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粒细胞前髓过氧化物酶由 HL-60 细胞中的蛋白前转化酶 furin 和 PC7 冗余加工。

Granulocyte pro-myeloperoxidase is redundantly processed by proprotein convertase furin and PC7 in HL-60 cells.

机构信息

TransBIOTech, Lévis, QC G6V 6Z3, Canada.

Nutraceuticals and Functional Foods Institute (INAF), Université Laval, Québec City, QC G1K 7P4, Canada.

出版信息

Biochem Cell Biol. 2024 Jun 1;102(3):275-284. doi: 10.1139/bcb-2023-0339. Epub 2024 Mar 14.

DOI:10.1139/bcb-2023-0339
PMID:38484367
Abstract

Neutrophil myeloperoxidase/HO/chloride system is a key mechanism to control pathogen infection. This enzyme, myeloperoxidase, plays a pivotal role in the arsenal of azurophilic granules that are released through degranulation upon neutrophil activation, which trigger local hypochlorous acid production. Myeloperoxidase gene encodes a protein precursor named promyeloperoxidase that arbors a propeptide that gets cleaved later during secretory routing in post-endoplasmic reticulum compartments. Although evidence suggested that this processing event was performed by one or different enzymes from the proprotein convertases family, the identity of this enzyme was never investigated. In this work, the naturally producing myeloperoxidase promyelocytic cell line HL-60 was used to investigate promyeloperoxidase cleavage during granulocytic differentiation in response to proprotein convertase inhibitors decanoyl-RVKR-chloromethylketone and hexa-d-arginine. Stable PC knockdown of endogenously expressed proprotein convertases, furin and PC7, was achieved using lentiviral delivery of shRNAs. None of the knockdown cell line could reproduce the effect of the pan-proprotein convertases inhibitor decanoyl-RVKR-chloromethylketone that accumulated intracellular promyeloperoxidase stores in HL-60 cells, therefore illustrating that both furin and PC7 redundantly process this proprotein.

摘要

中性粒细胞髓过氧化物酶/HO/氯体系是控制病原体感染的关键机制。这种酶,髓过氧化物酶,在嗜中性粒细胞活化时通过脱颗粒释放的嗜天青颗粒的储备中发挥关键作用,这触发了局部次氯酸的产生。髓过氧化物酶基因编码一种名为前髓过氧化物酶的蛋白前体,该蛋白前体带有一个前肽,在高尔基体内腔室中的分泌途径中随后被切割。尽管有证据表明,这个加工事件是由蛋白原转化酶家族的一种或多种酶来执行的,但这种酶的身份从未被研究过。在这项工作中,使用自然产生髓过氧化物酶的髓样前体细胞系 HL-60 来研究粒细胞分化过程中前髓过氧化物酶的切割,以响应蛋白原转化酶抑制剂癸酰基-RVKR-氯甲基酮和六聚精氨酸。使用慢病毒递送 shRNA 实现了内源性表达的蛋白原转化酶,如 furin 和 PC7 的稳定 PC 敲低。没有一种敲低细胞系能够重现 pan-蛋白原转化酶抑制剂癸酰基-RVKR-氯甲基酮的效果,该抑制剂会在 HL-60 细胞中积累细胞内髓过氧化物酶储存,因此说明 furin 和 PC7 冗余地处理这种蛋白原。

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Biochem Cell Biol. 2024 Jun 1;102(3):275-284. doi: 10.1139/bcb-2023-0339. Epub 2024 Mar 14.
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Implication of the proprotein convertases in iron homeostasis: proprotein convertase 7 sheds human transferrin receptor 1 and furin activates hepcidin.蛋白转化酶在铁稳态中的作用:前蛋白转化酶 7 切割人转铁蛋白受体 1,而弗林蛋白酶激活铁调素。
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