4.5 Review

Protein damage by reactive electrophiles: Targets and consequences

Journal

CHEMICAL RESEARCH IN TOXICOLOGY
Volume 21, Issue 1, Pages 117-128

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/tx700235t

Keywords

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Funding

  1. NATIONAL CANCER INSTITUTE [R01CA104590] Funding Source: NIH RePORTER
  2. NATIONAL INSTITUTE OF ENVIRONMENTAL HEALTH SCIENCES [P30ES000267, T32ES007028, P01ES013125, R01ES011811, R01ES010056] Funding Source: NIH RePORTER
  3. NCI NIH HHS [R01 CA104590, CA104590] Funding Source: Medline
  4. NIEHS NIH HHS [P01 ES013125-020004, R01 ES011811-01, R01 ES011811, ES001811, ES013125, P01 ES013125-01A19001, P01 ES013125, R01 ES011811-03, T32 ES007028, ES010056, P01 ES013125-030004, R01 ES010056-01, R01 ES010056-06, ES007028, R01 ES010056-08, P01 ES013125-029001, R01 ES010056-09, R01 ES010056-05, P01 ES013125-039001, R01 ES010056-04, R01 ES011811-05, R01 ES011811-04, R01 ES010056-02, P01 ES013125-01A10004, R01 ES010056-07, R01 ES011811-02, R01 ES010056-03, ES000267, P30 ES000267, R01 ES010056] Funding Source: Medline

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It has been 60 years since the Millers first described the covalent binding of carcinogens to tissue proteins. Protein covalent binding was gradually overshadowed by the emergence of DNA adduct formation as the dominant paradigm in chemical carcinogenesis but re-emerged in the early 1970s as a critical mechanism of drug and chemical toxicity. Technology limitations hampered the characterization of protein adducts until the emergence of mass spectrometry -based proteomics in the late 1990s. The time since then has seen rapid progress in the characterization of the protein targets of electrophiles and the consequences of protein damage. Recent integration of novel affinity chemistries for electrophile probes, shotgun proteomics methods, and systems modeling tools has led to the identification of hundreds of protein targets of electrophiles in mammalian systems. The technology now exists to map the targets of damage to critical components of signaling pathways and metabolic networks and to understand mechanisms of damage at a systems level. The implementation of sensitive, specific analyses for protein adducts from both xenobiotic-derived and endogenous electrophiles offers a means to link protein damage to clinically relevant health effects of both chemical exposures and disease processes.

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