Abstract
Pathogenic germline DICER1 variants are associated with pleuropulmonary blastoma, multinodular goiter, embryonal rhabdomyosarcoma and other tumour types, while mosaic missense DICER1 variants in the RNase IIIb domain are linked to cause GLOW (global developmental delay, lung cysts, overgrowth, and Wilms' tumor) syndrome. Here, we report four families with germline DICER1 pathogenic variants in which one member in each family had a more complex phenotype, including skeletal findings, facial dysmorphism and developmental abnormalities. The developmental features occur with a variable expressivity and incomplete penetrance as also described for the neoplastic and dysplastic lesions associated with DICER1 variants. Whole exome sequencing (WES) was performed on all four cases and revealed no further pathogenic or likely pathogenic dominant, homozygous or compound heterozygous variants in three of them. Notably, a frameshift variant in ARID1B was detected in one patient explaining part of her phenotype. This series of patients shows that pathogenic DICER1 variants may be associated with a broader phenotypic spectrum than initially assumed, including predisposition to different tumours, skeletal findings, dysmorphism and developmental abnormalities, but genetic work up in syndromic patients should be comprehensive in order not to miss additional underlying /modifying causes.
Highlights
DICER1 is a member of ribonuclease III (RNaseIII) family and responsible for microRNA processing
Germline pathogenic variants in DICER1 cause a tumour predisposition syndrome (OMIM 601200), which is characterized by occurrence of pleuropulmonary blastoma, Sertoli-Leydig cell tumour, cystic nephroma, multinodular goiter, embryonic rhabdomyosarcoma of the cervix uteri and other tumour types [1]
Mosaic somatic missense DICER1 variants in the RNase IIIb domain are linked to GLOW syndrome, an acronym from the reported core features of global developmental delay, lung cysts, overgrowth, and Wilms’ tumour
Summary
DICER1 is a member of ribonuclease III (RNaseIII) family and responsible for microRNA processing. The patient is 6 years old and shows developmental delay, dystrophy and mild respiratory insufficiency with overall good quality of life Her family history was unremarkable for DICER1-associated tumors or unusual phenotypic features. The oldest son was born with severe Pierre-Robin-sequence (Fig. 1A, B), shortening of the left arm and leg and bilateral hip dysplasia Chest imaging has shown no lung cysts, histoplasmosis was incidentally discovered and successfully treated She remains alive and well 14 years following resection of her ovarian tumour. The fourth individual was born preterm at 33 weeks of gestation to non-consanguineous parents She showed mild dysmorphic facial features such as a bulging underlip, Fig. 1 A, B Front and side view of patient 1 with severe PierreRobin-sequence.
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