自体消化假说:流变和心血管细胞功能障碍中的蛋白水解受体裂解1。

IF 1 4区 医学 Q4 BIOPHYSICS
Biorheology Pub Date : 2016-01-01 DOI:10.3233/BIR-17131
Geert W Schmid-Schönbein
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引用次数: 1

摘要

循环白细胞从休眠状态转变为具有改变流变特性的激活状态,导致其在微循环中的行为发生重大转变。低水平的假足形成或粘附分子的表达有助于相对自由地通过微血管,而具有假足的活化白细胞和增强的粘附膜蛋白被困在微血管中,附着在内皮细胞上并迁移到组织中。白细胞进入激活状态的转变在许多疾病中都可以看到。虽然感染、组织创伤以及非生理生化或生物物理暴露引起的激活机制得到了很好的认识,但许多疾病中的激活机制还没有像这些传统机制那样得到最终的认同,并且仍然未知。我们总结了我们最近的证据,表明消化酶在小肠中作为白细胞激活和微血管紊乱的根本原因的主要和令人惊讶的作用。在正常的食物消化过程中,消化酶被肠粘膜上皮屏障分隔在肠腔内。当这种屏障的渗透性增加时,这些强大的降解酶就会渗入肠壁,进入体循环。消化酶的渗漏发生在生理休克和多器官衰竭。消化酶进入小肠壁导致肠道组织在自体消化过程中降解。消化酶和组织/食物碎片的产生不仅会激活白细胞,还会引起许多细胞功能障碍。例如,发生膜受体、血浆蛋白和其他生物分子的蛋白水解破坏。我们的结论是,消化酶从肠道逃逸是细胞功能障碍、发病率甚至死亡率的主要来源,包括在流变学研究中看到的异常白细胞活化。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The autodigestion hypothesis: Proteolytic receptor cleavage in rheological and cardiovascular cell dysfunction1.

The autodigestion hypothesis: Proteolytic receptor cleavage in rheological and cardiovascular cell dysfunction1.

The autodigestion hypothesis: Proteolytic receptor cleavage in rheological and cardiovascular cell dysfunction1.

The autodigestion hypothesis: Proteolytic receptor cleavage in rheological and cardiovascular cell dysfunction1.

Transformation of circulating leukocytes from a dormant into an activated state with changing rheological properties leads to a major shift of their behavior in the microcirculation. Low levels of pseudopod formation or expression of adhesion molecules facilitate relatively free passage through microvessels while activated leukocytes with pseudopods and enhanced levels of adhesion membrane proteins become trapped in microvessels, attach to the endothelium and migrate into the tissue. The transformation of leukocytes into an activated state is seen in many diseases. While mechanisms for activation due to infections, tissue trauma, as well as non-physiological biochemical or biophysical exposures are well recognized, the mechanisms for activation in many diseases have not been conclusively liked to these traditional mechanisms and remain unknown. We summarize our recent evidence suggesting a major and surprising role of digestive enzymes in the small intestine as root causes for leukocyte activation and microvascular disturbances. During normal digestion of food digestive enzymes are compartmentalized in the lumen of the intestine by the mucosal epithelial barrier. When permeability of this barrier increases, these powerful degrading enzymes leak into the wall of the intestine and into the systemic circulation. Leakage of digestive enzymes occurs for example in physiological shock and multi-organ failure. Entry of digestive enzymes into the wall of the small intestine leads to degradation of the intestinal tissue in an autodigestion process. The digestive enzymes and tissue/food fragments generate not only activate leukocytes but also cause numerous cell dysfunctions. For example, proteolytic destruction of membrane receptors, plasma proteins and other biomolecules occurs. We conclude that escape of digestive enzymes from the intestinal track serves as a major source of cell dysfunction, morbidity and even mortality, including abnormal leukocyte activation seen in rheological studies.

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来源期刊
Biorheology
Biorheology 医学-工程:生物医学
CiteScore
2.00
自引率
0.00%
发文量
5
审稿时长
>12 weeks
期刊介绍: Biorheology is an international interdisciplinary journal that publishes research on the deformation and flow properties of biological systems or materials. It is the aim of the editors and publishers of Biorheology to bring together contributions from those working in various fields of biorheological research from all over the world. A diverse editorial board with broad international representation provides guidance and expertise in wide-ranging applications of rheological methods to biological systems and materials. The scope of papers solicited by Biorheology extends to systems at different levels of organization that have never been studied before, or, if studied previously, have either never been analyzed in terms of their rheological properties or have not been studied from the point of view of the rheological matching between their structural and functional properties. This biorheological approach applies in particular to molecular studies where changes of physical properties and conformation are investigated without reference to how the process actually takes place, how the forces generated are matched to the properties of the structures and environment concerned, proper time scales, or what structures or strength of structures are required.
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