Improved volume CLEM revealed that aberrant phagophores and RB1CC1/FIP200-containing clusters appear surround SQSTM1/p62 aggregates in Atg9a-deficient cells

Autophagy reports Pub Date : 2023-09-15 DOI:10.1080/27694127.2023.2256599

Soichiro Kakuta, Junji Yamaguchi, Chigure Suzuki, Isei Tanida, Yasuo Uchiyama

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Abstract

ATG9A is an important membrane protein in mammalian macroautophagy. The formation of autophagosomes and phagophores is blocked in atg9a KO cells. However, it remains possible that residual membrane formation activity exists in these cells. These precursor structures that precede phagophores are, if they exist, rare and may be difficult to find. Here, we introduce the modified volume correlative light and electron microscopy (CLEM) method to analyze these structures three-dimensionally. In addition to target proteins, mitochondria were labeled as a landmark for precise correlation of slice images by a confocal fluorescence microscope and a focused ion beam scanning electron microscope. We found phagophores and small membrane vesicles near SQSTM1/p62 aggregates in atg9a KO cells, indicating that phagophores could be formed in atg9a-deficient cells, although they were immature and inefficient. Furthermore, we found that RB1CC1/FIP200-positive structures formed clusters around SQSTM1/p62 with ferritin and TAX1BP1. Taken together, our method contributes to the understanding of undiscovered fine structures.

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改进的体积CLEM显示，在atg9a缺陷细胞中，在SQSTM1/p62聚集体周围出现了异常的吞噬团和RB1CC1/FIP200-containing团

ATG9A是哺乳动物巨噬过程中重要的膜蛋白。atg9a KO细胞中自噬体和吞噬细胞的形成被阻断。然而，仍有可能在这些细胞中存在残留的膜形成活性。这些在吞噬体之前的前体结构，如果存在的话，是罕见的，可能很难找到。在此，我们引入了改进的体积相关光电子显微镜(CLEM)方法对这些结构进行三维分析。除靶蛋白外，线粒体被标记为共聚焦荧光显微镜和聚焦离子束扫描电镜切片图像精确相关的里程碑。我们在atg9a KO细胞的SQSTM1/p62聚集体附近发现了吞噬团和小膜泡，这表明atg9a缺陷细胞可以形成吞噬团，尽管它们不成熟且效率低下。此外，我们发现RB1CC1/ fip200阳性结构与铁蛋白和TAX1BP1在SQSTM1/p62周围形成簇。总之，我们的方法有助于理解未被发现的精细结构。

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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Autophagy reports

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