Multiple roles for endothelin in melanocyte development: regulation of progenitor number and stimulation of differentiation.

IF 3.7 2区 生物学 Q1 DEVELOPMENTAL BIOLOGY
K Reid, A M Turnley, G D Maxwell, Y Kurihara, H Kurihara, P F Bartlett, M Murphy
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引用次数: 0

Abstract

Melanocytes in the skin are derived from the embryonic neural crest. Recently, mutations in endothelin 3 and the endothelin receptor B genes have been shown to result in gross pigment defects, indicating that this signalling pathway is required for melanocyte development. We have examined the effects of endothelins on melanocyte progenitors in cultures of mouse neural crest. Firstly, they stimulate an increase in progenitor number and act synergistically with another factor, Steel factor, in the survival and proliferation of the progenitors. These findings are consistent with findings from mice with natural mutations in the endothelin receptor B gene, which show an early loss of melanocyte progenitors. Secondly, endothelins induce differentiation of the progenitors into fully mature pigmented melanocytes. This finding is consistent with the expression of endothelins in the skin of mice at the initiation of pigmentation. The melanocytes generated in endothelin-treated cultures also become responsive to alpha melanocyte-stimulating hormone, which then acts to regulate the activity of the pigmentation pathway. These findings indicate two key roles for endothelin in melanocyte development: regulation of expansion of the progenitor pool and differentiation of progenitors into mature melanocytes.

内皮素在黑素细胞发育中的多重作用:调节祖细胞数量和刺激分化。
皮肤中的黑素细胞来源于胚胎神经嵴。最近,内皮素3和内皮素受体B基因的突变被证明会导致严重的色素缺陷,这表明这一信号通路是黑素细胞发育所必需的。我们研究了内皮素对小鼠神经嵴黑素细胞祖细胞的影响。首先,它们刺激祖细胞数量的增加,并与另一个因子钢铁因子协同作用于祖细胞的存活和增殖。这些发现与内皮素受体B基因自然突变小鼠的发现一致,内皮素受体B基因显示黑色素细胞祖细胞的早期丢失。其次,内皮素诱导祖细胞分化为完全成熟的黑色素细胞。这一发现与色素沉着开始时小鼠皮肤内皮素的表达一致。在内皮素处理的培养物中产生的黑素细胞也对α -黑素细胞刺激激素产生反应,该激素随后调节色素沉着途径的活性。这些发现表明内皮素在黑素细胞发育中的两个关键作用:调节祖细胞池的扩张和祖细胞向成熟黑素细胞的分化。
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来源期刊
Development
Development 生物-发育生物学
CiteScore
6.70
自引率
4.30%
发文量
433
审稿时长
3 months
期刊介绍: Development’s scope covers all aspects of plant and animal development, including stem cell biology and regeneration. The single most important criterion for acceptance in Development is scientific excellence. Research papers (articles and reports) should therefore pose and test a significant hypothesis or address a significant question, and should provide novel perspectives that advance our understanding of development. We also encourage submission of papers that use computational methods or mathematical models to obtain significant new insights into developmental biology topics. Manuscripts that are descriptive in nature will be considered only when they lay important groundwork for a field and/or provide novel resources for understanding developmental processes of broad interest to the community. Development includes a Techniques and Resources section for the publication of new methods, datasets, and other types of resources. Papers describing new techniques should include a proof-of-principle demonstration that the technique is valuable to the developmental biology community; they need not include in-depth follow-up analysis. The technique must be described in sufficient detail to be easily replicated by other investigators. Development will also consider protocol-type papers of exceptional interest to the community. We welcome submission of Resource papers, for example those reporting new databases, systems-level datasets, or genetic resources of major value to the developmental biology community. For all papers, the data or resource described must be made available to the community with minimal restrictions upon publication. To aid navigability, Development has dedicated sections of the journal to stem cells & regeneration and to human development. The criteria for acceptance into these sections is identical to those outlined above. Authors and editors are encouraged to nominate appropriate manuscripts for inclusion in one of these sections.
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