True MEN1 or phenocopy? Evidence for geno-phenotypic correlations in MEN1 syndrome

Kövesdi, Annamária; Tóth, Miklós; Butz, Henriett; Szücs, Nikolette; Sármán, Beatrix; Pusztai, Péter; Tőke, Judit; Reismann, Péter; Fáklya, Mónika; Tóth, Géza; Somogyi, Anikó; Borka, Katalin; Erdei, Annamária; Nagy, Endre; Deák, Veronika; Valkusz, Zsuzsanna; Igaz, Péter; Patócs, Attila; Grolmusz, Vince

doi:10.1007/s12020-019-01932-x

Cited by 22 publications

(15 citation statements)

References 33 publications

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“…We conclude that structural analysis provides a useful tool in understanding the impact of missense variants in MEN1, and that integration of proteomic with genomic data could potentially contribute to the classification of novel variants in this disease. collagenomas and meningiomas (11), resulting in a range of clinical symptoms which may overlap with other diseases of different genetic etiology (12)(13)(14). This overlap presents one of the key problems in assessing genetic variants in cases of MEN1.…”

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confidence: 99%

Using structural analysis in silico to assess the impact of missense variants in MEN1

Caswell

Owens

Gunning

et al. 2019

Preprint

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Previous studies have shown that thermodynamic analysis of protein structure in silico can discriminate between groups of benign and pathogenic missense variants. However, although structures exist for many human disease-associated proteins, such analysis remains largely unexploited in clinical laboratories. Here, we analysed the predicted effect of 338 known missense variants on the structure of Menin, the MEN1 gene product. Results provided strong discrimination between pathogenic and benign variants, with a threshold of >4 kcal/mol for the predicted change in stability providing a strong indicator of pathogenicity. Subsequent analysis of 7 novel missense variants identified during clinical testing of MEN1 patients showed that all 7 were predicted to destabilise Menin by >4 kcal/mol. We conclude that structural analysis provides a useful tool in understanding the impact of missense variants in MEN1, and that integration of proteomic with genomic data could potentially contribute to the classification of novel variants in this disease. collagenomas and meningiomas (11), resulting in a range of clinical symptoms which may overlap with other diseases of different genetic etiology (12)(13)(14). This overlap presents one of the key problems in assessing genetic variants in cases of MEN1. While a large number of pathogenic variants in MEN1 have been reported, genetic testing continues to uncover novel missense substitutions which require assessment of their potential pathogenicity. A further confounding issue is the often later onset of disease, with reported age-related penetrance of 10-43% at 20 years and 81-94% by 50 years (10, 15), which may lead to apparent non-segregation of a variant with disease within a family pedigree.

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confidence: 99%

Using structural analysis in silico to assess the impact of missense variants in MEN1

Caswell

Owens

Gunning

et al. 2019

Preprint

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“…In keeping with these indications, the novel missense variant herein reported c.836C>A resulting in the amino acid change p.A279D in heterozygous state, leads to a change from alanine to aspartic acid with potential aggressive behavior. At odds with studies minimizing the clinical impact of missense mutations compared to frameshift or non-sense mutations (20,24), the missense variant described in our index case stands out for its aberrant and aggressive clinical manifestations developing long after the first clinical manifestation of MEN1.…”

Section: Discussionmentioning

confidence: 88%

“…Lack of mutations have been reported in 5-25% of patients with a clinical diagnosis of MEN1, constituting the so-called "phenocopies" (15,22,23). Of note, a recent study on 189 patients with typical MEN1 phenotype described a higher prevalence (74%) of mutation-negative cases than previously reported (24).…”

Section: Introductionmentioning

confidence: 94%

“…However, genetic testing in MEN1 patients meeting the clinical criteria could be negative (23,89). Some studies demonstrated that negative testing for mutations is frequent in clinical MEN1-like presentations including a combination of pituitary and parathyroid tumors (136,137), while GEP NET appeared more frequently and earlier in MEN1-positive probands, and its development under 30 years seems to be a predictor of a positive genetic test (24).…”

Section: Diagnosis and Management Of Men1mentioning

confidence: 99%

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Phenotypes Associated With MEN1 Syndrome: A Focus on Genotype-Phenotype Correlations

et al. 2020

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“…Importantly, though, significant discordance has been recognized between index cases meeting clinical diagnostic criteria and their genetic test results wherein up to 10-30% of index MEN1 cases that meet clinical diagnostic criteria do not have an identifiable germline pathogenic variant in MEN1 (Thakker et al 2012, de Laat et al 2016, Isailovic et al 2019. Furthermore, there have now been several studies published by different groups comparing the phenotypes of gene-positive and gene-negative MEN1 cases, identifying significant differences between these groups (de Laat et al 2016, Pardi et al 2017, Kovesdi et al 2019. Of additional importance, the gene-negative cases often have a weaker or nonexistent family history of MEN1, supporting the idea that these individuals may represent a different entity altogether from highly penetrant MEN1 due to a confirmed germline pathogenic MEN1 variant (Isailovic et al 2019).…”

Section: The Right Approach For Clinical Diagnosesmentioning

confidence: 99%

HEREDITARY ENDOCRINE TUMOURS: CURRENT STATE-OF-THE-ART AND RESEARCH OPPORTUNITIES: Challenges and opportunities in genetic counseling for hereditary endocrine neoplasia syndromes

Brock

Geurts

Galen

et al. 2020

Endocrine-Related Cancer

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The Genetic Counseling Working Group from the 16th International Workshop on Multiple Endocrine Neoplasia (MEN 2019) convened to discuss contemporary challenges and opportunities in the area of genetic counseling for individuals and families affected by hereditary endocrine neoplasia syndromes. As healthcare professionals with multidisciplinary training in human genetics, risk assessment, patient education, psychosocial counseling, and research methodology, genetic counselors bring a unique perspective to working toward addressing these challenges and identifying their subsequent opportunities. This Working Group focused on the following broad areas: (1) genetic counseling resources for endocrine neoplasias, (2) candidate gene discovery, (3) implications of increasingly sensitive and expansive genetic testing technologies for both the germline and the tumors, and (4) situating clinical diagnoses for hereditary endocrine neoplasia syndromes in the context of present-day knowledge.

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True MEN1 or phenocopy? Evidence for geno-phenotypic correlations in MEN1 syndrome

Cited by 22 publications

References 33 publications

Using structural analysis in silico to assess the impact of missense variants in MEN1

Using structural analysis in silico to assess the impact of missense variants in MEN1

Phenotypes Associated With MEN1 Syndrome: A Focus on Genotype-Phenotype Correlations

HEREDITARY ENDOCRINE TUMOURS: CURRENT STATE-OF-THE-ART AND RESEARCH OPPORTUNITIES: Challenges and opportunities in genetic counseling for hereditary endocrine neoplasia syndromes

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