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The extended substrate recognition profile of the dog mast cell chymase reveals similarities and differences to the humann chymase

机译:狗肥大细胞糜酶的底物识别特性得到扩展,揭示了与人糜酶的相似性和差异

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摘要

Human chymase (HC) constitutes a major granule protease in one of the two human mast cell (MC) types. The main biological role of this haematopoietic serine protease is probably not yet known, although it has been implicated in a large number of functions. Dogs, like humans, have only one chymase. This enzyme is closely related to its human homologue, and the MC subtypes of human and dog appear to be similar as well. Therefore, the functions of the dog chymase (DC) may closely reflect the functions of the HC. Moreover, dogs may serve as good models for studies of human MC functions and MC-related diseases. To reveal functional similarities and differences between the DC and HC, we have determined the extended cleavage specificity of the DC by substrate phage display. This method allows the simultaneous permutation of primed and unprimed substrate positions. The DC was found to have very similar preferences to its human counterpart for substrate positions P1, P3, P4 and P3′, whereas their preferences differ at positions P2, P1′ and P2′. Therefore, the HC and DC may have co-evolved with a substrate where positions P1, P3, P4 and P3′ are conserved between dogs and humans, whereas positions P2 and P1′ are not and P2′differs to a minor extent. The differences observed between these two enzymes suggest that results obtained from dog models cannot be directly extrapolated to human clinical settings but need to be evaluated carefully concerning potential differences in substrate preferences.
机译:人糜酶(HC)构成两种人肥大细胞(MC)类型之一中的主要颗粒蛋白酶。尽管该造血丝氨酸蛋白酶具有许多功能,但其主要生物学作用可能尚不清楚。狗和人类一样,只有一种糜酶。该酶与其人类同源物密切相关,人与狗的MC亚型也似乎相似。因此,狗糜酶(DC)的功能可能紧密反映HC的功能。此外,狗可以作为研究人类MC功能和MC相关疾病的良好模型。为了揭示DC和HC之间的功能相似性和差异,我们通过底物噬菌体展示确定了DC扩展的切割特异性。这种方法允许同时对打底和未打底的基板位置进行排列。发现DC对于底物位置P1,P3,P4和P3'具有与其人类对应物非常相似的偏好,而它们的偏好在位置P2,P1'和P2'上不同。因此,HC和DC可能与在狗和人之间保守位置P1,P3,P4和P3'的底物共同进化,而位置P2和P1'不在,而P2'差异很小。这两种酶之间观察到的差异表明,从狗模型获得的结果不能直接外推至人类临床环境,但需要仔细评估底物偏好方面的潜在差异。

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