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光保护黑色素在角质形成细胞的储存溶酶体中得以维持。

Photoprotective Melanin Is Maintained within Keratinocytes in Storage Lysosomes.

作者信息

Neto Matilde V, Hall Michael J, Charneca João, Escrevente Cristina, Seabra Miguel C, Barral Duarte C

机构信息

iNOVA4Health, NOVA Medical School, Faculdade de Ciências Médicas, NMS, FCM, Universidade NOVA de Lisboa, Lisboa, Portugal.

iNOVA4Health, NOVA Medical School, Faculdade de Ciências Médicas, NMS, FCM, Universidade NOVA de Lisboa, Lisboa, Portugal.

出版信息

J Invest Dermatol. 2025 May;145(5):1155-1165.e3. doi: 10.1016/j.jid.2024.08.023. Epub 2024 Sep 18.

DOI:10.1016/j.jid.2024.08.023
PMID:39303907
Abstract

In the skin, melanin is synthesized by melanocytes within melanosomes and transferred to keratinocytes. After being phagocytosed by keratinocytes, melanin polarizes to supranuclear caps that protect against the genotoxic effects of UVR. We provide evidence that melanin-containing phagosomes undergo a canonical maturation process, with the sequential acquisition of early and late endosomal markers. Subsequently, these phagosomes fuse with active lysosomes, leading to the formation of a melanin-containing phagolysosome that we named melanokerasome. Melanokerasomes achieve juxtanuclear positioning through lysosomal trafficking regulators Rab7 and RILP. Mature melanokerasomes exhibit lysosomal markers, elude connections with the endo/phagocytic pathway, are weakly degradative, retain undigested cargo, and are likely tethered to the nuclear membrane. We propose that they represent a lysosomal-derived storage compartment that has exited the lysosome cycle, akin to the formation of lipofuscin in aged cells and dysfunctional lysosomes in lysosomal storage and age-related diseases. This storage lysosome allows melanin to persist for long periods, where it can exert its photoprotective effect efficiently.

摘要

在皮肤中,黑色素由黑素小体内的黑素细胞合成并转移至角质形成细胞。被角质形成细胞吞噬后,黑色素极化至核上帽,以抵御紫外线辐射的基因毒性作用。我们提供的证据表明,含黑色素的吞噬体经历典型的成熟过程,依次获得早期和晚期内体标志物。随后,这些吞噬体与活性溶酶体融合,导致形成一种我们命名为黑素角蛋白体的含黑色素吞噬溶酶体。黑素角蛋白体通过溶酶体运输调节因子Rab7和RILP实现近核定位。成熟的黑素角蛋白体表现出溶酶体标志物,与内吞/吞噬途径无连接,降解能力弱,保留未消化的货物,并且可能与核膜相连。我们提出,它们代表了一个已脱离溶酶体循环的溶酶体衍生储存隔室,类似于衰老细胞中脂褐素的形成以及溶酶体贮积症和与年龄相关疾病中功能失调的溶酶体。这种储存溶酶体使黑色素能够长期存在,在其中它可以有效地发挥其光保护作用。

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