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Single-cell protein activity analysis reveals aberrant myogenesis and IGF2-PI3K pathway dependencies in MYOD1-mutant rhabdomyosarcoma - PubMed

3 hours ago
  • #IGF2-PI3K pathway
  • #single-cell analysis
  • #rhabdomyosarcoma
  • Single-cell protein activity analysis identifies aberrant myogenesis and IGF2-PI3K pathway dependencies in MYOD1-mutant rhabdomyosarcoma.
  • MYOD1L122R-mutant spindle cell rhabdomyosarcoma (SRMS) is a rare, treatment-resistant sarcoma with poor outcomes.
  • Regulatory network analysis of single-nucleus RNA sequencing (snRNA-seq) from six patient tumors reveals disrupted myogenesis and actionable master regulator dependencies across three tumor cell states.
  • Three coexisting tumor cell states identified: MYOD1-enriched progenitor-like state, proliferative transition state, and partially differentiated state with reduced MYOD1 activity.
  • Ligand-receptor analysis uncovers paracrine IGF2-IGF1R-PI3K signaling from progenitor to transition/differentiated states, with therapeutic potential demonstrated in ex vivo drug screens.
  • Inhibition of IGF2-PI3K signaling significantly improved disease control in a patient-derived xenograft model.
  • Oncogenic master regulators were recapitulated in 24 bulk RNA profiles, while 20 DNA profiles revealed recurrent IGF2/PI3K/AKT alterations.
  • Findings suggest IGF1R-PI3K/AKT/mTOR inhibitors as potential therapeutic options for MYOD1L122R-mutant SRMS.
  • Highlights the utility of single-cell regulatory network analysis for uncovering actionable dependencies in rare, transcriptionally complex cancers.
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