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Studies on the status of lysine residues in phospholipase A2 from Naja naja atra (Taiwan cobra) snake venom

机译:台湾眼镜蛇蛇毒磷脂酶A2中赖氨酸残基状态的研究

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pPhospholipase A2 (PLA2) from Naja naja atra (Taiwan cobra) snake venom was subjected to lysine modification with trinitrobenzene sulphonic acid (TNBS), and two major trinitrophenylated (TNP) derivatives, TNP-1 and TNP-2, were separated by h.p.l.c. TNP-1 contained only one TNP group on Lys-6 and showed a marked decrease in enzymic activity, but still retained 45% of the lethal toxicity. Both Lys-6 and Lys-65 were modified in TNP-2, and modification of Lys-65 caused a further reduction of the lethal toxicity to 12.6%. However, the antigenicity of both TNP-1 and TNP-2 remained unchanged. The reactivity of Lys-6 and Lys-65 toward TNBS was greatly enhanced by Ca2+ and dihexanoyl-lecithin, suggesting that the two Lys residues are not directly involved in the binding of Ca2+ and substrate. The modified derivatives retained their affinity for Ca2+, indicating that Lys-6 and Lys-65 did not participate in the Ca2+ binding. The TNP derivatives could be regenerated with hydrazine hydrochloride. The biological activities of the regenerated PLA2 are almost the same as those of native PLA2. These results indicate that Lys-6 and Lys-65 are important for the biological activities of PLA2, and incorporation of a bulky TNP group on Lys-6 and Lys-65 might give rise to a distortion of the active conformation of PLA2./p
机译:p对来自眼镜蛇蛇毒(台湾眼镜蛇)的磷脂酶A2(PLA2)进行三硝基苯磺酸(TNBS)的赖氨酸修饰,并分离出两个主要的三硝基苯化(TNP)衍生物TNP-1和TNP-2。由hplc TNP-1仅在Lys-6上包含一个TNP基团,并显示出明显的酶活性降低,但仍保留了45%的致命毒性。 Lys-6和Lys-65都在TNP-2中进行了修饰,Lys-65的修饰导致致死毒性进一步降低至12.6%。但是,TNP-1和TNP-2的抗原性保持不变。 Ca2 +和二己酰基-卵磷脂大大增强了Lys-6和Lys-65对TNBS的反应性,表明两个Lys残基不直接参与Ca2 +和底物的结合。修饰的衍生物保留了它们对Ca2 +的亲和力,表明Lys-6和Lys-65不参与Ca2 +结合。 TNP衍生物可以用盐酸肼再生。再生的PLA2的生物活性与天然PLA2几乎相同。这些结果表明,Lys-6和Lys-65对于PLA2的生物学活性很重要,而在Lys-6和Lys-65上掺入大量的TNP基团可能会导致PLA2的活性构象变形。 >

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