Biphasic effects of minoxidil on the proliferation and differentiation of normal human keratinocytes.

N Boyera, I Galey, B A Bernard
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引用次数: 33

Abstract

Minoxidil is the most used drug with proved effects in the treatment of androgenetic alopecia (AGA), but little is known about its pharmacological activity and target cells in hair follicles. As AGA is characterized by follicle atrophy, accelerated hair cycles and hair fiber thinning, we postulated that keratinocyte proliferation/differentiation is affected and we tested Minoxidil's effects on those parameters. Normal human keratinocytes (NHK) of follicular or epidermal origin were cultured in the presence of Minoxidil (0, 0.1, 1, 10, 100, 1,000 microM) during 5-8 days in various media (high-/low-calcium content, with or without serum). Proliferation was assessed by mitochondrial dehydrogenase activity (XTT), BrdU incorporation, lysosome numeration (neutral red incorporation) and total protein dosage. Drug-induced cytotoxicity was measured by lactate dehydrogenase release in culture supernatant, and pro-differentiating effects were evaluated by relative involucrin expression (ELISA dosage). On this basis, we showed that Minoxidil had biphasic effects on the proliferation and differentiation of NHK: Minoxidil stimulated NHK proliferation at micromolar doses, while antiproliferative, pro-differentiative and partially cytotoxic effects were observed with millimolar concentrations. We can hypothesize that Minoxidil hypertrichotic activity in vivo is possibly mediated by the maintenance of proliferative potential in follicular keratinocytes precociously committed to differentiation.

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米诺地尔对正常人角质形成细胞增殖和分化的双相影响。
米诺地尔是治疗雄激素性脱发(AGA)最常用的药物,但对其药理活性和毛囊中的靶细胞知之甚少。由于AGA的特点是毛囊萎缩,头发周期加快和头发纤维变薄,我们假设角质细胞增殖/分化受到影响,我们测试了米诺地尔对这些参数的影响。在米诺地尔(0、0.1、1、10、100、1000微米)的存在下,在各种培养基(高/低钙含量,含或不含血清)中培养5-8天,滤泡或表皮来源的正常人角质形成细胞(NHK)。通过线粒体脱氢酶活性(XTT)、BrdU掺入、溶酶体数量(中性红掺入)和总蛋白剂量评估增殖情况。通过培养上清乳酸脱氢酶释放量检测药物诱导细胞毒性,通过酶联免疫吸附法(ELISA)检测天花素的相对表达量。在此基础上,我们发现米诺地尔对NHK的增殖和分化具有双相作用:米诺地尔在微摩尔剂量下刺激NHK的增殖,而在毫摩尔浓度下观察到抗增殖、促分化和部分细胞毒性作用。我们可以假设米诺地尔在体内的多毛活性可能是通过维持早熟分化的滤泡角质形成细胞的增殖潜能来介导的。
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