THE POLYMORPHISM OF METALLOPROTEINASES 1 AND 13 AND POSTTRAUMATIC ELBOW STIFFNESS

THE POLYMORPHISM OF METALLOPROTEINASES 1 AND 13 AND POSTTRAUMATIC ELBOW STIFFNESS

To evaluate the relationship between the genetic polymorphism of matrix metalloproteinases 1 and 13 and posttraumatic elbow stiffness, as well as the association of other risk factors with this condition. We evaluated 20 patients with posttraumatic elbow stiffness and 12 controls with traumatic elbo...

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Published in:Acta ortopedica brasileira Vol. 30; no. 1; p. e253503
Main Authors: Pinto, Gustavo DE Mello Ribeiro, Assunção, Jorge Henrique, Santos, Maria Cristina Leme Godoy Dos, Godoy-Santos, Alexandre Leme, Gracitelli, Mauro Emilio Conforto, Malavolta, Eduardo Angeli, Silva, Fernando Brandão DE Andrade E, Neto, Arnaldo Amado Ferreira
Format: Journal Article
Language:English
Published: Brazil ATHA EDITORA 01-01-2022
Sociedade Brasileira de Ortopedia e Traumatologia
Subjects:
Articular rigidity
Capsule contracture
Elbow
Genetic polymorphism
Metalloproteinases
Original
ORTHOPEDICS
Trauma
Articular rigidity
Metalloproteinases
Elbow
Trauma
Capsule contracture
Genetic polymorphism
Metaloproteinases
Polimorfismo genético
Contratura capsular
Cotovelo
Rigidez articular
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Summary:To evaluate the relationship between the genetic polymorphism of matrix metalloproteinases 1 and 13 and posttraumatic elbow stiffness, as well as the association of other risk factors with this condition. We evaluated 20 patients with posttraumatic elbow stiffness and 12 controls with traumatic elbow disorders without contracture. Deoxyribonucleic acid (DNA) was obtained from buccal mucosa epithelial cells of the volunteers. The MMP-1 and MMP-13 genotypes were determined using PCR-restriction fragment length polymorphism assays. We did not find any significant differences in the frequency of genotypes and alleles between the test and control groups for the polymorphism of metalloproteinases 1 and 13. We observed that genotypes 1G/2G and 2G/2G of MMP-1 were present in 65% (13/20) of patients with articular stiffness and 50% (6/12) of controls (p = 0.599). Genotypes A/A and A/G of MMP-13 were obtained in 95% (19/20) of patients and 91.6% (11/12) of controls (p = 0.491). Among the prognostic factors for elbow stiffness, only immobilization time correlated positively. The mean immobilization time for cases and controls were 16 ± 10 days and 7 ± 7 days, respectively (p = 0.017). The genetic polymorphism of MMP-1 at position -1607 and MMP-13 at position -77 was not associated with post-traumatic elbow stiffness.
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AUTHORS’ CONTRIBUTION: GMRP: conceived and planned the activities that led to the study, wrote the Original Draft and participated in the review process of the manuscript; JHA: conceived and planned the activities that led to the study, development the design of methodology, interpreted the results of the study, participated in the review process of the manuscript; MCLGS: provided study material and scientific support; ALGS: development the design of methodology, provided study material and scientific support; MECG: participated in the review process of the manuscript; EAM: participated in the review process of the manuscript; FBAS: participated in the review process of the manuscript; AAFN: supervision of the study, participated in the review process of the manuscript. All authors have read and approved the final article, and also authorized its publication.
All authors declare no potential conflict of interest related to this article.
ISSN:1413-7852
1809-4406
1809-4406
DOI:10.1590/1413-785220223001e253503