Identifying Sequence Variants of 18 Hereditary Ovarian Cancer-Associated Genes in Chinese Epithelial Ovarian Cancer Patients

Objectives. The causes of ovarian cancer (OC) have been confirmed to be closely related to genetic factors. Identifying sequence variants of hereditary ovarian cancer (HOC) susceptibility genes can increase clinical surveillance, facilitate early detection, and provide personalized treatment for patients. This study is aimed at investigating the variation frequency of HOC susceptibility genes in the Chinese population and providing information for the etiology and genetics of OC. Methods. 118 epithelial OC patients were recruited in this clinical study. Variants of 18-gene panel were detected in blood samples by next-generation sequencing (NGS) technology. Results. Overall, 36.44% (43/118) of patients carried at least one pathogenic variant. Among these, BRCA1 pathogenic variants were detected in 31 (26.27%) patients, and 5 (4.24%) patients carried pathogenic variants of BRCA2. Moreover, 27.12% (32/118) of patients carried variants of unknown significance (VUSs). Importantly, we detected eight variants that were not reported previously. Conclusions. Our study enlarged the spectrum of HOC-associated gene sequence variants in the Chinese population and also proved the necessity of multigene testing in epithelial OC patients. The identification of patients with HOC will allow family members to undergo cascade testing where identification of unaffected carriers can facilitate early detection, risk reduction, or prevention of OC and ultimately improve long-term outcomes.

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Prevalence of pathogenic variants and variants of unknown significance in patients at high risk of breast cancer: A systematic review and meta-analysis of gene-panel data

Critical Reviews in Oncology/Hematology ◽

10.1016/j.critrevonc.2018.09.009 ◽

2018 ◽

Vol 132 ◽

pp. 138-144 ◽

Cited By ~ 8

Author(s):

C. van Marcke ◽

A. Collard ◽

M. Vikkula ◽

F.P. Duhoux

Keyword(s):

Breast Cancer ◽

Systematic Review ◽

High Risk ◽

Panel Data ◽

Meta Analysis ◽

Gene Panel ◽

Variants Of Unknown Significance ◽

Pathogenic Variants ◽

Unknown Significance

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Factors affecting surgical decision-making in carriers of BRCA1/2 pathogenic variants undergoing risk-reducing surgery at a dedicated hereditary ovarian cancer clinic

Menopause ◽

10.1097/gme.0000000000001900 ◽

2021 ◽

Vol Publish Ahead of Print ◽

Author(s):

Michelle R. Jacobson ◽

Melissa Walker ◽

Gabrielle E.V. Ene ◽

Courtney Firestone ◽

Marcus Q. Bernardini ◽

...

Keyword(s):

Ovarian Cancer ◽

Decision Making ◽

Hereditary Ovarian Cancer ◽

Surgical Decision ◽

Factors Affecting ◽

Pathogenic Variants ◽

Risk Reducing ◽

Surgical Decision Making ◽

Cancer Clinic

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Whole‐Exome Sequencing of a Saudi Epilepsy Cohort Reveals Association Signals in Known and Potentially Novel Loci

10.21203/rs.3.rs-915593/v1 ◽

2021 ◽

Author(s):

Amein Kadhem AlAli ◽

Abdulrahman Al-Enazi ◽

Ahmed Ammar ◽

Mahmoud Hajj ◽

Cyril Cyrus ◽

...

Keyword(s):

Exome Sequencing ◽

Whole Exome Sequencing ◽

Rare Variants ◽

High Rate ◽

Variants Of Unknown Significance ◽

Pathogenic Variants ◽

Whole Exome ◽

Novel Variants ◽

Unknown Significance ◽

Rare Genetic Variants

Abstract Background Epilepsy, a serious chronic neurological condition effecting up to 100 million people globally, has clear genetic underpinnings including common and rare variants. In Saudi Arabia the prevalence of epilepsy is high and caused mainly by perinatal and genetic factors. No whole-exome sequencing (WES) studies have been performed to date in Saudi Arabian Epilepsy cohorts. This offers a unique opportunity for the discovery of rare genetic variants impacting this disease as there is a high rate of consanguinity amongst large tribal pedigrees. Results We performed WES on 144 individuals diagnosed with epilepsy, to interrogate known Epilepsy related genes for known and functional novel variants. We also used an American College of Medical Genetics (ACMG) guideline based variant prioritization approach in an attempt to discover putative causative variants. We identified a 32 potentially causative pathogenic variants across 30 different genes in 44/144 (30%) of these Saudi Epilepsy individuals. We also identified 232 variants of unknown significance (VUS) across 101 different genes in 133/144 (92%) subjects. Strong enrichment of variants of likely pathogenicity were observed in previously described epilepsy-associated loci, and a number of putative pathogenic variants in novel loci are also observed. Conclusion Several putative pathogenic variants known to be epilepsy-related loci were identified for the first time in our population, in addition to several potential new loci have been identified which may be prioritized for further investigation.

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Large next-generation sequencing gene panels in genetic heart disease: yield of pathogenic variants and variants of unknown significance

Netherlands Heart Journal ◽

10.1007/s12471-019-1250-5 ◽

2019 ◽

Vol 27 (6) ◽

pp. 304-309 ◽

Cited By ~ 8

Author(s):

F. H. M. van Lint ◽

O. R. F. Mook ◽

M. Alders ◽

H. Bikker ◽

R. H. Lekanne dit Deprez ◽

...

Keyword(s):

Heart Disease ◽

Next Generation Sequencing ◽

Next Generation ◽

Variants Of Unknown Significance ◽

Pathogenic Variants ◽

Unknown Significance ◽

Gene Panels ◽

Genetic Heart Disease ◽

Generation Sequencing

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Sorting Rare ALS Genetic Variants by Targeted Re-Sequencing Panel in Italian Patients: OPTN, VCP, and SQSTM1 Variants Account for 3% of Rare Genetic Forms

Journal of Clinical Medicine ◽

10.3390/jcm9020412 ◽

2020 ◽

Vol 9 (2) ◽

pp. 412 ◽

Cited By ~ 3

Author(s):

Viviana Pensato ◽

Stefania Magri ◽

Eleonora Dalla Bella ◽

Pierpaola Tannorella ◽

Enrica Bersano ◽

...

Keyword(s):

Genetic Variants ◽

Next Generation Sequencing Technology ◽

Variants Of Unknown Significance ◽

Pathogenic Variants ◽

Unknown Significance ◽

Rare Gene ◽

Motor Neuron Loss ◽

Generation Sequencing ◽

Lateral Sclerosis ◽

Diagnostic Investigations

Amyotrophic lateral sclerosis (ALS) is an adult-onset progressive neurodegenerative disease due to motor neuron loss variably associated with frontotemporal dementia (FTD). Next generation sequencing technology revealed an increasing number of rare and novel genetic variants and interpretation of their pathogenicity represents a major challange in the diagnosis of ALS. We selected 213 consecutive patients with sporadic or familial (16%) ALS, tested negative for SOD1, FUS, TARDBP, and C9orf72 mutations. To reveal rare forms of genetic ALS, we performed a comprehensive multi-gene panel screening including 46 genes associated with ALS, hereditary motor neuronopathies, spastic paraplegia, and FTD. Our study allowed the identification of pathogenic or likely pathogenic variants in 4.2% of patients. The genes with the highest percentage of pathogenic variants were OPTN (1%), VCP (1%) SQSTM1(1%), SETX (0.4%), FIG4 (0.4%), and GARS1 (0.4%) genes. We also found 49 novel or rare gene variants of unknown significance in 30 patients (14%), 44 unlikely pathogenic variants (39%), and 48 variants in ALS susceptibility genes. The results of our study suggest the screening of OPTN, VCP, and SQSTM1 genes in routine diagnostic investigations for both sporadic and familial cases, and confirm the importance of diagnosis and couselling for patients and their relative family members.

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Genetic Spectrum of Left Ventricular Non-Compaction in Paediatric Patients

Cardiology ◽

10.1159/000510439 ◽

2020 ◽

Vol 145 (11) ◽

pp. 746-756

Author(s):

Tatiana Vershinina ◽

Yulia Fomicheva ◽

Alexey Muravyev ◽

John Jorholt ◽

Alexandra Kozyreva ◽

...

Keyword(s):

Ion Channel ◽

Age Groups ◽

Left Ventricular ◽

Barth Syndrome ◽

Reduced Ejection Fraction ◽

Variants Of Unknown Significance ◽

Pathogenic Variants ◽

Paediatric Patients ◽

Unknown Significance ◽

Sarcomeric Genes

Introduction: Left ventricular non-compaction (LVNC) represents a genetically heterogeneous cardiomyopathy which occurs in both children and adults. Its genetic spectrum overlaps with other types of cardiomyopathy. However, LVNC phenotypes in different age groups can have distinct genetic aetiologies. The aim of the study was to decipher the genetic spectrum of LVNC presented in childhood. Patient Group and Methods: Twenty patients under the age of 18 years diagnosed with LVNC were enrolled in the study. Target sequencing and whole-exome sequencing were performed using a panel of 108 cardiomyopathy-associated genes. Pathogenic, likely pathogenic, and variants of unknown significance found in genes highly expressed in cardiomyocytes were considered as variants of interest for further analysis. Results: The median age at presentation was 8.0 (0.1–17) years, with 6 patients presenting before 1 year of age. Twelve (60%) patients demonstrated reduced ejection fraction. Right ventricular (RV) dilation was registered in 6 (30%), often in combination with reduced RV contractility (25%). Almost half (45%) of the patients demonstrated biventricular involvement already at disease presentation. For pathogenic and likely pathogenic variants, the positive genotyping rate was 45%, and these variants were found mainly in non-contractile structural sarcomeric genes (ACTN2, MYPN, and TTN) or in metabolic and signal transduction genes (BRAF and TAZ). Likely pathogenic TAZ variants were detected in all 5 patients suspected of having Barth syndrome. No pathogenic or likely pathogenic variants were found in genes encoding for sarcomeric contractile proteins, but variants of unknown significance were detected in 3 out of 20 patients (MYH6, MYH7, and MYLK2). In 4 patients, variants of unknown significance in ion-channel genes were detected. Conclusion: We detected a low burden of contractile sarcomeric variants in LVNC patients presenting below the age of 18 years, with the major number of variants residing in non-contractile structural sarcomeric genes. The identification of the variants in ion-channel and related genes not previously associated with LVNC in paediatric patients requires further examination of their functional role.

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A likelihood‐based approach to assessing frequency of pathogenicity among variants of unknown significance in susceptibility genes

Statistics in Medicine ◽

10.1002/sim.8791 ◽

2020 ◽

Vol 40 (3) ◽

pp. 593-606

Author(s):

Yunqi Yang ◽

Christine Hong ◽

Jane W. Liang ◽

Stephen Gruber ◽

Giovanni Parmigiani ◽

...

Keyword(s):

Susceptibility Genes ◽

Variants Of Unknown Significance ◽

Unknown Significance

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Functional assessment of variants associated with Wolfram syndrome

Human Molecular Genetics ◽

10.1093/hmg/ddz212 ◽

2019 ◽

Vol 28 (22) ◽

pp. 3815-3824

Author(s):

Melissa Riachi ◽

Sebahat Yilmaz ◽

Erdal Kurnaz ◽

Zehra Aycan ◽

Semra Çetinkaya ◽

...

Keyword(s):

Neurodegenerative Disorder ◽

Molecular Genetic ◽

Wolfram Syndrome ◽

Neurological Complications ◽

Variants Of Unknown Significance ◽

Pathogenic Variants ◽

Unknown Significance ◽

Genetic Mechanisms ◽

Allelic Variations

Abstract Wolfram syndrome (WS) is a heterogeneous multisystem neurodegenerative disorder with two allelic variations in addition to a separate subtype known as WS type 2. The wide phenotypic spectrum of WS includes diabetes mellitus and optic atrophy which is often accompanied by diabetes insipidus, deafness, urological and neurological complications in combination or in isolation. To date, the understanding of the genotype-phenotype relationship in this complex syndrome remains poorly understood. In this study, we identified and explored the functionality of rare and novel variants in the two causative WS genes WFS1 and CISD2 by assessing the effects of the mutations on the encoded proteins Wolframin and ERIS, in a cohort of 12 patients with autosomal recessive WS, dominant WS and WS type 2. The identified pathogenic variants included missense changes, frameshift deletions and insertions in WFS1 and an exonic deletion in CISD2 which all altered the respective encoded protein in a manner that did not correlate to the phenome previously described. These observations suggest the lack of genotype-phenotype correlation in this complex syndrome and the need to explore other molecular genetic mechanisms. Additionally, our findings highlight the importance of functionally assessing variants for their pathogenicity to tackle the problem of increasing variants of unknown significance in the public genetic databases.

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Molecular Autopsy of Sudden Cardiac Death in the Genomics Era

Diagnostics ◽

10.3390/diagnostics11081378 ◽

2021 ◽

Vol 11 (8) ◽

pp. 1378

Author(s):

Vincenzo Castiglione ◽

Martina Modena ◽

Alberto Aimo ◽

Enrica Chiti ◽

Nicoletta Botto ◽

...

Keyword(s):

Diagnostic Features ◽

Molecular Autopsy ◽

Variants Of Unknown Significance ◽

Pathogenic Variants ◽

Genome Wide ◽

Unknown Significance ◽

New Challenges ◽

Next Generation Sequencing Ngs ◽

Cascade Genetic Screening ◽

Generation Sequencing

Molecular autopsy is the process of investigating sudden death through genetic analysis. It is particularly useful in cases where traditional autopsy is negative or only shows non-diagnostic features, i.e., in sudden unexplained deaths (SUDs), which are often due to an underlying inherited arrhythmogenic cardiac disease. The final goal of molecular autopsy in SUD cases is to aid medico-legal inquiries and to guide cascade genetic screening of the victim’s relatives. Early attempts of molecular autopsy relied on Sanger sequencing, which, despite being accurate and easy to use, has a low throughput and can only be employed to analyse a small panel of genes. Conversely, the recent adoption of next-generation sequencing (NGS) technologies has allowed exome/genome wide examination, providing an increase in detection of pathogenic variants and the discovery of newer genotype-phenotype associations. NGS has nonetheless brought new challenges to molecular autopsy, especially regarding the clinical interpretation of the large number of variants of unknown significance detected in each individual.

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NOTCH3 Variants and Genotype-Phenotype Features in Chinese CADASIL Patients

Frontiers in Genetics ◽

10.3389/fgene.2021.705284 ◽

2021 ◽

Vol 12 ◽

Author(s):

Yacen Hu ◽

Qiying Sun ◽

Yafang Zhou ◽

Fang Yi ◽

Haiyun Tang ◽

...

Keyword(s):

Clinical Data ◽

Retrospective Studies ◽

Autosomal Dominant ◽

Small Vessel Disease ◽

Coding Region ◽

Variants Of Unknown Significance ◽

Pathogenic Variants ◽

Unknown Significance ◽

Epidermal Growth ◽

Distinctive Phenotype

Cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy (CADASIL) is a cerebral small vessel disease caused by mutations in the NOTCH3 gene. Archetypal disease-causing mutations are cysteine-affecting variants within the 34 epidermal growth factor-like repeat (EGFr) region of the Notch3 extracellular subunit. Cysteine-sparing variants and variants outside the EGFr coding region associated with CADASIL phenotype have been reported. However, the linkage between untypical variants and CADASIL is unclear. In this study, we investigated the spectrum of NOTCH3 variants in a cohort of 38 probands from unrelated families diagnosed as CADASIL. All coding exons of the NOTCH3 gene were analyzed, and clinical data were retrospectively studied. We identified 23 different NOTCH3 variants including 14 cysteine-affecting pathogenic variants, five cysteine-sparing pathogenic variants, two reported cysteine-sparing variants of unknown significance (VUS), and two novel VUS outside EGFr region. In retrospective studies of clinical data, we found that patients carrying cysteine-sparing pathogenic variants showed later symptom onset (51.36 ± 7.06 vs. 44.96 ± 8.82, p = 0.023) and milder temporal lobe involvement (1.50 ± 1.74 vs. 3.11 ± 2.32, p = 0.027) than patients carrying cysteine-affecting pathogenic variants. Our findings suggested that untypical variants comprise a significant part of NOTCH3 variants and may be associated with a distinctive phenotype.

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