Timing underpins the benefits associated with injectable collagen biomaterial therapy for the treatment of myocardial infarction.

Biomaterials

Division of Cardiac Surgery, University of Ottawa Heart Institute, Ottawa K1Y 4W7, Canada; Department of Cellular and Molecular Medicine, University of Ottawa, Ottawa K1H 8M5, Canada. Electronic address:

Published: January 2015

AI Article Synopsis

  • Injectable hydrogel biomaterials, like collagen matrices, show potential for repairing heart tissue after a heart attack (MI).
  • The timing of delivery is crucial; administering the treatment within 3 hours post-MI yields significantly better outcomes than waiting 1 or 2 weeks.
  • The collagen matrix not only avoids inducing immediate inflammation but also helps to improve heart tissue health by influencing cytokines, promoting blood vessel growth (angiogenesis), and decreasing scarring and cell death long-term.

Article Abstract

Injectable hydrogel biomaterials are promising therapies to promote repair and regeneration post-myocardial infarction (MI). However, the timing of delivery and the mechanisms through which biomaterial treatments confer their benefits are translational issues that remain to be addressed. We assessed the efficacy of an injectable collagen matrix at 3 different delivery time points post-MI. Infarcted mice received the matrix or control (saline) treatment at 3 h, 1 week or 2 weeks after MI. The earlier treatment delivery better prevented negative ventricular remodeling and long-term deterioration of cardiac function (up to 3 months), whereas waiting longer to administer the matrix (1 and 2 weeks post-MI) reduced the therapeutic effects. Collagen matrix delivery did not stimulate an inflammatory response acutely and favorably modulated inflammation in the myocardium long-term. We found that the matrix interacts with the host tissue to alter the myocardial cytokine profile, promote angiogenesis, and reduce fibrosis and cell death. This work highlights that the timing of delivery can significantly affect the ability of an injectable hydrogel to protect the post-MI environment, which will be an important consideration in the clinical translation of cardiac biomaterial therapy.

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Source
http://dx.doi.org/10.1016/j.biomaterials.2014.11.004DOI Listing

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