- Comprehensive characterisation of TRND in 76 patients with mono-allelic predicted loss-of-function TCF7L2 variants, defining core features including speech delay and autism.
- Phenotype: speech delay (95.3%), autism (62.1%), craniofacial dysmorphism (73.3%), ophthalmologic conditions (65.5%), orthopaedic abnormalities (52.6%).
- No genotype-phenotype clustering by variant type or genomic locus; adult biobank data show nominal association with type 2 diabetes with renal manifestations, OR 5.8, p=0.03.
Genet Med. 2026 Jul 7:102642. doi: 10.1016/j.gim.2026.102642. Online ahead of print.
ABSTRACT
PURPOSE: TCF7L2 (OMIM:602228; HGNC:11641) is a transcription factor and critical effector of the Wnt/β-Catenin pathway. In 2021, 11 pediatric patients with mono-allelic predicted loss-of-function (pLOF) TCF7L2 variants and syndromic features were observed. Characterization of patients with pLOF TCF7L2 variants and neurodevelopmental features – herein referred to as TCF7L2-related neurodevelopmental disorder (TRND) – is urgently needed.
METHODS: We leveraged multiple methods (GeneMatcher, DECIPHER, literature review, public/private repositories) to identify an international cohort of 76 patients with pLOF TCF7L2 variants and neurodevelopmental features and phenotypically characterized them. We also retrospectively searched for an independent cohort of adults with pLOF TCF7L2 variants (n = 11) from 60,000+ PennMedicine BioBank (PMBB) patients.
RESULTS: Among 76 patients with pLOF TCF7L2 variants, speech delay (95.3%), craniofacial dysmorphisms (73.3%), ophthalmologic conditions (65.5%), autism (62.1%), and orthopedic abnormalities (52.6%) were most commonly observed. Phenotypic differences did not cluster by variant type or genomic locus. Among PMBB patients, an association of nominal significance with type 2 diabetes with renal manifestations (OR = 5.8; p-value = 0.03) was detected, warranting further investigation.
CONCLUSIONS: This represents the most comprehensive characterization to date of TRND, a novel neurodevelopmental disorder, defining its genotypic and phenotypic spectrum. We opened a Simons Searchlight natural history study (https://www.simonssearchlight.org/research/what-we-study/tcf7l2/) to enhance understanding of this condition.
PMID:42417140 | DOI:10.1016/j.gim.2026.102642
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