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Risk characterization

In the last step, a hazard quotient (HQ) as an indicator of risks associated with health effects other than cancer and excess cancer risk (ECR) as the incremental probability of an exposed person developing cancer over a lifetime, are calculated by integrating toxicity and exposure information, as shown below. If HQ>1, there may be concern for potential adverse systemic health effects in the exposed individuals. If HQ ≤ 1, there may be no concern. It should be noted that HQs are scaling factors and they are not statistically based. The EPA's acceptable criterion for carcinogenic risks is based on public policy as described in the National Contingency Plan (NCP) and is the exposure concentration that represent an ECR in the range of 10 -4 – 10 -6 , i.e. 1 in 10,000 to 1 in 1,000,000 excess cancer cases ( EPA, 1990 ).

Noncancer Risk: HazardQuotient ( HQ ) = ADD RfD size 12{ ital "HazardQuotient" \( ital "HQ" \) = { { ital "ADD"} over { ital "RfD"} } } {}

Excess Cancer Risk (ECR): ECR = L ( ADD ) xCSF size 12{ ital "ECR"=L \( ital "ADD" \) ital "xCSF"} {}

To account for exposures to multiple COCs via multiple pathways, individual HQs are summed to provide an overall Hazard Index (HI). If HI>1, COCs are segregated based on their critical health end-point and separate target organ-specific HIs are calculated. Only if target organ-specific HI>1, is there concern for potential health effects for that end-point (e.g. liver, kidney, respiratory system).

Cumulative Noncancer Risk: HazardIndex = HI = COC NC = 1 n ( HQ o + HQ d + HQ i ) size 12{ ital "HazardIndex"= ital "HI"= Sum cSub { size 8{ ital "COC" rSub { size 6{ ital "NC"} } =1} } cSup {n} { \( ital "HQ" rSub { size 8{o} } + ital "HQ" rSub { size 8{d} } + ital "HQ" rSub { size 8{i} } \) } } {}

Cumulative Excess Cancer Risk: COC C = 1 n ECR = COC C = 1 n ( ECR o + ECR d + ECR i ) size 12{ Sum cSub { size 8{ ital "COC" rSub { size 6{C} } =1} } cSup {n} { ital "ECR"} size 12{ {}= Sum cSub { ital "COC" rSub { size 6{C} } =1} cSup {n} { \( ital "ECR" rSub {o} size 12{+ ital "ECR" rSub {d} } size 12{+ ital "ECR" rSub {i} } size 12{ \) }} }} {}

Here, o, d and i subscripts express oral (ingestion), dermal contact and inhalation pathways.

As discussed above, the HQ, HI, and ECR estimates are performed for RME and CTE scenarios separately in the case of deterministic risk assessment. Although EPA published the probabilistic risk assessment guidelines in 2001 ( EPA, 2001 ), its application has so far been limited. Proper evaluation of uncertainties, which are associated with compounded conservatism and potential underestimation of quantitative risk estimates (e.g. due to the presence of COCs without established toxicity values), is intrinsic to any risk-based scientific assessment. In general, uncertainties and limitations are associated with sampling and analysis, chemical fate and transport, exposure parameters, exposure modeling, and human dose-response or toxicity assessment (derivation of CSFs/RfDs, extrapolation from high animal doses to low human doses), and site-specific uncertainties.

Conclusion

The improvement in the scientific quality and validity of health risk estimates depends on advancements in our understanding of human exposure to, and toxic effects associated with, chemicals present in environmental and occupational settings. For example, life-cycle of and health risks associated with pharmaceuticals in the environment is poorly understood due to lack of environmental concentration and human exposure data despite extensive toxicological data on drugs. There are many other examples for which either data on exposure or toxicity or both have not yet been developed, preventing quantitative assessment of health risks and development of policies that protect the environment and public health at the same time. Therefore, it is important to continue to develop research data to refine future risk assessments for informed regulatory decision-making in environmental sustainability and to ensure that costs associated with different technological and/or engineering alternatives are scientifically justified and public health-protective. One area that, particularly, requires advancement is the assessment of health risks of chemical mixtures. Current risk assessment approaches consider one chemical at a time. However, chemicals are present in mixtures in the environment. Furthermore, physical, chemical and biological transformations in the environment and interactions among chemicals in the environment may change the toxic potential of the mixture over time. Thus, risk assessment is an evolving scientific discipline that has many uncertainties in all of the four steps. These uncertainties should be thoroughly documented and discussed and the risk assessment results should be interpreted within the context of these uncertainties.

Questions & Answers

A golfer on a fairway is 70 m away from the green, which sits below the level of the fairway by 20 m. If the golfer hits the ball at an angle of 40° with an initial speed of 20 m/s, how close to the green does she come?
Aislinn Reply
cm
tijani
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John Reply
what is physics
Siyaka Reply
A mouse of mass 200 g falls 100 m down a vertical mine shaft and lands at the bottom with a speed of 8.0 m/s. During its fall, how much work is done on the mouse by air resistance
Jude Reply
Can you compute that for me. Ty
Jude
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David Reply
what is viscosity?
David
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emma Reply
what is chemistry
Youesf Reply
what is inorganic
emma
Chemistry is a branch of science that deals with the study of matter,it composition,it structure and the changes it undergoes
Adjei
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Adjanou
chemistry could also be understood like the sexual attraction/repulsion of the male and female elements. the reaction varies depending on the energy differences of each given gender. + masculine -female.
Pedro
A ball is thrown straight up.it passes a 2.0m high window 7.50 m off the ground on it path up and takes 1.30 s to go past the window.what was the ball initial velocity
Krampah Reply
2. A sled plus passenger with total mass 50 kg is pulled 20 m across the snow (0.20) at constant velocity by a force directed 25° above the horizontal. Calculate (a) the work of the applied force, (b) the work of friction, and (c) the total work.
Sahid Reply
you have been hired as an espert witness in a court case involving an automobile accident. the accident involved car A of mass 1500kg which crashed into stationary car B of mass 1100kg. the driver of car A applied his brakes 15 m before he skidded and crashed into car B. after the collision, car A s
Samuel Reply
can someone explain to me, an ignorant high school student, why the trend of the graph doesn't follow the fact that the higher frequency a sound wave is, the more power it is, hence, making me think the phons output would follow this general trend?
Joseph Reply
Nevermind i just realied that the graph is the phons output for a person with normal hearing and not just the phons output of the sound waves power, I should read the entire thing next time
Joseph
Follow up question, does anyone know where I can find a graph that accuretly depicts the actual relative "power" output of sound over its frequency instead of just humans hearing
Joseph
"Generation of electrical energy from sound energy | IEEE Conference Publication | IEEE Xplore" ***ieeexplore.ieee.org/document/7150687?reload=true
Ryan
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Maurice Reply
what are the types of wave
Maurice
answer
Magreth
progressive wave
Magreth
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Muhammad Reply
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Mohammed
hi
Mujahid
A string is 3.00 m long with a mass of 5.00 g. The string is held taut with a tension of 500.00 N applied to the string. A pulse is sent down the string. How long does it take the pulse to travel the 3.00 m of the string?
yasuo Reply
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Source:  OpenStax, Sustainability: a comprehensive foundation. OpenStax CNX. Nov 11, 2013 Download for free at http://legacy.cnx.org/content/col11325/1.43
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