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Publication : Prolactin Regulates Pain Responses via a Female-Selective Nociceptor-Specific Mechanism.

First Author  Patil M Year  2019
Journal  iScience Volume  20
Pages  449-465 PubMed ID  31627131
Mgi Jnum  J:311667 Mgi Id  MGI:6717594
Doi  10.1016/j.isci.2019.09.039 Citation  Patil M, et al. (2019) Prolactin Regulates Pain Responses via a Female-Selective Nociceptor-Specific Mechanism. iScience 20:449-465
abstractText  Many clinical and preclinical studies report an increased prevalence and severity of chronic pain among females. Here, we identify a sex-hormone-controlled target and mechanism that regulates dimorphic pain responses. Prolactin (PRL), which is involved in many physiologic functions, induces female-specific hyperalgesia. A PRL receptor (Prlr) antagonist in the hind paw or spinal cord substantially reduced hyperalgesia in inflammatory models. This effect was mimicked by sensory neuronal ablation of Prlr. Although Prlr mRNA is expressed equally in female and male peptidergic nociceptors and central terminals, Prlr protein was found only in females and PRL-induced excitability was detected only in female DRG neurons. PRL-induced excitability was reproduced in male Prlr(+) neurons after prolonged treatment with estradiol but was prevented with addition of a translation inhibitor. We propose a novel mechanism for female-selective regulation of pain responses, which is mediated by Prlr signaling in sensory neurons via sex-dependent control of Prlr mRNA translation.
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