ӳ��ý

PMCID

PMC12976905

Gene Portals: A Framework for Integrating Clinical, Functional, and Structural Evidence into Rare Disease Variant Classification.

medRxiv : the preprint server for health sciences

Authors	Tobias Brünger Ilona Krey Suyeon Kim Chiara Klöckner Scott Myers Katrine Johannesen Arthur Stefanski Gary Taylor Eduardo Perez-Palma Marie Macnee Stephanie Schorge Rebekka Dahl Hongjie Yuan Riley Perszyk Sukhan Kim Sunanjay Bajaj Ingo Helbig Jen Pan Mark Farrant Lonnie Wollmuth David Wyllie Erkin Kurganov David Baez Sameer Zuberi Christian Boßelmann Holger Lerche Massimo Mantegazza Sandrine Cestèle Patrick May Alina Ivaniuk Mary Meskis Veronica Hood Leah Schust Kimberly Goodspeed Jing-Qiong Kang Amber Freed Cornelius Gati Ludovica Montanucci Arthur Wuster Marena Trinidad Steven Froelich Alexander Deng Ángel Serrano Artem Borovikov Artem Sharkov Arjan Bouman M Hajianpour Deb Pal Leslie Danvoye Damien Lederer Tugce Balci Eveline Hagebeuk Alexis Heidlebaugh Kathryn Oetjens Trevor Hoffman Pasquale Striano Sarah Williams Kalene van Engelen Katherine Howell Jean Khoury Tim Benke Vincent Strehlow Konrad Platzer Amy Ramsey Lisa Manaster Sunitha Malepati Pangkong Fox Jeffrey Noebels Wendy Chung Annapurna Poduri Laina Stripe Sarah Ruggiero Stacey Cohen Lacey Smith Sylvia Boesch Olivia Wilmarth Anna Prentice Esther Cha Nikita Budnik Marina Hommersom Audra Kramer Carlos Vanoye Guo-Qiang Zhang Michael Nothnagel Aarno Palotie Mark Daly Alfred George Yuri Zarate Andreas Brunklaus Stephen Traynelis Rikke Møller Johannes Lemke Dennis Lal
Abstract	Rare Mendelian disorders affect 300-400 million people globally. Although genetic testing has become widely adopted, gene-specific evidence for tailored variant interpretation remains scattered across resources. We present Gene Portals, a framework for gene-centered multimodal knowledge bases that co-localize expert-harmonized clinical data, functional assays, population variation, structural annotations and gene-specific ACMG/AMP specifications within a single resource. A modular interface integrates this unified evidence with VCEP-refined ACMG specifications to enable automated gene-specific variant classification, infer molecular mechanisms, and support cross-gene analyses. We demonstrate the framework's utility across five Gene portals spanning eleven neurodevelopmental disorder-associated genes, integrating data from 4,423 individuals with 2,838 unique variants, 36,149 ClinVar submissions, and 1,044 expert-curated molecular readouts. By organizing evidence that is otherwise dispersed across multiple sources into a unified, queryable framework, the SCN, GRIN, CACNA1A, SATB2 and SLC6A1 Gene Portals became widely used community resources and provide an extensible template for standardized rare-disease variant interpretation and mechanism-aware discovery.
Year of Publication	2026
Journal	medRxiv : the preprint server for health sciences
Date Published	03/2026
DOI	10.64898/2026.03.05.26347086
PubMed ID	41822692
Links

Recent ӳ��ý Publications

Chromatin accessibility regulates age-dependent nuclear mechanotransduction.

Herpesvirus-encoded lncRNA targets host splicing by interacting with splicing factors.

Population genomics of , the principal South American malaria vector mosquito.

Adaptation of the multiplexed CRISPR-Cas13 CARMEN RVP assay for longitudinal detection of respiratory pathogens from air samples.

Underutilization of syndrome-specific ICD-10 codes for genetic epilepsies: Implications for precision medicine.