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磺酰氟丝氨酸蛋白酶抑制剂可使RNK - 16淋巴细胞颗粒蛋白酶失活,并减少颗粒提取物和穿孔素引起的细胞裂解。

Sulfonyl fluoride serine protease inhibitors inactivate RNK-16 lymphocyte granule proteases and reduce lysis by granule extracts and perforin.

作者信息

Ewoldt G R, Winkler U, Powers J C, Hudig D

机构信息

School of Medicine, University of Nevada, Reno 89557.

出版信息

Mol Immunol. 1992 Jun;29(6):713-21. doi: 10.1016/0161-5890(92)90181-v.

Abstract

Cytolytic granules purified from natural killer lymphocytes (NK) contain a pore-forming protein (perforin) and a number of serine proteases. When these proteases are inhibited by serine protease-specific isocoumarin reagents the serine proteases are inactivated and the cytolytic activity of the granules is decreased. Paradoxically, it has been found that the general serine protease inhibitor phenylmethylsulfonyl fluoride (PMSF) frequently cannot block killing even though it inhibits many of the serine proteases. At the same time it has been reported that "purified" perforin alone can lyze cells. To address these inconsistencies we first compared the ability of PMSF and four new sulfonyl fluoride serine protease inhibitors to inhibit proteases and cell lysis. We determined the effects on lysis and the second order inhibition rate constants for five granule protease activities: ly-tryptase, ly-chymase, Met-ase (methionine cleaving), Ser-ase (serine cleaving) and Asp-ase (aspartic acid cleaving). One compound, 2-(Z-NH(CH2)2CONH)C6SO2F, was a potent inhibitor of Met-ase activity (k(obsd)/[I] = 162 M-1 s-1), ly-chymase activity (k(obsd)/[I] = 147 M-1 s-1), and granule-mediated as well as perforin-mediated lysis. PMSF was a poor inhibitor of granule proteases (k(obsd)/[I]'s less than 7 M-1 s-1 for four activities and no inhibition of Ser-ase); the lack of reactivity is consistent with the failure of PMSF to block granule lytic activity. We also prepared enriched perforin by anion exchange chromatography and showed that a ly-chymase and a Met-ase associated with perforin. By inhibiting these proteases we also inhibited lytic activity.

摘要

从自然杀伤淋巴细胞(NK)中纯化得到的溶细胞颗粒含有一种成孔蛋白(穿孔素)和多种丝氨酸蛋白酶。当这些蛋白酶被丝氨酸蛋白酶特异性异香豆素试剂抑制时,丝氨酸蛋白酶失活,颗粒的溶细胞活性降低。矛盾的是,已发现通用的丝氨酸蛋白酶抑制剂苯甲基磺酰氟(PMSF)尽管能抑制许多丝氨酸蛋白酶,但常常无法阻断杀伤作用。同时,有报道称单独的“纯化”穿孔素就能裂解细胞。为了解决这些不一致的情况,我们首先比较了PMSF和四种新的磺酰氟丝氨酸蛋白酶抑制剂抑制蛋白酶和细胞裂解的能力。我们测定了它们对五种颗粒蛋白酶活性(ly-胰蛋白酶、ly-糜蛋白酶、Met-酶(切割甲硫氨酸)、Ser-酶(切割丝氨酸)和Asp-酶(切割天冬氨酸))的裂解作用及二级抑制速率常数的影响。一种化合物2-(Z-NH(CH2)2CONH)C6SO2F是Met-酶活性(k(obsd)/[I] = 162 M-1 s-1)、ly-糜蛋白酶活性(k(obsd)/[I] = 147 M-1 s-1)以及颗粒介导和穿孔素介导的裂解的有效抑制剂。PMSF是颗粒蛋白酶的弱抑制剂(四种活性的k(obsd)/[I]均小于7 M-1 s-1,且对Ser-酶无抑制作用);其缺乏反应性与PMSF未能阻断颗粒溶细胞活性一致。我们还通过阴离子交换色谱法制备了富集的穿孔素,并表明一种ly-糜蛋白酶和一种Met-酶与穿孔素相关。通过抑制这些蛋白酶,我们也抑制了裂解活性。

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