Mastoparan may activate GTP hydrolysis by Gi-proteins in HL-60 membranes indirectly through interaction with nucleoside diphosphate kinase

A Hagelüken; B Nürnberg; I Heilmann; I Schwaner; J Ervens; J F Klinker; K Wenzel-Seifert; L Grünbaum; R Harhammer; R Seifert; S Offermanns; T Müller

摘要

pThe wasp venom, mastoparan (MP), activates reconstituted pertussis toxin (PTX)-sensitive G-proteins in a receptor-independent manner. We studied the effects of MP and its analogue, mastoparan 7 (MP 7), on G-protein activation in HL-60 cells and a reconstituted system and on nucleoside diphosphate kinase (NDPK)-catalysed GTP formation. MP activated high-affinity GTP hydrolysis in HL-60 membranes with an EC50 of 1-2 microM and a maximum at 10 microM. Unlike the effects of the formyl peptide receptor agonist, N-formyl-L-methionyl-L-leucyl-L-phenylalanine (fMet-Leu-Phe), on GTPase, those of MP were only partially PTX-sensitive. MP-induced rises in cytosolic Ca2+ concentration and superoxide-anion formation in intact HL-60 cells were also only incompletely PTX-sensitive. N-Ethylmaleimide inhibited MP-stimulated GTP hydrolysis to a greater extent than that stimulated by fMet-Leu-Phe. Unlike the latter, MP did not enhance incorporation of GTP azidoanilide into, and cholera toxin-catalysed ADP-ribosylation of, Gi-protein alpha-subunits in HL-60 membranes. By contrast to fMet-Leu-Phe, MP did not or only weakly stimulated binding of guanosine 5′-[gamma-thio]triphosphate to Gi-protein alpha-subunits. MP 7 was considerably more effective than MP at activating the GTPase of reconstituted Gi/G(o)-proteins, whereas in HL-60 membranes, MP and MP 7 were similarly effective. MP and MP 7 were similarly effective at activating [3H]GTP formation from [3H]GDP and GTP in HL-60 membranes and by NDPK purified from bovine liver mitochondria. Our data suggest the following: (1) MP activates Gi-proteins in HL-60 cells, but (2) the venom does not simply mimic receptor activation. (3) MP and MP 7 may activate GTP hydrolysis in HL-60 membranes indirectly through interaction with NDPK. (4) MP 7 is a more effective direct activator of PTX-sensitive G-proteins than MP, whereas with regard to NDPK, MP and MP 7 are similarly effective./p

机译：>黄蜂毒液，Mastroparan（MP），以受体非依赖性方式激活重构的百日咳毒素（PTX）敏感的G蛋白。我们研究了MP及其类似物，Mastoparan 7（MP 7）对HL-60细胞和重构系统中G蛋白活化的影响以及对核苷二磷酸激酶（NDPK）催化的GTP形成的影响。 MP激活HL-60膜中的高亲和力GTP水解，EC50为1-2 microM，最大值为10 microM。与甲酰肽受体激动剂N-甲酰基-L-甲硫酰基-L-亮氨酰-L-苯丙氨酸（fMet-Leu-Phe）的作用不同，MP的作用仅对PTX敏感。 MP诱导的完整HL-60细胞中胞质Ca2 +浓度的升高和超氧阴离子的形成也仅对PTX不完全敏感。与fMet-Leu-Phe刺激相比，N-乙基马来酰亚胺对MP刺激的GTP水解的抑制作用更大。与后者不同，MP不会增强GTP叠氮基苯胺向HL-60膜中的Gi蛋白α亚基的结合以及霍乱毒素催化的ADP核糖基化。与fMet-Leu-Phe相反，MP没有或仅弱地刺激鸟苷5'-[γ-硫代]三磷酸与Gi蛋白α-亚基的结合。 MP 7在激活重构的Gi / G（o）蛋白的GTPase方面比MP有效得多，而在HL-60膜中，MP和MP 7同样有效。 MP和MP 7在激活HL-60膜中的[3H] GDP和GTP以及从牛肝线粒体纯化的NDPK上可有效激活[3H] GTP的形成。我们的数据表明：（1）MP激活HL-60细胞中的Gi蛋白，但是（2）毒液不能简单地模拟受体激活。（3）MP和MP 7可通过与NDPK相互作用间接激活HL-60膜中的GTP水解。（4）MP 7是一种对PTX敏感的G蛋白的直接激活剂，比MP更有效，而就NDPK而言，MP和MP 7的效果相似。

Mastoparan may activate GTP hydrolysis by Gi-proteins in HL-60 membranes indirectly through interaction with nucleoside diphosphate kinase

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