The novel p.E89K mutation in the SRY gene inhibits DNA binding and causes the 46,XY disorder of sex development

Abstract

In humans, male sex determination is controlled by the SRY gene, which encodes a transcriptional regulator with a conserved high mobility group box domain (HMG) required for DNA-binding. Mutations in the SRY HMG-box are known to affect the protein function leading to sex reversal phenotypes. In this study, we describe the novel p.E89K missense mutation in the SRY HMG-box. It was identified in a patient with 46,XY complete gonadal dysgenesis as a de novo mutation. Electrophoretic mobility shift assays showed that p.E89K almost completely abolished the SRY DNA-binding activity, suggesting that it is the cause of SRY function impairment. In addition, we report the occurrence of the p.G95R mutation in a 46,XY female with complete gonadal dysgenesis. Based on the three-dimensional structure of the SRY HMG-box, we discuss that the change of the acidic glutamic acid by the basic lysine in residue 89 introduces a positive charge adjacently to R86 and K92 residues and may cause electrostatic repulsion and destabilization of the interaction between SRY HMG-box helix 2 and its target DNA sequence. (AU)