4.7 Article

Microcurrent and adipose-derived stem cells modulate genes expression involved in the structural recovery of transected tendon of rats

期刊

FASEB JOURNAL
卷 34, 期 8, 页码 10011-10026

出版社

WILEY
DOI: 10.1096/fj.201902942RR

关键词

cell therapy; collagen; CTGF; electrical stimulation; tendon repair

资金

  1. Capes (Coordination for the Improvement of Higher Education Personnel)
  2. Herminio Ometto Foundation/FHO

向作者/读者索取更多资源

Tendon injuries are common and have a high incidence of re-rupture that can cause loss of functionality. Therapies with adipose-derived stem cells (ASC) and the microcurrent (low-intensity electrical stimulation) application present promising effects on the tissue repair. We analyzed the expression of genes and the participation of some molecules potentially involved in the structural recovery of the Achilles tendon of rats, in response to the application of both therapies, isolated and combined. The tendons were distributed in five groups: normal (N), transected (T), transected and ASC (C) or microcurrent (M) or with ASC, and microcurrent (MC). Microcurrent therapy was beneficial for tendon repair, as it was observed a statistically significant increase in the organization of the collagen fibers, with involvement of theTNC, CTGF, FN, FMDO,andCOL3A1genes as well as PCNA, IL-10, and TNF-alpha. ASC therapy significantly increased theTNCandFMDOgenes expression with no changes in the molecular organization of collagen. With the association of therapies, a significant greater collagen fibers organization was observed with involvement of theFMODgene. The therapies did not affect the expression ofCOL1A1, SMAD2,SMAD3,MKX,andEGR1genes, nor did they influence the amount of collagen I and III, caspase-3, tenomodulin (Tnmd), and hydroxyproline. In conclusion, the application of the microcurrent isolated or associated with ASC increased the organization of the collagen fibers, which can result in a greater biomechanical resistance in relation to the tendons treated only with ASC. Future studies will be needed to demonstrate the biological effects of these therapies on the functional recovery of injured tendons.

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