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Home › Dataset Library › Genome-Wide Analysis of Gene Program Activation by Defined Cardiac Transcription Factor Tbx5, Gata4 and Myocardin

Dataset: Genome-Wide Analysis of Gene Program Activation by Defined Cardiac Transcription Factor Tbx5, Gata4 and Myocardin

Background: Cardiac transcription factors are master regulators during heart development. Recently, some were shown to transdifferentiate...

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Background: Cardiac transcription factors are master regulators during heart development. Recently, some were shown to transdifferentiate noncardiac mesoderm cells and cardiac fibroblasts into cardiomyocytes. However, the individual roles of each transcription factors in activating cardiac gene program have not been elucidated. We examined cardiac-specific and genome-wide gene expression in fibroblasts induced with cardiac transcription factors Nkx2.5 (N), Tbx5 (T), Gata4 (G), Myocardin (M) alone or different combinations. Methodology/Principal Findings: We applied different combinations of human Nkx2.5 (N), Tbx5 (T), Gata4 (G) and Myocardin (M) lentiviruses into 10T1/2 fibroblasts. Immunostaining and quantitative reverse transcription polymerase chain reaction (qRT-PCR) showed that N, T, G or M alone did not induce expression of cardiac marker genes α-myosin heavy chain (αMHC) and cardiac troponin T (cTnT). Only T+M and T+G+M combinations induced αMHC and cTnT expression. Microarray-based gene ontology analysis revealed that T alone inhibited most genes involved in cardiac-related processes and activated genes involved in Wnt receptor signaling pathway and in aberrant processes. M alone inhibited genes involved in Wnt receptor signaling pathway and activated genes involved in cardiac-related processes and in aberrant processes. G alone inhibited genes involved in ectoderm development. T+G+M combination was the most effective activator of genes associated with cardiac-related processes including muscle cell differentiation, sarcomere, striated muscle contraction, regulation of heart contraction, and glucose metabolism and fatty acid oxidation (two significant forms of cardiomyocyte energy metabolism). And unlike T, M, G alone or T+M, T+G+M did not activate genes associated with aberrant processes. Conclusions: Tbx5, Gata4 and Myocardin play different roles in activating cardiac gene program and in avoiding aberrant gene program activation. The combination of T+G+M activated cardiac gene program and avoided aberrant gene program activation. Two weeks after doxycline induction, total RNA was isolated from 10T1/2-tTA cells infected with different combinations of Tbx5, Gata4, and Myocardin lentiviruses. Biological triplicated.

Species:
mouse

Samples:
24

Source:
E-GEOD-27329

PubMed:
23144723

Updated:
Dec.12, 2014

Registered:
Nov.11, 2014


Factors: (via ArrayExpress)
Sample LENTIVIRUS INFECTION
GSM675173 LacZ
GSM675173 LacZ
GSM675173 LacZ
GSM675555 Tbx5
GSM675555 Tbx5
GSM675555 Tbx5
GSM675618 Gata4
GSM675618 Gata4
GSM675618 Gata4
GSM675622 Myocardin
GSM675622 Myocardin
GSM675622 Myocardin
GSM675626 Tg
GSM675626 Tg
GSM675626 Tg
GSM675649 GM
GSM675649 GM
GSM675649 GM
GSM675654 TM
GSM675654 TM
GSM675654 TM
GSM675657 TGM
GSM675657 TGM
GSM675657 TGM

Tags

  • cell
  • ectoderm
  • fatty acid
  • genome
  • glucose
  • heart
  • mesoderm
  • muscle
  • muscle cell
  • myosin
  • myosin heavy chain
  • sarcomere
  • troponin

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