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α-人心房利钠肽反平行和平行二聚体的合成及生物学特性

Synthesis and biological properties of antiparallel and parallel dimers of alpha-human atrial natriuretic peptide.

作者信息

Chino N, Yoshizawa-Kumagaye K, Noda Y, Watanabe T X, Kimura T, Sakakibara S

出版信息

Biochem Biophys Res Commun. 1986 Dec 15;141(2):665-72. doi: 10.1016/s0006-291x(86)80224-8.

Abstract

To obtain antiparallel and parallel dimers of alpha-human atrial natriuretic peptide (alpha-hANP), two fully protected peptides I and II having the same amino acid sequence as alpha-hANP with different protective groups at the cysteinyl residues were synthesized, the former having Acm and Npys and the latter MeBzl and Acm. Equivalent amounts of peptides I and II were mixed and subjected to HF deprotection. Next, the first disulfide bond was linked between the remaining Npys group in I and the liberated SH group in II to form a monodisulfide dimer. The second disulfide bond was formed within the newly formed dimer between the remaining Acm groups by treatment with iodine, giving an antiparallel dimer. The parallel dimer of alpha-hANP was synthesized similarly starting from the protected peptide II. These dimers could be clearly segregated on HPLC. The retention time on HPLC of the antiparallel dimer was identical with that of natural beta-hANP. Both dimers showed biological activities as high as one third to one sixth of alpha-hANP in smooth muscle spasmolytic activity, and almost the same level of natriuretic activity as alpha-hANP at a high dose (10 nmol/kg) but about one fifth the activity at a low dose (1 nmol/kg). In these assay systems, the antiparallel dimer showed a slower onset and a tendency of longer duration than alpha-hANP.

摘要

为了获得α-人心房利钠肽(α-hANP)的反平行二聚体和平行二聚体,合成了两种完全保护的肽I和肽II,它们具有与α-hANP相同的氨基酸序列,但在半胱氨酸残基处具有不同的保护基团,前者具有Acm和Npys,后者具有MeBzl和Acm。将等量的肽I和肽II混合并进行HF脱保护。接下来,在肽I中剩余的Npys基团和肽II中游离的SH基团之间连接第一个二硫键,形成单二硫键二聚体。通过用碘处理,在新形成的二聚体内剩余的Acm基团之间形成第二个二硫键,得到反平行二聚体。α-hANP的平行二聚体以同样的方式从受保护的肽II开始合成。这些二聚体在HPLC上可以清晰地分离。反平行二聚体在HPLC上的保留时间与天然β-hANP相同。两种二聚体在平滑肌解痉活性方面均表现出高达α-hANP三分之一至六分之一的生物活性,在高剂量(10 nmol/kg)时利钠活性水平与α-hANP几乎相同,但在低剂量(1 nmol/kg)时约为α-hANP活性的五分之一。在这些测定系统中,反平行二聚体比α-hANP起效慢且有持续时间更长的趋势。

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