Germline PTCH1: c.361_362insAlu alteration identified by comprehensive exome and RNA sequencing in a patient with Gorlin syndrome.

Mochizuki, AY; Nagaraj, CB; Depoorter, D; Schieffer, KM; Kim, SY

Germline PTCH1: c.361_362insAlu alteration identified by comprehensive exome and RNA sequencing in a patient with Gorlin syndrome.

Mochizuki, AY Nagaraj, CB Depoorter, D Schieffer, KM Kim, SY

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Publisher:: Wiley
Publication Type:: Journal Article
Citation:: Am J Med Genet A, 2024, 194, (10), pp. e63788
Issue Date:: 2024-10

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Field	Value	Language
dc.contributor.author	Mochizuki, AY
dc.contributor.author	Nagaraj, CB
dc.contributor.author	Depoorter, D
dc.contributor.author	Schieffer, KM
dc.contributor.author	Kim, SY
dc.date.accessioned	2025-05-05T22:52:27Z
dc.date.available	2024-05-31
dc.date.available	2025-05-05T22:52:27Z
dc.date.issued	2024-10
dc.identifier.citation	Am J Med Genet A, 2024, 194, (10), pp. e63788
dc.identifier.issn	1552-4825
dc.identifier.issn	1552-4833
dc.identifier.uri	http://hdl.handle.net/10453/187192
dc.description.abstract	Gorlin syndrome can be caused by pathogenic/likely pathogenic (P/LP) variants in the tumor suppressor gene PTCH1 (9q22.1-q31), which encodes the receptor for the sonic hedgehog (SHH) ligand. We present a 12-month-old boy clinically diagnosed with Gorlin syndrome who was found to have significantly delayed development, palmar pitting, palmar and plantar keratosis, short hands, frontal bossing, coarse face, hypertelorism, a bifid rib, misaligned and missing teeth, and SHH-activated medulloblastoma. Genetic testing, including a pediatric cancer panel and genome sequencing with peripheral blood, failed to identify any P/LP variants in PTCH1. Paired tumor/normal exome sequencing was performed, which identified a germline NM_000264.5 (PTCH1): c.361_362ins? alteration through manual review of sequencing reads. Clinical RNA sequencing further demonstrated an Alu insertion at this region (PTCH1: c.361_362insAlu), providing molecular confirmation of Gorlin syndrome. This finding exemplifies a unique mechanism for PTCH1 disruption in the germline and highlights the importance of comprehensive analysis, including manual review of DNA sequencing reads and the utility of RNA analysis to detect variant types which may not be identified by routine genetic screening techniques.
dc.format	Print-Electronic
dc.language	eng
dc.publisher	Wiley
dc.relation.ispartof	Am J Med Genet A
dc.relation.isbasedon	10.1002/ajmg.a.63788
dc.rights	info:eu-repo/semantics/openAccess
dc.subject	0604 Genetics, 1103 Clinical Sciences
dc.subject.classification	3105 Genetics
dc.subject.classification	3202 Clinical sciences
dc.subject.mesh	Humans
dc.subject.mesh	Basal Cell Nevus Syndrome
dc.subject.mesh	Patched-1 Receptor
dc.subject.mesh	Male
dc.subject.mesh	Germ-Line Mutation
dc.subject.mesh	Infant
dc.subject.mesh	Exome
dc.subject.mesh	Exome Sequencing
dc.subject.mesh	Sequence Analysis, RNA
dc.subject.mesh	Phenotype
dc.subject.mesh	Genetic Predisposition to Disease
dc.subject.mesh	Humans
dc.subject.mesh	Basal Cell Nevus Syndrome
dc.subject.mesh	Genetic Predisposition to Disease
dc.subject.mesh	Sequence Analysis, RNA
dc.subject.mesh	Phenotype
dc.subject.mesh	Germ-Line Mutation
dc.subject.mesh	Infant
dc.subject.mesh	Male
dc.subject.mesh	Exome
dc.subject.mesh	Patched-1 Receptor
dc.subject.mesh	Exome Sequencing
dc.subject.mesh	Humans
dc.subject.mesh	Basal Cell Nevus Syndrome
dc.subject.mesh	Patched-1 Receptor
dc.subject.mesh	Male
dc.subject.mesh	Germ-Line Mutation
dc.subject.mesh	Infant
dc.subject.mesh	Exome
dc.subject.mesh	Exome Sequencing
dc.subject.mesh	Sequence Analysis, RNA
dc.subject.mesh	Phenotype
dc.subject.mesh	Genetic Predisposition to Disease
dc.title	Germline PTCH1: c.361_362insAlu alteration identified by comprehensive exome and RNA sequencing in a patient with Gorlin syndrome.
dc.type	Journal Article
utslib.citation.volume	194
utslib.location.activity	United States
utslib.for	0604 Genetics
utslib.for	1103 Clinical Sciences
pubs.organisational-group	University of Technology Sydney
pubs.organisational-group	University of Technology Sydney/Faculty of Health
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	2025-05-05T22:52:24Z
pubs.issue	10
pubs.publication-status	Published
pubs.volume	194
utslib.citation.issue	10

Abstract:

Gorlin syndrome can be caused by pathogenic/likely pathogenic (P/LP) variants in the tumor suppressor gene PTCH1 (9q22.1-q31), which encodes the receptor for the sonic hedgehog (SHH) ligand. We present a 12-month-old boy clinically diagnosed with Gorlin syndrome who was found to have significantly delayed development, palmar pitting, palmar and plantar keratosis, short hands, frontal bossing, coarse face, hypertelorism, a bifid rib, misaligned and missing teeth, and SHH-activated medulloblastoma. Genetic testing, including a pediatric cancer panel and genome sequencing with peripheral blood, failed to identify any P/LP variants in PTCH1. Paired tumor/normal exome sequencing was performed, which identified a germline NM_000264.5 (PTCH1): c.361_362ins? alteration through manual review of sequencing reads. Clinical RNA sequencing further demonstrated an Alu insertion at this region (PTCH1: c.361_362insAlu), providing molecular confirmation of Gorlin syndrome. This finding exemplifies a unique mechanism for PTCH1 disruption in the germline and highlights the importance of comprehensive analysis, including manual review of DNA sequencing reads and the utility of RNA analysis to detect variant types which may not be identified by routine genetic screening techniques.

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http://hdl.handle.net/10453/187192