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Fryns type mesomelic dysplasia of the upper limbs caused by inverted duplications of the HOXD gene cluster. | LitMetric

AI Article Synopsis

  • * Rare genetic abnormalities like duplications and rearrangements of HOXD genes can lead to mesomelic dysplasia, a condition affecting upper and lower limb formation.
  • * In two families with upper limb dysplasia, researchers discovered microduplications affecting HOXD genes, which likely disrupt gene regulation and contribute to the disease phenotype by misplacing a regulatory influence on specific HOXD genes.

Article Abstract

The HoxD cluster is critical for vertebrate limb development. Enhancers located in both the telomeric and centromeric gene deserts flanking the cluster regulate the transcription of HoxD genes. In rare patients, duplications, balanced translocations or inversions misregulating HOXD genes are responsible for mesomelic dysplasia of the upper and lower limbs. By aCGH, whole-genome mate-pair sequencing, long-range PCR and fiber fluorescent in situ hybridization, we studied patients from two families displaying mesomelic dysplasia limited to the upper limbs. We identified microduplications including the HOXD cluster and showed that microduplications were in an inverted orientation and inserted between the HOXD cluster and the telomeric enhancers. Our results highlight the existence of an autosomal dominant condition consisting of isolated ulnar dysplasia caused by microduplications inserted between the HOXD cluster and the telomeric enhancers. The duplications likely disconnect the HOXD9 to HOXD11 genes from their regulatory sequences. This presumptive loss-of-function may have contributed to the phenotype. In both cases, however, these rearrangements brought HOXD13 closer to telomeric enhancers, suggesting that the alterations derive from the dominant-negative effect of this digit-specific protein when ectopically expressed during the early development of forearms, through the disruption of topologically associating domain structure at the HOXD locus.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7028936PMC
http://dx.doi.org/10.1038/s41431-019-0522-2DOI Listing

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