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人血小板20S蛋白酶体:对其类胰凝乳蛋白酶活性的抑制及蛋白酶体激活剂PA28的鉴定。初步报告。

Human platelet 20S proteasome: inhibition of its chymotrypsin-like activity and identification of the proteasome activator PA28. A preliminary report.

作者信息

Ostrowska Halina, Ostrowska Justyna Kornelia, Worowski Krzysztof, Radziwon Piotr

机构信息

Department of Biology, Medical Academy of Bialystok, Poland.

出版信息

Platelets. 2003 May;14(3):151-7. doi: 10.1080/0953710031000092802.

Abstract

Earlier studies have demonstrated that human platelets contain the 20S proteasome, and its protein activator. However, understanding the potential role of the proteasome in human platelets requires a detailed knowledge about its chymotryptic-like activity, a crucial one for protein degradation in all eukaryotic cells. In this communication we have shown that human platelet 20S proteasome exhibited chymotryptic-like activity towards succinyl-Leu-Leu-Val-Tyr-7-amido-4-methylcoumarin as substrate at a broad pH range, with optimum between pH 7.5-8.0 and 5.0-5.5. These two activities were markedly inhibited by a 10 micromol/l concentration of two structurally unrelated proteasome inhibitors: lactacystin/beta-lactone or benzyloxycarbonyl-Ile-Glu(O-tert.-butyl)-Ala-leucinal, but not by ebelactone B, an inhibitor of lysosomal cathepsin A/deamidase. The chymotryptic-like activity of the 20S proteasome against succinyl-Leu-Leu-Val-Tyr-7-amido-4-methylcoumarin was also significantly inhibited in platelets, after exposure of platelet-rich plasma to 10 micromol/l lactacystin and benzyloxycarbonyl-Ile-Glu(O-tert.-butyl)-Ala-leucinal for up to 60 min. This indicates that these inhibitors can enter platelets and selectively inhibit 20S proteasome activity. We also demonstrated for the first time by Western blot analysis that human platelets contain a proteasome activator, PA28, which is known to play a key role in antigen processing by significant stimulation of the proteasomal chymotryptic-like activity. Since the platelet 20S proteasome was also present in a latent form, this suggests that its activity may be regulated in vivo in human platelets. All these results can therefore be beneficial in future studies on the role of the 20S proteasome in platelet biology.

摘要

早期研究表明,人类血小板含有20S蛋白酶体及其蛋白激活剂。然而,要了解蛋白酶体在人类血小板中的潜在作用,需要详细了解其类胰凝乳蛋白酶活性,这是所有真核细胞中蛋白质降解的关键活性。在本通讯中,我们表明人类血小板20S蛋白酶体在较宽的pH范围内对琥珀酰 - 亮氨酸 - 亮氨酸 - 缬氨酸 - 酪氨酸 - 7 - 氨基 - 4 - 甲基香豆素作为底物表现出类胰凝乳蛋白酶活性,最适pH在7.5 - 8.0和5.0 - 5.5之间。这两种活性被10微摩尔/升浓度的两种结构不相关的蛋白酶体抑制剂:乳胞素/β - 内酯或苄氧羰基 - 异亮氨酸 - 谷氨酸(叔丁酯) - 丙氨酸 - 亮氨酰显著抑制,但不被溶酶体组织蛋白酶A/脱酰胺酶抑制剂埃博霉素B抑制。在富含血小板血浆暴露于10微摩尔/升乳胞素和苄氧羰基 - 异亮氨酸 - 谷氨酸(叔丁酯) - 丙氨酸 - 亮氨酰长达60分钟后,血小板中20S蛋白酶体对琥珀酰 - 亮氨酸 - 亮氨酸 - 缬氨酸 - 酪氨酸 - 7 - 氨基 - 4 - 甲基香豆素的类胰凝乳蛋白酶活性也被显著抑制。这表明这些抑制剂可以进入血小板并选择性抑制20S蛋白酶体活性。我们还首次通过蛋白质印迹分析证明人类血小板含有蛋白酶体激活剂PA28,已知其通过显著刺激蛋白酶体类胰凝乳蛋白酶活性在抗原加工中起关键作用。由于血小板20S蛋白酶体也以潜伏形式存在,这表明其活性可能在人类血小板体内受到调节。因此,所有这些结果可能对未来关于20S蛋白酶体在血小板生物学中作用的研究有益。

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