ADAMTSL-6 Is a Novel Extracellular Matrix Protein That Binds to Fibrillin-1 and Promotes Fibrillin-1 Fibril Formation

Tsutsui, Ko; Manabe, Ri Ichiroh; Yamada, Takanobu; Nakano, Itsuko; Oguri, Yasuko; Keene, Douglas R.; Sengle, Gerhard; Sakai, Lynn Y.; Sekiguchi, Kiyotoshi

doi:10.1074/jbc.m109.076919

Cited by 94 publications

(116 citation statements)

References 61 publications

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“…These proteins are localized in connective tissues, including the skin, aorta, and perichondrocytes. Among the ADAMTSL6 family, ADAMTSL6␤ has been shown to associate with fibrillin-1 microfibrils through its direct interaction with the N-terminal region of fibrillin-1 and thereby promotes fibrillin-1 matrix assembly in vitro and in vivo (17). These findings suggest a potential clinical application of ADAMTSL6␤ as a novel MFS therapy by promoting fibrillin-1 microfibril assembly and regulating TGF-␤ activation.…”

Section: Marfan Syndrome (Mfs)mentioning

confidence: 81%

“…Expression and Purification of Recombinant Adamtsl6␤-The expression and purification of recombinant Adamtsl6␤ was performed using 293F cells (Invitrogen) and nickel-agarose (Qiagen, Hilden, Germany) as described previously (17). Briefly, pSecTag2A containing an Adamtsl6␤ segment fused with Myc and His tags at its C terminus was transfected into 293F cells, which were cultured for 3 days.…”

Section: Methodsmentioning

confidence: 99%

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ADAMTSL6β Protein Rescues Fibrillin-1 Microfibril Disorder in a Marfan Syndrome Mouse Model through the Promotion of Fibrillin-1 Assembly

Saito

Kurokawa

Oda

et al. 2011

Journal of Biological Chemistry

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Background:The pathology of Marfan syndrome is caused by insufficient fibrillin-1 microfibril formation in connective tissues. Results: Successful improvement of Marfan syndrome manifestations are induced by the direct administration of recombinant ADAMTSL6␤. Conclusion: This study demonstrated critical importance of microfibril regeneration in preventing Marfan syndrome. Significance: Our current data support a new concept that the regeneration of microfibrils using ADAMTSL6␤ is essential for improving Marfan syndrome.

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Section: Marfan Syndrome (Mfs)mentioning

confidence: 81%

Section: Methodsmentioning

confidence: 99%

ADAMTSL6β Protein Rescues Fibrillin-1 Microfibril Disorder in a Marfan Syndrome Mouse Model through the Promotion of Fibrillin-1 Assembly

Saito

Kurokawa

Oda

et al. 2011

Journal of Biological Chemistry

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“…Furthermore, ADAMTSL4 mutations occur in recessively inherited isolated ectopia lentis (31,32), and ADAMTS17 mutations result in ectopia lentis in dogs (33) and a WMS-like syndrome in humans (15). Recently, it was shown that ADAMTSL6 was capable of enhancing fibrillin-1 assembly into ECM (34).…”

Section: Discussionmentioning

confidence: 99%

ADAMTS10 Protein Interacts with Fibrillin-1 and Promotes Its Deposition in Extracellular Matrix of Cultured Fibroblasts

Kutz¹,

Wang²,

Bader³

et al. 2011

Journal of Biological Chemistry

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125

163

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Autosomal recessive and autosomal dominant forms of WeillMarchesani syndrome, an inherited connective tissue disorder, are caused by mutations in ADAMTS10 (encoding a secreted metalloprotease) and FBN1 (encoding fibrillin-1, which forms tissue microfibrils), respectively, yet they are clinically indistinguishable. This genetic connection prompted investigation of a potential functional relationship between ADAMTS10 and fibrillin-1. Specifically, fibrillin-1 was investigated as a potential ADAMTS10 binding partner and substrate, and the role of ADAMTS10 in influencing microfibril biogenesis was addressed. Using ligand affinity blotting and surface plasmon resonance, recombinant ADAMTS10 was found to bind to fibrillin-1 with a high degree of specificity and with high affinity. Two sites of ADAMTS10 binding to fibrillin-1 were identified, one toward the N terminus and another in the C-terminal half of fibrillin-1. Confocal microscopy and immunoelectron microscopy localized ADAMTS10 to fibrillin-1-containing microfibrils in human tissues. Furin-activated ADAMTS10 could cleave fibrillin-1, but innate resistance of ADAMTS10 zymogen to propeptide excision by furin was observed, suggesting that, unless activated, ADAMTS10 is an inefficient fibrillinase. To investigate the role of ADAMTS10 in microfibril biogenesis, fetal bovine nuchal ligament cells were cultured in the presence or absence of ADAMTS10. Exogenously added ADAMTS10 led to accelerated fibrillin-1 microfibril biogenesis. Conversely, fibroblasts obtained from a Weill-Marchesani syndrome patient with ADAMTS10 mutations deposited fibrillin-1 microfibrils sparsely compared with unaffected control cells. Taken together, these findings suggest that ADAMTS10 participates in microfibril biogenesis rather than in fibrillin-1 turnover.Inherited connective tissue disorders that result from mutations of genes encoding extracellular matrix (ECM) 3 components or their modifying enzymes are potentially insightful in identifying structural and regulatory roles of ECM constituents or their supramolecular assemblies. A classic example of such an ECM component is fibrillin-1, a large, secreted glycoprotein, which is a major component of 8 -12-nm-diameter tissue microfibrils (1). Bundles of microfibrils, containing fibrillin-1, fibrillin-2, and fibrillin-3 (in humans), are ubiquitous in the body but are especially abundant in tissues containing elastin (2). The structural role of microfibrils includes maintenance of the ocular lens in its appropriate position in the eye via the zonule of Zinn (the suspensory ligament of the lens), which comprises primarily fibrillin-1 microfibrils (2, 3). Inadequacy of the zonule or traumatic breakage of zonule fibers can result in subluxation or dislocation of the lens (ectopia lentis). Dominantly inherited FBN1 mutations lead to diverse connective tissue anomalies, the most common of which is Marfan syndrome (MFS) (4). Major features of MFS include musculoskeletal anomalies, aortic aneurysms, and ectopia lentis. Several features of MFS appear...

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“…These proteins are localized in connective tissues, including the skin, aorta and perichondrocytes. Among ADAMTSL6, ADAMTSL6β has shown to associated with fibrillin-1 microfibrils through its direct interaction with the N-terminal region of fibrillin-1 and promotes fibrillin-1 matrix assembly in vitro and in vivo [43]. These findings suggest a potential clinical application of ADAMTSL6β as a novel MFS therapy by promoting fibrillin-1 microfibril assembly and regulating TGF-β activation.…”

Section: Adamtsl6β Serves As a Novel Molecules That Regulate Microfibmentioning

confidence: 82%

Trends in Periodontal Regeneration Therapy: Potential Therapeutic Strategy of Extracellular Matrix Administration for Periodontal Ligament Regeneration

Saito

2015

Interface Oral Health Science 2014

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ADAMTSL-6 Is a Novel Extracellular Matrix Protein That Binds to Fibrillin-1 and Promotes Fibrillin-1 Fibril Formation

Cited by 94 publications

References 61 publications

ADAMTSL6β Protein Rescues Fibrillin-1 Microfibril Disorder in a Marfan Syndrome Mouse Model through the Promotion of Fibrillin-1 Assembly

ADAMTSL6β Protein Rescues Fibrillin-1 Microfibril Disorder in a Marfan Syndrome Mouse Model through the Promotion of Fibrillin-1 Assembly

ADAMTS10 Protein Interacts with Fibrillin-1 and Promotes Its Deposition in Extracellular Matrix of Cultured Fibroblasts

Trends in Periodontal Regeneration Therapy: Potential Therapeutic Strategy of Extracellular Matrix Administration for Periodontal Ligament Regeneration

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