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利用静电排斥失稳肽探针实现病理性胶原蛋白的原位成像

In Situ Imaging of Pathological Collagen by Electrostatic Repulsion-Destabilized Peptide Probes.

作者信息

Cai Xiangdong, Wei Wenyu, Liu Zhao, Bai Zhongtian, Lei Junqiang, Xiao Jianxi

机构信息

State Key Laboratory of Applied Organic Chemistry, Key Laboratory of Nonferrous Metal Chemistry and Resources Utilization of Gansu Province, College of Chemistry and Chemical Engineering, Lanzhou University, Lanzhou 730000, P. R. China.

The First Hospital of Lanzhou University, Lanzhou 730000, P. R. China.

出版信息

ACS Appl Bio Mater. 2020 Nov 16;3(11):7492-7499. doi: 10.1021/acsabm.0c00710. Epub 2020 Sep 22.

DOI:10.1021/acsabm.0c00710
PMID:35019491
Abstract

The development of robust collagen assays is crucial in the diagnosis and treatment of various pathological conditions. Peptide probes composed of the (Gly-Pro-Hyp) sequences have received extensive attention for their remarkable collagen-targeting capability, which unfortunately has been severely impaired by their high triple helical stability. Herein, we report an efficient strategy to reduce the triple helical propensity of the (Gly-Pro-Hyp) sequences by electrostatic repulsion. A series of peptides consisting of the (Gly-Pro-Hyp) sequence and a number of charged amino acid Asp have been investigated, indicating that the presence of six additional Asp pronouncedly weakened the triple helical stability of peptide probe FAM-PCTP-D6 under physiological conditions (pH 7.4). FAM-PCTP-D6 could be directly applied without any pretreatment to recognize denatured collagen with high selectivity, whereas another dye-labeled peptide probe ROX-PCTP-D6 specifically targeted pathological collagen in various connective tissues of animal disease models and human patients. The inclusion of extra charged natural amino acids has been demonstrated as a convenient approach to create biocompatible collagen-targeting peptide probes with much weaker triple helical stability. Without the need for preheating treatment, these electrostatic repulsion-driven peptide probes provide a handy tool for histopathology staining, showing promising applications in collagen-involved diseases.

摘要

强大的胶原蛋白检测方法的开发对于各种病理状况的诊断和治疗至关重要。由(甘氨酸-脯氨酸-羟脯氨酸)序列组成的肽探针因其卓越的胶原蛋白靶向能力而受到广泛关注,不幸的是,其高三螺旋稳定性严重损害了这种能力。在此,我们报告一种通过静电排斥降低(甘氨酸-脯氨酸-羟脯氨酸)序列三螺旋倾向的有效策略。对一系列由(甘氨酸-脯氨酸-羟脯氨酸)序列和多个带电荷氨基酸天冬氨酸组成的肽进行了研究,结果表明额外六个天冬氨酸的存在显著削弱了肽探针FAM-PCTP-D6在生理条件(pH 7.4)下的三螺旋稳定性。FAM-PCTP-D6无需任何预处理即可直接应用,以高选择性识别变性胶原蛋白;而另一种染料标记的肽探针ROX-PCTP-D6则特异性靶向动物疾病模型和人类患者各种结缔组织中的病理性胶原蛋白。已证明引入额外的带电荷天然氨基酸是一种方便的方法,可创建具有弱得多的三螺旋稳定性的生物相容性胶原蛋白靶向肽探针。无需预热处理,这些由静电排斥驱动的肽探针为组织病理学染色提供了一种便捷工具,在涉及胶原蛋白的疾病中显示出广阔的应用前景。

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