Abstract

Heavy metals such as lead (Pb) represent a major category of contaminants at Superfund sites. Pb has been demonstrated to cause neurological toxicity, behavioral deficits and immunotoxicity. Given the value of effective immune function, it is important to identify risk factors that may influence susceptibility to immunotoxicity. Possible risk modifiers include age and diet, both of which can affect immune status and may, therefore, alter susceptibility to Pb-induced immunotoxicity. In addition, therapeutic measures such as chelation, designed to modify the bioavailability of Pb in vivo, may alter the outcome of Pb exposure. During embryonic development, toxicant exposure may interfere with growth and differentiation, resulting in persistent abnormalities. The neurological effects of embryonic exposure have been described, but less is known about immunotoxic effects as a result of embryonic Pb exposure. Developmental immunotoxicity of Pb may not correlate with that of postnatal exposure, since immune function during development is quite distinct from that of the homeostatic immune system. This project will assess immune function in young animals following embryonic Pb exposure. Results will be obtained from two species (pregnant rat model and in ovo chicken model), thereby increasing possible applicability to other species. A panel of immune assessment assays will be utilized, including in vivo and in vitro measurements. Dietary intake and immune function are tightly linked. One dietary component which is associated with significant immunomodulation and which varies in populations exposed to Pb is protein, both quantity and quality (i.e., amino acid content). Decreases in protein intake have also been shown to amplify Pb retention and subsequent toxicity to other physiological systems. The interactions between altered immune function and altered Pb metabolism as a result of dietary changes could provide useful mechanistic information; in addition, dietary intake in exposed individuals may have predictive and/or therapeutic value. This proposal examines the effect of alterations in dietary protein (quantity and specific amino acid intake) on Pb-induced immunotoxicity in the rat. Chelation, in vivo control of Pb bioavailability, is a primary therapeutic measure for Pb exposure. Dimercaptosuccinate (DMSA), a chelator to be utilized in a proposal regarding rat neurobehavior (Project under Drs. Strupp and Levitski), will be administered to the pregnant rats to examine the abrogation of maternal vs. embryonic Pb- induced immunotoxicity. Results of these two projects will furnish information on DMSA protection of multiple target systems in similar embryonic models by controlling in vivo availability. The proposed research should provide a solid foundation of information regarding the immunotoxic effects of embryonic Pb exposure and the interaction of factors which may modify that immunotoxicity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Hazardous Substances Basic Research Grants Program (NIEHS) (P42)
Project #
3P42ES005950-08S2
Application #
6340936
Study Section
Project Start
1999-04-20
Project End
2001-03-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
8
Fiscal Year
2000
Total Cost
$134,428
Indirect Cost

  Institution

Name
Cornell University
Department
Type
DUNS #
872612445
City
Ithaca
State
NY
Country
United States
Zip Code
14850

  Publications

Smith, Donald; Strupp, Barbara J (2013) The scientific basis for chelation: animal studies and lead chelation. J Med Toxicol 9:326-38
Beaudin, Stephane A; Stangle, Diane E; Smith, Donald R et al. (2007) Succimer chelation normalizes reactivity to reward omission and errors in lead-exposed rats. Neurotoxicol Teratol 29:188-202
Stangle, Diane E; Smith, Donald R; Beaudin, Stephane A et al. (2007) Succimer chelation improves learning, attention, and arousal regulation in lead-exposed rats but produces lasting cognitive impairment in the absence of lead exposure. Environ Health Perspect 115:201-9
Quimby, Fred W; Casey, Ann C; Arquette, Mary Fadden (2005) From dogs to frogs: how pets, laboratory animals, and wildlife aided in elucidating harmful effects arising from a hazardous dumpsite. ILAR J 46:364-9
Chen, Suping; Golemboski, Karen; Piepenbrink, Michael et al. (2004) Developmental immunotoxicity of lead in the rat: influence of maternal diet. J Toxicol Environ Health A 67:495-511
Stangle, Diane E; Strawderman, Myla S; Smith, Donald et al. (2004) Reductions in blood lead overestimate reductions in brain lead following repeated succimer regimens in a rodent model of childhood lead exposure. Environ Health Perspect 112:302-8
Driscoll, Lori L; Carroll, Jenna C; Moon, Jisook et al. (2004) Impaired sustained attention and error-induced stereotypy in the aged Ts65Dn mouse: a mouse model of Down syndrome and Alzheimer's disease. Behav Neurosci 118:1196-205
Lee, Ji-Eun; Dietert, Rodney R (2003) Developmental immunotoxicity of lead: impact on thymic function. Birth Defects Res A Clin Mol Teratol 67:861-7
Savage, Wesley K; Quimby, Fred W; DeCaprio, Anthony P (2002) Lethal and sublethal effects of polychlorinated biphenyls on Rana sylvatica tadpoles. Environ Toxicol Chem 21:168-74
Tang, Jixin; Liste, Hans-Holger; Alexander, Martin (2002) Chemical assays of availability to earthworms of polycyclic aromatic hydrocarbons in soil. Chemosphere 48:35-42

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