4.2 Article

Depolarization of Cellular Resting Membrane Potential Promotes Neonatal Cardiomyocyte Proliferation In Vitro

期刊

CELLULAR AND MOLECULAR BIOENGINEERING
卷 7, 期 3, 页码 432-445

出版社

SPRINGER
DOI: 10.1007/s12195-014-0346-7

关键词

Cell cycle; Potassium gluconate; Ouabain; Cardiac fibroblasts; Akt pathway

资金

  1. NIH-NHLBI via NRSA [F32 HL112538]
  2. NIH-NHLBI [R00HL093358, R21HL115570]
  3. G. Harold and Leila Y. Mathers Charitable Foundation
  4. DARPA [W911NF-09-1-0125]
  5. W. M. Keck Foundation

向作者/读者索取更多资源

Cardiomyocytes (CMs) undergo a rapid transition from hyperplastic to hypertrophic growth soon after birth, which is a major challenge to the development of engineered cardiac tissue for pediatric patients. Resting membrane potential (V (mem)) has been shown to play an important role in cell differentiation and proliferation during development. We hypothesized that depolarization of neonatal CMs would stimulate or maintain CM proliferation in vitro. To test our hypothesis, we isolated postnatal day 3 neonatal rat CMs and subjected them to sustained depolarization via the addition of potassium gluconate or Ouabain to the culture medium. Cell density and CM percentage measurements demonstrated an increase in mitotic CMs along with a similar to is an element of twofold increase in CM numbers with depolarization. In addition, depolarization led to an increase in cells in G2 and S phase, indicating increased proliferation, as measured by flow cytometry. Surprisingly depolarization of V (mem) with either treatment led to inhibition of proliferation in cardiac fibroblasts. This effect is abrogated when the study was carried out on postnatal day 7 neonatal CMs, which are less proliferative, indicating that the likely mechanism of depolarization is the maintenance of the proliferating CM population. In summary, our findings suggest that depolarization maintains postnatal CM proliferation and may be a novel approach to encourage growth of engineered tissue and cardiac regeneration in pediatric patients.

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