To the Editor:
In 1995, Hennekam and Cohen described a patient with an unknown syndrome of which they suspected a disturbed programmed cell death to be the cause [1]. This male had complete cutaneous syndactyly of the hands and feet, underdeveloped lacrimal ducts, narrow external ear canals, pharyngeal mucous membrane fold, unilateral cryptorchidism, bilateral cord-like vasa deferentia without a lumen and small epididymis.
Twenty-seven years later, we had the opportunity to re-study the patient and were able to detect the molecular background in this patient. The clinical phenotype was compatible with an unusual form of Fraser syndrome, so we screened through next generation sequencing the four known Fraser syndrome genes (FRAS1, FREM1, FREM2, GRIP1) and identified two compound heterozygous FRAS1 variants (NM_025074.6:c.8353del p.(Val2785Trpfs*33) (pathogenic) and c.1724G > A p.(Cys575Tyr) (likely pathogenic)). The original authors had already mentioned that the clinical features were reminiscent of Fraser syndrome, but at that time the patient did not fulfill the clinical criteria. However, the phenotype was now found to fulfill the present diagnostic criteria [2]. The molecular confirmation aided the patient to understand his phenotype and allowed his family-members to make informed decisions regarding reproduction.
The hypothesis suggested by Hennekam and Cohen that a disturbed programmed cell death could be the underlying pathology, was well estimated. The Fraser complex including FRAS1 is composed of extracellular matrix proteins, which are critical for the regulation of epidermal basement membrane adhesion and epidermal blistering [3]. It has been suggested that a loss of function of the Fraser complex thereby leads to disturbed programmed cell death and initiation of the kidney [4, 5], which likely explains most of the characteristics of our patient. To our knowledge, atresia of the vas deferens and a small epididymis have not previously been described in males with Fraser syndrome. Analyses of CFTR did not show any abnormalities and made Cystic fibrosis as an alternative cause unlikely. It is plausible that atresia of the vas deferens and the small epididymis can be part of the Fraser phenotype, since programmed cell death and blistering are involved in the fusion of the cloaca and mesonephric duct, from which the vas deferens and epididymis are formed during embryogenesis [5]. We suggest that examination of reproductive structures should be part of the clinical work up when establishing a diagnosis of Fraser syndrome, and it may be useful to evaluate individuals with (presumed) isolated vas deference atresia for variants in one of the genes known to cause Fraser syndrome.
Data availability
The datasets generated and/or analyzed during the current study are available from the corresponding author on reasonable request.
References
Hennekam RC, Cohen MM. Hypothesis: patient with possible disturbance in programmed cell death. Eur J Hum Genet. 1995;3:374–7.
van Haelst MM, Scambler PJ, Fraser Syndrome Collaboration Group, Hennekam RC. Fraser syndrome: a clinical study of 59 cases and evaluation of diagnostic criteria. Am J Med Genet A. 2007;143A:3194–203.
McGregor L, Makela V, Darling SM, Vrontou S, Chalepakis G, Roberts C, et al. Fraser syndrome and mouse blebbed phenotype caused by mutations in FRAS1/Fras1 encoding a putative extracellular matrix protein. Nat Genet. 2003;34:203–8.
Hines EA, Verheyden JM, Lashua AJ, Larson SC, Branchfield K, Domyan ET, et al. Syndactyly in a novel FRAS1rdf mutant results from interruption of signals for interdigital apoptosis. Dev Dyn. 2016;245:497–507.
Hoshi M, Reginensi A, Joens MS, Fitzpatrick JAJ, McNeill H, Jain S. Reciprocal spatiotemporally controlled apoptosis regulates Wolffian duct cloaca fusion. J Am Soc Nephrol. 2018;29:775–83.
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The authors would like to thank the patient for his kind cooperation.
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All authors were involved in the clinical care of the patients. LR drafted the paper and all authors critically revised and approved the final version of the paper.
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Rumping, L., Hennekam, R.C.M., Alders, M. et al. “Hypothesis: Patient with possible disturbance in programmed cell death”: further insights in pathogenicity and clinical features of Fraser syndrome. Eur J Hum Genet 31, 16–17 (2023). https://doi.org/10.1038/s41431-022-01175-x
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DOI: https://doi.org/10.1038/s41431-022-01175-x
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