Measurment of Health Edited PDF
Measurment of Health Edited PDF
disease
                 UNIVERSITY OF GONDAR
                COLLAGE OF MEDICINE AND HEALTH SCIENCE
                    INSTITUTE OF PUBLIC HEALTH
                  DEPARTMENT OF EPIDEMIOLOGY AND
                      BIOSTATISTICS
                                         Alemneh M. (BSc, MPH)
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Course objective
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Course contents
Chapter one: Introduction to public health
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Chapter Five: measurements of
association
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                   Chapter One
           Introduction to Public health
Definitions of terms:
Health is a difficult concept to define.
  WHO in 1948 defined health as “A state of complete
  physical, mental and social well being and not merely
  the absence of disease or infirmity.”
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            Clinical versus community medicine:
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           Methods of Community
                Diagnosis:
    Discussion with community leaders
     and health workers
    Survey of available health records
    Field survey.
    Compilation and analysis of the data.
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 It is impossible to address all the identified
   problems at the same time because of
   resource scarcity.
 Therefore the problems should be put in
   the order of priority using a set criterion.
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  Criteria for priority setting
 Magnitude (amount or frequency) of the
    problem
 Severity (to what extent is the problem
    disabling, fatal)
 Feasibility (availability of financial and
    material resource, effective control
    method)
 Community concern (whether it is a felt
    problem of the community)
 Government concern (policy support,
    political commitment)
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              Health p1   2   3   4
Magnitude
Severity
Feasibility
Community
concern
Gov’t
concern
Total
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EPIDEMIOLOGY
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           Components of the
              definition
  “Population” the focus of epidemiology is
   mainly on the population rather than
   individuals.
  “Frequency” shows epidemiology is
   mainly a quantitative science.
       Epidemiology is concerned with the frequency
        of diseases and other health related
        conditions.
       Frequency of diseases and deaths are
        measured by morbidity rates and mortality
        rates.
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 “Health      related   conditions”   are
  conditions which directly or indirectly
  affect or influence health. These may be
  injuries, vital events, health related
  behaviors, social factors, economic
  factors etc.
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 The part of epidemiology concerned with
  the frequency and distribution of diseases
  by time, person and place is named
  Descriptive Epidemiology.
                                                .
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Determinants” are        factors     which
determine whether or not a person will get a
disease.
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     Scope of Epidemiology
 Originally, epidemiology was concerned with
  epidemics of communicable diseases
  and epidemic investigations.
 Later it was extended to endemic
  communicable        diseases    and   non-
  communicable diseases
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At present epidemiologic methods are
 being applied to:
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           Purpose/Use of
            Epidemiology
The ultimate purpose of Epidemiology is
 prevention and control of disease, in an effort
 to improve the health status of populations.
This is realized through:
1. Elucidation of the natural history of disease
4. Evaluation of intervention
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  Fundamental Assumptions in
        Epidemiology
There are two basic assumptions in
  epidemiology.
1. Non random distribution of diseases
  i.e. the distribution of disease in human
  population is not random or by chance
2. Human diseases have causal and
  preventive      factors   that    can  be
  identified        through      systematic
  investigations of different populations.
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Risk factors could be:
      Factors related to the agent: Strain difference
      Factors related to the human host: Lack of
       specific immunity.
      Factors related to the environment:
       Overcrowding, Lack of ventilation
Risk factors may further be classified as:
• Factors susceptible to change: smoking
  habit, alcohol drinking habit
• Factors not amenable to change: age, sex,
  family history
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 In order to be able to prevent disease, it is
  vital to identify factors that can be changed.
 For some diseases, the specific causes are
  not known. In such cases it is very
  important to identify risk factors, especially
  those that can be changed and act on them.
 Epidemiology is mainly interested in those
  risk factors that are amenable to change as
  its ultimate purpose is to prevent and
  control disease and promote the health of
  the population.
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           Chapter Two
Epidemiological concept of disease
             causation
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      HOW THE DISEASE IS CAUSED?
2. Ecological theory
3. Germ theory
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                                             25
                                             25
     1. SUPERNATURAL THEORY OF DISEASE
• At least 10% of the people in developed countries
    and 30% in developing countries still believe in
    supernatural origin
•    Even today superstitions are becoming        major
    obstacles in disease control
• Most of the literates view that disease is the result of
    microbes
• Most of the uneducated people (90%) believe that
    disease is due to bad physical environment
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                                           26          26
        2. ECOLOGICAL THEORY
• Around 463 BC, hippocrates is the first
  epidemiologist who advised to search the
  environment for the cause of the disease.
• Mckeown has pointed out, improved health
  owes less to advances in medical science
  than to the operation of natural ecological
  laws
• He rightly advised to search air, water and
  places for the cause of a disease
• In ecological approach an agent is
  considered necessary but not sufficient
  cause
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           of a disease.
                                           27
                                            27
           3. GERM THEORY
               Germ       theory:    Microbes
               (germs)     were found to be
               the cause for many known
               diseases.
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           1. The epidemiologic triangle
                   Agent
 
Host
 Environment
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    Epidemiological triad model con’t…
• An agent is a factor whose presence or
  absence, excess or deficit is necessary for a
  particular disease or injury to occur.
• General classes of disease agents include;
1. Chemicals such as benzene, oxygen, and
  asbestos;
2. Microorganisms such as bacteria, viruses, fungi,
  and protozoa; and
3. Physical energy sources such as electricity and
  radiation.
• Many diseases and injuries have multiple agents.
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• The environment includes all external
   factors, other than the agent, that can
   influence health. These factors are further
   categorized according to whether they
   belong    in   the    social,   physical,   or
   biological environments.
• The       social      environment     including
   availability of medical care and health
   insurance; cultural “dos” and “don’ts”
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• The    physical    environment:-   climatic
  conditions, pollution…
• The biological environment:- vectors,
  humans and plants and animals acting as
  a reservoir
• The host is the actual or potential
  recipient or victim of disease or injury.
  Although the agent and environment
  combine to “cause” the illness or injury if
  the host is not susceptible disease will not
  occur.
• According to this model Disease and injury
  occur only when the interaction between
  the three factors is altered.
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                     2. The web of causation model
Hormones                                             physical
  inactivity
Smoking                  obesity
  heredity
    Blood clotting                  hardening of arteries
Heart disease              stroke                    hypertension
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   3. The Wheel model         The wheel consists of a
 hub (the host or human), which has genetic makeup
 as its core. Surrounding the host is the environment.
 The size of each part varies according to the type of
                    disease shown.
                              Social
               Physical       environment
               environment
                      Host
                      (man)
                          vc
                      Genetic
                      core
                   Biologic
                   environment
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   Natural History of Disease
    and Levels of Prevention
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Natural history of disease
  Is the course of a disease over time
  without      any     treatment      or
  intervention.
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   There are four stages in the natural
    history of a disease.
 These are:
   Stage of   susceptibility/exposure
   Stage of   pre-symptomatic (sub-clinical)
   disease
   Stage of   clinical disease and
   Stage of   disability or death
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1. Stage of susceptibility
   Disease has not yet developed, but there
      are factors that favor its occurrence
   Examples:
    A     person    practicing  casual   and
      unprotected sex has a high risk of
      getting HIV infection.
    An unvaccinated child is susceptible to
      measles.
    High cholesterol level increases the risk
      of coronary heart disease.
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     2.Stage of Pre-symptomatic
        (sub-clinical) disease
  In this stage there is no manifestation of
  the disease but pathogenic changes have
  started to occur.
  There are no detectable signs or symptoms.
  The disease can only be detected through
  special tests.
Examples:
 Detection of antibodies against HIV in an
  apparently healthy person.
 Ova of intestinal parasite in the stool of
  apparently healthy children.
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           3. The Clinical stage
 By this stage the person has developed signs and
   symptoms of the disease.
 The clinical stage of different diseases differs in
   duration, severity and outcome.
 The outcomes of this stage may be recovery,
   disability or death.
Examples:
 Common cold has a short and mild clinical stage
   and almost everyone recovers quickly.
 Polio has a severe clinical stage and many patients
   develop paralysis becoming disabled for the rest
   of their lives.
 Rabies has a relatively short but severe clinical
   stage and almost always results in death.
 HIV/ AIDS has a relatively longer clinical stage and
   eventually results in death.
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      4. Stage of disability or death
 The disease has occurred and left
  damage to the body that limits the
  activity of the victim(disability) or has
  ended with the death of the victim
Examples:
 Trachoma may cause blindness
 Meningitis may result in blindness,
   deafness or death.
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              Healthy person
   Recovery
                Clinical disease
   Recovery                          Death
                   Disability
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           Disease Prevention
 The major purpose in investigating the
  epidemiology of diseases is to learn how to
  prevent and control them.
 Disease prevention means to interrupt or
  slow the progression of disease.
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Levels of disease prevention
      1. Primary
            health promotion
            Prevention of exposure
            Prevention of disease
      2. Secondary prevention
            Screening
            Early detection and treatment
      3. Tertiary prevention
            Rehabilitation
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           1. Primary prevention
 Is aimed at preventing healthy people from
  becoming sick.
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       1.2 - Prevention of
            exposure
is the avoidance of factors which may
 cause disease if an individual is
 exposed to them.
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       1.3 - Prevention of
             disease
   Is the prevention of disease development
    after the individual has become exposed
    to the disease causing factors.
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2. Secondary prevention
  Detecting people who already have the
        disease as early as possible and treat
        them.
  It is carried out after the biological onset
        of the disease, but before permanent
        damage sets in.
  The objective of secondary prevention is
        to stop or slow the progression of
        disease and to prevent or limit
        permanent damage.
 Examples:
  Prevention of blindness from Trachoma
  Early detection and treatment of breast
        cancer to prevent its progression to the
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        invasive stage
  3. Tertiary prevention
 Is targeted towards people with chronic
  diseases and disabilities that cannot be
  cured.
 Tertiary prevention is needed in some
  diseases because primary and secondary
  prevention have failed, and in others
  because primary and secondary prevention
  are not effective.
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           Tertiary prevention
                  cont’d
It has two objectives:
 Treatment to prevent further disability or
    death and
 To limit the physical, psychological,
    social, and financial impact of disability,
    thereby improving the quality of life.
 This can be done through rehabilitation,
    which is the retaining of the remaining
    functions for maximal effectiveness.
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Level of prevention   Point of intervention
                                                            Natural history of disease
Primary               Health promotion
                      Prevention of exposure
                       
                                                                Clinical
                                                                onset
                      Early treatment
                      (prevention of permanent damage
                      )
                      Rehabilitation (prevention of
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                        Exercise -1
  for each of the following intervention , indicate what
             level of prevention is involved
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  Thank you!
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           CHAPTER THREE
       Measurement of Disease and
                 Death
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              Measurements of Disease
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Incidence Rate
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CI =          Number of new cases of a disease
               during a given period of time
           X 1000
                    Total population at risk
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2. Incidence Density
 An incidence rate whose denominator is calculated
  using person-time units.
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2. Prevalence rate
 Prevalence rate measures the number of
  people in a population who have a disease
  at a given time.
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 1. Period prevalence rate
 Period Prevalence rate measures the
  proportion of a population that is affected with
  a certain condition during a specified period of
  time.
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       Point Prevalence rate
 Measures the proportion of a population
  with a certain condition at a given point in
  time.
 This is not a true rate; rather it is a simple
  proportion.
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              Exercise 1
Each horizontal line in the next figure
 represents one of 10 persons who had
 giardiasis (a parasitic intestinal
 infection which doesn’t confer
 immunity against subsequent
 infections) in a population of 100.
The date of onset and duration of
 each episode indicated by a line of
 X’s .the vertical lines indicate specific
 dates.
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a.   Population at risk for giardiasis on Jan 1, 1990
b.   Incidence rate of giardiasis in 1990
c.   Point prevalence rate of giardiasis on Jan 1 1990
d.   The period prevalence of giardiasis in 1990
e.   The point prevalence of giardiasis on July1, 1990
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•   A=98
•   B=6/98*1000=6.1per1000
•   C=20per 1000
•   D=80per 1000
•   E=40per 1000
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Relationship between incidence and point prevalence
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   Factors influencing prevalence
                 rate
a) severity of illness - for highly fatal
   (lethal) diseases the prevalence rate is
   low.
b) duration of illness - short duration of
   disease leads to low prevalence rates.
c) the number of new cases - the higher
   the number of new cases the higher will
   be the prevalence.
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    Prevalence can be increased by
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           Prevalence can be
             decreased by
 Shorter duration of disease
 High case - fatality rate
 Decrease in new cases
 In-migration of healthy people
 Out-migration of cases
 Improved cure rate of cases
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  Prevalence rate is not a helpful measure to
  provide strong evidence of causation and
  risk of development of a disease.
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Incidence rate is important as
  A fundamental tool for etiologic studies
    of acute and chronic diseases
  A direct measure of risk
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           Limitations of prevalence
                    studies
 Prevalence studies favor inclusion of
  chronic over acute cases.
 Disease status and attribute are measured
  at the same time; hence, temporal
  relations cannot be established.
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Measurements of Death
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   Crude Death rate (CDR)
 CDR= Total no. of deaths reported X
  1000
          during a given time interval
             Estimated mid interval
  population
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    Age- specific mortality rate
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  Sex- specific mortality rate
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   Cause- specific mortality rate
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  Proportionate mortality ratio
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            Case Fatality Rate
CFR=   No. of deaths from a sp. disease during a given
 time x 100
        No. of cases of that disease during the same
 time
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Perinatal Mortality Rate
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     Neonatal Mortality Rate
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      Infant mortality rate
IMR=     No. of deaths under 1 yr during a given time
   X 1000
       No. of live births in the same area& during
   the same yr
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           Child mortality rate
= No. of deaths of 1-4 yrs of age during a given
   time X 1000
   Average (mid-interval) population of same age at
   same time
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   Maternal Mortality Ratio
MMR=Total no of female deaths due to complications of
 pregnancy,
      child birth & puerprium in an area in a year    x
 100,000
             No. of live births in the same area & year
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 When calculating (using) mortality rates it is
  important to understand their interpretations and
  how they differ from each other.
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 The case fatality rate asks the question: “what
  proportion of the people with the disease
  die of the disease?”
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 SCREENING AND SCREENING
   PROGRAM EVALUATION
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Definition
• Screening is the search for unrecognized disease or
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   Case finding (diagnosis)
• Occurs when clinicians search for diseases with
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  Objective of Screening Tests
• To lower morbidity and mortality of the
  disease in a population.
• Screening provides access to the medical
  care system which is not an actual goal of
  screening, but is a benefit.
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                   An ideal screening test should be
1. Inexpensive,
2. Easy to administer,
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           Validity of a screening test
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  Sensitivity and Specificity of a screening test
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Test                  Definitive diagnosis
resul                 Diseased   Non      Total
t                                diseased
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• Sensitivity: The probability of testing
  positive if the disease is truly present
  Sensitivity = a / (a + c)
                     = TP X 100
                      TP+FN
• Specificity: The probability of screening
  negative if the disease is truly absent
  Specificity = d / (b + d)
                    = TN X100
                        TN + FP
• Accuracy= a+d/a+b+c+d
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Predictive Value of a Screening Test
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     – Predictive Value of a Negative Test
       (PVNT) or Negative Predictive Value
       Shows the degree of confidence the
       disease can be ruled out by using this
       specific test.
              PVNT = TN X 100%
                     TN+FN
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• Predictive value of a test is determined by
  Sensitivity, Specificity and the Prevalence of the
  disease.
• The higher the prevalence, the more likely it is that a
  positive test is predictive of the diseases i.e. PVPT will
  be high.
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Reliability (Precision) of Screening Test
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1. The variability of a method- depends
   on such factors as the stability of the
   reagents used and fluctuation in the
   substance being measured ( e.g in
   relation to meals, diurnal variation).
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   Evaluation of screening program
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  Feasibility
The feasibility of a screening program is
  determined by
• The acceptability of the program to the
  potential screenees,
• Cost-effectiveness,
• The subsequent diagnosis and treatment
  of individuals who test positive,
• The yield of cases.
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                     Feasibility
Total screened
• Yield = TP X 100
                        TP + FN + TN + FP
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           Effectiveness
 The evaluation of the effectiveness of a
  screening program must be based on
  measures that reflect the impact of a
  program on the course of a disease.
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Exercise                     Diagnostic(Gold
standard Test)
                       Positive   Negative Total
                       350        50       400
Screeni     Positive
ng Test
                       150        450       600
            Negativ
            e
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     THANK YOU!
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              CHAPTER FOUR
EPIDEMIOLOGIC STUDIES
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       Epidemiological design
             strategies
o Epidemiology is primarily concerned with the
  distribution and determinants of disease in
  human populations
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                                   122      122
         Epidemiologic approaches
 1. DESCRIPTIVE
   Used to describe health and disease in the
 community
    What? by….Who?             When?        Where?
What are the      How many        Over what   Where do the
health problems people            period of   affected
of the community? are affected?   time?       people
                                              live, work or
                                              spend leisure
2.                                            time?
ANALYTI
 Used to identify etiology, prognosis and for
C Why? evaluation
program
                                  How?
       What are the causal            By what
agents?                             mechanism
       What factors affect
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                                              operate?   123
outcome?
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           124   124
              Descriptive studies
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                                    125        125
            What?
            Cases
 Person                     Time
Place
 Who?        Where?
When?
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                      126          126
           Category of descriptive
                  studies
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                                       127       127
                  Case report
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                                         129           129
Example 1:-
Both
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          case report and case series are able to
                                     132       132
 Disadvantages of case reports and
               series
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                                            134       134
                       Strength
Can be done quickly and inexpensively, often using
available data.
environmental exposures, eg
- Do heat waves increase death rate?
- Does soft drinks increase heart disease?
- Do economic recessions increase suicide rate?
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                                             135        135
                       Limitation
1. Inability to link exposure with disease.
  - Data on exposure and outcome are not linked at the
   individual level;
  - Correlation found with aggregate data may not apply
    to individuals (this is referred as ecological fallacy)
2. Lack of ability to control for effects of potential
    confounding factors
     - A correlation found between the high per capita
   color TV and mortality from CHD, again here it is
   obvious that color TV owning is not a good reason for
   increased mortality from CHD
3. It may mask a non-linear relationship between
    exposure and disease while it is exist
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                                       136   136
           Cross sectional study
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                       Cross-sectional studies
It is also called prevalence study (survey study)
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                                     140     140
Advantages
 Good design for hypothesis generation
 Highly generalizable
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                                                     141            141
                Disadvantage
Impractical for rare diseases and rare exposure – because we
need to take very large sample size
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                                                 142         142
      Analytical Study
          Designs
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                   143   143
              Learning objectives
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                                    144      144
    Introduction to analytic
Application: studies
 To search for cause - effect relationship and
 mechanism
  o Why?
o How?
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                            147   147
             Analytic studies...
Observational studies
o An investigator observes the natural course of an
   event
o An investigator measures but does not intervene
Interventional studies
o An investigator assigns study subjects to exposed
   and non-exposed and follows to measure for
   disease occurrence
o An investigator manipulates the intervention
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                                       148       148
 Observational analytic studies
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                                    149    149
 Case-Control Studies
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                150     150
   Definition of case-control
            studies
 A case control study is one in which persons
 with        a   condition   (“cases”)   and    suitable
 comparison           subjects     (“controls”)     are
 identified, and then the two groups are
 compared with respect to prior exposure to
 risk factors
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                                          151        151
      Definition of case-control
               studies…
o The investigator looks back in time to measure
    exposure of the study subjects to the risk factors
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                                             154        154
             What is case?
o It is the outcome of interest under study
o It can be:
   – A disease
     E.g. HIV status, malaria status
   – A behavior
     E.g. Alcohol drinking habit(yes/no),
     cigarette smoking(yes/no)
   - Event – traffic accident
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                                155     155
              What is control?
o It is the comparison group (reference)
under study)
– Incidents cases
  –11/14/19
     Chronic/prevalent cases
                                                   157            157
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           158   158
        Measuring exposure of
              interest
o Exposure status could be ascertained by interview
  (patient,   relative),   hospital   records,    laboratory
  analysis etc…
o May include analysis of pre-diagnostic biological
  specimens (nested case-control approach)
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                                            159         159
  Common bias in case-control
          studies
o Information bias
- recall bias
   - non-response bias
o Selection bias
              controls
         - the probability of selecting a real case and
  control
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                                           160        160
 Strengths of case-control studies
o To investigate rare disease (less than 10%)
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                  163   163
             Learning objectives
o Immigration cohort
o Treatment cohort
o Exposure cohort
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                                       165       165
           Definition of cohort studies
   A cohort study is an observational research design
  which begins when a cohort initially free of disease
  (outcome of interest) are classified according to a
  given exposure and then followed (traced) over time
 The investigator compares whether the sub-sequent
  development of a new cases of disease (other
  outcome of interest) differs between the exposed and
  non-exposed cohorts
 For example if a researcher want to investigate
  weather      drinking   more   than   five   cup     of
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                                         166         166
     Design of cohort studies
    = == > If we want to know weather exposure to
drinking coffee during pregnancy will result in abnormal
                          birth                Diseased
                              Exposed        Give abnormal
                             Drink more           baby
                           than five cup of
                           Coffee per day     Not diseased
               People
               without                      Give normal baby
Population
  at risk        the                           Diseased
              outcome       Not Exposed     Give abnormal
              Pregnant                           baby
                             Not drink
               mothers       any coffee
                                            Not diseased
                                          Give normal baby
                      Time
              Direction of enquiry
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                                          167        167
Basic features of cohort studies
“Disease free” or “without outcome” population at entry
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                                             168          168
   Types of cohort studies
 Cohort studies can be classified depending
 on the temporal relationship between the
 initiation of the study and the occurrence of
 the outcome of interest
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                                   169     169
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           170   170
  1. Prospective cohort studies
o Study participants are grouped on the basis of past
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                                         171           171
                        2. Retrospective cohort studies
o What
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                                                 173        and
                                                            173
    Which type of cohort studies
         should be used?
 The          decision   to   conduct   a   retrospective     or
    prospective study depends on:
     –
o Exposure is any risk factor that can associated with the
interview
o Death certificate
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Follow up period of cohort studies
o The follow-up is the most critical and demanding part
of a cohort study.
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Strength of cohort studies:
o Particularly efficient when exposure is rare
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                                             179       179
  Limitation of cohort studies:
o Costly and time consuming if disease is rare and/or
  records
o Exposure status may change during the course of
  study
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                                         180        180
                Experimental
            (Intervention studies)
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 Definition
An experiment is a set of
  observations,
conducted     under    controlled
  circumstances,
in     which     the   scientist
  manipulates the
conditions    to ascertain what
  effect such
manipulation     has   on     the
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             Key Features of
           Experimental Design
1) Investigator manipulates
   the condition under study
2) Always prospective
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           Types of intervention studies
  Eligible              B               P
              R
Individuals                                       With
                                                  outcome
              Not-
              received
                                                  Without
              Interventi                          outcome
              on
  R=randomization   B=double blinding       P=placebo
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              Prevention Trial
                                                    With
                                                    outcome
                   Vaccinate
                   d                                Without
                                                    outcome
  Health                   B               P
               R
Individuals                                          With
                   Not-                              outcome
                   Vaccinate
                                                     Without
                   d                                 outcome
C.1 Phase I
  Trial on small number of subjects to
  test a new drug with small dosage to
  determine the toxic effect
C.2 Phase II
  Trial on small group of people to
  determine the therapeutic effect
C.3 Phase III
• Study on large population
• Usually randomized controlled trial
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Problems of intervention studies
1. Ethical problem
• An independent group must be
  established.
• Purpose:
     – Safety of subjects
     – Maintaining the quality of the study
     – Maintain objectivity
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2)Cost
• Loss to follow-up
    – Select population who are both interested and reliable.
    – Arrange frequent contacts with individuals
    – Use incentives, such as providing medical information
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           Main steps in an RCT
1. Identify new
  drug/intervention/prevention
2. Identify comparison – e.g standard
  treatment versus placebo
3. Define eligible patient population/
  exclusions (i.e the sampling frame)
4. Define the outcomes and how to
  assess them
5. Write the protocol
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      Main steps in an RCT cont…
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           Assessment of
            compliance
  • Self-report
• Pills count
• Biochemical tests
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            Stopping Rules
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           The Quality of “Gold
               Standard"
• Randomization
• Blinding
• Use of Placebo
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              Chapter Five
     MEASURES OF ASSOCIATION
      AND EVALUATION OF EVIDENCE
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           Learning objectives
• After the end of this session, students will
  be expected to:
     – List common measures of association and
       measures of public health impact
     – Calculate and interpret
        • relative risk
        • odds ratio
        • attributable and population attributable risk
          and their percent
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           Definition of association
 An association is said to exist between two
    variables when a change in one variable parallels
    or coincides with a change in another ones
 An association is said to be causal when it can be
    proved that a change in the exposure variable
    produces a change in the outcome variable
    More appropriately, a causal relationship exists
    when exposure enters into the causation of disease
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o Statistical relationship between two or
  more variables
o A causal association exists when the risk
  factor causes change in the disease
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 Measuring an association
  Quantifies the strength of the relationship
    between an "exposure" and “outcome” of
    interest
  Quantifies the difference in occurrence of
    disease or death between two groups of
    people who differ on “exposure status”
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Two main options for comparison
 Calculate ratio of two measures of
  disease frequency
  o Relative comparison
  o Strength    of    relationship  between
    exposure and outcome
 Calculate    difference     between   two
  measures of disease frequency
  o Absolute comparison (attributable risk)
  o Public health impact of exposure
    (population attributable risk)
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How strong is the association?
  The strength of the association is
  commonly measured by the relative risk,
  odds ratio, attributable risk and population
  attributable risk and their percents
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   1. Relative Risk (RR) or Risk Ratio
 RR shows the magnitude of association
   between exposure & disease
 Indicates the likelihood of developing the
   disease in exposed group relative to those
   who are not exposed
 RR can also be used to compare risks of
   death, injury, and other possible outcomes
   of the exposure.
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 .
RR    Incidence of a disease among exposed (a/
   (a+b))
=       Incidence of a disease among non-
   exposed (c/(c+d))             Disease
                    .    a     .
                                                Yes (+)
                                       Exposu
  RR =                       a+b        re
                                              Noa(-) b
                                                       a+
                                       Yes (+)
                .
                                                        b
                .
            .
            .
                          c        .
                                   .
                                                 c   d
                        c +d            No (-)         c+
                                                        d
     – It is a direct measurement of a risk to
       develop the outcome of interest
     – It is usually used in cohort and
       experimental studies
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                                                            209
                    Example
     Table 1: data from a cohort study of oral
    contraceptive (OC) use and bacteruria
    among women aged 16-49 years
    Bacteruria
    Yes No Total
Current OC use
 Yes 27 455 482
 No 77 1831 1908
 Total 104 2286 2390
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 Calculate RR??????? Ans:- 1.4
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                        Interpretation
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• Values of RR less than one 1 indicate a
   negative association between the risk
   factor and the disease.(i.e. protective )
• In general the strength of association can
   be considered:
• High - if the RR is 3.0 or more
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           2. Odds Ratio (OR)
o Odds: The ratio of the probability of an
   event's occurring to the probability of its
   not occurring
o Odds Ratio: The ratio of two odds
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                      Cont’d…
 In case control studies, it is usually not possible
   to calculate the rate of development of disease
   in the exposed and non-exposed group.
 Hence, it is difficult to calculate the RR.
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• Odds Ratio: Odds of case being
  exposed
        Odds of control being exposed
   OR = a/c = ad
       b/d    bc
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                    Example
Table 3: Data from a case-control study of
 current oral contraceptive (OC) use and MI in
 pre-menopausal female nurses
   Myocardial infarction
   Yes No Total
Current OC use
 Yes 23 304 327
 No 133 2816 2949
 Total 156 3120 3276
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Calculate OR
 OR = ad       =     (23) (2816)   = 1.6
         bc        (304) (133)
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       Interpretation of the Odds
                 Ratio…
• OR = 1 then exposure Not related to
   disease
• OR >1      then exposure Positively
   related to disease
• OR <1      then exposure Negatively related
   to disease
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                Interpretation
• The odds of having the disease in question
   are     OR   times   greater   among   those
   exposed to the suspected risk factor than
   among those with no such exposure.
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                        Exercise
• Suppose study was conducted in US in order to find
   out     weather   mother’s   use   of   hormone   during
   pregnancy influenced her son’s risk of testicular
   cancer in later life. Investigator selected 500 peoples
   with cancer and 1000 without cancer. The study
   found 90 mothers in cases and 50 mothers in controls
   had used hormones during pregnancy.
• What study design were used
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           Odds Ratio as estimator of
                 Relative Risk
OR is a valid estimator of RR if:
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• What is the excess risk among
  exposed individuals?
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       Absolute Measures of Risk
o Absolute   risk:     a   measure      of   association
  indicating on an absolute scale how much
  greater the frequency of diseases is in an
  exposed group than in an unexposed group,
  assuming       the     association    between      the
  exposure and disease is causal
o Attributable    risk     is   also   known    as   risk
  difference or excess risk among exposed
  groups
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           Attributable Risk (AR) / Risk
                 Difference (RD)
 Provides information about the absolute effect of
  the exposure or the excess risk of disease in those
  exposed compared with those non exposed.
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                Cont’d…
 AR=0 no association
 AR > 0 indicates positive association
   the number of cases of the disease among
    the exposed that can be attributable to
    the exposure itself, or
   alternatively, the number of cases of the
    disease among the exposed that could be
    eliminated if the exposure were eliminated
 Thus, the AR can be useful as a measure
  of the public health impact of a
  particular exposure.
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• What proportion of cases is
  attributed to the actual exposure
  among exposed people?
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Attributable Risk Percent (AR
%)
 Estimates the proportion of the disease among
  the exposed that is attributable to the exposure,
  or
• AR % = 1566/100,000 X 100
             27/482
           = 27.96 %
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   Population Attributable Risk
              (PAR)
 Public health planners want to be able to
  anticipate the effect of eliminating the
  exposure on the population as a whole,
  rather than just on the exposed part of the
  population.
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• PAR = AR X prevalence rate of the
   exposure
Interpretation:
In a population of 100,000 smokers, 18 deaths from
  lung cancer per year could have been avoided by
  preventing them from smoking (this refers to AR).
In a general population of 100,000 with a prevalence
  rate of cigarette smoking of 20 %, about 18 deaths
  from lung cancer per year would be prevented by
  eliminating cigarette smoking (this refers to PAR).
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 Both AR and PAR are used to estimate the
  effect on disease incidence of eliminating a
  given risk factor, but while AR estimates
  reduction in disease incidence only in
  those      exposed,     PAR      estimates
  reduction in disease incidence in the
  population as a whole.
 The alternative formula for PAR is:
 PAR = Incidence rate in total population
  minus incidence rate in non-exposed
  population
           PAR = IT - Io
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• What proportion of cases is
  attributed to the actual exposure
  among the general population?
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           Population Attributable Risk
                Percent (PAR %)
 Expresses the proportion of disease in the study
  population that is attributable to the exposure and
  thus could be eliminated if the exposure were
  eliminated.
 PAR% is the percent of the incidence of a disease in
  the population (exposed and non exposed) that is
  due to exposure.
 PAR % = PAR              X100
     incidence rate in total population
Example:
 PAR = 17.8 per 100,000 per year
 Mortality rate in non-smokers = 7 per 100000
 Mortality rate in the total population = 24.8 per 10 5
  per year
 Calculate PAR %
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• PAR % =17.8 per 105 per year X100
       24.8 per 105 per year
=71.8%
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   Possible Outcomes In Studying The
   Relationship Between Disease And
                Exposure
1. No association between exposure and
  disease
        AR=0, RR=1 ,OR=1
2. Positive association between exposure
  and disease (more exposure, more
  disease)
       AR>0, RR>1 ,OR>1
3. Negative association between exposure
  and disease
   (more exposure, less disease)
                AR<0 (negative),     RR
  <1(fraction)OR<1
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                       Exercise
      There is some hint that coffee drinking causes
       peptic ulcer. One epidemiologist wanted to
       make sure whether this is true.
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                    EVALUATION OF EVIDENCE
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           Brain storming
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           Association Vs Causation
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                Accuracy
                    =
           Validity + precision
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  Validity of epidemiological studies
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            Types of validity
Internal validity:
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                      Precision
 Precision measures the extent by which our study
    result is similar (consistent) with other previous
    studies published on the area by different scholars
    in different population, area and methods.
 Precision is the extent to which random error alters
    the measurement of effects
    Threats to validity of study:
       - Random error (chance): is sampling error
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            The Bradford Hill Criteria
o It is the statement of epidemiological criteria
 of a causal association formulated in 1965 by
  Sir Austin Bradford Hill
1. Strength of association
2. Consistency of findings with other studies
3. Temporality
4. Biologic gradient
5. Biologic plausibility
6. Specificity of the association
7. Experimental evidence
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 Bradford……….
1. Strength of the Association - The stronger the
  association, the more likely that it is causal.
2. Consistency of the Relationship - The same
  association should be demonstrable in studies with
  different    methods,      conducted      by      different
  investigators, and in different populations.
3. Specificity of the Association - The association is
  more likely causal if a single exposure is linked to a
  single disease.
Single exposure         Single disease
    This works more to most living organisms as causes.
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 Bradford…….
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           7. Biological plausibility
Hypothesis should be coherent with what is
known about the disease; both biologically
and using laboratory.
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Which Hill’s criteria are essential?
 There are no completely reliable criteria for
 determining whether an association is causal or not
 In judging the different aspects of causation; not all
 criteria must be fulfilled to establish scientific
 causation
 The correct temporal relationship is more essential
         risk factor/cause         ---------------------
 outcome/effect
=== Once this has been found, weight should be
 given to:
  – Strength of the association
  – Biologic plausibility
   – Consistency
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   – Dose-response relationship
            CHAPTER SIX
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            Learning Objectives
After this session, students will be expected to:
system
 Systematic, ongoing…
   – Collection
   – Analysis               Health action
   – Interpretation
                           investigation
   – Dissemination
 …of health outcome       control
  data                     prevention
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   Components of Surveillance and
       Public Health Action
                      Public Health
Component of        Action
Surveillance         Priority setting
 o Collection        Planning,
 o Analysis          implementing and
 o Interpretation
                     evaluating disease
 o Dissemination
                      occurrence in that
                      community
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           Purpose of Surveillance
I. To be able to identify diseases, injuries,
     hazards and other health related factors as
     early as possible. prediction and early
     detection of outbreaks.
II. To provide scientific baseline data and
     information for priority setting, planning,
     implementing and evaluating disease
     control program for both communicable
     and non-communicable health problems.
III. To define the magnitude and distribution of
     diseases by time, person and place
     dimension
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           Types of Surveillance
1. Active surveillance
2. Passive surveillance
3. Sentinel surveillance
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                        Active Surveillance
activities
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Preconditions to institute an active surveillance
  system.
 For periodic evaluation of an ongoing program
 For programs with limited time of operation such
  as eradication program.
 In unusual situations such as .
  – New disease discovery
  – New mode of transmission
  – When a high-risk season/year is recognized.
  – When a disease is found to affect a new
     subgroup of the population.
  – When a previously eradicated disease reappears
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                            Passive Surveillance
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       Sentinel Surveillance Con’t...
The advantages of sentinel surveillance data are
  that they can be less expensive to obtain than those
  gained through active surveillance of the total
  population, and the data can be of higher quality
  than those collected through passive systems.
In        developing   countries,   sentinel   surveillance
  provides a practical alternative to population-based
  surveillance
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 Main Purposes of Sentinel Surveillance
   To detect changes
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Advantages of sentinel surveillance
 Relatively inexpensive
 Provides a practical alternative to population-
  based surveillance
 Can make productive use of data collected for
  other purposes
Disadvantages:
 The    selected    population   may    not    be
  representative of the whole population
 Use of secondary data may lead to data of lesser
  quality and timeliness
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           Process of Public Health Surveillance
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Criteria for selecting and prioritizing health
  conditions     for    surveillance     system
  includes:
 Public health importance of the problem:-
        • incidence, prevalence,
        • severity, sequela, disabilities,
        • mortality caused by the problem,
        • socioeconomic impact,
        • communicability,
        • potential for an outbreak,
        • public perception and concern, and
        • international requirements.
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 If disease has epidemic potential
 If required internationally
programs
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       Basic Principles of Surveillance
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     Elements of Surveillance
• Case definition
• Cycle of surveillance
• Confidentiality
• Incentives
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                    A) Case Definition
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            Standard case definition
 If the use of case definition is agreed by
 everyone in the country or across boundaries
 or continents it is standard case definition
o Surveillance using less specific criteria is
 sometimes referred as syndromic surveillance
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               Types of Case Definition
Confirmed case
o A case with laboratory verification
Probable case
o A case with typical clinical features of the
  disease without laboratory confirmation
Suspected case/possible
o A case presented with fewer of the typical
  clinical features of the disease without
  laboratory confirmation
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   Advantages of Case Definition
1) Facilitate   early     detection     and     prompt
   management           even   if   diagnosis   is   not
   confirmed by laboratory
3) Observation of trends
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       B) Population Under Surveillance
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           C) Cycle of Surveillance
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                D) Confidentiality
• Personal identifying information is necessary to:
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  Public Health Emergency Management (PHEM)
 Public health emergencies are events or disasters that
 threaten the health of communities at large
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                Preparedness
 Actions taken before an emergency to prepare for
 response
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                      Response
 Activities to address immediate and short-
   term effects of a disaster
    – Implement emergency management plan
           o Save lives
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                 Recovery
 Restore essential functions and normal operation
community
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Limitations of Surveillance System In Ethiopia
o Under reporting
o Lack of representativeness
o Lack of timeliness
o Lack of motivation
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            List of Priority Reportable Diseases In Ethiopia
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       Learning objectives
 After the end of this session, students will be able to:
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              Level of disease
                occurrences
 • Diseases occur in a community at different levels at a
    particular point in time.
 Occurrence at expected levels
 • Endemic: Presence of a disease at more or less stable level.
    --==Malaria is endemic in the lowland areas of Ethiopia.
 • Hyper endemic: Persistently high level of disease occurrence.
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  Excess of what is expected
  • Epidemic: The occurrence of health related
    condition/disease in excess of the usual frequency
  • Outbreak: Epidemics of shorter duration covering
    a more limited area.
  • Cluster: is an aggregation of cases in a given area
    over a particular period without regard to whether
    the number of cases is more than expected.
  • Pandemic:    An    epidemic    involving  several
    countries or continents affecting a large number
    of people.
      example : HIV/AIDS is a pandemic.
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           What is outbreak
            occurrence?
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             What does outbreak
            investigation & control?
  It is the process of identifying:
           o The cause of the epidemic
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    What are the objectives for
 outbreak investigation? Or reason
           to investigate
1)To initiate control & prevention measures/to
  evaluate existing preventive strategies i.e.
  vaccine
 The most important public health reasons for
  investigating an outbreak are to help guide disease
  prevention and control strategies.
 These disease control efforts depend on several factors,
  Including
     knowledge of the agent,
     The natural course of the outbreak,
     The usual transmission mechanism of the disease,
       and
     Available control measures
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            2) Research and training
                  opportunity
 o Each outbreak should be viewed as an experiment
     waiting to be analyzed
 o It presents a unique opportunity to study the
     natural history of the disease
 o It could be a good opportunity to gain additional
     knowledge on
    – The impact of prevention and control measures
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       3) Public, political and legal
                obligations
o Politicians and leaders are usually concerned with
   control of the epidemic or address public concern
   about the outbreak.
o Politicians and leaders may sometimes override
   scientific concerns
o The public are more concerned in cluster of
   disease and potentials of getting medication
o It       is   the   right   of   the   community   to   get
   treatment/service and it is government and our
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   duty to protect the community
              4) Program
            considerations
o Occurrence      of   an   outbreak    notifies   the
   presence of a program weakness
o This could help program directors to change
   or strengthen the program’s effort in the
   future   to   prevent    potential   episodes    of
   outbreak occurrence
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Goals of investigation
 Identify the etiologic agent
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      1. Common source
It occurs as a epidemic
                result of the exposure of a group of
  population to a common source (etiological agent)
o It can result from a single source/ exposure of
  the population to the agent
      E.g: contaminated water supply, or food in a
  certain restaurant
Three types
      1. Point common source
      2. Continuous common source
      3. Intermittent common source
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 A) Point common source
                epidemic
o Single/ones/limited time exposure to the source
o All exposed hosts will develop disease within one
  incubation period
o The      epidemic   usually   decline   after   a   few
  generations,    either   because    the   number     of
  susceptible hosts fall below some critical level, or
  because intervention measures become effective
o A rapid rise and gradual fall of an epidemic curve
  suggests a point source epidemic
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    E.g. Food borne outbreak in a
            wedding feast
                Commonly due to
                infectious diseases or
                May be from
                environmental
                pollution        Features of epidemic curve:
                                 1-Rises and falls rapidly, no
                                 secondary waves.
                                   2-Tends to be explosive, with
                                 clustering of cases within narrow
                                 interval of time. 3-All cases
                                 develop within one incubation
                                 period.
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       B) Continuous common source
                 epidemic
  If exposure to a common source continues over
   time for days, weeks
  The epidemic curve has a plateau (multimodal
   epi curve)/ long peak
  Range of exposures and range of incubation
   periods is different
                          1-The exposure from the same
                          source may be prolonged-
                          continuous,     repeated   or
                          intermittent
                          2-No explosive rise in number
                          of cases.
                          3-Cases occur over more than
                          one incubation period.
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 C) Intermittent common source
            epidemic
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      2. Propagative /progressive
o
                   epidemic
     It occurs as a result of transmission of an
     infectious agent from one person to another
     directly or indirectly
o There is a successive generations of cases
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                       Typical Propagated Epidemic Curve
  Of infectious origin, with person to person transmission (hepatitis A,E and polio epidemics).
  Gradual rise and tails off over longer period of time. Transmission continues till depletion of
  susceptible or susceptible individuals are no longer exposed to source of infection. Communicability
  (speed of spread) depends on herd immunity among exposed and opportunities for contact with
  infective dose and secondary attack rate.
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           3. Mixed Epidemic
 o It shows the features of both types of epidemics
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    Steps of outbreak investigation and control
   1.Prepare to field work
   2.Establish the existence of outbreak
   3.Verifying the diagnosis
   4.Case definition and case finding
   5.Perform descriptive epidemiology
   6.Formulate hypotheses
   7.Testing hypotheses
   8.Refine hypothesis and additional studies
   9.Implementing prevention and control activities
   10.Communicate findings
    In practice, however, several steps may be done
     at the same time, or
    The circumstances of the outbreak may dictate
     that a different order be followed
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  Step 1: Prepare for field
            work
 Before leaving for the field, an investigator
  must be well prepared to under take the
  investigation:
o Investigation (Knowledge in epidemiology
   and the disease of concern is important)
o Administrative (Logistics, administrative
   procedures, travel arrangements)
o Consultation (Health workers should know
   their role, and should participate in the
   planning phase)
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    Step 2: Establish the existence of
                outbreak
 o An outbreak is the occurrence of more cases of
    disease than expected level
 o The investigator has to compare previous case
    load with the current to assure the existence
    of the outbreak
 o But be careful, excess cases may not always
   indicate an outbreak occurrence rather it may
   be because:
     Change in population size
     Change in case definition
     Change in reporting procedure
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Step 3: Verifying the diagnosis
 o The initial report may be spurious and arise from
      misinterpretation of the clinical features
 o Review clinical and laboratory findings to establish
      diagnosis
 o Goals in verifying the diagnosis includes:
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    Step 4: A. Case definition and
             case finding
 • Define cases ( Establish case definition):
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Step 4: Case definition and case
         finding Cont…d
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 Define cases ( Establish case definition):
 1)Possible (suspected)
  Having fewer sign and symptoms
 2) Probable
  Having typical sign and symptoms
 3) Definite (confirmed)
  Laboratory confirmed
 Example : A patient hospitalized in the ICU from
   24th November 2017, with new or worsening of
   cough, Fever >38, with suggestive X-ray changes
   and cultures identify a respiratory microorganism.
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     B. Identify cases (line listing)
 o Identifying information
 e.g. Hospital admission number, unit, name, address,
   phone.
 o Demographics
 e.g. Age, sex, date of admission, date of surgery.
 o Risk factor information
  e.g. Type of surgery, co morbidity, catheters, implants
 o Clinical data
 • e.g. Onset of symptoms and signs, frequency and
   duration of clinical features, treatments, devices, etc
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  Step 5: Performing Descriptive
           Epidemiology
 o Once data is collected, it should be analyzed by time, place and
    person
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1.   Analysis of epidemic by time
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           Epidemic curve
Point source
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     2.   Analysis of epidemic
                 byisplace
       – A spot map   a simple and useful
           technique for illustrating where cases
           live, work or may have been exposed
       – Area map if large area is affected
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 John Snow’s spot map of the distribution of cholera
cases Golden London square August-September 1848
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    3. Analysis of epidemic
          by person
 o Characterizing an outbreak occurrence by person is how we
    determine what populations are at risk for the disease
 o Host characteristics: age, race, sex, or medical status and
    exposures-occupation, leisure activities, use of medications,
    tobacco and drug use etc…
 o These influence susceptibility to disease and opportunities
    for exposure to risk factors
 o We use attack rates to identify high risk groups
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                         Attack rate
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                         Step 6: Formulating Hypothesis
  Depending on the outbreak, the hypothesis may address
     o     The exposures that caused the disease
     o     The agent and its reservoir
     o     Risk factors that caused disease
     o     The mode of transmission
  Using :
     1.    Subject-matter knowledge
     2.    Descriptive epidemiology
     3.    Talking with patients
     4.    Talking with local officials
     The hypotheses should be testable
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           Step 7: Testing the hypothesis
  Evaluate the credibility of your hypotheses
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 Factors that should also be
  considered when evaluating
  possible causality:
 • Testing statistical significance
 • Consistency with other studies
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  Step 8: Refining hypotheses and
 o
         additional studies
    When analytic epidemiological studies do not confirm
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    Step 9: Implementing control and
              prevention
   In outbreak investigation, the
   primary goal is to control and
   prevent the outbreak.
   Implementing control measure
   should be done as soon as possible
   It should go in parallel to
   investigating the outbreak
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            Source/ Mode of Transmission
Causative
Agent
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               Control measures (do early)
 1. Measures Directed Against the Reservoir:
     – Reduce contact rate
     – Reduce infectious sources- destruction of infected animal
       /isolation
     – Reduce infectiousness- early treatment
- Immunization
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           DAY
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              Step 10: Communicating
              findings of investigation
  The final responsibility of the investigative team is to prepare a written report to document the
      investigations, findings and the recommendations
 The written report should follow the scientific reporting format which includes:
  o introduction
  o    methods
  o    results
  o    discussion
  o    conclusion, and
  o Recommendations
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 Summary of the investigation and control
   of an epidemic considering procedure
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                 Post-Epidemic
                  Surveillance
 o The efficacy of control measures should be assessed day to
     day during the outbreak, a final assessment being made
     after it has ended
 o     This   will   provide   a   logical   basis   for   post-epidemic
     surveillance, and preventive measures aimed at avoiding
     similar outbreaks in the future
 o Develop long term early warning system
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           The End!
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