OR27-07 Molecular Mechanism of Androgen Receptor Mutation in Multigenerational Mild Androgen Insensitivity Syndrome

Chang, R; Pandher, R; Hibbs, D; Du, J; McGrath, K; Heather, A; Jayadev, V; Handelsman, DJ

OR27-07 Molecular Mechanism of Androgen Receptor Mutation in Multigenerational Mild Androgen Insensitivity Syndrome

Chang, R Pandher, R Hibbs, D Du, J McGrath, K

Heather, A Jayadev, V Handelsman, DJ

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Publisher:: The Endocrine Society
Publication Type:: Journal Article
Citation:: Journal of the Endocrine Society, 2025, 9, (Supplement_1), pp. bvaf149.1961
Issue Date:: 2025-10-22

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Field	Value	Language
dc.contributor.author	Chang, R
dc.contributor.author	Pandher, R
dc.contributor.author	Hibbs, D
dc.contributor.author	Du, J
dc.contributor.author	McGrath, K https://orcid.org/0000-0002-6244-3929
dc.contributor.author	Heather, A
dc.contributor.author	Jayadev, V
dc.contributor.author	Handelsman, DJ
dc.date.accessioned	2026-04-09T04:38:34Z
dc.date.available	2026-04-09T04:38:34Z
dc.date.issued	2025-10-22
dc.identifier.citation	Journal of the Endocrine Society, 2025, 9, (Supplement_1), pp. bvaf149.1961
dc.identifier.issn	2472-1972
dc.identifier.issn	2472-1972
dc.identifier.uri	http://hdl.handle.net/10453/194622
dc.description.abstract	Abstract<p> Disclosure: R. Chang: None. R. Pandher: None. D. Hibbs: None. J. Du: None. K. McGrath: None. A. Heather: None. V. Jayadev: None. D.J. Handelsman: None.</p><p> Objective Androgen insensitivity syndrome (AIS) due to androgen receptor (AR) mutations create a spectrum of clinical presentations based on residual AR function. The mildest impairment of this condition is known as mild AIS (MAIS), whose undefined molecular mechanism and subtle clinical features leave it little understood and underdiagnosed. Methods and Result The clinical features of this mutation are discussed along with response to high dose testosterone in three cases of MAIS across a six-generation family pedigree with a missense AR exon 8 mutation (nucleotide aga --> gga, p. R872G arginine to glycine). All three cases of MAIS displayed consistent gynaecomastia and micropenis but variable fertility. High dose testosterone treatment for 3 years in one young man caused increased virilisation and height growth but was ineffective for micropenis. Genetic counselling allowed for effective prediction of MAIS risks in progeny for carrier and non-carrier sisters. This AR mutation, previously shown to display increased ligand dissociation rate from the mutated AR in binding assays, was shown by in silico structural modelling to demonstrate weakened closure energy of the “lid” of the ligand binding pocket allowing for easier ligand dissociation from binding site. An in vitro yeast-based androgen bioassay demonstrated unimpaired androgen bioactivity. Conclusion: The molecular mechanism of the p. R8729G mutation in exon 8 of the AR ligand binding domain demonstrated increased ligand dissociation from its binding site due to weakened closure of the binding pocket “lid” but without impact on androgen bioactivity. This novel molecular mechanism may be present in other cases of MAIS. Discrepancy between MAIS genotype and phenotype in those carrying the same AR mutation is known and may be present within our cohort.</p><p> Presentation: Monday, July 14, 2025</p>
dc.language	en
dc.publisher	The Endocrine Society
dc.relation.ispartof	Journal of the Endocrine Society
dc.relation.isbasedon	10.1210/jendso/bvaf149.1961
dc.rights	info:eu-repo/semantics/openAccess
dc.subject.classification	3201 Cardiovascular medicine and haematology
dc.title	OR27-07 Molecular Mechanism of Androgen Receptor Mutation in Multigenerational Mild Androgen Insensitivity Syndrome
dc.type	Journal Article
utslib.citation.volume	9
pubs.organisational-group	University of Technology Sydney
pubs.organisational-group	University of Technology Sydney/Faculty of Science
pubs.organisational-group	University of Technology Sydney/Faculty of Science/School of Life Sciences
pubs.organisational-group	University of Technology Sydney/UTS Groups
pubs.organisational-group	University of Technology Sydney/UTS Groups/Climate Change & Health Research Collaborative (CCHRC)
pubs.organisational-group	University of Technology Sydney/UTS Groups/Women & Children’s Health Research Collaborative (WCHC)
pubs.organisational-group	University of Technology Sydney/UTS Groups/Centre for Health Technologies (CHT)
utslib.copyright.status	open_access	*
dc.rights.license	This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License (CC BY-NC-ND 4.0). To view a copy of this license, visit https://creativecommons.org/licenses/by-nc-nd/4.0/
dc.date.updated	2026-04-09T04:38:33Z
pubs.issue	Supplement_1
pubs.publication-status	Published
pubs.volume	9
utslib.citation.issue	Supplement_1

Abstract:

Abstract

Disclosure: R. Chang: None. R. Pandher: None. D. Hibbs: None. J. Du: None. K. McGrath: None. A. Heather: None. V. Jayadev: None. D.J. Handelsman: None.

Objective Androgen insensitivity syndrome (AIS) due to androgen receptor (AR) mutations create a spectrum of clinical presentations based on residual AR function. The mildest impairment of this condition is known as mild AIS (MAIS), whose undefined molecular mechanism and subtle clinical features leave it little understood and underdiagnosed. Methods and Result The clinical features of this mutation are discussed along with response to high dose testosterone in three cases of MAIS across a six-generation family pedigree with a missense AR exon 8 mutation (nucleotide aga --> gga, p. R872G arginine to glycine). All three cases of MAIS displayed consistent gynaecomastia and micropenis but variable fertility. High dose testosterone treatment for 3 years in one young man caused increased virilisation and height growth but was ineffective for micropenis. Genetic counselling allowed for effective prediction of MAIS risks in progeny for carrier and non-carrier sisters. This AR mutation, previously shown to display increased ligand dissociation rate from the mutated AR in binding assays, was shown by in silico structural modelling to demonstrate weakened closure energy of the “lid” of the ligand binding pocket allowing for easier ligand dissociation from binding site. An in vitro yeast-based androgen bioassay demonstrated unimpaired androgen bioactivity. Conclusion: The molecular mechanism of the p. R8729G mutation in exon 8 of the AR ligand binding domain demonstrated increased ligand dissociation from its binding site due to weakened closure of the binding pocket “lid” but without impact on androgen bioactivity. This novel molecular mechanism may be present in other cases of MAIS. Discrepancy between MAIS genotype and phenotype in those carrying the same AR mutation is known and may be present within our cohort.

Presentation: Monday, July 14, 2025

Please use this identifier to cite or link to this item:

http://hdl.handle.net/10453/194622