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小眼畸形相关转录因子对色素细胞特异性基因表达的调控

Regulation of pigment cell-specific gene expression by MITF.

作者信息

Shibahara S, Yasumoto K, Amae S, Udono T, Watanabe K, Saito H, Takeda K

机构信息

Department of Molecular Biology and Applied Physiology, Tohoku University School of Medicine, Sendai, Miyagi, Japan.

出版信息

Pigment Cell Res. 2000;13 Suppl 8:98-102. doi: 10.1034/j.1600-0749.13.s8.18.x.

Abstract

Melanocyte and retinal pigment epithelium (RPE) specifically express tyrosinase and other melanin-producing enzymes. Microphthalmia-associated transcription factor (Mitf), encoded at the mouse microphthalmia locus, regulates the development and survival of many cell types, including melanocyte and RPE. MITF, the human homolog of Mitf, consists of at least four isoforms with distinct amino-termini, referred to as A, MITF-C, MITF-H, and MITF-M. MITF-M is exclusively expressed in melanocytes and melanoma cells, and thus represents the melanocyte lineage-specific isoform. In contrast, other isoforms are expressed in many cell types so far examined. These isoforms appear to function as transcriptional activators of the melanogenesis genes, as assessed by transient transfection assays in cultured cells. Functional significance of Mitf-M in melanocyte differentiation was verified by the molecular lesion of black-eyed white Mitf(mi-bw) mice, which lack melanocytes but have normal RPE. The Mitf gene of this mutant has the insertion of an L1 retrotransposable element in the intron between exon 3 and exon 4, leading to complete repression of Mitf-M mRNA expression. Taken together, these results suggest that melanogenesis in melanocyte and RPE is regulated by separate Mitf/MITF isoforms. Recent findings on the multiplicity of MITF isoforms are summarized.

摘要

黑素细胞和视网膜色素上皮(RPE)特异性表达酪氨酸酶和其他产生黑色素的酶。小眼畸形相关转录因子(Mitf),由小鼠小眼畸形基因座编码,调节包括黑素细胞和RPE在内的多种细胞类型的发育和存活。MITF是Mitf的人类同源物,由至少四种具有不同氨基末端的异构体组成,分别称为A、MITF-C、MITF-H和MITF-M。MITF-M仅在黑素细胞和黑色素瘤细胞中表达,因此代表黑素细胞谱系特异性异构体。相比之下,其他异构体在迄今为止检测的许多细胞类型中都有表达。通过培养细胞中的瞬时转染试验评估,这些异构体似乎作为黑素生成基因的转录激活因子发挥作用。黑眼白Mitf(mi-bw)小鼠的分子损伤验证了Mitf-M在黑素细胞分化中的功能意义,该小鼠缺乏黑素细胞但RPE正常。该突变体的Mitf基因在第3外显子和第4外显子之间的内含子中插入了一个L1反转录转座元件,导致Mitf-M mRNA表达完全受到抑制。综上所述,这些结果表明黑素细胞和RPE中的黑素生成受不同的Mitf/MITF异构体调节。本文总结了关于MITF异构体多样性的最新发现。

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