Homozygous GDF2 nonsense mutations result in a loss of circulating BMP9 and BMP10 and are associated with either PAH or an "HHT-like" syndrome in children.

Joshua Mark Hodgson Lidia Ruiz-Llorente Jamie McDonald Oliver W J QuarrellKelechi UgonnaJames BenthamRebecca MasonJennifer M Martin Alejandro Sifrim Katie Bergstrom Pinar Bayrak-Toydemir Whitney L Wooderchak-Donahue Nicholas W Morrell Robin Condliffe Carmelo Bernabéu Paul D Upton

Published in: Molecular genetics & genomic medicine (2021)

Collectively, these data show that homozygous GDF2 mutations, leading to a loss of circulating BMP9 and BMP10, can cause either pediatric PAH and/or "HHT-like" telangiectases and PAVMs. Although patients reported to date have manifestations that overlap with those of HHT, none meet the Curaçao criteria for HHT and seem distinct from HHT in terms of the location and appearance of telangiectases, and a tendency for tiny, diffuse PAVMs.

Keyphrases

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