AI Article Synopsis

  • The study investigates how HOX genes, crucial for the development of vertebrate spinal cord motor neurons, are activated in a specific sequence during differentiation.
  • Researchers found that the activation pace of these genes, termed the 'HOX clock', is influenced by FGF signaling; blocking this pathway halted gene activation, while increasing FGF accelerated it.
  • By manipulating the HOX clock through FGF and GDF11, the researchers could generate various human neuronal subtypes, offering potential for research and therapeutic applications.

Article Abstract

Rostro-caudal patterning of vertebrates depends on the temporally progressive activation of HOX genes within axial stem cells that fuel axial embryo elongation. Whether the pace of sequential activation of HOX genes, the 'HOX clock', is controlled by intrinsic chromatin-based timing mechanisms or by temporal changes in extrinsic cues remains unclear. Here, we studied HOX clock pacing in human pluripotent stem cell-derived axial progenitors differentiating into diverse spinal cord motor neuron subtypes. We show that the progressive activation of caudal HOX genes is controlled by a dynamic increase in FGF signaling. Blocking the FGF pathway stalled induction of HOX genes, while a precocious increase of FGF, alone or with GDF11 ligand, accelerated the HOX clock. Cells differentiated under accelerated HOX induction generated appropriate posterior motor neuron subtypes found along the human embryonic spinal cord. The pacing of the HOX clock is thus dynamically regulated by exposure to secreted cues. Its manipulation by extrinsic factors provides synchronized access to multiple human neuronal subtypes of distinct rostro-caudal identities for basic and translational applications.This article has an associated 'The people behind the papers' interview.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8034877PMC
http://dx.doi.org/10.1242/dev.194514DOI Listing

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