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Multicenter Study
. 2022 Jan;42(1):118-135.
doi: 10.1002/pd.6074. Epub 2021 Dec 11.

Terminal 6q deletions cause brain malformations, a phenotype mimicking heterozygous DLL1 pathogenic variants: A multicenter retrospective case series

Marion Lesieur-Sebellin  1   2 Marianne Till  3 Philippe Khau Van Kien  4 Bérénice Herve  5   6 Nicolas Bourgon  7 Céline Dupont  8 Anne-Claude Tabet  8   9 Mathilde Barrois  10 Aurélie Coussement  11 Laurence Loeuillet  1 Eve Mousty  12 Vuthy Ea  4 Amal El Assal  13 Laura Mary  14   15 Sylvie Jaillard  15   16 Claire Beneteau  17   18 Claudine Le Vaillant  19 Charles Coutton  20   21 Françoise Devillard  20 Carole Goumy  22 Amélie Delabaere  23 Sylvia Redon  24 Yves Laurent  25 Audrey Lamouroux  26   27 Jérôme Massardier  28 Catherine Turleau  1 Damien Sanlaville  3 Vincent Cantagrel  29   30 Pascale Sonigo  31 François Vialard  5   6 Laurent J Salomon  7   30 Valérie Malan  1   29   30
Affiliations
Multicenter Study

Terminal 6q deletions cause brain malformations, a phenotype mimicking heterozygous DLL1 pathogenic variants: A multicenter retrospective case series

Marion Lesieur-Sebellin et al. Prenat Diagn. 2022 Jan.

Abstract

Objective: Terminal 6q deletion is a rare genetic condition associated with a neurodevelopmental disorder characterized by intellectual disability and structural brain anomalies. Interestingly, a similar phenotype is observed in patients harboring pathogenic variants in the DLL1 gene. Our study aimed to further characterize the prenatal phenotype of this syndrome as well as to attempt to establish phenotype-genotype correlations.

Method: We collected ultrasound findings from 22 fetuses diagnosed with a pure 6qter deletion. We reviewed the literature and compared our 22 cases with 14 fetuses previously reported as well as with patients with heterozygous DLL1 pathogenic variants.

Results: Brain structural alterations were observed in all fetuses. The most common findings (>70%) were cerebellar hypoplasia, ventriculomegaly, and corpus callosum abnormalities. Gyration abnormalities were observed in 46% of cases. Occasional findings included cerebral heterotopia, aqueductal stenosis, vertebral malformations, dysmorphic features, and kidney abnormalities.

Conclusion: This is the first series of fetuses diagnosed with pure terminal 6q deletion. Based on our findings, we emphasize the prenatal sonographic anomalies, which may suggest the syndrome. Furthermore, this study highlights the importance of chromosomal microarray analysis to search for submicroscopic deletions of the 6q27 region involving the DLL1 gene in fetuses with these malformations.

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References

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