New roles of SHOX as regulator of target genes.

[achondroplasia]

The homeobox gene SHOX encodes a transcription factor which is important for normal limb development . Approximately 5 to 10 % of short patients exhibit a mutation or deletion in either the SHOX gene or its downstream enhancer regions . In humans , SHOX deficiency has been associated with various short stature syndromes as well as non-syndromic idiopathic short stature . A common feature of these syndromes is disproportionate short stature with a particular shortening of the forearms and lower legs . Madelung deformity , cubitus valgus , high-arched palate and muscular hypertrophy also differed markedly between patients with or without SHOX gene defects . A clinical trial in patients with SHOX deficiency and Turner syndrome demonstrated highly significant growth hormone-stimulated increases in height velocity and height SDS in both groups . Employing microarray analyses and cell culture experiments , a strong effect of SHOX on the expression of the natriuretic peptide BNP and the fibroblast growth factor receptor gene FGFR 3 could be demonstrated . We found that BNP was positively regulated , while Fgfr 3 was negatively regulated by SHOX . A regulation that occurs mainly in the mesomelic segments , a region where SHOX is known to be strongly expressed , offers a possible explanation for the phenotypes seen in patients with FGFR 3 (e .g . achondroplasia ) and SHOX defects (e .g . LÃ©ri-Weill dyschondrosteosis ).

Diseases
Validation

Diseases presenting "a region where shox is known to be strongly expressed" symptom

achondroplasia

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