Measures of Disease Occurrence

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Presentation transcript:

Measures of Disease Occurrence Dr Rufaidah Al Dabbagh, MBBS, MPH, DrPH Community Medicine Unit, Family & Community Medicine Department 18, 9, 2018

Objectives To define and distinguish the different types of measures of disease frequency To calculate the different measures of disease frequency To understand the difference between frequency, proportion, rate, and ratio To understand the difference between association and effect

Measures for Disease Occurrence Proportions: Prevalence Incidence proportion (risk) Rates: Incidence rates Ratio: odds for a certain disease Differences between proportions, rates and ratios will be explained at the end

What is Prevalence? Prevalence is a term referring to the number of existing and new cases of the disease present in a particular population at a given time It thus means that numerator includes all current cases; both the old and new cases. It is an important measure of the burden of disease in a community Prevalence is important to know the burden of a disease in the community. It is important to tell us how many clinics we need, how many services we need. It is a good indicator to use when planning health services.

Point Prevalence Prevalence The proportion of the population that has the disease at a specific point in time Prevalence = Number of current cases at a specific point in time Total population at that same point in time “Current cases” means new and pre-existing cases (all the cases that were there at that point in time) Period prevalence vs. point prevalence.

Period Prevalence Period Prevalence The proportion of the population that has the disease during a specified period of time Period Prevalence = Number of current cases during a specific period of time Average or mid-interval population Period prevalence vs. point prevalence.

Incidence Proportion (Risk) In a cohort study, investigators can also estimate the incidence proportion (risk) Risk= Number of new cases______________ total population at risk at the beginning of the study The population at risk is a well-defined population that is free of the disease at the beginning of the study and has certain characteristics that put them at risk for developing the disease

Why is it important to estimate risk? Gives us information about the new cases of the disease Important in order to estimate associations between exposure and outcome that can give us an idea about disease causes and risk factors Risk can only be interpreted in the period of time in which it was measured. e.g. it does not make sense to say that xx person has a risk of 3% for CVD, without explaining the period of time or the context.

Follow-up in Study D D D D D Population at risk D 1 y 2 y 3 y 4 y 5 y # of people at risk at baseline? # of cases developed during the 6 year follow-up period? Total person-time at risk?

What is the prevalence? risk? In a study that followed up people above 60 years of age for the development of CVD, there were 80 men with CVD when screened at baseline, and 60 women with CVD when screened at baseline. However, 200 men and 200 women did not have CVD at baseline. After 3 years follow-up, 50 new cases of CVD developed in men, and 30 new cases of CVD developed in women.

Relationship between prevalence and incidence Source: Gordis L. Epidemiology. 4th ed Saunders Elsevier; 2009.

Incidence Rate In a cohort study, investigators are usually interested in disease incidence rates Incidence Rate= Number of new cases______________ the total person time at risk over the study period of time Here we are taking into consideration the time that each person spent being at risk before developing the disease By contrast the incidence proportion only considers the total population at risk without also incorporating time in the equation Incidences of whatever we are interested in, disease, adverse effects, deaths………

Rate vs. Risk A study followed 3,000 males ages 45 years and older for 5 years to assess the development of MI. During the study period, 150 men developed MI, who accumulated a total person-time of 14,625 person- years. What is the incidence proportion after 5 years (risk)? What is the incidence rate after 5 years (rate)? Incidences of whatever we are interested in, disease, adverse effects, deaths………

Follow-up in Study D D D D D Population at risk D 1 y 2 y 3 y 4 y 5 y # of people at risk at baseline? # of cases developed during the 6 year follow-up period? Total person-time at risk?

Attack rate: is it really a rate? In the context of an outbreak: The proportion of new cases during a specific time period divided by the total population at risk during that same period Attack rate is the “incidence proportion” that they calculate during outbreak investigations for acute illnesses Attack rate for disease X = number of new cases with disease X Total population at risk Incidences of whatever we are interested in, disease, adverse effects, deaths………

Odds for disease a b c d Odds= prevalence/ 1-prevalence GD No GD Genetic variant present a b Genetic variant absent c d Odds among GV+ve = a/b Odds among GV-ve = c/d Odds ratio = (a/b) / (c/d) = ad / cb Odds= prevalence/ 1-prevalence Odds of GD in people with genetic variant: (a / a+b) / (b / a+b) = a / b

Risk, Rate or Odds? Cervical Ca No Cervical CA Total Person Time (person-years) Total Tobacco Use 64 106 35,000 170 No Tobacco Use 55 125 56,000 180 119 231 91,000 350 Risk = 119 / 350 = 0.34 (or 34%) Rate = 119 / 91000 = 1.3 per 1000 person-years Odds = 119 / 231 = 0.52 (or 52 in 100)

Risk, Rate or Odds It is important to distinguish between these measures of disease frequency, and not to mistake them with each other when interpreting your results The type of study determines the type of estimate we can use: If we can follow-up people through time (cohort study) then we will be able to calculate: Risk and Rate If we do not have the information from when the person was free of disease until they developed a disease then we can only estimate odds ratios (odds alone are rarely expressed)

Proportion, rate and ratio Proportions They are dimentionless (do not have a unit of measure, because the unit of measure in the denominator is the same as the numerator) Always lies between 0 or 1 Rates denominator is measured in time units Can exceed 1 if no. of new cases > person-time spent at risk Ratio Compares between two measures (two rates, odds or proportions) what is counted in numerator isn’t always in the denominator

Theory behind Cause and Effect a specific event or condition that is necessary for the occurrence of the disease at the moment it occurred, given that other conditions are fixed Effect: A change in a population measure brought upon by a certain event In other words, a cause is an event that must precede the disease in order for the disease to occur, in such a way that if we removed that event, given all other conditions being fixed, the disease would not have occurred.

We need a sufficient causal mechanism for the disease to occur viral infection suitable conditions for virus to grow low immunity

Cause and Effect Y X Effect Need assumptions in order to: Be certain that X caused Y Measure the “effect” of X on Y Not compatible with our world ! In order for me to be certain that X causes Y, I need to be able to measure all the component causes that would complete this causal mechanism, and be 100% certain that they all occurred. And that removing x from the equation will definitely make Y impossible to happen, given all other conditions are fixed.

In the same population, at the same time, all other things fixed Effect X (happens) Y ? Effect You will need to bring a population (let’s call them A), and then expose them to X, follow them over time to see if they develop Y or not. Then you go back in time, to the same population A, do not expose them to X, follow them over time to see if they develop Y or not, all other conditions similar to the first scenario. X (doesn’t happen) Y ?

We can only measure associations NOT effects In reality as researchers we can never measure effects, because there is no way we can compare occurrence of an event vs. absence of that event, given all other things fixed, in the SAME population, at the SAME exact period of time At best, we try to estimate effects by measuring association (after controlling for confounding and making many other assumptions)

Thank you Questions?