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Proton pumping V-ATPase inhibitor bafilomycin A1 affects Rab7 lysosomal localization and abolishes anterograde trafficking of osteoclast secretory lysosomes

机译:质子泵浦V-ATP酶抑制剂BafiLomycin A1影响Rab7溶酶体定位,并废除了骨质细胞分泌溶酶体的伪造贩运

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Osteoclast lysosomes secrete lytic enzymes into bone resorption lacunae, and sort the lysosomal proton pumping vacuolar-type ATPase (V-ATPase) to the plasma membrane to form the acidic environment required for bone digestion. The a3 isoform of V-ATPase is essential for outward trafficking of the secretory lysosomes and interacts physically with Rab7, a small GTPase that regulates trafficking of late endosomes and lysosomes, to recruit it to lysosomes. However, it is unclear whether organelle acidification by V-ATPase is required for the lysosome trafficking. Here, we showed that incubation of osteoclasts with the V-ATPase inhibitor bafilomycin A1 abolished the osteoclast-characteristic peripheral localization of secretory lysosomes, Rab7, and alpha-tubulin. Although bafilomycin A1 had little or no effect on Rab7 activation and its interaction with a3, treatment with the inhibitor significantly reduced the lysosomal localization of Rab7. Even constitutively active Rab7 did not localize to lysosomes in the presence of the inhibitor. These results suggest that organelle acidification by V-ATPase is required for localization of activated Rab7 to lysosomes. (C) 2019 Elsevier Inc. All rights reserved.
机译:骨髓溶质溶酶体分泌含裂变酵素的骨吸收雷,并将溶酶体质子泵送真空型ATP酶(V-ATP酶)分类到质膜中,形成骨消化所需的酸性环境。 V-ATP酶的A3同种型对于向外贩运分泌溶酶体并与Rab7的物理相互作用,这是一种调节贩运晚期内体和溶酶体的小GTP酶,将其募集到溶酶体中。然而,目前尚不清楚溶酶体贩运需要V-ATP酶的细胞器酸化。在此表明,随着V-ATP酶抑制剂BafiLomycin A1的疏松骨壳孵育废除了分泌溶酶体,RAB7和α-管蛋白的破骨细胞特征外周定。虽然Bafilomycin A1对RAB7活化几乎没有或没有影响,但其与A3的相互作用,抑制剂的治疗显着降低了RAB7的溶酶体定位。甚至组成型活性Rab7在抑制剂存在下没有本地化溶酶体。这些结果表明,通过V-ATP酶将活性Rab7定位所需的细胞器酸化在溶酶体中。 (c)2019 Elsevier Inc.保留所有权利。

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