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阿片样生长因子、[Met5]-脑啡肽和ζ阿片受体存在于人和小鼠的皮肤中,并持续发挥作用以抑制表皮中的DNA合成。

The opioid growth factor, [Met5]-enkephalin, and the zeta opioid receptor are present in human and mouse skin and tonically act to inhibit DNA synthesis in the epidermis.

作者信息

Zagon I S, Wu Y, McLaughlin P J

机构信息

Department of Neuroscience, The Pennsylvania State University, College of Medicine, Hershey, U.S.A.

出版信息

J Invest Dermatol. 1996 Mar;106(3):490-7. doi: 10.1111/1523-1747.ep12343712.

Abstract

Opioid peptides serve as tonically active negative growth factors in neural and non-neural cells, in addition to being neuromodulators. To investigate the involvement of opioids in homeostatic renewal of epithelial cells in the epidermis, mice were given systemic injections of the potent opioid antagonist, naltrexone (NTX) (20 mg/kg). Disruption of opioid-receptor interaction by NTX resulted in an elevation of 42 and 72% in DNA synthesis in skin from the dorsum and plantar surface of the hindfoot, respectively, within 2 h; response to NTX was dependent on the circadian rhythm in each region examined. Injection of the naturally occurring and potent opioid growth factor (OGF), [Met5]-enkephalin, at 1 mg/kg depressed DNA synthesis in the dorsum and plantar surface by 42 and 19%, respectively, within 2 h; the effects of OGF complied with the pattern of circadian rhythm in each area of skin. The decreases in labeling index evoked by OGF were blocked by concomitant administration of the opioid antagonist, naloxone (10 mg/kg); naloxone alone at the dosage utilized had no influence on cell replicative processes. In tissue culture studies, OGF and NTX respectively depressed and elevated DNA synthesis. Both OGF and its receptor, zeta, were detected in all but the cornified layer of the epidermis in murine skin from the dorsum, plantar surface, pinnae, and tail. In addition, both peptide and receptor were observed in basal and suprabasal cells of the human epidermis. These results lead to the suggestion that an endogenous opioid peptide and its receptor are present and govern cellular renewal processes in the skin in a direct manner, regulating DNA synthesis in a tonically inhibitory, circadian rhythm-dependent fashion.

摘要

阿片肽除作为神经调质外,在神经细胞和非神经细胞中还起着持续活跃的负生长因子的作用。为了研究阿片类物质在表皮上皮细胞稳态更新中的作用,给小鼠全身注射强效阿片拮抗剂纳曲酮(NTX)(20毫克/千克)。NTX破坏阿片受体相互作用导致后足背部和足底皮肤DNA合成在2小时内分别升高42%和72%;对NTX的反应取决于所检查每个区域的昼夜节律。注射1毫克/千克天然存在的强效阿片生长因子(OGF)[Met5] - 脑啡肽,在2小时内分别使背部和足底表面的DNA合成降低42%和19%;OGF的作用符合皮肤各区域的昼夜节律模式。OGF引起的标记指数下降被同时给予的阿片拮抗剂纳洛酮(10毫克/千克)阻断;所用剂量的纳洛酮单独对细胞复制过程没有影响。在组织培养研究中,OGF和NTX分别降低和升高DNA合成。在小鼠背部、足底表面、耳廓和尾巴皮肤的表皮除角质层外的所有层中均检测到OGF及其受体ζ。此外,在人类表皮的基底细胞和基底上层细胞中也观察到了该肽和受体。这些结果表明,内源性阿片肽及其受体存在,并以直接方式控制皮肤中的细胞更新过程,以昼夜节律依赖的方式调节DNA合成。

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