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在发育中的肌腱中,胶原蛋白 V 和 XI 与胶原蛋白的协调相互作用,调节胶原原纤维的成核和初始纤维的组装。

Regulation of collagen fibril nucleation and initial fibril assembly involves coordinate interactions with collagens V and XI in developing tendon.

机构信息

Myriad Genetic Laboratories, Inc., Salt Lake City, Utah 84108, USA.

出版信息

J Biol Chem. 2011 Jun 10;286(23):20455-65. doi: 10.1074/jbc.M111.223693. Epub 2011 Apr 5.

Abstract

Collagens V and XI comprise a single regulatory type of fibril-forming collagen with multiple isoforms. Both co-assemble with collagen I or II to form heterotypic fibrils and have been implicated in regulation of fibril assembly. The objective of this study was to determine the roles of collagens V and XI in the regulation of tendon fibrillogenesis. Flexor digitorum longus tendons from a haplo-insufficient collagen V mouse model of classic Ehlers Danlos syndrome (EDS) had decreased biomechanical stiffness compared with controls consistent with joint laxity in EDS patients. However, fibril structure was relatively normal, an unexpected finding given the altered fibrils observed in dermis and cornea from this model. This suggested roles for other related molecules, i.e. collagen XI, and compound Col5a1(+/-),Col11a1(+/-) tendons had altered fibril structures, supporting a role for collagen XI. To further evaluate this, transcript expression was analyzed in wild type tendons. During development (E18-P10) both collagen V and XI were comparably expressed; however, collagen V predominated in mature (P30) tendons. The collagens had a similar expression pattern. Tendons with altered collagen V and/or XI expression (Col5a1(+/-); Col11a1(+/-); Col5a1(+/-),Col11a1(+/-); Col11a1(-/-); Col5a1(+/-),Col11a1(-/-)) were analyzed at E18. All genotypes demonstrated a reduced fibril number and altered structure. This phenotype was more severe with a reduction in collagen XI. However, the absence of collagen XI with a reduction in collagen V was associated with the most severe fibril phenotype. The data demonstrate coordinate roles for collagens V and XI in the regulation of fibril nucleation and assembly during tendon development.

摘要

V 型和 XI 型胶原是一种具有多种同工型的单一调节性纤维形成胶原。两者都与 I 型或 II 型胶原共同组装形成异质纤维,并被认为参与了纤维组装的调节。本研究的目的是确定 V 型和 XI 型胶原在调节肌腱原纤维发生中的作用。与对照相比,经典型埃勒斯-当洛斯综合征(EDS)杂合不足胶原 V 鼠模型的屈肌腱具有较低的生物力学刚度,这与 EDS 患者的关节松弛一致。然而,纤维结构相对正常,这与该模型的真皮和角膜中观察到的改变纤维的预期结果不同。这表明其他相关分子,即胶原 XI 的作用,而复合 Col5a1(+/-),Col11a1(+/-)肌腱的纤维结构发生改变,支持胶原 XI 的作用。为了进一步评估这一点,在野生型肌腱中分析了转录表达。在发育过程中(E18-P10),V 型和 XI 型胶原的表达相当;然而,在成熟(P30)肌腱中,V 型胶原占优势。两种胶原具有相似的表达模式。改变了胶原 V 和/或 XI 表达的肌腱(Col5a1(+/-);Col11a1(+/-);Col5a1(+/-),Col11a1(+/-);Col11a1(-/-);Col5a1(+/-),Col11a1(-/-))在 E18 时进行了分析。所有基因型均表现出纤维数量减少和结构改变。胶原 XI 减少时,这种表型更为严重。然而,胶原 V 减少而胶原 XI 缺乏时,与最严重的纤维表型相关。该数据表明,在肌腱发育过程中,胶原 V 和 XI 协同作用于纤维核的形成和组装的调节。

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