Literature DB >> 21790323

Nitric oxide signaling as a common target of organohalogens and other neuroendocrine disruptors.

Margarita C Currás-Collazo1.   

Abstract

Organohalogen compounds such as polychlorinated biphenyls (PCB) and polybrominated diphenyl ethers (PBDE) are global environmental pollutants and highly persistent, bioaccumulative chemicals that produce adverse effects in humans and wildlife. Because of the widespread use of these organohalogens in household items and consumer products, indoor contamination is a significant source of human exposure, especially for children. One significant concern with regard to health effects associated with exposure to organohalogens is endocrine disruption. Toxicological studies on organohalogen pollutants primarily focused on sex steroid and thyroid hormone actions, and findings have largely shaped the way one envisions their disruptive effects occurring. Organohalogens exert additional effects on other systems including other complex endocrine systems that may be disregulated at various levels of organization. Over the last 20 years evidence has mounted in favor of a critical role of nitric oxide (NO) in numerous functions ranging from neuroendocrine functions to learning and memory. With its participation in multiple systems and action at several levels of integration, NO signaling has a pervasive influence on nervous and endocrine functions. Like blockers of NO synthesis, PCBs and PBDEs produce multifaceted effects on physiological systems. Based on this unique set of converging information it is proposed that organohalogen actions occur, in part, by hijacking processes associated with this ubiquitous bioactive molecule. The current review examines the emerging evidence for NO involvement in selected organohalogen actions and includes recent progress from our laboratory that adds to our current understanding of the actions of organohalogens within hypothalamic neuroendocrine circuits. The thyroid, vasopressin, and reproductive systems as well as processes associated with long-term potentiation were selected as sample targets of organohalogens that rely on regulation by NO. Information is provided about other toxicants with demonstrated interference of NO signaling. Our focus on the convergence between NO system and organohalogen toxicity offers a novel approach to understanding endocrine and neuroendocrine disruption that is particularly problematic for developing organisms. This new working model is proposed as a way to encourage future study in elucidating common mechanisms of action that are selected with a better operational understanding of the systems affected.

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Year:  2011        PMID: 21790323     DOI: 10.1080/10937404.2011.578564

Source DB:  PubMed          Journal:  J Toxicol Environ Health B Crit Rev        ISSN: 1093-7404            Impact factor:   6.393


  6 in total

1.  Perinatal exposure to octabromodiphenyl ether mixture, DE-79, alters the vasopressinergic system in adult rats.

Authors:  Mhar Y Alvarez-Gonzalez; Eduardo Sánchez-Islas; Samuel Mucio-Ramirez; Patricia de Gortari; María I Amaya; Prasada Rao S Kodavanti; Martha León-Olea
Journal:  Toxicol Appl Pharmacol       Date:  2020-02-04       Impact factor: 4.219

2.  Perinatal exposure to organohalogen pollutants decreases vasopressin content and its mRNA expression in magnocellular neuroendocrine cells activated by osmotic stress in adult rats.

Authors:  Samuel Mucio-Ramírez; Eduardo Sánchez-Islas; Edith Sánchez-Jaramillo; Margarita Currás-Collazo; Victor R Juárez-González; Mhar Y Álvarez-González; L E Orser; Borin Hou; Francisco Pellicer; Prasada Rao S Kodavanti; Martha León-Olea
Journal:  Toxicol Appl Pharmacol       Date:  2017-06-01       Impact factor: 4.219

3.  Diverse influences of androgen-disrupting chemicals on immune responses mounted by macrophages.

Authors:  Kyong Hoon Kim; Seung-min Yeon; Hyun Gyung Kim; Hyun Suk Choi; Hyojeung Kang; Hee-Deung Park; Tae Won Park; Seung Pil Pack; Eun Hee Lee; Youngjoo Byun; Sang-Eun Choi; Kenneth Sung Lee; Un-Hwan Ha; Yong Woo Jung
Journal:  Inflammation       Date:  2014-06       Impact factor: 4.092

4.  Persistent autism-relevant behavioral phenotype and social neuropeptide alterations in female mice offspring induced by maternal transfer of PBDE congeners in the commercial mixture DE-71.

Authors:  Elena V Kozlova; Matthew C Valdez; Maximillian E Denys; Anthony E Bishay; Julia M Krum; Kayhon M Rabbani; Valeria Carrillo; Gwendolyn M Gonzalez; Gregory Lampel; Jasmin D Tran; Brigitte M Vazquez; Laura M Anchondo; Syed A Uddin; Nicole M Huffman; Eduardo Monarrez; Duraan S Olomi; Bhuvaneswari D Chinthirla; Richard E Hartman; Prasada Rao S Kodavanti; Gladys Chompre; Allison L Phillips; Heather M Stapleton; Bernhard Henkelmann; Karl-Werner Schramm; Margarita C Curras-Collazo
Journal:  Arch Toxicol       Date:  2021-10-23       Impact factor: 5.153

5.  The PBDE metabolite 6-OH-BDE 47 affects melanin pigmentation and THRβ MRNA expression in the eye of zebrafish embryos.

Authors:  Wu Dong; Laura J Macaulay; Kevin Wh Kwok; David E Hinton; P Lee Ferguson; Heather M Stapleton
Journal:  Endocr Disruptors (Austin)       Date:  2014

Review 6.  Endocrine Disruption of Vasopressin Systems and Related Behaviors.

Authors:  Heather B Patisaul
Journal:  Front Endocrinol (Lausanne)       Date:  2017-06-19       Impact factor: 5.555

  6 in total

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