Abstract

The mechanisms by which lead (Pb) alters immune reactivities are multifactorial, both MHC and non-MHC genes are likely involved, in that there appear to be independent effects on T cells, B cells and macrophages, and these effects appear to involve different cytokines and signaling/transcription factors. The long-term goal of this project is to determine the sub cellular mechanisms by which Pb alters lymphocyte development (naive to memory cells) and the activation and reactivity of memory T cells which could influence immunity causing hypo- or hyper-responsiveness. This proposal tests the hypothesis that the heavy metal Pb can alter immune status by biochemical and molecular modulations resulting in a preferential environment for development of type-2 responses, and dependent on the particular type of immune response needed for defense against an infectious agent, cancer or regulation of self-reactive response, this """"""""skewing"""""""" may increase pathologies associated with lessened type-] and enhanced lype-2 immune responses. Synergies between chemical, physical and/or emotional stresses can enhance the skewing of immune reactivities toward type-] or type-2 responses; short-term imbalance is needed for appropriate defenses, but long-term imbalance exacerbates pathologies. Thus, an environmental agent such as Pb may alter the balance enough to increase morbidity. Mutant (genetic over-expressing or deficient) H-2d mice will be employed to assess the involvement of specific genes in the """"""""skewing"""""""" phenomenon. Specific questions to be addressed are: how Pb alters kinetic production of IFN?gamma; how macrophage reactivities, such as production of ILl 0, ILl 2 or ILl 8, are altered, and whether cellular thiol modifications are involved; whether Pb """"""""skewing"""""""" can be achieved with T cells specific only to OVA or whether T cells with self-reactivity (or metal-related specificities) are needed, whether B cells or a particular type of T cell subset (e.g., NK-like T cells) are required and within what particular cytokine environment; what molecular mechanisms are involved with the IL-4 reactivities of T cells; and what cells are responsible for the type-2 environment induced by Pb. Cell types will be assayed by flow cytometry and immunofluorescence microscopy. The presence of cytokines and signaling factors will be assessed by ELISA, microarray analysis (or RNAse protection) and western analyses. Pb heads the ATSDR list of toxic substances and its potential to induce or modify incidence of diseases associated with immune reactivities needs to be better understood. This cellular and molecular approach should identify the mechanisms by which Pb is immunomodulatory and assist evaluation of its health hazard and the molecular basis for the risks in exposure.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Project (R01)
Project #
5R01ES011135-02
Application #
6623926
Study Section
Alcohol and Toxicology Subcommittee 4 (ALTX)
Program Officer
Mastin, Patrick
Project Start
2002-03-27
Project End
2005-12-31
Budget Start
2003-01-01
Budget End
2003-12-31
Support Year
2
Fiscal Year
2003
Total Cost
$273,006
Indirect Cost

  Institution

Name
Wadsworth Center
Department
Type
DUNS #
153695478
City
Menands
State
NY
Country
United States
Zip Code
12204

  Publications

Zhang, Yubin; Bolivar, Valerie J; Lawrence, David A (2013) Maternal exposure to mercury chloride during pregnancy and lactation affects the immunity and social behavior of offspring. Toxicol Sci 133:101-11
Zhang, Yubin; Bolivar, Valerie J; Lawrence, David A (2012) Developmental exposure to mercury chloride does not impair social behavior of C57BL/6 ýý BTBR F(1) mice. J Immunotoxicol 9:401-10
Kasten-Jolly, Jane; Pabello, Nina; Bolivar, Valerie J et al. (2012) Developmental lead effects on behavior and brain gene expression in male and female BALB/cAnNTac mice. Neurotoxicology 33:1005-20
Kasten-Jolly, Jane; Heo, Yong; Lawrence, David A (2011) Central nervous system cytokine gene expression: modulation by lead. J Biochem Mol Toxicol 25:41-54
Zhang, Yubin; Gao, Donghong; Bolivar, Valerie J et al. (2011) Induction of autoimmunity to brain antigens by developmental mercury exposure. Toxicol Sci 119:270-80
Gao, Donghong; Lawrence, David A (2010) Dendritic cells in immunotoxicity testing. Methods Mol Biol 598:259-81
Kasten-Jolly, Jane; Heo, Yong; Lawrence, David A (2010) Impact of developmental lead exposure on splenic factors. Toxicol Appl Pharmacol 247:105-15
Emeny, Rebecca T; Marusov, Gregory; Lawrence, David A et al. (2009) Manipulations of metallothionein gene dose accelerate the response to Listeria monocytogenes. Chem Biol Interact 181:243-53
Lawerence, David A; Bolivar, Valerie J; Hudson, Chad A et al. (2007) Erratum to ""Antibody induction of lupus-like neuropsychiatric manifestations"" [J.Neuroimmunol.182(2007) 185-194]. J Neuroimmunol 192:235
Gao, Donghong; Mondal, Tapan K; Lawrence, David A (2007) Lead effects on development and function of bone marrow-derived dendritic cells promote Th2 immune responses. Toxicol Appl Pharmacol 222:69-79

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