p62 sorts Lupus La and selected microRNAs into breast cancer-derived exosomes.

bioRxiv : the preprint server for biology Pub Date : 2025-03-20 DOI:10.1101/2025.03.20.644464

Jordan Matthew Ngo, Justin Krish Williams, Morayma Mercedes Temoche-Diaz, Abinayaa Murugupandiyan, Randy Schekman

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Abstract

Exosomes are multivesicular body-derived extracellular vesicles that are secreted by metazoan cells. Exosomes have utility as disease biomarkers, and exosome-mediated miRNA secretion has been proposed to facilitate tumor growth and metastasis. Previously, we demonstrated that the Lupus La protein (La) mediates the selective incorporation of miR-122 into metastatic breast cancer-derived exosomes; however, the mechanism by which La itself is sorted into exosomes remains unknown. Using unbiased proximity labeling proteomics, biochemical fractionation, superresolution microscopy and genetic tools, we establish that the selective autophagy receptor p62 sorts La and miR-122 into exosomes. We then performed small RNA sequencing and found that p62 depletion reduces the exosomal secretion of tumor suppressor miRNAs and results in their accumulation within cells. Our data indicate that p62 is a quality control factor that modulates the miRNA composition of exosomes. Cancer cells may exploit p62-dependent exosome cargo sorting to eliminate tumor suppressor miRNAs and thus to promote cell proliferation.

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p62 将狼疮 La 和选定的 microRNA 运送到乳腺癌衍生的外泌体中。

外泌体是源于多囊体的细胞外囊泡，由类动物细胞分泌。外泌体可作为疾病生物标记物，外泌体介导的 miRNA 分泌被认为可促进肿瘤生长和转移。此前，我们证明狼疮 La 蛋白（La）介导了 miR-122 有选择性地纳入转移性乳腺癌外泌体；然而，La 本身被分选到外泌体中的机制仍然未知。利用无偏接近标记蛋白质组学、生化分馏、超分辨率显微镜和遗传工具，我们确定了选择性自噬受体p62将La和miR-122分选到外泌体中。然后，我们进行了小 RNA 测序，发现 p62 的耗竭会减少肿瘤抑制 miRNA 的外泌体分泌，并导致它们在细胞内的积累。我们的数据表明，p62 是一种质量控制因子，可调节外泌体的 miRNA 组成。癌细胞可能会利用 p62 依赖性外泌体货物分拣来消除肿瘤抑制miRNA，从而促进细胞增殖。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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bioRxiv : the preprint server for biology

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