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κ-酪蛋白和 β-乳球蛋白的共聚集产生形态独特的淀粉样纤维。

Coaggregation of κ-Casein and β-Lactoglobulin Produces Morphologically Distinct Amyloid Fibrils.

机构信息

CSIRO Agriculture and Food, Werribee, Victoria, 3031, Australia.

AgResearch Limited, Grasslands Research Centre, Tennent Drive, Palmerston North, 4442, New Zealand.

出版信息

Small. 2017 Apr;13(14). doi: 10.1002/smll.201603591. Epub 2017 Feb 1.

Abstract

The unfolding, misfolding, and aggregation of proteins lead to a variety of structural species. One form is the amyloid fibril, a highly aligned, stable, nanofibrillar structure composed of β-sheets running perpendicular to the fibril axis. β-Lactoglobulin (β-Lg) and κ-casein (κ-CN) are two milk proteins that not only individually form amyloid fibrillar aggregates, but can also coaggregate under environmental stress conditions such as elevated temperature. The aggregation between β-Lg and κ-CN is proposed to proceed via disulfide bond formation leading to amorphous aggregates, although the exact mechanism is not known. Herein, using a range of biophysical techniques, it is shown that β-Lg and κ-CN coaggregate to form morphologically distinct co-amyloid fibrillar structures, a phenomenon previously limited to protein isoforms from different species or different peptide sequences from an individual protein. A new mechanism of aggregation is proposed whereby β-Lg and κ-CN not only form disulfide-linked aggregates, but also amyloid fibrillar coaggregates. The coaggregation of two structurally unrelated proteins into cofibrils suggests that the mechanism can be a generic feature of protein aggregation as long as the prerequisites for sequence similarity are met.

摘要

蛋白质的展开、错误折叠和聚集导致了多种结构物种的出现。其中一种形式是淀粉样纤维,这是一种高度有序、稳定的纳米纤维结构,由垂直于纤维轴的β-折叠片组成。β-乳球蛋白(β-Lg)和κ-酪蛋白(κ-CN)是两种乳蛋白,它们不仅可以单独形成淀粉样纤维状聚集物,而且在高温等环境胁迫条件下也可以共同聚集。据推测,β-Lg 和 κ-CN 之间的聚集是通过形成二硫键导致无定形聚集物进行的,尽管确切的机制尚不清楚。本文使用一系列生物物理技术表明,β-Lg 和 κ-CN 共同聚集形成形态不同的共淀粉样纤维状结构,这种现象以前仅限于来自不同物种的蛋白质同工型或来自单个蛋白质的不同肽序列。提出了一种新的聚集机制,即β-Lg 和 κ-CN 不仅形成二硫键连接的聚集物,还形成淀粉样纤维状共聚集物。两种结构上不相关的蛋白质共同聚集形成共纤维,这表明只要满足序列相似性的前提条件,该机制就可以成为蛋白质聚集的通用特征。

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