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1. Phenotypes of carriers of two mutated alleles in major cancer susceptibility genes.

Author

Laitman, Yael, Niskakoski, Anni, Bernstein-Molho, Rinal, Koskinen, Lotta, Rabina, Daniel, Koskenvuo, Juha, and Friedman, Eitan

Abstract

Purpose: While cancer phenotypes in carriers of a single mutant allele in most major cancer susceptibility genes are well-established, there is a paucity of data on the phenotype of carriers of two pathogenic variants—double heterozygotes (DH) or homozygous carriers. Here, we describe the phenotype of carriers of homozygous and DH pathogenic sequence variants (PSVs) in major cancer susceptibility genes. Methods: Individuals referred for multigene panel testing at Blueprint Genetics laboratory were included. Ethically approved comparison of cancer type and age at diagnosis between DH, homozygous, and single PSV carriers was performed per gene. Results: Of 6,685 eligible participants, 928 (13.9%) were single heterozygous PSV carriers, 6 (0.09%) were homozygous PSV carriers, and 17 (0.25%) were DH PSV carriers. Mean age at diagnosis of any cancer among single PSV age was 46.8 ± 14.9 years and among DH PSV carriers 37.6 ± 13.0 years (P < 0.0001). Notably, age at diagnosis for breast cancer among single BRCA1 PSV carriers (n = 59) was 43.8 ± 8.7 years (p = 0.7606), among single BRCA2 PSV carriers (n = 52)—47.9 ± 13.0 years (p = 0.2274) compared with 42.3 ± 13.0 years among DH PSV carriers (n = 10- 9 of whom were carriers of either BRCA1 or BRCA2). Conclusion: DH for PSV in two cancer susceptibility genes is a rare event, and the mean age at cancer diagnosis is younger in DH PSV carriers compared with single PSV carriers. [ABSTRACT FROM AUTHOR]

Published
2024
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2. A novel BRCA1 splicing variant detected in an early onset triple-negative breast cancer patient additionally carrying a pathogenic variant in ATM: A case report.

Author

Colombo, Mara, Mondini, Patrizia, Minenza, Elisa, Foglia, Claudia, Mosconi, Annamaria, Molica, Carmen, Pistola, Lorenza, Ludovini, Vienna, and Radice, Paolo

Subjects
GENETIC variation, TRIPLE-negative breast cancer, BRCA genes, CANCER patients, CANCER genes
Abstract

The widespread adoption of gene panel testing for cancer predisposition is leading to the identification of an increasing number of individuals with clinically relevant allelic variants in two or more genes. The potential combined effect of these variants on cancer risks is mostly unknown, posing a serious problem for genetic counseling in these individuals and their relatives, in whom the variants may segregate singly or in combination. We report a female patient who developed triple-negative high grade carcinoma in the right breast at the age of 36 years. The patient underwent bilateral mastectomy followed by combined immunotherapy and chemotherapy (IMpassion030 clinical trial). Two years later she developed a skin recurrence on the right anterior chest wall. Despite intensive treatment, the patient died at 40-year-old due to disease progression. Gene panel testing of patient's DNA revealed the presence of a protein truncating variant in ATM [c.1672G>T; p.(Gly558Ter)] and of a not previously reported variant in the BRCA1 exon 22 donor splice site [c.5406 +6T>G], whose clinical significance was unknown. The analysis of patient's RNA revealed the up-regulation of two alternative BRCA1 mRNA isoforms derived from skipping of exon 22 and of exons 22-23. The corresponding predicted protein products, p.(Asp1778GlyfsTer27) and p.(Asp1778_His1822del) are both expected to affect the BRCA1 C Terminus (BRCT) domain. The two variants were observed to co-occur also in the proband's brother who, in addition, was heterozygous for a common variant (c.4837A>G) mapped to BRCA1 exon 16. This allowed to ascertain, by transcript-specific amplification, the lack of functional mRNA isoforms expressed by the c.5406+6T>G allele and provided evidence to classify the BRCA1 variant as pathogenic, according to the guidelines of the Evidence-based Network for the Interpretation of Germline Mutant Alleles (ENIGMA) consortium. To our knowledge, excluding two cases detected following the screening of population specific recurrent variants, only one ATM/BRCA1 double heterozygote has been reported in the literature, being the case here described the one with the youngest age at cancer onset. The systematic collection of cases with pathogenic variants in more than one cancer predisposition gene is needed to verify if they deserve ad hoc counseling and clinical management. [ABSTRACT FROM AUTHOR]

Published
2023
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3. Corrigendum: A novel BRCA1 splicing variant detected in an early onset triple-negative breast cancer patient additionally carrying a pathogenic variant in ATM: a case report

Author

Mara Colombo, Patrizia Mondini, Elisa Minenza, Claudia Foglia, Annamaria Mosconi, Carmen Molica, Lorenza Pistola, Vienna Ludovini, and Paolo Radice

Subjects
BRCA1, ATM, double heterozygote, spliceogenic variant, case report, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Published
2023
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4. Penetrance of CHEK2 and BRCA1 Double Heterozygotes in Breast and/or Ovarian Cancer Patients.

Author

Berga-Švītiņa, Egija, Pirsko, Valdis, Nakazawa-Miklaševiča, Miki, Maksimenko, Jeļena, Gardovskis, Jānis, and Miklaševičs, Edvīns

Subjects
*CHECKPOINT kinase 2, *OVARIAN cancer, *BRCA genes, *BREAST, *CANCER patients, *GENETIC carriers
Abstract

Germline pathogenic BRCA1 variants confer increased risk of breast and/or ovarian cancer. The penetrance of BRCA1 pathogenic variants is variable due to the effects of other genetic factors. The interaction between CHEK2 and BRCA1 proteins is crucial in homology directed DNA repair pathway. The aim of this study was to assess the effect of three pathogenic/likely pathogenic variants of the CHEK2 gene on BRCA1 pathogenic allelic variant penetrance. The analysis included 380 DNA samples of women with confirmed positive BRCA1 status for one of founder variants c.4035del and c.5266dup. The c.444+1G>A and c.470T>C variants of CHEK2 gene were identified by Sanger's sequencing, and the del5395 variant was detected by multiplex PCR. The studied CHEK2 variants were found in 13 double heterozygous cases (c.444+1G>A, n = 1; c.470T>C, n = 11, del5395, n = 1). Although the prevalence of CHEK2 variants in the ovarian cancer group was comparatively high (5.41%), the increase of the ovarian cancer risk was not statistically significant (OR = 1.56; 95% CI: 0.32–9.94; p = 0.73). The association of the age at the onset of cancer with the presence of particular CHEK2 variant was not consistent. [ABSTRACT FROM AUTHOR]

Published
2023
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5. A novel BRCA1 splicing variant detected in an early onset triple-negative breast cancer patient additionally carrying a pathogenic variant in ATM: A case report

Author

Mara Colombo, Patrizia Mondini, Elisa Minenza, Claudia Foglia, Annamaria Mosconi, Carmen Molica, Lorenza Pistola, Vienna Ludovini, and Paolo Radice

Subjects
BRCA1, ATM, double heterozygote, spliceogenic variant, case report, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

The widespread adoption of gene panel testing for cancer predisposition is leading to the identification of an increasing number of individuals with clinically relevant allelic variants in two or more genes. The potential combined effect of these variants on cancer risks is mostly unknown, posing a serious problem for genetic counseling in these individuals and their relatives, in whom the variants may segregate singly or in combination. We report a female patient who developed triple-negative high grade carcinoma in the right breast at the age of 36 years. The patient underwent bilateral mastectomy followed by combined immunotherapy and chemotherapy (IMpassion030 clinical trial). Two years later she developed a skin recurrence on the right anterior chest wall. Despite intensive treatment, the patient died at 40-year-old due to disease progression. Gene panel testing of patient’s DNA revealed the presence of a protein truncating variant in ATM [c.1672G>T; p.(Gly558Ter)] and of a not previously reported variant in the BRCA1 exon 22 donor splice site [c.5406+6T>G], whose clinical significance was unknown. The analysis of patient’s RNA revealed the up-regulation of two alternative BRCA1 mRNA isoforms derived from skipping of exon 22 and of exons 22-23. The corresponding predicted protein products, p.(Asp1778GlyfsTer27) and p.(Asp1778_His1822del) are both expected to affect the BRCA1 C Terminus (BRCT) domain. The two variants were observed to co-occur also in the proband’s brother who, in addition, was heterozygous for a common variant (c.4837A>G) mapped to BRCA1 exon 16. This allowed to ascertain, by transcript-specific amplification, the lack of functional mRNA isoforms expressed by the c.5406+6T>G allele and provided evidence to classify the BRCA1 variant as pathogenic, according to the guidelines of the Evidence-based Network for the Interpretation of Germline Mutant Alleles (ENIGMA) consortium. To our knowledge, excluding two cases detected following the screening of population specific recurrent variants, only one ATM/BRCA1 double heterozygote has been reported in the literature, being the case here described the one with the youngest age at cancer onset. The systematic collection of cases with pathogenic variants in more than one cancer predisposition gene is needed to verify if they deserve ad hoc counseling and clinical management.

Published
2023
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6. The Role of Double Heterozygotes of SLC3A1 and SLC7A9 in the Prevalence of Cystine Stones.

Author

Wu CW, Patel I, Lovrenert K, Eisner B, Meeks N, Chun-Hui Tsai A, Baum M, Berry G, and Schumacher FR

Abstract

Purpose: Cystine stones, an autosomal recessive disorder caused by cystinuria, result from pathogenic variants of SLC3A1 and SLC7A9. Previous publications revealed clinical prevalence is higher than genetically predicted prevalence. Heterozygous carriers in either gene are not stone formers. However, double heterozygotes (DH), individuals with two heterozygous pathogenic variants in both genes, were never evaluated and may explain the gap between clinical and genetic prevalence., Methods: Due to the rarity of the condition, direct clinical observation is impractical. We perform this population study as a surrogate by identifying the observed DH, deriving the theoretical/expected DH, and testing the null hypothesis (NH) that the observed DH frequency is equal or greater than expected. This NH biologically correlates to DH are asymptomatic and without cystine stone., Results: Using the 1000 Genome Database, we identified 0 DH. We derived the theoretical/expected DH with Hardy-Weinberg Equilibrium and Mendel's law of independent assortment, as 4.94x10-s. Population proportion test revealed Z= -0.353, and p= 0.362, the NH cannot be rejected., Conclusion: Statistical testing does not support that DH are symptomatic, i.e. DH of SLC3A1 and SLC7A9 may not present with cystine stone, and other factors responsible for the gap that current genetics knowledge cannot explain., (Copyright © 2024. Published by Elsevier Inc.)

Published
2024
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7. Double heterozygous pathogenic variants in the BRCA1 and BRCA2 genes in a patient with bilateral metachronous breast cancer.

Author

Mampel, Alejandra, Sottile, Mayra L., Denita-Juárez, Silvina P., Vargas, Ana L., and Vargas-Roig, Laura M.

Subjects
*GENETIC variation, *BRCA genes, *BREAST cancer, *BREAST, *DUCTAL carcinoma, *HETEROZYGOSITY
Abstract

Double heterozygosity pathogenic variants in BRCA1 and BRCA2 genes are a very rare finding, particularly in non-Ashkenazi individuals. We described the first case of double heterozygosity variants in a non-Ashkenazi Argentinean woman with metachronous bilateral breast cancer. The proband is a 65-year-old female diagnosed with invasive ductal carcinoma in the left breast at 45 years old and invasive carcinoma in the right breast at 65 years old. She underwent a multi-gene panel testing indicating the presence of two concurrent heterozygous germline deleterious variants NM_007300.4(BRCA1):c.4201C>T (p.Gln1401Ter), and NM_000059.3(BRCA2):c.5146_5149del (p.Tyr1716fs).. The patient's son (40 years-old) was found to have the inherited pathogenic variant in BRCA2 gene. There are few reports of double heterozygosity variants in BRCA1 and BRCA2 genes in Latin America. The two pathogenic variants identified in our patient have not been described together so far. [ABSTRACT FROM AUTHOR]

Published
2022
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8. Lack of phenotypic additive effect of familial defective apolipoprotein B3531 in familial hypercholesterolaemia.

Author

Giammanco, Antonina, Spina, Rossella, Fayer, Francesca, Barbagallo, Carlo M., Noto, Davide, Cefalù, Angelo B., and Averna, Maurizio R.

Subjects
*SEQUENCE analysis, *GENETIC mutation, *FAMILIAL hypercholesterolemia, *GENETIC carriers, *APOLIPOPROTEINS, *PHENOTYPES
Abstract

Familial defective apolipoprotein (apo) B (FDB) and familial hypercholesterolaemia (FH) are the two common genetic conditions that cause hypercholesterolaemia. R3531C mutation of the APOB gene is a rare cause of FDB. Individuals with both FDB and FH are rare. A 51‐year‐old man with hypercholesterolaemia (11.4 mmol/L) and his family were studied. Low‐density lipoprotein (LDL) receptor (LDLR) and APOB genes were analysed by direct sequencing. LDL of four subjects were studied in a fibroblast LDL receptor‐binding displacement assay. We found a mutation of the LDLR gene (p.Y398X) in the proband and in four other family members: the p.R3531C APOB gene mutation was also found in the proband, his father and his children. The proband and his son were thus compound heterozygotes for both FH and FDB. Double heterozygotes did not show higher cholesterol levels compared to carriers of LDLR gene mutation alone. LDL from one of the carriers of the p.R3531C alone exhibited a binding ability, which was similar to a normal subject. This is the first report in Italy of the p.R3531C mutation, and our results show that this mutation has no effect in LDLR p.Y398X/APOB p.R3531C double heterozygotes. [ABSTRACT FROM AUTHOR]

Published
2021
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9. Recurrent moderate‐risk mutations in Finnish breast and ovarian cancer patients.

Author

Nurmi, Anna, Muranen, Taru A., Pelttari, Liisa M., Kiiski, Johanna I., Heikkinen, Tuomas, Lehto, Sini, Kallioniemi, Anne, Schleutker, Johanna, Bützow, Ralf, Blomqvist, Carl, Aittomäki, Kristiina, and Nevanlinna, Heli

Subjects
BRCA genes, OVARIAN cancer, BREAST cancer, CANCER patients, HEREDITARY cancer syndromes
Abstract

Mutations in BRCA1 and BRCA2 genes predispose to breast and ovarian cancer (BC/OC) with a high lifetime risk, whereas mutations in PALB2, CHEK2, ATM, FANCM, RAD51C and RAD51D genes cause a moderately elevated risk. In the Finnish population, recurrent mutations have been identified in all of these genes, the latest being CHEK2 c.319+2T>A and c.444+1G>A. By genotyping 3,156 cases and 2,089 controls, we estimated the frequencies of CHEK2 c.319+2T>A and c.444+1G>A in Finnish BC patients. CHEK2 c.319+2T>A was detected in 0.7% of the patients, and it was associated with a high risk of BC in the unselected patient group (OR = 5.40 [95% CI 1.58–18.45], p = 0.007) and similarly in the familial patient group. CHEK2 c.444+1G>A was identified in 0.1% of all patients. Additionally, we evaluated the combined prevalence of recurrent moderate‐risk gene mutations in 2,487 BC patients, 556 OC patients and 261 BRCA1/2 carriers from 109 families. The overall frequency of the mutations was 13.3% in 1,141 BRCA1/2‐negative familial BC patients, 7.5% in 1,727 unselected BC patients and 7.2% in 556 unselected OC patients. At least one moderate‐risk gene mutation was found in 12.5% of BRCA1 families and 7.1% of BRCA1 index patients, as well as in 17.0% of BRCA2 families and 11.3% of BRCA2 index patients, and the mutations were associated with an additional risk in the BRCA1/2 index patients (OR = 2.63 [1.15–5.48], p = 0.011). These results support gene panel testing of even multiple members of BC families where several mutations may segregate in different individuals. What's new? In the Finnish population, a small number of recurrent mutations account for the majority of deleterious variations in breast and ovarian cancer susceptibility genes. The authors investigated 12 recurrent moderate‐risk mutations in Finnish breast and ovarian cancer patients. These mutations were found with similar frequency in unselected patients and BRCA1/2‐positive familial index patients, twice as often as in population controls. In addition, a novel association was identified between breast cancer risk and CHEK2 variant c.319+2T>A. The findings highlight the relevance of gene panel testing for breast and ovarian cancer risk assessment and its potential use for assessing breast cancer families with members who may carry different mutations. [ABSTRACT FROM AUTHOR]

Published
2019
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12. Exome sequencing reveals blended phenotype of double heterozygous FBN1 and FBN2 variants in a fetus.

Author

Aggarwal, Shagun, Das Bhowmik, Aneek, Tandon, Ashwani, and Dalal, Ashwin

Subjects
*EXOMES, *PHENOTYPES, *PATHOGENIC microorganisms, *GENETIC carriers, *SCOLIOSIS
Abstract

We report a 29 week fetus with arthrogryposis multiplex congenita, multiple joint dislocations, scoliosis and dysmorphism who was detected to be double heterozygote for putatively pathogenic FBN1 (NM_000138.4:c.6004C > T; p.Pro2002Ser) and FBN2 (NM_001999.3:c.2945G > T; p.Cys982Phe) variants on exome sequencing. The de-novo status of these variants is not confirmed as parental genotypes could not be ascertained. A comparison of the post-mortem findings of the fetus with reported phenotypes of Beals and Marfan syndromes indicated overlapping clinical features suggestive of a blended phenotype. [ABSTRACT FROM AUTHOR]

Published
2018
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13. Hb Hornchurch [β43(CD2)Glu→Lys; HBB : c.130G>A] Compromises the Molecular Diagnosis of β-Thalassemia in a Chinese Family.

Author

Zhao, Yuan, Huang, Lv-Yin, Jiang, Fan, Zhou, Jian-Ying, Xie, Xing-Mei, and Li, Dong-Zhi

Subjects
*THALASSEMIA diagnosis, *HEMOGLOBIN polymorphisms, *GLOBIN genes, *GENETIC carriers, *DISEASE prevalence, *CHINESE people, *DISEASES
Abstract

The combination of β-thalassemia (β-thal) and a hemoglobin (Hb) variant is not uncommon in regions with a high prevalence of thalassemia. Although most of the β-globin chain variants will not aggravate the β-thal, some can compromise the accurate molecular diagnosis. In this study, we present a rare case of coinheritance of β-thal and Hb Hornchurch [β43(CD2)Glu→Lys;HBB: c.130G>A], that compromises the molecular diagnosis of homozygous β-thal. [ABSTRACT FROM AUTHOR]

Published
2017
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14. Genetically diagnosed Birt-Hogg-Dubé syndrome and familial cerebral cavernous malformations in the same individual: a case report.

Author

Whitworth, James, Stausbøl-Grøn, Brian, and Skytte, Anne-Bine

Abstract

When faced with an unusual clinical feature in a patient with a Mendelian disorder, the clinician may entertain the possibilities of either the feature representing a novel manifestation of that disorder or the co-existence of a different inherited condition. Here we describe an individual with a submandibular oncocytoma, pulmonary bullae and renal cysts as well as multiple cerebral cavernous malformations and haemangiomas. Genetic investigations revealed constitutional mutations in FLCN, associated with Birt-Hogg-Dubé syndrome (BHD) and CCM2, associated with familial cerebral cavernous malformation. Intracranial vascular pathologies (but not cerebral cavernous malformation) have recently been described in a number of individuals with BHD (Kapoor et al. in Fam Cancer 14:595-597, , 2015) but it is not yet clear whether they represent a genuine part of that conditions' phenotypic spectrum. We suggest that in such instances of potentially novel clinical features, more extensive genetic testing to consider co-existing conditions should be considered where available. The increased use of next generation sequencing applications in diagnostic settings is likely to lead more cases such as this being revealed. [ABSTRACT FROM AUTHOR]

Published
2017
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15. Coinheritance of Hb City of Hope (HBB: c.208G>A) and β-Thalassemia: Compromising the Molecular Diagnosis of the Codons 71/72 (+A) (HBB: c.216_217insA) Mutation by Reverse Dot-Blot Hybridization.

Author

Zhou, Jian-Ying, Jiang, Fan, Li, Jian, Chen, Gui-Lan, and Li, Dong-Zhi

Subjects
*MOLECULAR diagnosis, *GENETIC code, *HEMOGLOBIN polymorphisms, *GLOBIN genes
Abstract

More than 900 abnormal hemoglobin (Hb) β chain variants have now been characterized. The majority are due to point mutations resulting in a single amino acid substitution within the globin gene involved, with nearly twice as many β chain variants identified compared to α chain variants. Although most of these variants are clinically and hematologically silent, they can interact with different thalassemia mutations, which could sometimes render laboratory diagnostics in a routine setting difficult. In this study, we present a case of coinheritance of Hb City of Hope [β69(E13)Gly→Ser; HBB: c.208G>A] and β-thalassemia (β-thal), that compromises the molecular diagnosis of β-thal trait. [ABSTRACT FROM AUTHOR]

Published
2019
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16. Recurrent moderate‐risk mutations in Finnish breast and ovarian cancer patients

Author

Anne Kallioniemi, Johanna Schleutker, Liisa M. Pelttari, Kristiina Aittomäki, Carl Blomqvist, Sini Lehto, Heli Nevanlinna, Ralf Bützow, Tuomas Heikkinen, Anna Nurmi, Taru A. Muranen, Johanna I. Kiiski, Lääketieteen ja terveysteknologian tiedekunta - Faculty of Medicine and Health Technology, Tampere University, Department of Clinical Chemistry, BioMediTech, HUS Gynecology and Obstetrics, Department of Obstetrics and Gynecology, University of Helsinki, Genome-Scale Biology (GSB) Research Program, University Management, Department of Pathology, Department of Oncology, Clinicum, HUS Comprehensive Cancer Center, Research Programs Unit, Kristiina Aittomäki / Principal Investigator, HUSLAB, and Department of Medical and Clinical Genetics

Subjects
Cancer Research, Datasets as Topic, Gene mutation, Gastroenterology, FAMILY-HISTORY, Cohort Studies, 0302 clinical medicine, FANCM, Prevalence, CONFER SUSCEPTIBILITY, Family history, Medical History Taking, skin and connective tissue diseases, Finland, Aged, 80 and over, Ovarian Neoplasms, double heterozygote, RAD51C, moderate-risk gene, Middle Aged, 3. Good health, ovarian cancer, Oncology, 030220 oncology & carcinogenesis, Female, Adult, Heterozygote, medicine.medical_specialty, PALB2, 3122 Cancers, Breast Neoplasms, Risk Assessment, Cancer Genetics and Epigenetics, Young Adult, 03 medical and health sciences, breast cancer, Breast cancer, Genetiikka, kehitysbiologia, fysiologia - Genetics, developmental biology, physiology, Internal medicine, Biomarkers, Tumor, medicine, Humans, Genetic Predisposition to Disease, BRCA2 MUTATIONS, Genetic Testing, CHEK2, Genotyping, Aged, business.industry, 217 Medical engineering, medicine.disease, GENE, PREDISPOSITION, moderate‐risk gene, Case-Control Studies, ATM, Mutation, C.5791C-GREATER-THAN-T, Ovarian cancer, business
Abstract

Mutations in BRCA1 and BRCA2 genes predispose to breast and ovarian cancer (BC/OC) with a high lifetime risk, whereas mutations in PALB2, CHEK2, ATM, FANCM, RAD51C and RAD51D genes cause a moderately elevated risk. In the Finnish population, recurrent mutations have been identified in all of these genes, the latest being CHEK2 c.319+2T>A and c.444+1G>A. By genotyping 3,156 cases and 2,089 controls, we estimated the frequencies of CHEK2 c.319+2T>A and c.444+1G>A in Finnish BC patients. CHEK2 c.319+2T>A was detected in 0.7% of the patients, and it was associated with a high risk of BC in the unselected patient group (OR = 5.40 [95% CI 1.58–18.45], p = 0.007) and similarly in the familial patient group. CHEK2 c.444+1G>A was identified in 0.1% of all patients. Additionally, we evaluated the combined prevalence of recurrent moderate‐risk gene mutations in 2,487 BC patients, 556 OC patients and 261 BRCA1/2 carriers from 109 families. The overall frequency of the mutations was 13.3% in 1,141 BRCA1/2‐negative familial BC patients, 7.5% in 1,727 unselected BC patients and 7.2% in 556 unselected OC patients. At least one moderate‐risk gene mutation was found in 12.5% of BRCA1 families and 7.1% of BRCA1 index patients, as well as in 17.0% of BRCA2 families and 11.3% of BRCA2 index patients, and the mutations were associated with an additional risk in the BRCA1/2 index patients (OR = 2.63 [1.15–5.48], p = 0.011). These results support gene panel testing of even multiple members of BC families where several mutations may segregate in different individuals., What's new? In the Finnish population, a small number of recurrent mutations account for the majority of deleterious variations in breast and ovarian cancer susceptibility genes. The authors investigated 12 recurrent moderate‐risk mutations in Finnish breast and ovarian cancer patients. These mutations were found with similar frequency in unselected patients and BRCA1/2‐positive familial index patients, twice as often as in population controls. In addition, a novel association was identified between breast cancer risk and CHEK2 variant c.319+2T>A. The findings highlight the relevance of gene panel testing for breast and ovarian cancer risk assessment and its potential use for assessing breast cancer families with members who may carry different mutations.

Published
2019

17. Identification of a breast cancer family double heterozygote for RAD51C and BRCA2 gene mutations.

Author

Ahlborn, Lise, Steffensen, Ane, Jønson, Lars, Djursby, Malene, Nielsen, Finn, Gerdes, Anne-Marie, and Hansen, Thomas

Abstract

Next-generation sequencing has entered routine genetic testing of hereditary breast cancer. It has provided the opportunity to screen multiple genes simultaneously, and consequently has identified new complex genotypes. Here we report the first identification of a woman double heterozygote for mutations in the RAD51C and BRCA2 genes. The RAD51C missense mutation p.Arg258His has previously been identified in a homozygous state in a patient with Fanconi anemia. This mutation is known to affect the DNA repair function of the RAD51C protein. The BRCA2 p.Leu3216Leu synonymous mutation has not been described before and mini-gene splicing experiments revealed that the mutation results in skipping of exon 26 containing a part of the DNA-binding domain. We conclude that the woman has two potential disease-causing mutations and that predictive testing of family members should include both the RAD51C and BRCA2 mutation. This study illustrates the advantage of sequencing gene panels using next-generation sequencing in terms of genetic testing. [ABSTRACT FROM AUTHOR]

Published
2015
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18. Double heterozygotes among breast cancer patients analyzed for BRCA1, CHEK2, ATM, NBN/NBS1, and BLM germ-line mutations.

Author

Sokolenko, Anna, Bogdanova, Natalia, Kluzniak, Wojciech, Preobrazhenskaya, Elena, Kuligina, Ekatherina, Iyevleva, Aglaya, Aleksakhina, Svetlana, Mitiushkina, Natalia, Gorodnova, Tatiana, Bessonov, Alexandr, Togo, Alexandr, Lubiński, Jan, Cybulski, Cezary, Jakubowska, Anna, Dörk, Thilo, and Imyanitov, Evgeny

Abstract

17 double heterozygous (DH) breast cancer (BC) patients were identified upon the analysis of 5,391 affected women for recurrent Slavic mutations in BRCA1, CHEK2, NBN/NBS1, ATM, and BLM genes. Double heterozygosity was found for BRCA1 and BLM (4 patients), BRCA1 and CHEK2 (4 patients), CHEK2 and NBS1 (3 patients), BRCA1 and ATM (2 patients), CHEK2 and BLM (2 patients), CHEK2 and ATM (1 patient), and NBS1 and BLM (1 patient). DH BC patients were on average not younger than single mutation carriers and did not have an excess of bilateral BC; an additional non-breast tumor was documented in two BRCA1/BLM DH patients (ovarian cancer and lymphoplasmacytic lymphoma). Loss-of-heterozygosity (LOH) analysis of involved genes was performed in 5 tumors, and revealed a single instance of somatic loss of the wild-type allele (LOH at CHEK2 locus in BRCA1/CHEK2 double heterozygote). Distribution of mutations in patients and controls favors the hypothesis on multiplicative interaction between at least some of the analyzed genes. Other studies on double heterozygosity for BC-predisposing germ-line mutations are reviewed. [ABSTRACT FROM AUTHOR]

Published
2014
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19. Lack of phenotypic additive effect of familial defective apolipoprotein B3531 in familial hypercholesterolaemia

Author

Angelo B. Cefalù, Maurizio Averna, Davide Noto, Carlo M. Barbagallo, Francesca Fayer, Rossella Spina, Antonina Giammanco, Giammanco A., Spina R., Fayer F., Barbagallo C.M., Noto D., Cefalu A.B., and Averna M

Subjects
Proband, Male, medicine.medical_specialty, Apolipoprotein B, 030204 cardiovascular system & hematology, Compound heterozygosity, Hyperlipoproteinemia Type II, 03 medical and health sciences, chemistry.chemical_compound, FDB3531, 0302 clinical medicine, Internal medicine, Internal Medicine, medicine, Humans, 030212 general & internal medicine, Apolipoproteins B, double heterozygote, biology, business.industry, Cholesterol, LDL receptor, nutritional and metabolic diseases, Heterozygote advantage, Middle Aged, Endocrinology, chemistry, Italy, Receptors, LDL, Mutation (genetic algorithm), Mutation, familial hypercholesterolaemia, biology.protein, lipids (amino acids, peptides, and proteins), business, Lipoprotein
Abstract

Familial defective apolipoprotein (apo) B (FDB) and familial hypercholesterolaemia (FH) are the two common genetic conditions that cause hypercholesterolaemia. R3531C mutation of the APOB gene is a rare cause of FDB. Individuals with both FDB and FH are rare. A 51-year-old man with hypercholesterolaemia (11.4 mmol/L) and his family were studied. Low-density lipoprotein (LDL) receptor (LDLR) and APOB genes were analysed by direct sequencing. LDL of four subjects were studied in a fibroblast LDL receptor-binding displacement assay. We found a mutation of the LDLR gene (p.Y398X) in the proband and in four other family members: the p.R3531C APOB gene mutation was also found in the proband, his father and his children. The proband and his son were thus compound heterozygotes for both FH and FDB. Double heterozygotes did not show higher cholesterol levels compared to carriers of LDLR gene mutation alone. LDL from one of the carriers of the p.R3531C alone exhibited a binding ability, which was similar to a normal subject. This is the first report in Italy of the p.R3531C mutation, and our results show that this mutation has no effect in LDLR p.Y398X/APOB p.R3531C double heterozygotes.

Published
2020

20. Exome sequencing reveals blended phenotype of double heterozygous FBN1 and FBN2 variants in a fetus

Author

Ashwani Tandon, Aneek Das Bhowmik, Ashwin Dalal, and Shagun Aggarwal

Subjects
musculoskeletal diseases, 0301 basic medicine, Marfan syndrome, Heterozygote, Contracture, Fibrillin-2, Fibrillin-1, Joint Dislocations, Scoliosis, 030105 genetics & heredity, Biology, Double heterozygote, 03 medical and health sciences, Fetus, Genotype, Genetics, medicine, Humans, Abnormalities, Multiple, Exome, Connective Tissue Diseases, Genetics (clinical), Exome sequencing, Arthrogryposis, Arthrogryposis multiplex congenita, Sequence Analysis, DNA, General Medicine, medicine.disease, Phenotype, Arachnodactyly, 030104 developmental biology
Abstract

We report a 29 week fetus with arthrogryposis multiplex congenita, multiple joint dislocations, scoliosis and dysmorphism who was detected to be double heterozygote for putatively pathogenic FBN1 (NM_000138.4:c.6004C > T; p.Pro2002Ser) and FBN2 (NM_001999.3:c.2945G > T; p.Cys982Phe) variants on exome sequencing. The de-novo status of these variants is not confirmed as parental genotypes could not be ascertained. A comparison of the post-mortem findings of the fetus with reported phenotypes of Beals and Marfan syndromes indicated overlapping clinical features suggestive of a blended phenotype.

Published
2018

21. Coinheritance of Hb City of Hope (HBB: c.208G>A) and β-Thalassemia: Compromising the Molecular Diagnosis of the Codons 71/72 (+A) (HBB: c.216_217insA) Mutation by Reverse Dot-Blot Hybridization

Author

Jian-Ying Zhou, Jian Li, Gui-Lan Chen, Dong-Zhi Li, and Fan Jiang

Subjects
Mutation, Thalassemia, Point mutation, Biochemistry (medical), Clinical Biochemistry, Hematology, Biology, medicine.disease_cause, medicine.disease, Molecular biology, Abnormal hemoglobin, Double heterozygote, medicine, Single amino acid, Globin gene, Genetics (clinical), Reverse dot blot
Abstract

More than 900 abnormal hemoglobin (Hb) β chain variants have now been characterized. The majority are due to point mutations resulting in a single amino acid substitution within the globin gene involved, with nearly twice as many β chain variants identified compared to α chain variants. Although most of these variants are clinically and hematologically silent, they can interact with different thalassemia mutations, which could sometimes render laboratory diagnostics in a routine setting difficult. In this study, we present a case of coinheritance of Hb City of Hope [β69(E13)Gly→Ser; HBB: c.208G>A] and β-thalassemia (β-thal), that compromises the molecular diagnosis of β-thal trait.

Published
2019

22. Identification of a Danish breast/ovarian cancer family double heterozygote for BRCA1 and BRCA2 mutations.

Author

Steffensen, Ane, Jønson, Lars, Ejlertsen, Bent, Gerdes, Anne-Marie, Nielsen, Finn, and Hansen, Thomas

Abstract

Mutations in the two breast cancer susceptibility genes BRCA1 and BRCA2 are associated with increased risk of breast and ovarian cancer. Patients with mutations in both genes are rarely reported and often involve Ashkenazi founder mutations. Here we report the first identification of a Danish breast and ovarian cancer family heterozygote for mutations in the BRCA1 and BRCA2 genes. The BRCA1 nucleotide 5215G > A/c.5096G > A mutation results in the missense mutation Arg1699Gln, while the BRCA2 nucleotide 859 + 4A > G/c.631 + 4A > G is novel. Exon trapping experiments and reverse transcriptase (RT)–PCR analysis revealed that the BRCA2 mutation results in skipping of exon 7, thereby introducing a frameshift and a premature stop codon. We therefore classify the mutation as disease causing. Since the BRCA1 Arg1699Gln mutation is also suggested to be disease-causing, we consider this family double heterozygote for BRCA1 and BRCA2 mutations. [ABSTRACT FROM AUTHOR]

Published
2010
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24. Report of a family segregating mutations in both the APC and MSH2 genes: juvenile onset of colorectal cancer in a double heterozygote.

Author

Uhrhammer, N. and Bignon, Y.-J.

Subjects
*COLON cancer, *CANCER patients, *DNA, *GENES, *GENETIC mutation, *UTERUS, *KIDNEYS, *BLADDER
Abstract

Mutations in DNA mismatch repair genes are associated with high risk of digestive malignancies [hereditary non-polyposis colorectal cancer (HNPCC); Lynch syndrome]; mutations of APC and MYH are associated with classic and attenuated familial adenomatous polyposis (FAP). Although the early onset of tumors in both syndromes is characteristic of their genetic origin, pediatric malignancies remain rare. Certain reports have found familial colorectal cancer (CRC) occurring in very young patients associated with mutations in more than one gene. A family corresponding to the Amsterdam criteria for HNPCC, including two cases of colorectal cancer before the age of 25 years, was analyzed for mutations in the MSH2 genes by sequencing. Because polyposis was observed in a patient who developed CRC at age 16, the APC gene was also sequenced. A truncating mutation in the MSH2 gene, c.258_259delTG, was carried by patients developing cancer of the colon (two patients), uterus, kidney, bladder, and/or small intestine at ages 16, 24, 43, 44, 45, and 57, respectively. A patient with CRC at age 16 was found to carry the APC c.3183_3187del5 mutation as well as the MSH2 mutation, and it is inferred that her father, deceased of CRC at age 24, was also a double heterozygote. These results confirm that vigilance is required when interpreting molecular results for families with very young patients, as more than one gene may contribute to the genetic risk. Cancer screening measures must also be adapted to the earlier and more penetrant risk to double heterozygotes. [ABSTRACT FROM AUTHOR]

Published
2008
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25. Severe factor VII deficiency with recurrent intracranial haemorrhages owing to double heterozygosity for a splice site mutation of an IVS4 and a novel nonsense mutation in exon 8 (Gln211→Term).

Author

Takamiya, Osamu and Okimoto, Yuri

Subjects
*HEMORRHAGIC diseases in children, *GENETIC mutation, *NONSENSE mutation, *EXONS (Genetics)
Abstract

Genetic analysis of a 10-month-old Japanese baby boy with recurrent intrathoracic bleeding, cerebral haemorrhages and gastrointestinal bleeding secondary to severe factor VII (FVII) deficiency revealed evidence of two distinct mutations of FVII: a splice site mutation of G→A at nucleotide 6071 in the IVS4 splice site and a novel nonsense mutation (Gln211→Term) in exon 8. His bleeding was difficult to control without prophylactic infusion of FVII. We detected a heterozygous splice site mutation of the IVS4 in his mother and a heterozygous nonsense mutation in exon 8 (Gln211→Term) in his father. The parents' FVII levels are both 50% of normal controls. The FVII:C in plasma from the proband was < 1·5% of normal controls. FVII:antigen (Ag) was < 1% of normal controls, using a monoclonal antibody (mAb) hVII-B101/1 that specifically reacts with FVII epidermal growth factor 1 (EGF-1), and 5% of normal controls, using a rabbit polyclonal antibody against human FVII. After immunoadsorption with mAb hVII-B101/B1–Sepharose 4B, FVII levels of both the proband and his mother were 5% of normal controls; after immunoadsorption the FVII levels of normal subjects were < 1%. We hypothesize that secretion of a small amount of dysfunctional FVII lacking EGF-1 into the circulation accounts for this observation. [ABSTRACT FROM AUTHOR]

Published
2001
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26. Band 3 Cape Town (E90K) causes severe hereditary spherocytosis in combination with band 3 Prague III.

Author

Bracher, Natalie A., Lyons, Cheryl A., Wessels, Glynn, Mansvelt, Erna, and Coetzer, Thérèsa L.

Subjects
*HEMOLYTIC anemia, *GENETIC disorders, *ERYTHROCYTE disorders, *GENETIC mutation, *DNA damage
Abstract

Hereditary spherocytosis (HS) is an inherited haemolytic anaemia, characterized by spheroidal, osmotically fragile red blood cells. This disorder exhibits heterogeneity in terms of both clinical severity and underlying molecular defect. We have studied a South African Cape Coloured individual with severe HS owing to a band 3 deficiency caused by two mutations, occurring in trans, in the band 3 gene: a novel variant that we have designated band 3 Cape Town and a previously described mutation, band 3 Prague III. Analysis of erythrocyte membrane proteins indicated a deficiency of both band 3 and protein 4·2, as well as a decreased functional capacity of band 3 to transport anions. Band 3 Cape Town is defined by a GAG→AAG point mutation at codon 90, substituting a glutamic acid with a lysine in the cytoplasmic domain of the molecule, while band 3 Prague III is a codon 870 CGG→TGG point mutation, replacing an arginine with a tryptophan in the transmembrane region of band 3. mRNA is transcribed from both mutant alleles, implying that mutant proteins are synthesized, but are either degraded prior to membrane incorporation or insertion is impaired. We conclude that the combination of these two mutations exacerbated the clinical presentation of the proband. [ABSTRACT FROM AUTHOR]

Published
2001
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27. Hb Hornchurch [β43(CD2)Glu→Lys; HBB: c.130GA] Compromises the Molecular Diagnosis of β-Thalassemia in a Chinese Family

Author

Yuan Zhao, Dong-Zhi Li, Jian-Ying Zhou, Fan Jiang, Lv-Yin Huang, and Xing-Mei Xie

Subjects
Male, China, Thalassemia, Hemoglobins, Abnormal, Clinical Biochemistry, Hb Hornchurch, Double heterozygote, 03 medical and health sciences, 0302 clinical medicine, Asian People, Pregnancy, hemic and lymphatic diseases, Rare case, Medicine, Humans, Chinese family, Genetics (clinical), Genetics, business.industry, Biochemistry (medical), Homozygote, beta-Thalassemia, A hemoglobin, Hematology, medicine.disease, 030220 oncology & carcinogenesis, Child, Preschool, Female, business, 030215 immunology
Abstract

The combination of β-thalassemia (β-thal) and a hemoglobin (Hb) variant is not uncommon in regions with a high prevalence of thalassemia. Although most of the β-globin chain variants will not aggravate the β-thal, some can compromise the accurate molecular diagnosis. In this study, we present a rare case of coinheritance of β-thal and Hb Hornchurch [β43(CD2)Glu→Lys; HBB: c.130G>A], that compromises the molecular diagnosis of homozygous β-thal.

Published
2018

28. Профилактика внезапной сердечной смерти у больного с диффузно-генерализованной гипертрофической кардиомиопатией, обусловленной двумя мутациями в генах MYH7 и MyBPC3

Subjects
ГИПЕРТРОФИЧЕСКАЯ КАРДИОМИОПАТИЯ, МУТАЦИИ DE NOVO, HYPERTROPHIC CARDIOMYOPATHY, IMPLANTABLE CARDIOVERTER-DEFIBRILLATOR, ДВОЙНАЯ ГЕТЕРОЗИГОТА, EXPANDED MYOECTOMY, ИМПЛАНТИРУЕМЫЙ КАРДИОВЕРТЕР-ДЕФИБРИЛЛЯТОР, DOUBLE HETEROZYGOTE, RISK ASSESSMENT OF SUDDEN CARDIAC DEATH, MYH7, MYBPC3, ОЦЕНКА РИСКА ВНЕЗАПНОЙ СЕРДЕЧНОЙ СМЕРТИ, РАСШИРЕННАЯ МИОЭКТОМИЯ, MUTATIONS DE NOVO
Abstract

Гипертрофическая кардиомиопатия (ГКМП) это частое наследственное заболевание, характеризующееся выраженной клинической и генетической гетерогенностью. Причины значительной вариабельности клинических проявлений среди членов одной семьи недостаточно изучены. Развитие хирургических методов лечения этого заболевания позволили снизить смертность при ГКМП с 2 до 0,5% в год, в основном за счет профилактики внезапной смерти. Однако подходы к оценке риска ВСС, отбор пациентов для ИКД и сроки вмешательств до сих пор остаются дискуссионными. Особенно тревожен в отношении риска внезапной сердечной смерти и раннего прогрессирования сердечной недостаточности фенотип, отличающийся гипертрофией всей перегородки (а не только ее базальных отделов) с генерализацией процесса на верхушку, переднюю боковую стенку и увеличением числа и объема папиллярных мышц. В настоящей работе приведен анализ истории болезни 15-летнего больного с семейной формой ГКМП, необычно тяжелым диффузно-генерализованным фенотипом и комбинацией 2 гетерозиготных мутаций p.G263R в гене MyBPC3 и p.G741R в гене MYH7. Пациенту была выполнена расширенная миоэктомия с иммобилизацией папиллярных мышц и имплантация ИКД. Считаем, что указанные особенности генотипа и фенотипа в настоящем наблюдении являются абсолютным показанием к проведению миоэктомии в условиях искусственного кровообращения и имплантации ИКД. Такое сочетанное хирургическое вмешательство должно служить залогом предотвращения внезапной сердечной смерти и прогрессирования сердечной недостаточности., Hypertrophic cardiomyopathy (HCM) is a common inherited disease characterized by pronounced clinical and genetic heterogeneity. The causes for the considerable variability in clinical manifestations of the HCM among family members remain unclear. The development of surgical approaches for HCM treatment allowed reducing annual mortality in HCM patients from 2% to 0.5%, mainly due to sudden cardiac death (SCD) prevention. However, SCD risk assessment, the selection of patients for implantable cardioverter-defibrillator (ICD), and the timing of interventions are still debatable. The most threatening HCM phenotype with a high risk of SCD and early progression of heart failure characterized by hypertrophy of the entire septum (and not just its basal parts) with generalization of the process to the apex, anterior lateral wall, and exceed and hypertrophic papillary muscles. Here we discuss a clinical history of 15 year-old patient with a familial form of HCM, unusually severe diffuse generalized phenotype, and a combination of two heterozygous mutations, p.G263R in the MyBPC3 gene and p.G741R in the MYH7 gene. The patient underwent an expanded myectomy with immobilization of the papillary muscles, and ICD implantation. We believe that combination of complex genotype with diffuse generalized cardiac phenotype might be considered as an absolute indication for septal myectomy with cardiopulmonary bypass and ICD implantation. Such a combined surgical intervention should prevent sudden cardiac death and the heart failure progression.

Published
2018
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29. Double red blood cell donors with increased ferritin levels: a descriptive study

Author

André Lebrun, Yves Grégoire, and Gilles Delage

Subjects
biology, business.industry, Iron levels, Immunology, Ferritin levels, Increased ferritin, Physiology, Heterozygote advantage, Hematology, medicine.disease, Ferritin, Double heterozygote, Red blood cell, medicine.anatomical_structure, biology.protein, Immunology and Allergy, Medicine, business, Hemochromatosis
Abstract

BACKGROUND One of the measures proposed to mitigate iron loss in blood donors is monitoring of their ferritin levels. Occasionally, high ferritin levels are found in monitored donors. We report the results of the clinical and laboratory investigation of 80 double red blood cell (DRBC) donors with high ferritin levels. STUDY DESIGN AND METHODS All DRBC donors’ ferritin levels were measured during each visit for a donation. Donors with high ferritin levels who agreed to participate underwent a clinical and laboratory evaluation. RESULTS A total of 165 of 2757 DRBC donors had at least one high ferritin level. Five were already known to suffer from hemochromatosis. A full investigation was available for 80 other donors. A total of 61 of 80 donors had normalized their ferritin level at the time of their laboratory evaluation. Only 16 donors had high serum iron levels, of whom four had increased saturation index. Genetic analysis gave the following results: C282Y homozygous, two; H63D homozygous, six; C282Y/HC3D double heterozygote, six; C282Y heterozygote, six; H63D heterozygote, 19; and no mutations, 39. None of the other laboratory investigations contributed data explaining the high ferritin levels observed. CONCLUSION In most donors with high ferritin levels, the phenomenon was transient, with normal ferritin levels found in follow-up. Less than 10% of these donors had evidence of iron overload. Only eight were homozygous for mutations associated with hemochromatosis. An extensive laboratory investigation by the treating physician should only be recommended in donors with persistently high ferritin levels.

Published
2015

30. Multiple jejunal cancers resulting from combination of germline APC and MLH1 mutations.

Author

Lindor, Noralane, Smyrk, Tom, Buehler, Sheila, Gunawardena, Shanaka, Thomas, Brittany, Limburg, Paul, Kirmani, Salman, and Thibodeau, Stephen

Abstract

Double heterozygotes for mutations in APC and a DNA mismatch repair gene are extremely rare. We report on an individual who had truncating mutations in APC and MLH1 whose clinical presentation initially resembled Familial Adenomatous Polyposis but then emerged as a novel phenotype with multiple jejunal carcinomas. We have reviewed the relevant literature on double heterozygotes and based on what has been reported to date, this phenotype was not anticipated. It may be useful for clinicians to be aware of this observation as clinical screening guidelines are proposed for such individuals. [ABSTRACT FROM AUTHOR]

Published
2012
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31. Genetically diagnosed Birt-Hogg-Dubé syndrome and familial cerebral cavernous malformations in the same individual:a case report

Author

James Whitworth, Anne-Bine Skytte, Brian Stausbøl-Grøn, Whitworth, James [0000-0003-2747-4006], and Apollo - University of Cambridge Repository

Subjects
0301 basic medicine, Pathology, medicine.medical_specialty, Cancer Research, Hemangioma, Cavernous, Central Nervous System, Short Communication, Cerebral cavernous malformations, Birt–Hogg–Dubé syndrome, Birt-Hogg-Dube Syndrome, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, Proto-Oncogene Proteins, medicine, Genetics, Humans, Oncocytoma, Genetics(clinical), Folliculin, Genetics (clinical), Genetic testing, Cerebral cavernous malformation, medicine.diagnostic_test, business.industry, Tumor Suppressor Proteins, Cancer, Middle Aged, medicine.disease, Human genetics, 030104 developmental biology, Oncology, Double heterozygote, FOS: Biological sciences, Mutation, Mendelian inheritance, symbols, Female, business, Carrier Proteins, 030217 neurology & neurosurgery
Abstract

When faced with an unusual clinical feature in a patient with a Mendelian disorder, the clinician may entertain the possibilities of either the feature representing a novel manifestation of that disorder or the co-existence of a different inherited condition. Here we describe an individual with a submandibular oncocytoma, pulmonary bullae and renal cysts as well as multiple cerebral cavernous malformations and haemangiomas. Genetic investigations revealed constitutional mutations in FLCN, associated with Birt-Hogg-Dubé syndrome (BHD) and CCM2, associated with familial cerebral cavernous malformation. Intracranial vascular pathologies (but not cerebral cavernous malformation) have recently been described in a number of individuals with BHD (Kapoor et al. in Fam Cancer 14:595-597, 10.1007/s10689-015-9807-y , 2015) but it is not yet clear whether they represent a genuine part of that conditions' phenotypic spectrum. We suggest that in such instances of potentially novel clinical features, more extensive genetic testing to consider co-existing conditions should be considered where available. The increased use of next generation sequencing applications in diagnostic settings is likely to lead more cases such as this being revealed.

Published
2017

32. Five Hemoglobin Variants in a Double Heterozygote for α- and β-Globin Chain Defects

Author

Kritsada Singha, Supan Fucharoen, and Goonnapa Fucharoen

Subjects
Adult, Erythrocyte Indices, Male, Heterozygote, Double heterozygosity, Hemoglobins, Abnormal, beta-Globins, Biology, Double heterozygote, Hemoglobins, alpha-Globins, alpha-Thalassemia, Protein Interaction Mapping, Humans, Genetic Testing, Globin, Hemoglobin Q Thailand, Chromatography, High Pressure Liquid, Genetics, Electrophoresis, Capillary, Hemoglobin variants, Globin chain, Sequence Analysis, DNA, Hematology, General Medicine, Blood Protein Electrophoresis, Thailand, Hemoglobinopathies, Phenotype, Hemoglobin Tak
Abstract

Genetic interactions of different defective globin chains could render laboratory diagnostics in a routine setting difficult. We report a hitherto undescribed condition of double heterozygosity for hemoglobin (Hb) Q-Thailand with α+-thalassemia and Hb Tak found in 2 adult Thai individuals. Both patients were healthy and had no pertinent past medical history. A complete blood count revealed slight elevations of Hb and HCT values with low MCV and MCH. Interestingly, Hb analysis demonstrated, in addition to Hb A, A2, and F, as many as 5 Hb variants including Hb Tak (αA2βTak2), Q-Thailand (αQT2βA2), QA2 (αQT2δ2), QF (αQT2γ2), and a novel variant, Hb QTak (αQT2βTak2). Hematological findings of these unusual cases were compared with those of pure heterozygotes for Hb Q-Thailand and Hb Tak found in our series. Hb analysis using combined HPLC and capillary electrophoresis did help in the initial recognition and in making presumptive diagnoses, but definite diagnoses of these cases with complex α- and β-hemoglobinopathies could only be obtained after DNA analysis.

Published
2013

34. Linkage

Author

Doolittle, Donald P., Bresler, E., editor, Thomas, G. W., editor, Van Vleck, L. D., editor, and Doolittle, Donald P.

Published
1987
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40. Identification of a Danish breast/ovarian cancer family double heterozygote for BRCA1 and BRCA2 mutations

Author

Ane Y. Steffensen, Lars Jønson, Bent Ejlertsen, Thomas v. O. Hansen, Finn Cilius Nielsen, and Anne-Marie Gerdes

Subjects
Male, Heterozygote, Cancer Research, endocrine system diseases, Denmark, Genes, BRCA2, Molecular Sequence Data, Genes, BRCA1, Mutation, Missense, Breast Neoplasms, Biology, medicine.disease_cause, Article, Breast Neoplasms, Male, Frameshift mutation, Exon, Breast cancer, Exon trapping, Ovarian cancer, Genetics, medicine, Humans, Missense mutation, Genetics(clinical), Family, Genetic Predisposition to Disease, Frameshift Mutation, skin and connective tissue diseases, Genetics (clinical), Ovarian Neoplasms, Mutation, Base Sequence, Reverse Transcriptase Polymerase Chain Reaction, Heterozygote advantage, Middle Aged, BRCA1, medicine.disease, BRCA2, female genital diseases and pregnancy complications, Pedigree, Oncology, Double heterozygote, Cancer research, Female
Abstract

Mutations in the two breast cancer susceptibility genes BRCA1 and BRCA2 are associated with increased risk of breast and ovarian cancer. Patients with mutations in both genes are rarely reported and often involve Ashkenazi founder mutations. Here we report the first identification of a Danish breast and ovarian cancer family heterozygote for mutations in the BRCA1 and BRCA2 genes. The BRCA1 nucleotide 5215G > A/c.5096G > A mutation results in the missense mutation Arg1699Gln, while the BRCA2 nucleotide 859 + 4A > G/c.631 + 4A > G is novel. Exon trapping experiments and reverse transcriptase (RT)–PCR analysis revealed that the BRCA2 mutation results in skipping of exon 7, thereby introducing a frameshift and a premature stop codon. We therefore classify the mutation as disease causing. Since the BRCA1 Arg1699Gln mutation is also suggested to be disease-causing, we consider this family double heterozygote for BRCA1 and BRCA2 mutations.

Published
2010

41. A New Variant of Glucosephosphate Isomerase Deficiency with Mild Haemolytic Anaemia (GPI-MYTHO)

Author

Colette Galand, Pierre Boivin, M. Torres, and J. P. Bourgeaud

Subjects
Male, chemistry.chemical_classification, Anemia, Hemolytic, Silent gene, Erythrocytes, Glucosephosphate isomerase deficiency, Electrophoresis, Starch Gel, Glucose-6-Phosphate Isomerase, Anemia, Hemolytic, Congenital Nonspherocytic, Hematology, New variant, Biology, Molecular biology, Phenotype, Double heterozygote, Isoelectric point, Enzyme, Biochemistry, chemistry, Humans, Female, Isoelectric Focusing, Molecular instability, Child
Abstract

A new case of glucosephosphate isomerase deficiency with mild haemolytic anaemia was observed in a 6-year-old girl. Deficient enzyme was characterized by a profoundly decreased activity in the red cells, a normal electrophoretic phenotype, normal isoelectric point, normal optimum pH, a molecular instability and a clearly decreased Michaelis constant for fructose-6-phosphate. Propositus was double heterozygote for a 'silent gene' inherited from the mother and an abnormal enzyme from the father. Because this abnormal enzyme has undescribed characteristics, it responds to a new variant for which we propose the name GPI-MYTHO.

Published
2009

45. Instrument Comparison for Heterozygote Scanning of Single and Double Heterozygotes: A Correction and Extension of Herrmann et al., Clin Chem 2006;52:494-503

Author

Karl V. Voelkerding, Carl T. Wittwer, L. Kathryn Bromley, Mark G. Herrmann, and Jacob D. Durtschi

Subjects
Double heterozygote, Genetics, Biochemistry (medical), Clinical Biochemistry, Heterozygote advantage, Locus (genetics), Sequence variation, Biology, Molecular biology, Heteroduplex
Abstract

We have discovered that the DNA sample used in our recent paper (1) as a control heterozygote at the sickle cell locus of β-globin (17A→T, also known as HBB c.20A→T by HUGO nomenclature) contained an additional variant. Subsequent sequencing revealed a double heterozygote, HBB c.[9C→T; 20A→T]. The HBB c. 9C→T is a silent variant for the 3rd amino acid, histidine. In view of this additional sequence variation, we reevaluated the heteroduplex scanning capabilities of the instruments, as reported in the original Fig. 3, to ascertain their ability to distinguish melting curves of heteroduplexes caused by single and double heterozygotes from melting curves of homoduplexes. The c. 9C→T is a …

Published
2007

46. Polymorphism of Arylamine-N-acetyltransferase 2 Gene Is Associated with the Risk of Atopic Dermatitis

Author

V. A. Vavilin, S. I. Makarova, G. G. Ivanova, E. M. Dodunova, L. F. Kaznacheeva, and V. V. Lyakhovich

Subjects
Male, Heterozygote, medicine.medical_specialty, Adolescent, Arylamine N-Acetyltransferase, Glycine, Polymerase Chain Reaction, General Biochemistry, Genetics and Molecular Biology, Dermatitis, Atopic, Double heterozygote, Atopy, Sex Factors, Gene Frequency, Risk Factors, medicine, Humans, Genetic Predisposition to Disease, Child, Gene, Alleles, Polymorphism, Genetic, Arylamine N-acetyltransferase, business.industry, Incidence, Infant, DNA, General Medicine, Atopic dermatitis, medicine.disease, Dermatology, body regions, Amino Acid Substitution, Case-Control Studies, Child, Preschool, Female, business
Abstract

A case--control study was conducted to evaluate the relationship between C481T and G590A polymorphisms of arylamine-N-acetyltransferase 2 and predisposition to atopic dermatitis in children. Double heterozygote 481C/T and 590G/A in girls is a factor of resistance to atopic dermatitis, especially in the absence of smoking-related effects.

Published
2005

47. Lemierre's syndrome with double heterozygote status in the methylenetetrahydrofolate reductase gene

Author

Abdollah Karimi, Mostafa Behpour-Oskooee, and Shirin Sayyahfar

Subjects
Male, medicine.medical_specialty, Heterozygote, Double heterozygote, Lemierre's syndrome, Medicine, Humans, Child, Methylenetetrahydrofolate Reductase (NADPH2), biology, business.industry, Maternal and child health, Clindamycin, Ceftriaxone, Anticoagulants, Lemierre Syndrome, Heparin, Low-Molecular-Weight, medicine.disease, Surgery, Anti-Bacterial Agents, Treatment Outcome, Methylenetetrahydrofolate reductase, Pediatrics, Perinatology and Child Health, Immunology, Methylenetetrahydrofolate reductase gene, biology.protein, Drug Therapy, Combination, business, Biomarkers
Abstract

There are some risk factors being more vulnerable to Lemierre's syndrome such as a hypercoagulable state.We report a rare case of Lemierre's syndrome with ethmoid and maxillary sinusitis, bilateral mastoiditis, and sigmoid sinus thrombosis.Genetic study revealed a double heterozygote status in the methylenetetrahydrofolate reductase gene including C677T and A1298C.It is suggested to screen patients with Lemierre's syndrome for a hypercoagulable state to consider anticoagulant therapy.

Published
2012

48. A spurious haemoglobin A(1c) result associated with double heterozygote for haemoglobin Raleigh (β1[NA1]Val → Ala) and α(+)-thalassaemia

Author

Kritsada Singha, Attawut Chaibunruang, Paripat Netnee, Goonnapa Fucharoen, and Supan Fucharoen

Subjects
Adult, Male, Heterozygote, Hemoglobins, Abnormal, Clinical Biochemistry, DNA Mutational Analysis, Molecular Sequence Data, High-performance liquid chromatography, Double heterozygote, Diagnosis, Differential, Capillary electrophoresis, Asian People, alpha-Thalassemia, Polymorphism (computer science), Diabetes mellitus, medicine, Humans, Multiplex, Cation Exchange Resins, Chromatography, High Pressure Liquid, Glycated Hemoglobin, medicine.diagnostic_test, Base Sequence, Haemoglobin A1c, Chemistry, Genetic Variation, General Medicine, medicine.disease, Molecular biology, Immunoassay
Abstract

Background Accurate measurement of haemoglobin A1c (HbA1c) is useful for long-term glycaemic control in patients with diabetes. Many Hb variants can interfere with HbA1c measurement and cause inaccurate results. Methods The subject was a 31-year-old Thai man who was discovered because of an unexpected HbA1c result; other diabetic parameters were within the normal range. Abnormal Hb was investigated using automated high-pressure liquid chromatography (HPLC) and a capillary electrophoresis system. Mutation analysis was done by cDNA sequencing, polymerase chain reaction–restriction fragment length polymorphism (PCR–RFLP) and multiplex allele-specific PCR assays. Results Evaluation of HbA1c by cation-exchange HPLC showed a value of 34.9% (reference interval, 4.0–6.0%), but a value of only 4.0% (reference value, 4.8–5.9%) was found with a turbidimetric immunoassay. Haematological analysis revealed a mild anaemia but other parameters were within the normal range. Hb-HPLC analysis demonstrated an unknown Hb variant (47.0%) separating from HbA (46.7%), but capillary electrophoresis identified no abnormal peaks. Mutation analysis identified the Hb Raleigh ( β1[NA1]Val → Ala [G TG → G CG]) mutation in combination with an α+-thalassaemia, a hitherto undescribed association. The Hb Raleigh mutation could be detected by PCR–RFLP or a multiplex allele-specific PCR assay. Conclusions Hb Raleigh can cause falsely increased HbA1c values on cation-exchange HPLC. Definitive diagnosis of this variant using combined Hb and DNA analyses is therefore essential.

Published
2012

50. Situation de la drepanocytose au Togo

Author

A. K. Messie, Imd Kueviakoe, ad Gbadoe, A. Vovor, jk Assimadi, and A. Y. Segbena

Subjects
Double heterozygote, Gynecology, Pediatrics, medicine.medical_specialty, business.industry, medicine, business, Sickle cell disease, management, Togo
Abstract

Sickle cell disease is the most important hemoglobin abnormalities in our country where this disease is an impotant public health concern. The gene frequency of Hb S is estimated to 16.1%. The frequency of homozygous sickle cell disease is about 1.3% and 2.6% for SC sickle cell disease patients. We estimate that 171.600 people suffering from major sickle cell disease in Togo. Regarding Sickle cell disease the major problems are the lack of national program for the control of the disease; no neonatal screening is available and the lack of sickle cell disease center for the management of the patients. La drepanocytose est l’anomalie hemoglobinique la plus importante dans notre pays ou elle constitue un probleme de sante publique. La frequence du gene de l’HbS est estimee a 16,1 %, celle de la drepanocytose homozygote est de 1,3 % et celle de la forme double heterozygote de 2,6 %. On estime qu’environ 200.000 Togolais ont une forme majeure de drepanocytose. Les differents problemes observes sont lies a l’inexistence d’un programme national de lutte contre la maladie, l’absence de depistage neonatal et le manque de structures specifiques de prise en charge.

Published
2009

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