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Type XIV Collagen Regulates Fibrillogenesis: PREMATURE COLLAGEN FIBRIL GROWTH AND TISSUE DYSFUNCTION IN NULL MICE*

机译:XIV型胶原蛋白调节原纤维形成:胶原蛋白原纤维 NULL中的增长和组织功能异常 老鼠*

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摘要

Type XIV collagen is a fibril-associated collagen with an interrupted triple helix. This collagen interacts with the fibril surface and has been implicated as a regulator of fibrillogenesis; however, a specific role has not been elucidated. Functional roles for type XIV collagen were defined utilizing a new type XIV collagen-deficient mouse line. This line was produced using a conventional targeted knock-out approach. Col14a1(–/–) mice were devoid of type XIV collagen, whereas heterozygous mice had reduced synthesis. Both mutant Col14a1 genotypes were viable with a grossly normal phenotype; however, mature skin exhibited altered mechanical properties. Prior to evaluating tendon fibrillogenesis in type XIV collagen-deficient mice, the developmental expression patterns were analyzed in wild-type flexor digitorum longus (FDL) tendons. Analyses of mRNA and protein expression indicated tissue-specific temporal expression that was associated with the early stages in fibrillogenesis. Ultrastructural analyses of wild-type and null tendons demonstrated premature fibril growth and larger fibril diameters in tendons from null mice at postnatal day 4 (P4). However, fibril structure in mature tendons was normal. Biomechanical studies established a direct structure/function relationship with reduced strength in P7-null tendons. However, the biomechanical properties in P60 tendons were comparable in null and wild-type mice. Our results indicate a regulatory function for type XIV collagen in early stages of collagen fibrillogenesis with tissue differences.
机译:XIV型胶原蛋白是与原纤维相关的胶原蛋白,具有三螺旋间断。这种胶原蛋白与原纤维表面相互作用,并被认为是原纤维形成的调节剂。但是,具体角色尚未阐明。 XIV型胶原蛋白的功能角色是使用新型的XIV型胶原蛋白缺乏小鼠系定义的。该生产线使用常规的靶向剔除方法生产。 Col14a1(– / –)小鼠缺乏XIV型胶原,而杂合小鼠则合成减少。两种突变的Col14a1基因型均具有大致正常的表型;然而,成熟的皮肤表现出改变的机械性能。在评估XIV型胶原蛋白缺乏小鼠的肌腱原纤维形成之前,先分析野生型趾长屈肌(FDL)肌腱的发育表达模式。对mRNA和蛋白表达的分析表明,组织特异性的时间表达与原纤维形成的早期阶段有关。野生型和无效肌腱的超微结构分析表明,出生后第4天(P4),无效小鼠的肌腱中纤维过早生长,纤维直径较大。但是,成熟肌腱的原纤维结构是正常的。生物力学研究建立了直接的结构/功能关系,降低了P7零筋的强度。但是,P60肌腱的生物力学特性在空和野生型小鼠中是可比的。我们的结果表明在胶原原纤维形成的早期具有组织差异的XIV型胶原的调节功能。

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