The metalloproteinase-proteoglycans ADAMTS7 and ADAMTS12 provide an innate, tendon-specific protective mechanism against heterotopic ossification
Timothy J. Mead, … , David E. Birk, Suneel S. Apte
Timothy J. Mead, … , David E. Birk, Suneel S. Apte
Published April 5, 2018
Citation Information: JCI Insight. 2018;3(7):e92941. https://doi.org/10.1172/jci.insight.92941.
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Research Article Bone biology Genetics

The metalloproteinase-proteoglycans ADAMTS7 and ADAMTS12 provide an innate, tendon-specific protective mechanism against heterotopic ossification

Abstract

Heterotopic ossification (HO) is a significant clinical problem with incompletely resolved mechanisms. Here, the secreted metalloproteinases ADAMTS7 and ADAMTS12 are shown to comprise a unique proteoglycan class that protects against a tendency toward HO in mouse hindlimb tendons, menisci, and ligaments. Adamts7 and Adamts12 mRNAs were sparsely expressed in murine forelimbs but strongly coexpressed in hindlimb tendons, skeletal muscle, ligaments, and meniscal fibrocartilage. Adamts7–/– Adamts12–/– mice, but not corresponding single-gene mutants, which demonstrated compensatory upregulation of the intact homolog mRNA, developed progressive HO in these tissues after 4 months of age. Adamts7–/– Adamts12–/– tendons had abnormal collagen fibrils, accompanied by reduced levels of the small leucine-rich proteoglycans (SLRPs) biglycan, fibromodulin, and decorin, which regulate collagen fibrillogenesis. Bgn–/0 Fmod–/– mice are known to have a strikingly similar hindlimb HO to that of Adamts7–/– Adamts12–/– mice, implicating fibromodulin and biglycan reduction as a likely mechanism underlying HO in Adamts7–/– Adamts12–/– mice. Interestingly, degenerated human biceps tendons had reduced ADAMTS7 mRNA compared with healthy biceps tendons, which expressed both ADAMTS7 and ADAMTS12. These results suggest that ADAMTS7 and ADAMTS12 drive an innate pathway protective against hindlimb HO in mice and may be essential for human tendon health.

Authors

Timothy J. Mead, Daniel R. McCulloch, Jason C. Ho, Yaoyao Du, Sheila M. Adams, David E. Birk, Suneel S. Apte

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Figure 2

Adamts7 and Adamts12 are expressed in hindlimb tendons and menisci and show mutual compensation.

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Adamts7 and Adamts12 are expressed in hindlimb tendons and menisci and ...
(A) Adamts7 (β-gal staining, blue nuclei, eosin counterstain is red) and Adamts12 expression (RNA in situ hybridization [red signal]) are shown in 18.5-day-old embryo hindlimbs. Expression is seen in the quadriceps (QT), patellar (PT), and Achilles tendons (AT) and meniscal fibrocartilage. The data are representative of n = 5. F, femur; T, tibia; P, patella; M, meniscus. Scale bars: 200 μm. (B) RT-PCR analysis of newborn, 1-month-old (juvenile), and 4-month-old (adult) tendons to show widespread expression of Adamts7 and Adamts12. EDLT, extensor digitorum longus tendon. The data are representative of n = 3. (C) qRT-PCR analysis of Adamts7 and Adamts12 mRNA levels in quadriceps tendons showing a decline with age. n = 6. Error bars represent ± SEM. (D) qRT-PCR analysis of Adamts7 and Adamts12 mRNAs in wild-type, Adamts7–/–, Adamts12–/–, and Adamts7–/– Adamts12–/– double-knockout mice shows mutual compensation by Adamts7 and Adamts12. n = 3. Error bars represent ± SEM. *P ≤ 0.01; #P ≤ 0.05 by Student’s t test.