Philip Morris
Tools of Risk Analysis Applications of Epidemiology
Fields
- Author
- Cole, P.
- Area
- LOGUE,MAYADA/OFFICE
- Type
- OUTL, OUTLINE
- Site
- N426
- Named Person
- Austin, H.
- Cole, P.
- Delzell, E.
- Cole, P.
- Request
- Stmn/R1-072
- Document File
- 2025545619/2025546382/Harvard University Office of
- Continuing Education Short Course Program Harvard School
- of Public Health
- Continuing Education Short Course Program Harvard School
- Named Organization
- Am J Epidemiol
- OSHA, Occupational Safety & Health Administration
- Litigation
- Stmn/Produced
- Characteristic
- EXTR, EXTRA
- MARG, MARGINALIA
- Master ID
- 2025545673/6381
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- Date Loaded
- 24 May 1999
- UCSF Legacy ID
- bkp02a00
Document Images
TOOLS OF RISK ANALYSIS
Applications of Epidemiology
I. Overview
II. Risk assessment epidemiology
A. Definition: a description of the change in the
incidence rate of a disease due to
a known change in the level of
exposure to a cause
B. Purposes: - guide public health policies
- guide the regulatory process
__~ assist in tort resolution
C. Foundations - basic science - ~Q~e ~ ~~~e~
~ - animal studies `dcseribe eney
D. Growing importance of epidemiology : - 0-5u-3~3 tkie-
~-'advances in methodology a tj~-F IcLat.
!~ reduced reliance on animal
research CSF~_c~ts oaU~~~
bases in law
~'nlmciCs hcwe c~ stnc~ l~ expo:~~ o rx~ ~hC_ destre_ ~~rc&~ e. o rz oS{'ec"E-
III. Epidemiology - general
A. Definitions: the study of the distribution and
determinants of disease in man
an observational science dealing
with the environmental causes of
diseases of human beings
B. Strengths - human beings
- human lifestyles
C. Limitations - non-experimental
- often qualitative
IV. Selected measures
A. Incidence rate
I = new cases/(population x time)
~
example: the incidence rate of leukemia is ~
i
k 10.1 cases per 100,000 person-years N
~
B. R
s R = new cases/population C11
L
example:
the lifetime risk of developing
leukemia is 700 per 100,000 *
lk
C11
~
persons, or 0.7%
~
;A

2
C. Relative incidence rate (relative risk, RR)
R?q= the incidence rate in an exposed group
divided by that in a non-exposed group
example: the RI of leukemia among rubber
workers is 4.5 (base = 1.0) D. Standardized mortality ratio
SMR = the number of deaths observed (usually
in an occupational group) divided by
the number of deaths expected
example: among pliofilm workers the SMR
is 337 (base = 100)
V. Study designs - general
A. Descriptive studies aF, `1~ »cl~vrcluc~ ~'~0c`~ ~ejn-c~ u
s~ud~~ C~rrela E~,~Q 5~~d~es
o_qroucto 1.3
B. Follow-up (cohort) studies
a. prospective is
b. retrospective +
C. Case-control- lcss «,j2,,4,,+ ~~- R A- s elec~n- °-6
\DXI,tr) w;-~h PeePz, wO"rt ar'd wi1'hoLd' drstLLse 14 de1ermrne exFb2U'u_
D. Proportional mortality ratio (PMR)
VI. Study designs - specific
Limitations:
A. The retrospective follow-up design
Example: 1165 rubber hydrochloride (pliofilm)
workers followed-up from 1950-81 experi-
enced 9 deaths from leukemia with 2.7
expected, an SMR of 337
Advantages: fast, inexpensive (- -0
exposure based
profile of effects (all causes of death)
relatively free of bias ( s'{6ic,omct~l~ cc-rcr~
inadequate exposure-possible (jn~a
inadequate exposure documentation -
usual
~
prone to chance-
0
prone to confounding N
C11

- 3 -
B. The case-control design 0~'fcr) ct6cd -A- R14
~ o~ ~f s r~ ereal -a) 0 J- (J ~i cJ }~reer s~
Example: 138 adults with leukemia, resident in
Olmsted County M, were compared with
276 adults without leukemia. Informa-
tion on benzene exposure was abstracted
from medical records. Among persons
with benzene exposure, the RI of leuke-
mia was 3.3 compared to persons without
exposure.
Advantages : fast 6 s
profile of exposures
control confounding
precise (not prone to chance)
suitable for rare disease
Limitations: single disease
only relative measures cp juests ~
prone to bias -c/rffrc.c,~ -1-o fi)+-ove-. 7"h-G2?Le 4'u~ 'Ae sa me 2s ~, e, ~cs
VI I. Interpretations -4-0-w Ck0_t)Vf_5f_
I~lu e r~e ~ oczf ~e~rn ~
A. Chance
B. Bias
d ~s~ c~n ~hc~~e i u
C. Confounding -
D. Valid d 1seQ.,SeS
causal
null
Comment: not mutually exclusive
not permanent
VIII. Causality
A. Individual study
strength
internal consistency
biological credibility
B. Abstract, general case
external consistency
response to manipulation

- 4 -
C. Specific individual case - ~or CC.-ses
relevant exposure
absence of alternative cause
IX. Benzene and leukemia - A model risk assessment
A. Basic science
not genotoxic n 'c-
damages chromosomes -~nv'- ciec- hcd
~-nec i anlsy~
B. Animal studies
carcinogenic
leukemogenicity problematic 14 p~
C. Epidemiologic studies l'7 s1;eg
~~~\,generally positive for AML -r\ecc-~,Ue~
S~~zs ~G; ~poor quantification of exposure
some potential confounding - o{-t,,r so1,;{rrt
D. Epidemiologic data*
- observed deaths : CL 19
- expected deaths: 9.6
- total deaths: 1273
- mean cum. exposure: 42 ppm-yrs
E. Risk assessment
- excess deaths: 19-9.6 = 9.4
- excess deaths/1000: 9. 4/1 .273 = 7. 4/1000 -~~1'~'~~
- baseline risk: 7/1000
- doubling dose: -
~ (14/14.7)(42 ppm-yrs) = 40 ppm-yrs
~'rn c~es ~ ,~eed ~ be cxposed 4-0 do«b!e AhL P ts iC
X. The OSHA standard ~~G Pp-ft.U
A. For many years
= 10 ppm 8 hr TWA
30 yrs x 10 ppm = 300 ppm-yrs
ti 7 doublings = 800/1000 = unacceptable
1.7 additions ti 56 deaths/1000
B. Currently =IL ppm 8 hr TWA
'3
` 30 ppm yrs
ti 1.75 baseline ti 5 excess
deaths/1000 exposed

- 5 -
C. Issues - _A'lodel CissLCmes -
- linear dose response
- non-threshold
- other
4 September 1991
Philip Cole, M.D.
Austin H, Delzell E, Cole P: Benzene and leukemia: A review of
thE: literature and a risk assessment. Am J Epidemiol
127: 419-439, 1988.
