AI Article Synopsis

  • Trisomy 21 (Down syndrome) is the most common chromosomal abnormality and leads to various health issues, necessitating a better cellular model for research.
  • Researchers derived induced pluripotent stem cells (iPSCs) from mid-trimester amniotic fluid stem cells to study the syndrome's hematopoietic and neurological features.
  • The iPSCs demonstrated embryonic stem cell-like properties, retained their genetic profiles, differentiated into specialized cell types, and showed pluripotency markers, paving the way for future studies and potential treatments for trisomy 21.

Article Abstract

Trisomy 21 is the most common chromosomal abnormality and is associated primarily with cardiovascular, hematological, and neurological complications. A robust patient-derived cellular model is necessary to investigate the pathophysiology of the syndrome because current animal models are limited and access to tissues from affected individuals is ethically challenging. We aimed to derive induced pluripotent stem cells (iPSCs) from trisomy 21 human mid-trimester amniotic fluid stem cells (AFSCs) and describe their hematopoietic and neurological characteristics. Human AFSCs collected from women undergoing prenatal diagnosis were selected for c-KIT(+) and transduced with a Cre-lox-inducible polycistronic lentiviral vector encoding SOX2, OCT4, KLF-4, and c-MYC (50,000 cells at a multiplicity of infection (MOI) 1-5 for 72 h). The embryonic stem cell (ESC)-like properties of the AFSC-derived iPSCs were established in vitro by embryoid body formation and in vivo by teratoma formation in RAG2(-/-), γ-chain(-/-), C2(-/-) immunodeficient mice. Reprogrammed cells retained their cytogenetic signatures and differentiated into specialized hematopoietic and neural precursors detected by morphological assessment, immunostaining, and RT-PCR. Additionally, the iPSCs expressed all pluripotency markers upon multiple rounds of freeze-thawing. These findings are important in establishing a patient-specific cellular platform of trisomy 21 to study the pathophysiology of the aneuploidy and for future drug discovery.

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Source
http://dx.doi.org/10.1089/cell.2013.0091DOI Listing

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