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Glucocorticoid treatment rescues early lethality in a mouse model of geleophysic dysplasia.


ABSTRACT: Geleophysic dysplasia (GD) is a rare genetic disorder characterized by severe cardiorespiratory dysfunction and poor prognosis. With no cure available, current treatments focus on symptomatic management. Using a cellular model of ADAMTSL2 p.A165T variant, our screening of 2,321 FDA-approved drugs identified several glucocorticoids, particularly betamethasone dipropionate (BMD), which significantly enhance secretion of two crucial proteins for GD, ADAMTSL2 and FBN1 while improving extracellular matrix organization. In a mouse model carrying the Adamtsl2 p.A165T variant, we observed a high early mortality rate, mirroring the short lifespan seen in GD patients. Around only 60% of homozygous p.A165T mice survived beyond two days after birth, while hemizygous p.A165T/- mice had an even lower survival rate of 40%. Notably, BMD administration at birth significantly improved survival rates to 80% and 69%, respectively. These findings suggest that BMD offers a promising therapeutic approach to prevent early mortality in GD patients.

SUBMITTER: Morales AA 

PROVIDER: S-EPMC12658166 | biostudies-literature | 2025 Nov

REPOSITORIES: biostudies-literature

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Glucocorticoid treatment rescues early lethality in a mouse model of geleophysic dysplasia.

Morales Alejo Antonio AA   Camarena Vladimir V   Walz Katherina K   Wang Gaofeng G   Tekin Mustafa M  

Communications biology 20251126 1


Geleophysic dysplasia (GD) is a rare genetic disorder characterized by severe cardiorespiratory dysfunction and poor prognosis. With no cure available, current treatments focus on symptomatic management. Using a cellular model of ADAMTSL2 p.A165T variant, our screening of 2,321 FDA-approved drugs identified several glucocorticoids, particularly betamethasone dipropionate (BMD), which significantly enhance secretion of two crucial proteins for GD, ADAMTSL2 and FBN1 while improving extracellular m  ...[more]

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