78 results on '"Prenatal Diagnosis"'
Search Results
2. Prevalence of thalassemia in the Vietnamese population and building a clinical decision support system for prenatal screening for thalassemia.
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Danh Cuong Tran, Anh Linh Dang, Thi Ngoc Lan Hoang, Chi Thanh Nguyen, Thi Minh Phuong Le, Thi Ngoc Mai Dinh, Van Anh Tran, Thi Kim Phuong Doan, and Thi Trang Nguyen
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EXPERT systems , *CLINICAL decision support systems , *PRENATAL diagnosis , *ALPHA-Thalassemia , *GENETIC mutation , *CROSS-sectional method , *GENETIC testing , *PREGNANT women , *ARTIFICIAL intelligence , *SPOUSES , *DISEASE prevalence , *MEDICAL records , *DESCRIPTIVE statistics , *RESEARCH funding , *THALASSEMIA , *STATISTICAL sampling , *POLYMERASE chain reaction , *BETA-Thalassemia - Abstract
The prevalence of thalassemia among the Vietnamese population was studied, and clinical decision support systems (CDSSs) for prenatal screening of thalassemia were created. A cross-sectional study was conducted on pregnant women and their husbands visiting from October 2020 to December 2021. A total of 10,112 medical records of first-time pregnant women and their husbands were collected. CDSS including two different types of systems for prenatal screening for thalassemia (expert system [ES] and four artificial intelligence [AI]-based CDSS) was built. 1,992 cases were used to train and test machine learning (ML) models while 1,555 cases were used for specialized ES evaluation. There were 10 key variables for AI-based CDSS for ML. The four most important features in thalassemia screening were identified. Accuracy of ES and AI-based CDSS was compared. The rate of patients with alpha thalassemia is 10.73% (1,085 patients), the rate of patients with beta-thalassemia is 2.24% (227 patients), and 0.29% (29 patients) of patients carry both alpha-thalassemia and beta-thalassemia gene mutations. ES showed an accuracy of 98.45%. Among AI-based CDSS developed, multilayer perceptron model was the most stable regardless of the training database (accuracy of 98.50% using all features and 97.00% using only the four most important features). AI-based CDSS showed satisfactory results. Further development of such systems is promising with a view to their introduction into clinical practice. [ABSTRACT FROM AUTHOR]
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- 2023
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3. Cord Blood Hematological Parameters of Fetuses Detected Different Thalassemia Genotypes in the Second Trimester of Pregnancy.
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Yenilmez, Ebru Dündar and Tuli, Abdullah
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REFERENCE values , *ALPHA-Thalassemia , *HEMOGLOBINS , *SEQUENCE analysis , *PRENATAL diagnosis , *CROSS-sectional method , *GENETIC testing , *MANN Whitney U Test , *CORD blood , *DESCRIPTIVE statistics , *GENOTYPES , *SECOND trimester of pregnancy , *BLOOD testing , *DATA analysis software , *GENE amplification , *POLYMERASE chain reaction , *DECISION making in clinical medicine , *BETA-Thalassemia , *PREGNANCY - Abstract
Background: Hemoglobinopathies are the most common inherited diseases in humans resulting from impaired globin chain synthesis of hemoglobin. The progression of thalassemia rates is prevented with prenatal screening methods. Aims: To evaluate the hematological parameters of α- and β-thalassemia and normal fetuses aged 17-25 weeks of gestation. Study Design: A cross-sectional study. Methods: Pregnant women who underwent cordocentesis in the second trimester because of the risk of having a baby with thalassemia were included in the study. Hematological indices and molecular DNA methods were analyzed from the cord blood samples of 129 women who were 17-25 weeks into pregnancy. The HPLC method was used for Hb fraction analysis. Amplification refractory mutation system, restriction enzyme analysis, multiplex polymerase chain reaction, and sequencing methods were used for the molecular analysis. Maternal contamination was eliminated by the short tandem repeat method. Results: In total, 112 of the fetuses carry α- and β-thalassemia heterozygous or homozygous (α: 37, β: 58, mixed: 17) and 17 fetuses had a normal genotype for thalassemia. Significant differences in adult hemoglobin (HbA), fetal hemoglobin (HbF), Hb Barts, MCV, MCH, and RDW were detected in three groups compared with the normal group (p < 0.001, except for RBC, Hb, HCT, and MCHC). Differences in HbF, Hb Barts, MCV, MCH, and RDW were observed in the α-thalassemia groups compared with the normal group (p < 0.001). Among the five β-thalassemia subgroups, only HbA and RDW were different from the normal group (p < 0.001). Conclusion: This study could be a good reference for future studies and prenatal diagnostic applications in emphasizing the importance of changes in the blood parameters of fetuses before molecular genotyping. These hematological data give valuable information to clinicians about the fetus to enlighten families in making appropriate decisions during prenatal diagnosis. [ABSTRACT FROM AUTHOR]
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- 2023
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4. Research Progress of Cell-Free Fetal DNA in Non-Invasive Prenatal Diagnosis of Thalassemia.
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Liu, Dewen, Nong, Chen, Lai, Fengming, Tang, Yulian, and Wang, Taizhong
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CELL-free DNA , *PRENATAL diagnosis , *CIRCULATING tumor DNA , *THALASSEMIA , *SINGLE nucleotide polymorphisms , *BETA-Thalassemia - Abstract
Thalassemia is a genetic disease that seriously affects the health of the fetus. At present, invasive prenatal diagnosis is the main method of thalassemia screening, but invasive prenatal diagnosis has the risk of fetal abortion. The discovery of cell-free fetal DNA (cffDNA) in the peripheral blood of pregnant women provides the possibility for non-invasive prenatal diagnosis (NIPD). Rapid and efficient capture of mutational information on cffDNA in maternal plasma can help prevent the birth of children with thalassemia major. Currently, strategies for cffDNA-based NIPD of thalassemia include the detection of paternal mutations in maternal plasma, detection of a proportion of wild and mutant alleles in maternal plasma, linkage disequilibrium single nucleotide polymorphism (SNP) based on pedigree probands, and prediction of fetal genotypes by bioinformatics combined with population information. Therefore, this paper will focus on the above aspects, in order to provide an essential reference to the prevention and treatment of thalassemia. [ABSTRACT FROM AUTHOR]
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- 2023
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5. Evaluation of Factors influencing the birth of Thalassemia in Family Members with Thalassemia Major in Southeast Iran in 2021.
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Majid, Naderi, Sahar, Najafi, Hossein, Ahmadi Mohammad, Fariba, Ramezani Siakhulak, Saeedeh, Yaghoubi, and Younes, Sadeghi Bojd
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BETA-Thalassemia , *THALASSEMIA , *POOR families , *COUPLES counseling , *MARRIAGE - Abstract
Background & Objectives: Beta-thalassemia is one of the complex diseases that causes many social and economic problems for the patient and his family. This study aimed to investigate factors influencing the birth of thalassemia (intermedia or major) in family members with thalassemia major in Sistan and Baluchistan province. Materials & Methods: This descriptive-analytical study was conducted by census sampling on 48 families of thalassemia major patients with at least two children with thalassemia (intermedia or major) in their members. Data were collected through direct interviews and a review of patients' documents. The results were analyzed by SPSS (version 22) and Mann-Whitney U, Independent t-test, Wilcoxon, and Chi-square tests. Results: In this study, statistical evaluations showed that the birth of thalassemia in family members with thalassemia major whose mothers are housewives was 100% and in families that had no premarital counseling was 91.7%. There was a significant relationship between variables related to mothers' awareness of thalassemia, including their place of residence and Sistani and Baluchestani ethnics, and the birth of thalassemia in family members with thalassemia major (in both cases, P-value = 0.05); However, there was no significant relationship between other variables related to mothers' awareness such as age groups and maternal education with the birth of thalassemia in family members with thalassemia major (P-Value = 0.98 and P-Value = 0.22, respectively). Conclusion: Informing and educating before marriage for high-risk families with thalassemia children, as well as financial support for low-income families can inform parents, prevent the birth of thalassemia, and improve the quality of life of these patients. [ABSTRACT FROM AUTHOR]
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- 2023
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6. Noninvasive prenatal testing of beta-thalassemia for common Pakistani mutations: a comparative study using cell-free fetal DNA from maternal plasma and chorionic villus sampling.
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Afzal, Muhammad, Naeem, Muhammad Abdul, Ahmed, Suhaib, Amin, Nayyar, Rahim, Amena, Munawar, Manazza, Ishaq, Mansoor, Rathore, Ali, and Maria, K.
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CHORIONIC villus sampling , *CELL-free DNA , *CIRCULATING tumor DNA , *PRENATAL diagnosis , *BETA-Thalassemia , *SEX determination - Abstract
The discovery of circulating cell-free fetal DNA (cff-DNA) in maternal plasma has inspired the noninvasive prenatal testing (NIPT) approaches for various genetic fetal screening including rhesus D typing, sex determination, aneuploidies, and single-gene disorders. Noninvasive determination of paternally inherited beta-thalassemia mutations in maternal total cell-free DNA (cf-DNA) by using allele-specific amplification refractory mutation system (ARMS) real-time PCR (RT-PCR) in concordance with the conventional invasive method. An observational study was conducted at the Armed Forces Institute of Blood Transfusion in collaboration with the genetics resource center from March 2021 to August 2021. A total number of 26 couples were selected having a history of previously affected children with beta-thalassemia. A routine chorionic villus sampling (CVS) invasive procedure was carried out, and the mutation analysis was done using conventional PCR. To assess NIPT, a total cf-DNA was also extracted from maternal plasma and analyzed using allele-specific ARMS RT-PCR. Based on conventional PCR testing, 13 of 26 couples were found having beta-thalassemia carriers with homozygous mutation, and 13 couples were carriers with heterozygous mutations. Further to assess NIPT, the cf-DNA of 13 pregnant females among the couples with different mutational patterns was analyzed by allele-specific ARMS RT-PCR to detect paternally inherited mutations. In comparison with conventional PCR, 11 cases (84.6%) were matched successfully, while two cases (15.4%) had no concordance with conventional invasive prenatal testing (IPT). NIPT using maternal cf-DNA by allele-specific ARMS RT-PCR can be feasible to screen paternal inherited mutant alleles to rule out pregnant women from invasive procedures where the test would be negative for paternal inheritance. However, a low amount of fetal DNA in maternal plasma is a limiting factor and required further improvement to enrich fetal cf-DNA for complete concordance with conventional IPT. [ABSTRACT FROM AUTHOR]
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- 2022
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7. Noninvasive Prenatal Diagnosis of Beta-Thalassemia Disease by Using Digital PCR Analysis of Cell-Free Fetal DNA in Maternal Plasma.
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Charoenkwan, Pimlak, Traisrisilp, Kuntharee, Sirichotiyakul, Supatra, Phusua, Arunee, Sanguansermsri, Torpong, and Tongsong, Theera
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CELL-free DNA , *NONINVASIVE diagnostic tests , *PRENATAL diagnosis , *DIAGNOSIS , *FETAL diseases - Abstract
Introduction: Prenatal diagnosis of thalassemia disease was usually based on invasive technique. Noninvasive diagnosis using cell-free fetal DNA (cff-DNA) was described with various laboratory techniques. The aim of this study was to identify the performance of dPCR for analyzing cff-DNA in maternal plasma to diagnose fetal beta-thalassemia diseases. Methods: Thirty-five couples at risk of fetal beta-thalassemia disease caused by four common mutations of HBB were enrolled at 12–18 weeks. The dPCR assay was designed to detect and quantify paternally inherited beta-thalassemia allele (PIB) and maternally inherited beta-thalassemia allele (MIB) from cff-DNA in maternal plasma. Results: Of 29 couples with different paternal/maternal mutations, all cases who inherited paternal mutation had detectable PIB-M. The MIB-mutant/wild-type (MIB-M/MIB-N) ratio in the mothers whose fetuses did not inherit maternal mutation was 0.87 ± 0.07 which was significantly lower than that of the mothers whose fetuses inherited maternal mutation, 1.01 ± 0.05. The sensitivity and specificity of MIB-M/MIB-N ratio >0.95 in predicting fetus inheriting maternal mutation were 100 and 92.3%, respectively. In four couples with same paternal/maternal mutation, IB-M/IB-N ratio of >0.95 correctly predicted the presence of an inheritance of at least one beta-thalassemia allele. In two couples with paternal Hb E/beta-thalassemia, the presence of PIB-M and the MIB-M/MIB-N ratio of >0.95 correctly predicted the presence of paternal/maternal mutations, respectively. Conclusions: The method of analyzing cff-DNA in maternal plasma by dPCR is efficient for prenatal diagnosis of beta-thalassemia. [ABSTRACT FROM AUTHOR]
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- 2022
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8. SCREENING FOR B-THALASSEMIA CARRIERS AMONG STUDENTS IN SECONDARY SCHOOL FAQUOS, SHARKIA.
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Hesham, Mervat Abdallah, Ahmed, Adel Sherif, Gaballah, Ahmed Mohamed, and Ahmed, Mohamed Abdel Rahman
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BETA-Thalassemia , *BLOOD transfusion reaction , *VIRUS disease transmission , *HYPOCHROMIC anemia , *PRENATAL diagnosis , *SECONDARY school students - Abstract
Background: Beta-thalassemia represents a major public health problem in Egypt. The carrier rate varies between 5.5% to = 9%.Unfortunately, most patients suffer from complications of blood transfusions, mainly transfusion transmitted viral infections and iron overload. Prevention by carrier detection and prenatal diagnosis is needed in populations with high incidence of the disease, such as Egypt. This study aimed at identifying thalassemia carriers among secondary school children in Faquos city, EL-Sharkia Governorate to be taken in consideration of prevention program of ß-thalassemia and to update carrier rate data in EL-Sharkia Governorate. Methods: This was a prospective cross-sectional study conducted on 350 se condary school students in Faquos, Sharkia Governorate. All subjects were subjected to the following: Complete blood count, Serum ferritin level, Serum iron level, total iron binding capacity(TIBC). Subjects with microcytic anemia were subjected to specific laboratory tests: High Performance Liquid Chromatography(HPLC) which include hemoglobin A2(HbA2). Results: Headache and pallor were the most common findings in all studied subjects. Investigations of all studied subjects (350) revealed that 200 (57.14%) subjects were non anemic, 150 (42.86 %) subjects were anemic. Among anemic group, 45 (12.85%) subjects had normocytic anemia and 105 (30%) subjects had microcytic anemia. Beta-thalassemia carrier rate was 10% among all the studied group. Beta-thalassemia carrier rate was 33.3% among microcytic anemia group. There was significant decrease in the mean value of red blood cells count, hemoglobin, hematocrite, mean corpuscular volume and mean cell hemoglobin in B-thalassaemia carriers compared to non-carriers among microcytic anemia group. There was a significant increase in hemoglobin A2 level in ß-thalassemia carrier group compared to noncarrier group among microcytic anemia group. Conclusion: Carrier rate among secondary school students in Faquos, Sharkia Governorate was 10%.Hemoglobin A2 is the gold standard for B-thalassemia carrier screening. [ABSTRACT FROM AUTHOR]
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- 2022
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9. Early prenatal diagnosis of Hb Lepore Boston‐Washington and β‐thalassemia on fetal celomatic DNA.
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Giambona, Antonino, Leto, Filippo, Cassarà, Filippo, Tartaglia, Viviana, Marchese, Giuseppe, Orlandi, Emanuela, Cigna, Valentina, Picciotto, Francesco, Maggio, Aurelio, and Vinciguerra, Margherita
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HEMOGLOBINS , *PRENATAL diagnosis , *DNA , *GENETIC mutation , *AMNIOCENTESIS , *PREGNANT women , *GESTATIONAL age , *HEALTH outcome assessment , *GENES , *GENOTYPES , *DESCRIPTIVE statistics , *POLYMERASE chain reaction , *BETA-Thalassemia , *EARLY diagnosis - Abstract
Introduction: Analysis of fetal DNA in at risk couples for thalassemia is performed from fetal trophoblast or amniotic fluid cells. Although these procedures are in common use, the main limitation is essentially due to the late gestation week in which diagnosis is performed. The celomic cavity develops around 4 weeks of pregnancy within the extraembryonic mesoderm and contains embryonic erythroid precursor cells as a source of fetal DNA that can be used to perform invasive prenatal diagnosis. Methods: Celomatic fluids were obtained at 8 weeks of gestation in thirteen women with high‐risk pregnancies. Twelve of these couples were at risk for Hb Lepore disease and β‐thalassemia and one couple represented a rare case in which both parents were carriers of Hb Lepore Boston‐Washington. Fetal cells were isolated by micromanipulator and nested polymerase chain reactions were performed. Results: The analysis was successfully performed in all examined cases. Two fetuses were found to have a compound heterozygosity for β‐thalassemia and Hb Lepore Boston‐Washington, three fetuses were found to be carriers of β‐thalassemia, three fetuses of Hb Lepore, five were found without parental mutations. The genotypic analysis, carried out both by amniocentesis and on abortive tissue or after birth, showed concordance with results obtained on fetal celomic DNA. Conclusion: Our results unequivocally show that fetal DNA can be obtained by nucleated fetal cells present in celomatic fluid and demonstrate for the first time that prenatal diagnosis of β‐thalassemia and Hb Lepore may be feasible in an earlier time of pregnancy than other procedures. [ABSTRACT FROM AUTHOR]
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- 2022
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10. Spectrum of Haemoglobinopathies Detected on Antenatal Screening and Diagnostic Work-up in an Urban Healthcare Set-up: A Retrospective Study.
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CHERIAN, SUSAN, SINGH, PARUL, PATIL, SONIYA, BHANDARKAR, PRASHANT, and JADHAV, VAISHALI R.
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SICKLE cell trait , *PRENATAL diagnosis , *SICKLE cell anemia , *BETA-Thalassemia , *GENETIC disorders , *CELLULOSE acetate , *COUPLES therapy - Abstract
Introduction: Haemoglobinopathies are inherited disorders of haemoglobin (Hb) and consist of Thalassemias and many other structurally variant haemoglobins. Out of these, beta-thalassemia major and clinically significant sickle cell disorders are of great public health importance in India. Lack of awareness regarding their prevalence and knowledge about diagnostic methods, has resulted in failure of community control of birth of these otherwise totally preventable genetic disorders in India. Aim: To study the spectrum of haemoglobinopathies in the study population and to assess the effectiveness of the antenatal screening program, in identifying the couples at-risk and providing prenatal intervention. Materials and Methods: This retrospective cohort study was performed at a community healthcare set-up in Mumbai. from August 2021 to October 2021 on medical records of 10,025 patients including women who were part of antenatal screening, patients investigated for anemia and who underwent haemoglobin electrophoresis over 12 years (October 2007 to October 2019). Alkaline Electrophoresis test was performed using the InterlabGenios analyser on cellulose acetate and the findings were interpreted along with haemogram parameters. Finding of various conditions were presented in terms of prevalence rates and mean values of relevant blood count parameters were presented as mean±SD. Results: An abnormal haemoglobin pattern was seen in 544 (5.42%) of the 10,025 cases with age group ranged from 1 year to 84 years. Most common haemoglobinopathies detected were beta (β) thalassemia trait 378 (3.77%) followed by sickle cell trait (0.9%), Hb D trait (0.26%), HbE trait (0.24%) and others. Carriers of haemoglobinopathies were detected in 186(3.74%) of 4968 women, on antenatal screening. A total of 18 couples-at-risk were identified. One child with thalassemia major and another with sickle cell disease were born in this population over 12 years. Conclusion: The b-Thalassemia trait and HbS trait are the commonest haemoglobinopathies detected. Antenatal screening programme and timely intervention is an effective strategy to control clinically significant major hemoglobinopathies. [ABSTRACT FROM AUTHOR]
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- 2022
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11. Professionally responsible management of the ethical and social challenges of antenatal screening and diagnosis of β-thalassemia in a high-risk population.
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Corda, Valentina, Murgia, Federica, Dessolis, Francesca, Murru, Stefania, Chervenak, Frank A., McCullough, Laurence B., and Monni, Giovanni
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NEWBORN screening , *PROFESSIONAL ethics , *PRENATAL diagnosis , *PREIMPLANTATION genetic diagnosis , *SOCIOECONOMIC factors , *AT-risk people , *BETA-Thalassemia - Abstract
Thalassemias are among the most frequent genetic disorders worldwide. They are an important social and economic strain in high-risk populations. The benefit of β-thalassemia screening programs is growing evident but the capacity to diagnose fetal β-thalassemia exceeds the treatment possibilities and even when treatment before birth becomes feasible, difficult decisions about the relative risks will remain. This paper can be of practical and ethically justified aid when counseling women about screening, diagnosis, and treatment of β-thalassemia. It takes in consideration various social challenges, medical issues such as antenatal screening, preimplantation genetic diagnosis, prenatal diagnosis, non-invasive prenatal testing and prenatal therapy. We also describe the Sardinian experience in applying and promoting high-risk population screening and diagnosis programs and future trends in the management of β-thalassemia. [ABSTRACT FROM AUTHOR]
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- 2021
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12. Direct Amplification of Whole Blood and Amniotic Fluid Specimens for Prenatal and Postnatal Diagnosis of Hb E-β 0-Thalassemia Diseases.
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Wichian, Phongsathorn, Yamsri, Supawadee, Sanchaisuriya, Kanokwan, and Fucharoen, Supan
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BLOOD , *GENETIC mutation , *PRENATAL diagnosis , *AMNIOTIC liquid , *SEVERITY of illness index , *PUERPERIUM , *RESEARCH funding , *DESCRIPTIVE statistics , *GENOTYPES , *CARRIER state (Communicable diseases) , *POLYMERASE chain reaction , *COLLECTION & preservation of biological specimens , *BETA-Thalassemia - Abstract
Objective Prenatal and postnatal diagnosis of hemoglobin E-β 0-thalassemia can be made using polymerase chain reaction (PCR) analysis mostly on purified DNA. We have establihed a direct amplification method without DNA extraction on whole blood (WB) and amniotic fluid (AF) specimens to diagnose the disease. Methods Three reactions of WB PCR assays and 7 reactions of AF PCR tests were developed for postnatal and prenatal diagnosis, respectively. Assays were validated against routine tests in a blinded trial. Results The results showed 100% concordance with routine DNA PCR assays. Among 309 β-thalassemia carriers, 191 patients (61.8%) carried common β-thalassemia mutations. Among 448 AF specimens, 116 (25.9%) fetuses were found to be affected, 247 (55.1%) fetuses were carriers, and 85 (19%) fetuses were unaffected. Conclusion We found that WB and AF PCR assays are simple, rapid, and reliable. The developed techniques could be applicable in routine settings. [ABSTRACT FROM AUTHOR]
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- 2021
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13. Presentation of two new mutations in the 3'untranslated region of the β-globin gene and evaluating the molecular spectrum of thalassemia mutations in the Mediterranean region of Turkey.
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Arpaci, Abdullah, Gul, Bahar Unlu, Ozcan, Oguzhan, Ilhan, Gul, El, Cigdem, Dirican, Emre, Elmacioglu, Sibel, and Kaya, Hasan
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MOLECULAR spectra , *THALASSEMIA , *GENETIC mutation , *GENETIC counseling , *GENETIC disorders , *GLUCOSE-6-phosphate dehydrogenase deficiency , *HEMOGLOBINS , *ALPHA-Thalassemia , *GENETIC polymorphisms , *RNA , *RETROSPECTIVE studies , *BETA-Thalassemia - Abstract
Thalassemia is a common genetic disorder. We aimed to present thalassemia mutation data that covers a period of 7 years from the Mediterranean region of Turkey by comparing with hemoglobin indices and to contribute to prenatal diagnosis and genetic counseling studies which should be decided very quickly. In this study, in which a retrospective archive was scanned, the cases were first grouped as α and β thalassemia, and then β thalassemia mutations were examined in a total of 5 groups as UTR-Pro, Codon, IVS, β0, and β+. We have reached the family of the proband that analyzed their Hb indices and genetic mutation. All mutations were statistically compared with Hb indices, HbF, and HbA2. We have identified two new β thalassemia mutations that have the feature of not being defined previously [HBB:C*62 A>G. (3'UTR+1536 A>G) and HBB:C*1 G>A (3'UTR+1475 G>A)]. The most commonly encountered 23 mutations account for 74.7% of all mutations which is unlike the literature. In the β thalassemia group, 73 different mutations were detected. The most common β thalassemia mutation was HBB: c.93-21 G>A (IVS I-110 G>A) with a frequency of 19.72%. A statistically significant difference was found when comparing the mutation groups with Hb indices. We think that it may be useful to evaluate the mutations we have newly identified too together with the Hb indices especially in evaluating the carriers of thalassemia and it will contribute to prenatal diagnosis and genetic counseling studies which should be decided very quickly. [ABSTRACT FROM AUTHOR]
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- 2021
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14. Factors affecting Thai pregnant women's decisions concerning prenatal diagnosis and termination of pregnancy for β‐thalassemia.
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Phaophan, Amprapha, Mongkolchat, Nadda, Chuenwattana, Prakong, and Viboonchart, Sommai
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ABORTION , *CONTENT analysis , *DECISION making , *INTERVIEWING , *RESEARCH methodology , *PREGNANCY & psychology , *PRENATAL diagnosis , *THEMATIC analysis , *BETA-Thalassemia - Abstract
Aim: To investigate the factors influencing decisions concerning prenatal diagnosis (PND) and termination of pregnancy for β‐thalassemia in Thai pregnant women. Methods: A total of 142 Thai Buddhist pregnant women waiting for PND were asked to undertake semi‐structured interviews regarding their reasons for PND and their decisions and reasoning concerning pregnancy if the fetus was found to be affected. The interviews were analyzed using a thematic content approach. Results: Thai pregnant women accepted PND for three reasons: to know whether their pregnancies were affected, to confirm that their pregnancies were unaffected and to terminate if their pregnancies were affected. Three decisions identified among the women were to terminate the pregnancy, to continue the pregnancy and undecided. The interview analysis identified five themes and nine sub‐themes affecting pregnancy‐related decision‐making: (i) quality of life (suffering or no disability); (ii) burden (difficulty or acceptability); (iii) sense of motherhood (the best way for the child or I cannot hurt my child); (iv) significant others (support to terminate, support to continue or support to wait for the test result) and (v) conflict in deciding. Conclusion: An acceptance of PND in Thai pregnant women was not always associated with pregnancy termination. Multiple factors influenced the decision to terminate, but not their religious affiliation. [ABSTRACT FROM AUTHOR]
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- 2021
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15. Noninvasive prenatal diagnosis for pregnancies at risk for β-thalassaemia: a retrospective study.
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Lv, W, Linpeng, S, Li, Z, Liang, D, Jia, Z, Meng, D, Cram, DS, Zhu, H, Teng, Y, Yin, A, Wu, L, and Cram, D S
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PRENATAL diagnosis , *NONINVASIVE diagnostic tests , *INVASIVE diagnosis , *SINGLE molecules , *PREGNANCY tests , *CELL-free DNA , *DIAGNOSIS of fetal diseases , *PILOT projects , *HEMOGLOBINS , *MOLECULAR diagnosis , *RETROSPECTIVE studies , *FETAL diseases , *GENOTYPES , *RESEARCH funding , *BETA-Thalassemia - Abstract
Objective: To evaluate the clinical feasibility of noninvasive prenatal diagnosis (NIPD) for β-thalassaemia using circulating single molecule amplification and re-sequencing technology (cSMART).Design: Through carrier screening, 102 pregnant Chinese couples carrying pathogenic HBB gene variants were recruited to the study. Pregnancies were managed using traditional invasive prenatal diagnosis (IPD). Retrospectively, we evaluated the archived pregnancy plasma DNA by NIPD to evaluate the performance of our cSMART assay for fetal genotyping.Setting: Chinese prenatal diagnostic centres specialising in thalassaemia testing.Population: Chinese carrier couples at high genetic risk for β-thalassaemia.Methods: Fetal cell sampling was performed by amniocentesis and HBB genotypes were determined by reverse dot blot. NIPD was performed by a newly designed HBB cSMART assay and fetal genotypes were called by measuring the allelic ratios in the maternal cell-free DNA.Main Outcome Measures: Concordance of HBB fetal genotyping between IPD and NIPD and the sensitivity and specificity of NIPD.Results: Invasive prenatal diagnosis identified 29 affected homozygotes or compound heterozygotes, 54 heterozygotes and 19 normal homozygotes. Compared with IPD results, 99 of 102 fetuses (97%) were correctly genotyped by our NIPD assay. Two of three discordant samples were false positives and the other sample involved an incorrect call of a heterozygote carrier as a homozygote normal. Overall, the sensitivity and specificity of our NIPD assay was 100% (95% CI 88.06-100.00%) and 97.26% (95% CI 90.45-99.67%), respectively.Conclusions: This study demonstrates that our cSMART-based NIPD assay for β-thalassaemia has potential clinical utility as an alternative to IPD for pregnant HBB carrier couples.Tweetable Abstract: A new noninvasive test for pregnancies at risk for β-thalassaemia. [ABSTRACT FROM AUTHOR]- Published
- 2021
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16. AN EXPERIENCE OF CHORIONIC VILLUS SAMPLING IN LADY READING HOSPITAL, PESHAWAR.
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Syed, Wajeeha, Hayat, Nazish, Liaqat, Nazia, and Rafiq, Sonia
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CHORIONIC villus sampling , *UTERINE hemorrhage , *GENETIC disorder diagnosis , *BETA-Thalassemia , *REPRODUCTIVE history , *PRENATAL diagnosis - Abstract
Objective: To determine the outcome of chorionic villus sampling for prenatal diagnosis of inherited diseases. Methodology: This descriptive study was conducted on 70 antenatal ladies having 11 to 14 weeks singleton pregnancy and with history of genetic disorders in family or children. It was carried in the Department of Obstetrics and Gynaecology, Lady Reading Hospital, Peshawar. Chorionic villus sampling (CVS) was performed by Obstetrics and Gynae consultants via transabdominal route under local anaesthesia and ultrasound guidance. Written informed consent was taken from all the participating couples before starting the process. By using SPSS version 23, statistical analysis was done. Results: A total of 70 samplings were done. Miscarriage as a result of the procedure occurred in 1/70 (1.42%), significant pain requiring intramuscular analgesia occurred in 40 (57%) patients and there were no reported cases of infection. Failure to retrieve sample occurred in 4 (5.7%) patients requiring repeat procedure after 10 days. 3 (4.2%) patients reported vaginal bleeding within a week after the procedure. After DNA analysis of the submitted samples, it showed thalassemia major 15 (21.42%), thalassemia minor 30 (42.85%), no mutation 22 (31.42%) and down syndrome 1 (1.42%). Conclusion: Chorionic villus sampling was found to be a safe procedure for prenatal diagnosis of genetic disorders in first trimester. [ABSTRACT FROM AUTHOR]
- Published
- 2020
17. Prevalence of globin gene modifiers encountered in fetuses during antenatal diagnosis of hemoglobinopathies.
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Mehta, Pallavi, Sawant, Pratibha, Gorivale, Manju, Nadkarni, Anita, Colah, Roshan, and Mukherjee, Malay B.
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HEMOGLOBINOPATHY genetics , *ANEUPLOIDY , *GENES , *GENETIC polymorphisms , *GLOBULINS , *GENETIC mutation , *PRENATAL diagnosis , *SICKLE cell anemia , *BETA-Thalassemia - Abstract
Introduction: The hemoglobinopathies are the commonest group of single gene disorders in the Indian subcontinent. Although genetic modifiers are known to have a remarkable effect on phenotypic expression, the effects of the possible co‐inheritance of different modifiers are not taken into account during prenatal diagnosis. The present study was undertaken to look for the frequency of globin gene modifiers like the types of β‐globin gene mutations, α thalassemia, α gene triplication, and the Xmn1 polymorphism in fetuses during antenatal diagnosis of hemoglobinopathies. Materials and methods: A total of 580 fetuses with different diagnoses were screened for the presence of genetic modifiers. Results: Twenty‐two different β‐globin gene mutations were identified of which 3.5% were milder mutations. Among the affected fetuses, 29.6% of the β‐thalassemia major and 52.9% of the sickle cell anemia (SCA) fetuses had one genetic modifier while 3.7% of the β‐thalassemia major and 41.1% of the SCA fetuses had co‐inherited two modifiers. α‐gene triplication was detected in 16 (3.5%) β‐thalassemia/sickle cell heterozygous and normal fetuses of which 5 babies (2 β‐thalassemia heterozygous and 3 normal) could be followed up. Of the 2 β‐thalassemia heterozygous babies, one had a severe clinical presentation. Conclusion: Many fetuses had one or two gene modifiers. However, the impact of these on ameliorating the severity of the disease could not be evaluated as all the fetuses with β thalassemia major or sickle cell disease were terminated. Parents having heterozygous fetuses with α gene triplication should be followed up periodically after birth for better management of these babies. [ABSTRACT FROM AUTHOR]
- Published
- 2020
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18. SAFETY AND EFFECTIVENESS OF TRANSABDOMINAL CHORIONIC VILLOUS SAMPLING FOR PRENATAL DIAGNOSIS OF β-THALASSEMIA.
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Shams, Roeda, Raza, Fazia, and Nawaz, Aman
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CHORIONIC villus sampling , *PRENATAL diagnosis , *BETA-Thalassemia , *RECURRENT miscarriage , *CONSANGUINITY , *UTERINE hemorrhage , *DNA analysis - Abstract
Objectives: To assess safety and effectiveness of trans abdominal, chorionic villus sampling( CVS) for pre-natal diagnosis of B-thalassemia. Material & Methods: This is prospective observational study conducted over a period from Jan 2018 to Dec 2018 in Rehman Medical Institute of Peshawar-Pakistan. Total of 50 patients were recruited in study. All couples who were carriers of thalassemia trait or had previous child with thalassemia major were included. Patients with multiple gestation, active vaginal bleeding before procedure, gestational age > 16 weeks, recurrent unexplained abortions, medical disease such as overt diabetes, chronic hypertension and patients who refused termination in case of positive diagnosis were excluded from the study A written consent about the CVS procedure, its complications and decision for termination in case of positive diagnosis was taken from all couples. Period of gestation was calculated by booking ultrasound and LMP and procedure was performed between 10-14 weeks. The procedure was conducted in interventional radiology unit of RMI through Trans abdominal route under aseptic technique and local anesthesia (5-10ml of 2% xylocaine). Results: DNA analysis of chorionic villus sampling showed that 17(34%) fetuses had thalassemia major, 10 fetuses (20%) thalassemia trait and 23 (46%) had no Beta Thalassemia mutation. Twentyeight (56%) couples had consanguineous marriages. Only one patient (2%) had procedure related spontaneous miscarriage. None of sample was reported as insufficient or in adequate. Conclusion; Trans abdominal approach for chorionic villus sampling is a safe and effective tool for prenatal diagnosis of thalassemia major provided done with skilled hands. [ABSTRACT FROM AUTHOR]
- Published
- 2020
19. Early prenatal diagnosis of hemoglobinopathy via celocentesis: Is it ready for use in routine clinical practice?
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Zhao, Yuan and Li, Dong‐Zhi
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HEMOGLOBINS , *PRENATAL diagnosis , *DNA , *GESTATIONAL age , *GENES , *BETA-Thalassemia , *EARLY diagnosis - Abstract
The article offers information on first trimester chorionic villus sampling which is the widely accepted method of prenatal diagnosis for single gene disorders. Topics include medians several researchers give considerable attention to another approach of prenatal diagnosis known as celocentesis and considered unlike CVS which cannot be performed until the very late in the first trimester, celocentesis can be undertaken as early as 7–9 weeks of gestation.
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- 2023
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20. India's First Child using PGT-M, PGT-A and HLA Matching for Helping a Sibling having β-Thalassemia Major.
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Banker, Jwal M., Arora, Parul, Khajuria, Rajni, and Banker, Manish
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HEMATOPOIETIC stem cell transplantation , *HLA histocompatibility antigens , *GENETIC testing , *SIBLINGS , *BETA-Thalassemia , *PRENATAL diagnosis - Abstract
β-thalassemia is a common single-gene disorder in India, with hematopoietic stem cell transplantation (HSCT) being the only cure. HSCT with matched unrelated donor is less successful, whereas finding a human leukocyte antigen (HLA)-matched related donor is difficult. Preimplantation genetic testing for monogenic diseases (PGT-M) with HLA matching is a novel option to have a matched sibling for HSCT for couples having an affected child. We present the first such case report in India. A couple, both carriers of β-thalassemia and having an affected son, underwent PGT-M with HLA matching combined with preimplantation genetic testing for aneuploidies of embryos to have a β - thalassemia-free child. This resulted in birth of a 10/10 HLA-matched sibling. [ABSTRACT FROM AUTHOR]
- Published
- 2019
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21. Noninvasive prenatal screening test for compound heterozygous beta thalassemia using an amplification refractory mutation system real-time polymerase chain reaction technique.
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Suwannakhon, Narutchala, Pangeson, Tanapat, Seeratanachot, Teerapat, Mahingsa, Khwanruedee, Pingyod, Arunee, Bumrungpakdee, Wanwipa, and Sanguansermsri, Torpong
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BETA-Thalassemia , *POLYMERASE chain reaction , *PRENATAL diagnosis , *SYMPTOMS , *INVASIVE diagnosis , *CYCLODEXTRINS - Abstract
We propose using a modified amplification refractory mutation system real-time polymerase chain reaction (ARMS RTPCR) technique to exclude the invasive prenatal diagnosis for a non-paternally inherited beta thalassemia mutation in couples atrisk for having a baby with CHBT. The ARMS RT-PCR method was performed for 36 at-risk couples by using isolated fetal cell-free DNA from maternal plasma. The modified ARMS RT-PCR primers targeted one of the following paternally inherited beta thalassemia mutation: -28 A→G, CD17 A→T, CD 26 G→A, IVS1-1 G→T and CD 41-42 -CTTT. The method could be successfully employed for NIPST starting with the 7th week of gestation. The results showed that 19 pregnant women were negative for PIBTM (53%). After an on-track and on-time of one year, including postnatal thalassemia blood tests, none of the babies showed symptoms or signs of beta thalassemia disease. We concluded that the modified ARMS RT-PCR method was an accurate, cost-effective and feasible method for use as a NIPST for at-risk couples with the potential of having a baby with CHBT. [ABSTRACT FROM AUTHOR]
- Published
- 2019
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22. Mutational analysis of thalassemia in transfusion-dependent beta-thalassemia patients from central India.
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Shrivastava, Manisha, Bathri, Rashmi, and Chatterjee, Nirupama
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BLOOD transfusion , *GENETIC counseling , *HEMOGLOBINOPATHY , *HETEROCYCLIC compounds , *GENETIC mutation , *POLYMERASE chain reaction , *PRENATAL diagnosis , *PURINES , *RISK assessment , *PHENOTYPES , *GENETIC testing , *SICKLE cell trait , *BETA-Thalassemia , *GENOTYPES , *DISEASE risk factors - Abstract
BACKGROUND: Thalassemia and hemoglobin (Hb) disorders are the most common genetic disorders among humans. These disorders entail huge morbidity, economic, and psychological burden on the families of the affected. Genetic counseling and prenatal diagnosis are the steps, which helps to reduce this burden. At present, there is paucity of data on the mutational spectrum of thalassemia from the central Indian region. METHODS: Blood samples were collected from 62 transfusion-dependent patients, demographic and relevant data were collected and screened for the two rare mutations − 88 (C-T) and CAP + 1 (A-G) using amplification refractory mutation system-polymerase chain reaction (PCR) and GAP PCR technique. PCR was performed for rare Hb disorders such as Hb Lepore and δ β chain disorder by GAP PCR in addition to five common Indian beta-thalassemia mutations IVS1-5 (G-C), IVS1-1 (G-T), Cd41/42 (−TCTT), Cd8/9 (+G), 619 bp deletion. RESULTS: Overall 93.5% of the mutations could be identified. Among the abnormal Hb, sickle cell and HbE were found at 4% and 3% of all the loci studied. We also reported two loci with Hb δ β and one locus with Hb Lepore in the present samples. IVS I-5 (G–C) was the common mutation (46%) followed by IVS I-1 (G–T) (12%) and 619 bp (9%). CONCLUSION: The identification of the genotypes helps to define the severity of the phenotype, plan therapy and form the basis of the comprehensive diagnostic database that would be useful not only for genetic counseling but prenatal diagnosis as well, contributing to the current focus of the National Policy to prevent and control hemoglobinopathies. [ABSTRACT FROM AUTHOR]
- Published
- 2019
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23. The phenotypic and molecular diversity of hemoglobinopathies in India: A review of 15 years at a referral center.
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Nadkarni, Anita H., Gorakshakar, Ajit C., Sawant, Pratibha M., Italia, Khushnooma Y., Upadhye, Dipti S., Gorivale, Manju S., Mehta, Pallavi R., Hariharan, Priya, Ghosh, Kanjaksha, and Colah, Roshan B.
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HEMOGLOBINOPATHY genetics , *CHROMOSOME abnormalities , *DNA , *ELECTROPHORESIS , *GENETIC polymorphisms , *HEMOGLOBINS , *HEMOGLOBINOPATHY , *HIGH performance liquid chromatography , *MOLECULAR biology , *GENETIC mutation , *NUCLEIC acid hybridization , *POLYMERASE chain reaction , *PRENATAL diagnosis , *PHENOTYPES , *ALPHA-Thalassemia , *BETA-Thalassemia , *SEQUENCE analysis , *TERTIARY care , *GENOTYPES ,HEMOGLOBINOPATHY diagnosis - Abstract
Introduction: The hemoglobinopathies pose a significant health burden in India. Apart from the β thalassemias and sickle cell disorders, α thalassemias and structural hemoglobin variants are also common. Here we have reviewed the phenotypic and molecular diversity of hemoglobinopathies encountered at a referral center in western India over a period of 15 years. Materials and Methods: Screening for hemoglobinopathies was done using HPLC and cellulose acetate electrophoresis. Molecular characterization was done using Covalent Reverse Dot Blot Hybridization (CRDB), Amplification Refractory Mutation System (ARMS), GAP PCR and direct DNA sequencing. Results: The study includes 31 075 individuals who were referred for diagnosis of hemoglobinopathies and prenatal diagnosis. Of these 14 423 individuals showed various hemoglobin abnormalities. Beta genotyping in 5615 individuals showed the presence of 49 β thalassemia mutations. 143 β thalassemia heterozygotes had normal or borderline HbA2 levels. We identified three δ gene mutations (HbA2 Pellendri, HbA2 St.George, HbA2 Saurashtra) in β thalassemia heterozygotes leading to normal HbA2 levels. The commonest defects among the raised Hb F determinants were Gγ(Αγδβ)0 Indian inversion and the HPFH‐3 Indian deletion. A total of 312 individuals showed the presence of α thalassemia, of which 12.0% had a single α gene deletion (−α/αα). HbH disease was identified in 29 cases with 10 different genotypes. Alpha globin gene triplication was seen in 2.1% of β thalassemia heterozygotes with a thalassemia intermedia phenotype. Seven unusual α chain variants and eight uncommon β chain variants were identified. Conclusion: The repertoire of molecular defects seen in the different globin genes will be valuable for management and control of these disorders both in India as well as in other countries where there is a huge influx of migrant populations from India. [ABSTRACT FROM AUTHOR]
- Published
- 2019
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24. The sensitive detection of IVSII-1(G˃A) mutation in beta globin gene using a Nano-based ligation genotyping system.
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Heidari sharafdarkolaee, Somaye, Motovali-Bashi, Majid, and Gill, Pooria
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BETA-Thalassemia , *GENETIC disorders , *PRENATAL diagnosis , *QUANTUM dots , *MAGNETIC nanoparticles - Abstract
Beta-thalassemia (β-thalassemia) is a globally genetic diseases, and is most prevalent in the Middle East, particularly in Iran. Carrier detection and prenatal diagnosis are the best ways to managing it, and to prevent new community cases from emerging. We report on a simple method for rapid detection of the worst β-thalassemia point mutation in Iran (IVS-II-1 G>A), using a nano-based ligation assay, this was performed using probes with labeled magnetic nanoparticles and quantum dots. After optimizing the technique, 50 DNA samples were genotyped with this method. We found a frequency of 72% for IVSII-1 (G˃A) mutation (42% heterozygote, and 30% mutant homozygote) with a highly sensitive nano-based ligation genotyping system, offering excellent sensitivity and specificity for point mutation detection; it has been demonstrated to be inaccurate, sensitive, cost-effective, and rapid technique for single nucleotide polymorphism (SNP) genotyping. [ABSTRACT FROM AUTHOR]
- Published
- 2018
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25. Fast Temperature-Gradient COLD PCR for the enrichment of the paternally inherited SNPs in cell free fetal DNA; an application to non-invasive prenatal diagnosis of β-thalassaemia.
- Author
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Byrou, Stefania, Makrigiorgos, G. Mike, Christofides, Agathoklis, Kallikas, Ioannis, Papasavva, Thessalia, and Kleanthous, Marina
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BETA-Thalassemia , *SINGLE nucleotide polymorphisms , *POLYMERASE chain reaction , *MOLECULAR genetics , *GENE amplification , *DIAGNOSIS - Abstract
Objective: To develop a sensitive, specific, simple, cost-effective and reproducible platform for the non-invasive prenatal detection of paternally inherited alleles for β-thalassaemia. The development of such an assay is of major significance in order to replace currently-applied invasive methods containing inherent fetal loss risks. Methods: We present a fast Temperature-Gradient Co-amplification at Lower Denaturation Temperature Polymerase Chain Reaction (fast TG COLD PCR) methodology for the detection of the paternally-inherited fetal alleles in maternal plasma. Two single-nucleotide polymorphisms (SNPs), rs7480526 (G/T) and rs968857 (G/A) that are located on the β-globin gene cluster and exhibit a high degree of heterozygosity in the Cypriot population were selected for evaluation. Seventeen maternal plasma samples from pregnancies at risk for β-thalassemia were analysed for the selected SNPs using the novel fast TG COLD PCR assay. Results: Using fast TG COLD PCR, the paternally inherited allele in cell free fetal DNA was correctly determined for all the 17 maternal plasma samples tested, showing full agreement with the Chorionic Villus Sampling (CVS) analysis. Conclusions: Our findings are encouraging and demonstrate the efficiency and sensitivity of fast TG COLD PCR in detecting the minor paternally-inherited fetal alleles in maternal plasma for the development of a NIPD assay for β-thalassaemia. [ABSTRACT FROM AUTHOR]
- Published
- 2018
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26. Non-invasive prenatal testing for fetal inheritance of maternal β-thalassaemia mutations using targeted sequencing and relative mutation dosage: a feasibility study.
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Xiong, L., Barrett, A. N., Hua, R., Ho, S. S. Y., Jun, L., Chan, K. C. A., Mei, Z., Choolani, M., Ho, Ssy, and Chan, Kca
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DIAGNOSIS of fetal diseases , *FETAL diseases , *GENETICS , *GENETIC mutation , *PRENATAL diagnosis , *PILOT projects , *BETA-Thalassemia , *SEQUENCE analysis , *DIAGNOSIS - Abstract
Objective: To evaluate whether targeted sequencing and relative mutation dosage can be used to diagnose correctly inheritance of maternal β-thalassaemia mutations in cell-free DNA.Design: Feasibility study using samples collected in a prenatal clinic.Setting: South East Asia.Population: Couples where both partners were known to be carriers of one of four common β-thalassaemia mutations or an HbE mutation, and therefore at risk of carrying a fetus affected with β-thalassaemia.Methods: 49 samples previously identified as having inherited a paternal β-thalassaemia mutation were amplified using nested polymerase chain reaction (PCR), and then sequencing. Relative mutation dosage was used to classify the fetus as having inherited the wild-type or mutant maternal allele.Main Outcome Measures: Classification of the fetus as 'unaffected' (if the maternal wild-type allele was inherited) or 'affected' with β-thalassaemia (if the maternal mutant allele was inherited).Results: A classification for inheritance of maternal allele was obtained in 48/49 samples (98.0%). A concordant call was made in 44/48 cases (91.7%): one false-positive and three false-negatives were obtained. Thus, we had an overall sensitivity of 87.5% [95% confidence interval (CI) 67.6-97.3%] and a specificity of 95.8% (95% CI 78.9-99.9%) for inheritance of maternal genotype.Conclusions: RMD for detection of inheritance of maternal β-thalassaemia mutations has potential for clinical use. Our sequential approach could be applied to other single-gene disorders.Tweetable Abstract: NIPT for β-thalassaemia achieved using nested-PCR followed by relative mutation dosage. [ABSTRACT FROM AUTHOR]- Published
- 2018
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27. Molecular Characterization of β-Thalassemia Mutations Via the Amplification Refractory Mutation System-Polymerase Chain Reaction Method at the North Waziristan Agency, Pakistan.
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Khan, Noor M., Rehman, Shoaib Ur., Shakeel, Muhammad, Khan, Saadullah, Ahmed, Usman, Rehman, Hazir, Yaseen, Tabassum, and Javid, Asad
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BETA-Thalassemia , *HYPOCHROMIC anemia , *POLYMERASE chain reaction , *GENETIC mutation , *PRENATAL diagnosis - Abstract
β-Thalassemia (β-thal) is a monogenic disease characterized by mutations on the HBB gene, affecting the production of globin that results in hypochromic and microcytic anemia. The aim of this study was to determine the prevalence of six common β-thal mutations, and their frequency and inheritance pattern in affected populations of North Waziristan Agency, Pakistan. In this study, 130 blood samples from 37 unrelated β-thalassemic families having a minimum of one transfusion-dependent child with β-thal major (β-TM), were retrieved either from the Thalassaemia Centre for Women and Children Hospital Bannu or their home towns situated in Noth Waziristan Agency. All samples were analyzed by the amplification refractory mutation system-polymerase chain reaction (ARMS-PCR) using six allele-specific primers for the presence of the six β-thal mutations common in the Pakistani population. Of the six common mutations, our study demonstrated five HBB mutations comprising HBB: c.27_28insG, HBB: c.92+5G>C, HBB: c.126_129delCTTT, HBB: c.92+1G>T and HBB: c.17_18delCT from the families studied, while mutation HBB: c.47G>A [codon 15 (G>A)] was not detected in any of the studied families. Furthermore, the HBB: c.27_28insG and HBB: c.92+5G>C were noted to be the most common with frequencies of 42.85 and 31.42%, respectively. The findings of the present study may be useful in launching carrier screening and prenatal diagnosis (PND) programs by screening analyzed and other unanalyzed affected families for the possible presence of common mutations through the ARMS-PCR technique that will help to control the disease. [ABSTRACT FROM AUTHOR]
- Published
- 2018
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28. A National Registry of Thalassemia in Turkey: Demographic and Disease Characteristics of Patients, Achievements, and Challenges in Prevention.
- Author
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Aydınok, Yeşim, Oymak, Yeşim, Atabay, Berna, Aydoğan, Gönül, Yeşilipek, Akif, Ünal, Selma, Kılınç, Yurdanur, Oflaz, Banu, Akın, Mehmet, Vergin, Canan, Evim, Melike Sezgin, Çalışkan, Ümran, Ünal, Şule, Bay, Ali, Kazancı, Elif, İleri, Talia, Atay, Didem, Patıroğlu, Türkan, Kahraman, Selda, and Söker, Murat
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CHELATION therapy , *REPORTING of diseases , *HEMATOPOIETIC stem cell transplantation , *HEMOGLOBINOPATHY , *GENETIC mutation , *PRENATAL diagnosis , *SPLENECTOMY , *BETA-Thalassemia , *THALASSEMIA , *SYMPTOMS , *PREVENTION - Abstract
Objective: The Turkish Society of Pediatric Hematology set up a National Hemoglobinopathy Registry to demonstrate the demographic and disease characteristics of patients and assess the efficacy of a hemoglobinopathy control program (HCP) over 10 years in Turkey. Materials and Methods: A total of 2046 patients from 27 thalassemia centers were registered, of which 1988 were eligible for analysis. This cohort mainly comprised patients with β-thalassemia major (n=1658, 83.4%) and intermedia (n=215, 10.8%). Results: The majority of patients were from the coastal areas of Turkey. The high number of patients in Southeastern Anatolia was due to that area having the highest rates of consanguineous marriage and fertility. The most common 11 mutations represented 90% of all β-thalassemia alleles and 47% of those were IVS1-110(G->A) mutations. The probability of undergoing splenectomy within the first 10 years of life was 20%, a rate unchanged since the 1980s. Iron chelators were administered as monotherapy regimens in 95% of patients and deferasirox was prescribed in 81.3% of those cases. Deferasirox administration was the highest (93.6%) in patients aged <10 years. Of the thalassemia major patients, 5.8% had match-related hemopoietic stem cell transplantation with a success rate of 77%. Cardiac disease was detected as a major cause of death and did not show a decreasing trend in 5-year cohorts since 1999. Conclusion: While the HCP has been implemented since 2003, the affected births have shown a consistent decrease only after 2009, being at lowest 34 cases per year. This program failure resulted from a lack of premarital screening in the majority of cases. Additional problems were unawareness of the risk and misinformation of the at-risk couples. In addition, prenatal diagnosis was either not offered to or was not accepted by the at-risk families. This study indicated that a continuous effort is needed for optimizing the management of thalassemia and the development of strategies is essential for further achievements in the HCP in Turkey. [ABSTRACT FROM AUTHOR]
- Published
- 2018
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29. Haplotypes inside the beta-globin gene: use as new biomarkers for beta-thalassemia prenatal diagnosis in north of Iran.
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Hashemi-Soteh, Mohammad Bagher, Mousavi, Seyed Saeed, and Tafazoli, Alireza
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HAPLOTYPES , *GLOBIN genes , *BIOMARKERS , *BETA-Thalassemia , *PRENATAL diagnosis - Abstract
Background: Beta-thalassemia is common in the Mediterranean area as well as the Middle East and India. Official report in Iran revealed the average prevalence rate of carriers about 4%. More than 20 restriction fragment length polymorphisms (RFLPs) are known in the beta-globin gene cluster and used in the prenatal diagnosis (PND) services. Some of these locations may have low allele frequency and are not informative in the prenatal diagnosis. The current study aims to find new haplotypes and polymorphisms with high allele frequency in the local population. Methods: Two thousand three hundred fifty samples (1,321 male and 1,029 female) from the northern Iran, whom suspected to be the carriers either for alpha or beta thalassemia and referred to the local diagnostic laboratory as a routine services were investigated during five years, (2010-2015). The beta-globin gene was sequenced for all samples. Results: Heterozygosity for five SNPs in the beta-globin gene was calculated separately. 383 individuals (16.29%) showed no sign of nucleotide change in the beta-globin gene sequence. In total, codon2 (C/T) 31.72%, IVSII-16 (C/G) 31.72%, IVSII- 74 (G/T) 54.71%, IVSII-81 (C/T) 19.47%, and IVSII-666 (T/C) 31.72% were seen respectively. Although all five polymorphisms showed reasonably high heterozygosity, IVSII-74 (G/T) [GG wild type (36.5%), G/T (54.71%) and TT (8.8%)] revealed the highest heterozygosity rate. Four combinations of these five SNPs were defined as new haplotypes named M1 to M4. ARMS-PCR also were designed and applied to detect IVSII-74 (G/T) nucleotide position. Conclusions: This study represents an intragenic polymorphism, IVSII-74, a reliable position with high heterozygosity rates in Iranian population for PND analysis. Trial registration: Retrospectively registered. [ABSTRACT FROM AUTHOR]
- Published
- 2017
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30. Use of Chorionic Villous Sampling for Prenatal Diagnosis of Beta Thalassaemia: Attitudes and Practices of Parents.
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Ali, Sundas, Zawar, Asfa, Amanat, Samina Tufail, Jiskani, Shahzad Ali, Sohail, Aliena, Rizwan, Humaira, and Jamal, Sara
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BETA-Thalassemia , *CHORIONIC villus sampling , *PRENATAL diagnosis , *PREGNANCY , *PARENT attitudes - Abstract
Background: To assess the attitudes and practices of parents of Beta-Thalassaemia Major children regarding Chorionic Villous Sampling (CVS), as prenatal diagnosis in subsequent pregnancies. Methods: In this cross-sectional study a predesigned questionnaire was used to evaluate the socio-demographic profile and attitudes of parents of 210 registered thalassaemic children, regarding CVS.Only those parents who had one or more pregnancies after the index case were included in the study. Results were entered and analyzed on SPSS version 20. Results: After the index case, 36.2% parents underwent CVS in all subsequent pregnancies. The common reasons not to utilize this facility were lack of knowledge (47.7%), careless attitude (41.7%), family pressure (4.4%) and financial issues (1.5%). Religious reason was not found in any of the cases. Majority of the families (54.3%) belonged to lower middle class financial status. There was a significant association between CVS practice and educational level of the mother and genetic counselling at the time of diagnosis of index case. In future pregnancies, 52.8% parents had no planning, while 15.7% showed interest in undergoing CVS in next pregnancies. Conclusion: Despite the availability of CVS in the country, very few families had opted for it; the major reasons being lack of knowledge, careless attitude and family pressure. As against the common thought, religious reason was not a significant factor. [ABSTRACT FROM AUTHOR]
- Published
- 2017
31. A Pilot Study of Noninvasive Prenatal Diagnosis of Alpha- and Beta-Thalassemia with Target Capture Sequencing of Cell-Free Fetal DNA in Maternal Blood.
- Author
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Wang, Wenjuan, Yuan, Yuan, Zheng, Haiqing, Wang, Yaoshen, Zeng, Dan, Yang, Yihua, Yi, Xin, Xia, Yang, and Zhu, Chunjiang
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THALASSEMIA , *BETA-Thalassemia , *PRENATAL diagnosis , *BODY fluids , *GENETIC disorders - Abstract
Aims: Thalassemia is a dangerous hematolytic genetic disease. In south China, ∼24% Chinese carry alpha-thalassemia or beta-thalassemia gene mutations. Given the fact that the invasive sampling procedures can only be performed by professionals in experienced centers, it may increase the risk of miscarriage or infection. Thus, most people are worried about the invasive operation. As such, a noninvasive and accurate prenatal diagnosis is needed for appropriate genetic counseling for families with high risks. Here we sought to develop capture probes and their companion analysis methods for the noninvasive prenatal detection of deletional and nondeletional thalassemia. Materials and Methods: Two families diagnosed as carriers of either beta-thalassemia gene or Southeast Asian deletional alpha-thalassemia gene mutation were recruited. The maternal plasma and amniotic fluid were collected for prenatal diagnosis. Probes targeting exons of the genes of interest and the highly heterozygous SNPs within the 1Mb flanking region were designed. The target capture sequencing was performed with plasma DNA from the pregnant woman and genomic DNA from the couples and their children. Then the parental haplotype was constructed by the trios-based strategy. The fetal haplotype was deduced from the parental haplotype with a hidden Markov model-based algorithm. Results: The fetal genotypes were successfully deduced in both families noninvasively. The noninvasively constructed haplotypes of both fetuses were identical to the invasive prenatal diagnosis results with an accuracy rate of 100% in the target region. Conclusion: Our study demonstrates that the effective noninvasive prenatal diagnosis of alpha-thalassemia and beta-thalassemia can be achieved with the targeted capture sequencing and the haplotype-assisted analysis method. [ABSTRACT FROM AUTHOR]
- Published
- 2017
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32. A Novel -72 (T→A) β-Promoter Mutation Causing Slightly Elevated HbA2 in a Vietnamese Heterozygote.
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Pirastru, Monica, Mereu, Paolo, Nguyen, Chau Quynh, Nguyen, Nhan Viet, Nguyen, Thang Duy, and Manca, Laura
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BETA-Thalassemia , *FAMILIES , *GENE expression , *GENES , *GENETIC mutation , *PRENATAL diagnosis , *GENETICS - Abstract
We report a novel β+-thalassemia mutation found in a Vietnamese family. The molecular defect T→A lies at -72 of the β-globin gene promoter, within the conserved CCAAT box. The index case was a 5-year-old child having red blood cells indices close to normal and slightly increased level of HbA2 (3.96%). The expression of the mutated β allele was inferred by luciferase reporter assay in K562 cells. The β -72 determinant is the eighth β-thalassemic mutation identified in Vietnam and it was not previously reported in any population. The absence of homozygous or compound heterozygous states did not allow us to precisely predict either its clinical impact or its relevance in management programs. Our results further underline the importance of identifying and characterizing new or rare β+-thalassemic alleles in carrier screening and prenatal diagnosis. [ABSTRACT FROM AUTHOR]
- Published
- 2017
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33. Non invasive prenatal diagnosis of β- Thalassemia, A narrative review study.
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Zafari, M., Kowsaryan, M., Gill, P., and Banihashemi, A.
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PRENATAL diagnosis , *BETA-Thalassemia , *GENETIC mutation , *CHORIONIC villus sampling , *AMNIOCENTESIS - Abstract
β- Thalassemia is major monogenic disorder. A practical way to prevention of Thalassemia is identification of carries couples; genetic counseling and offer prenatal diagnose services for both carrier couples. Routine prenatal diagnose are chorionic villus sampling and amniocentesis, but both of them are invasive method and they can be ended to bleeding and pregnancy loss. Recently non invasive prenatal diagnosis has been done by researchers for early detection of pre-eclampsia, chromosomal aneuploidies, RhD-genotyping. Regarding non invasive prenatal diagnosis of β- Thalassemia, detection of paternally inherited mutation in maternal plasma is possible. If the fetus inherited normal paternal allele the performance of invasive method it is not necessary, so this method can be eliminate 50% performance of routine prenatal diagnosis. [ABSTRACT FROM AUTHOR]
- Published
- 2017
- Full Text
- View/download PDF
34. The pros and cons of the fourth revision of thalassaemia screening programme in Iran.
- Author
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Moafi, Alireza, Vallian, Reihaneh, Vallian, Sadeq, Rahgozar, Soheila, Torfenajad, Mohammad, and Moafi, Hadi
- Subjects
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THALASSEMIA , *BETA-Thalassemia , *ERYTHROCYTES , *BLOOD testing , *BLOOD protein electrophoresis , *CONFIDENCE intervals , *DIAGNOSIS , *HEMOGLOBINS , *MARRIAGE , *MEDICAL screening , *MOLECULAR diagnosis , *PARENTS , *PRENATAL diagnosis , *GENETIC testing , *DESCRIPTIVE statistics , *PREVENTION - Abstract
Objective To evaluate the repercussions of recent changes to the cut-offs used in the first screening step of the pre-marital screening programme for thalassaemia prevention in Iran. Methods The profiles of 984 subjects referred to a genetic laboratory, and the tests of 242 parents of children with thalassaemia major were assessed for red blood cell (RBC) indices, haemoglobin (Hb) A2 levels and results of Hb electrophoresis. Results Of 407 suspected thalassaemia minor (STM) cases, 18 proved positive for thalassaemia minor on molecular analysis (18/407, confidence interval 2.6–6.9%). If the revised screening cut-offs had been used to determine who would undergo molecular analysis, two of these cases would not have been identified. Only 4.4% of suspected cases with lower than normal RBC indices (mean corpuscular volume <80 fl and mean corpuscular Hb <27 pg) and HbA2 (<3.5%) were diagnosed with thalassaemia minor. Conclusion The thalassaemia major prevention programme is performed in two separate steps. One step involves the screening of subjects and identification of β-thalassaemia minor, suspected cases for thalassaemia minor (STM), and normal subject groups. The other step concerns the identification of thalassaemia minor in the STM group. Changing the cut-offs at the first screening step does not result in significant improvement from an economic view, and is associated with significant risk at the second screening step. [ABSTRACT FROM AUTHOR]
- Published
- 2017
- Full Text
- View/download PDF
35. Characterization of a novel β-globin gene cluster deletion causing (Aγδβ)0-thalassemia by next-generation sequencing.
- Author
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Wu, M.‐Y., Li, J., Yan, J.‐M., Zhang, Y., and Li, D.‐Z.
- Subjects
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CHROMOSOME analysis , *BETA-Thalassemia , *CHINESE people , *GENEALOGY , *GENETIC techniques , *GENETIC mutation , *POLYMERASE chain reaction , *PRENATAL diagnosis , *GENETIC carriers , *SEQUENCE analysis , *GENETICS , *DIAGNOSIS - Abstract
A letter to the editor is presented on characterization of a novel beta-globin gene cluster deletion which causes a form of thalassemia.
- Published
- 2017
- Full Text
- View/download PDF
36. Q Sepharose micro-column chromatography: A simple screening method for identifying beta thalassemia traits and hemoglobin E carriers.
- Author
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Wong, Peerapon, Sritippayawan, Suchila, Suwannakhon, Narutchala, Tapprom, Akamon, Deoisares, Rawisut, and Sanguansermsri, Torpong
- Subjects
- *
BETA-Thalassemia , *PREGNANCY complications , *PRENATAL diagnosis , *HEMOGLOBINS , *SEPHAROSE , *COLUMN chromatography , *MEDICAL screening , *PREVENTION - Abstract
Objectives For beta thalassemia control program in pregnancy, mass screening of the carrier state by determination of the hemoglobin (Hb) A 2 and Hb E proportions and mutation analysis is a preferred method for making prenatal diagnoses. Q Sepharose micro-column chromatography, developed for the determination of Hb A 2 and Hb E for screening purposes, was compared with high performance liquid chromatography (HPLC) to ascertain its relative accuracy and reliability. Design and methods Results using Q Sepharose micro-column chromatography in 350 blood specimens, including 50 samples genetically proven to be beta thalassemia heterozygotes, were compared to HPLC for validation. An additional study was conducted to test a clinical application on a large-scale survey for beta thalassemia in 1581 pregnant women and their spouses. Results The mean (± SD) Hb A 2 proportions in the normal and genetically proven beta thalassemia heterozygotes were 2.70 ± 0.40% and 6.30 ± 1.23%, respectively, as determined by Q-Sepharose micro-column chromatography, and 2.65 ± 0.31% and 5.37 ± 0.96%, respectively, as determined by HPLC. The mean Hb E proportions in the Hb E heterozygotes were 23.25 ± 4.13% and 24.72 ± 3.5% as determined by Q Sepharose micro-column chromatography and HPLC, respectively. In the large-scale survey for beta thalassemia, 23 at risk couples were detected. Seven affected fetuses were identified by prenatal diagnosis. Conclusions Q Sepharose micro-column chromatography was found to be reliable, reproducible and well-suited for large-scale surveys. Additionally, by being reusable and convenient, this simple and economical chromatography method may be an alternative means to screen for beta thalassemia and Hb E carriers in the mass population. [ABSTRACT FROM AUTHOR]
- Published
- 2016
- Full Text
- View/download PDF
37. High-resolution melting analysis for noninvasive prenatal diagnosis of IVS-II-I (G-A) fetal DNA in minor beta-thalassemia mothers.
- Author
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Zafari, Mandana, Gill, Pooria, Kowsaryan, Mehrnoush, Alipour, Abbass, and Banihashemi, Ali
- Subjects
- *
PRENATAL care , *BETA-Thalassemia , *LABOR (Obstetrics) , *PREGNANCY , *FETAL development , *DELIVERY (Obstetrics) , *MATERNAL health , *MATERNAL health services - Abstract
Objectives: The high-resolution melting (HRM) technique is fast, effective and successful method for mutation detection. The aim of this study was to determine the sensitivity and specificity of the HRM method for detection of a paternally inherited mutation in a fetus as a noninvasive prenatal diagnosis of β-thalassemia.Methods: Genomic DNAs were prepared from 50 β-thalassemia minor couples whose pregnancy was at risk for homozygous β-thalassemia. Ten milliliters of the maternal blood from each pregnant woman were collected and after separating plasma stored at -80 °C until analysis. The extracted DNAs were analyzed by HRM real-time PCR for detection of IVS-II-I (G-A) as a paternally inherited mutation. The gold standard was the result of a chorionic villus sampling by a standard reverse dot blotting test.Results: The sensitivity and specificity of HRM real-time PCR were 92.6% and 82.6%, respectively. Also, the positive and negative predictive values were 86.2% and 90.47%, respectively.Conclusions: HRM real-time PCR was a sensitive and specific method for determining the paternally inherited mutation in the fetus at risk with thalassemia major. [ABSTRACT FROM AUTHOR]- Published
- 2016
- Full Text
- View/download PDF
38. Detection of paternally inherited fetal point mutations for β-thalassemia in maternal plasma using simple fetal DNA enrichment protocol with or without whole genome amplification: an accuracy assessment.
- Author
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Ramezanzadeh, Mahboubeh, Salehi, Mansour, Farajzadegan, Ziba, Kamali, Sara, and Salehi, Rasoul
- Subjects
- *
PRENATAL diagnosis , *MEDICAL protocols , *CHORIONIC villi , *CHORIONIC villus sampling , *DNA , *COMPARATIVE studies , *CORD blood , *RESEARCH methodology , *MEDICAL cooperation , *GENETIC mutation , *POLYMERASE chain reaction , *RESEARCH , *GENETIC testing , *EVALUATION research , *GENETIC carriers , *BETA-Thalassemia , *GENOTYPES , *DIAGNOSIS - Abstract
Objective: To design and evaluate a noninvasive protocol for prenatal diagnosis (PND) of β-thalassemia, using cell free fetal DNA (cff-DNA) in maternal circulation. Traditional current PND which is mainly based on chorionic villous sampling (CVS), amplification refractory mutation system and sequencing holds as gold standard.Methods: Ten thalassemia trait couples with distinct mutations for the husband and wife were included in this study. The mutations in carrier fathers were IVSI-1, IVSI-5, FR8/9 and CD44. After maternal plasma isolation and free DNA extraction, all samples subjected to designed protocol including DNA size separation on agarose gel, elution of DNA from the gel slices using a simple and efficient manual purification method, with or without whole genome amplification and the detection method was allele-specific real-time PCR.Results: Presence or absence of the paternal mutant allele was correctly determined in all of cases and the accuracy of designed protocol was determined 100%.Conclusions: The protocol described here is very simple, inexpensive and easy to perform, but with satisfactory accuracy in detection of paternal mutations in cff-DNA. Due to the risk of fetal loss with current invasive sampling for PND, a noninvasive alternative is highly demanded in clinical setting. [ABSTRACT FROM AUTHOR]- Published
- 2016
- Full Text
- View/download PDF
39. Non-invasive prenatal diagnosis of β-thalassemia by detection of the cell-free fetal DNA in maternal circulation: a systematic review and meta-analysis.
- Author
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Zafari, Mandana, Kosaryan, Mehrnoush, Gill, Pooria, Alipour, Abbass, Shiran, Mohammadreza, Jalalli, Hossein, Banihashemi, Ali, and Fatahi, Fatemeh
- Subjects
- *
THALASSEMIA diagnosis , *BETA-Thalassemia , *DIAGNOSIS of fetal diseases , *PRENATAL diagnosis , *HEMOGLOBINOPATHY , *PRENATAL genetic testing , *METABOLISM in the fetus , *CELLS , *DNA , *META-analysis , *SYSTEMATIC reviews , *DIAGNOSIS ,RESEARCH evaluation - Abstract
The discovery of fetal DNA (f-DNA) opens the possibility of early non-invasive procedure for detection of paternally inherited mutation of beta-thalassemia. Since 2002, some studies have examined the sensitivity and specificity of this method for detection of paternally inherited mutation of thalassemia in pregnant women at risk of having affected babies. We conducted a systematic review of published articles that evaluated using this method for early detection of paternally inherited mutation in maternal plasma. A sensitive search of multiple databases was done in which nine studies met our inclusion criteria. The sensitivity and specificity was 99 and 99 %, respectively. The current study found that detection of paternally inherited mutation of thalassemia using analysis of cell-free fetal DNA is highly accurate. This method could replace conventional and invasive methods. [ABSTRACT FROM AUTHOR]
- Published
- 2016
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- View/download PDF
40. Prenatal diagnosis of hemoglobinopathies in Tunisia: an 18 years of experience.
- Author
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Ouali, F., Siala, H., Bibi, A., Hadj Fredj, S., Dakhlaoui, B., Othmani, R., Ouenniche, F., Zouari, F., Bouguerra, B., Rezigua, H., Fattoum, S., and Messaoud, T.
- Abstract
Hemoglobinopathies are the most common genetic disease in Tunisia with a total carrier prevalence of 4.48%. Objective The aim of this study was to report an 18-year fully achieved experience of prenatal diagnosis (PND) of hemoglobinopathies (1994-2012) and to assess the impact of this prevention program. Patient and methods A total of 461 fetuses of 340 at-risk couples have been the subject of PND for beta-thalassemia major risk (41%), for sickle cell anemia risk (40.3%), for S/beta-thal risk (14.7%). The remainder fetuses were at risk for a compound heterozygote hemoglobinopathies (S/O, O/beta-thal, S/C....). Fetal DNA was studied by PCR procedure including the reverse dot-blot technique and the amplification refractory mutation system and direct sequencing. Results and discussion Only 13.8% of the fetal samplings were conducted by chorionic villus sampling. The molecular result for beta-thalassemia risk has shown 13 beta-thal mutations, with two common: codon 39 (C>T) and IVS1-110 (G>A). The last 3 years, STR study has permitted to reduce the problems of maternal cell contamination. Among the 461 tested fetuses, 121 were affected, and then the pregnancy was terminated except for 13 cases, because of religious considerations and this despite the abortion legality in Tunisia. The conducted PND is only about 30 PND per year corresponding essentially to the couples living in Tunis City and surrounding area. PND number has increased from 1994 to 2009. This evolution has brutally decreased after the Tunisian revolution (2010). Conclusion Although the good running of the PND, it covers only the Tunis city with low impact because it prevent apparition of only a mean of 7.3% of new cases. The reduced number of PND is not a technical inconvenience but rather a lack of a preventive program. [ABSTRACT FROM AUTHOR]
- Published
- 2016
- Full Text
- View/download PDF
41. Pregnancy outcomes among women with beta-thalassemia trait.
- Author
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Charoenboon, Chitrakan, Jatavan, Phudit, Traisrisilp, Kuntharee, and Tongsong, Theera
- Subjects
- *
BETA-Thalassemia , *PREGNANT women , *PREGNANCY complications , *RETROSPECTIVE studies , *DISEASE prevalence , *GESTATIONAL age , *HEALTH outcome assessment , *PATIENTS , *LOW birth weight , *BLOOD diseases , *FETAL growth retardation , *PREMATURE infants , *EVALUATION of medical care , *PREGNANCY , *PRENATAL diagnosis , *CASE-control method , *DISEASE complications - Abstract
Objective: To compare the obstetric outcomes between pregnant women affected by beta-thalassemia trait and normal controls.Methods: A retrospective cohort study was conducted on singleton pregnant women complicated by beta-thalassemia trait and normal controls, randomly selected with the controls-to-case ratio of 2:1. All were low-risk pregnancies without underlying medical diseases and fetal anomalies. The pregnancies undergoing invasive prenatal diagnosis were excluded.Results: A total of 597 pregnant women with beta-thalassemia trait and 1194 controls were recruited. Baseline characteristics and maternal outcomes in the two groups were similar, except that hemoglobin levels were slightly lower in the study group. The prevalence of small for gestational age and preterm birth tended to be higher in the study group but not reached the significant levels but the rate of low birth weight was significantly higher in the study group (relative risk 1.25; 95 % CI 1.00-1.57). Additionally, abortion rate was also significantly higher in the study group (relative risk 3.25; 95 % CI 1.35-7.80).Conclusion: Beta-thalassemia trait could minimally, but significantly, increase risk of low birth weight but did not increase rates of maternal adverse outcomes. [ABSTRACT FROM AUTHOR]- Published
- 2016
- Full Text
- View/download PDF
42. Evaluation of α-Globin Gene Mutations Among Different Ethnic Groups in Khuzestan Province, Southwest Iran.
- Author
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Khosravi, Abbas, Jalali-Far, Mohammadali, Saki, Najmaldin, Hosseini, Hossein, Galehdari, Hamid, Kiani-Ghalesardi, Omid, Paridar, Mostafa, Azarkeivan, Azita, and Magaji-Hamid, Kabir
- Subjects
- *
BETA-Thalassemia , *GENE frequency , *PRENATAL diagnosis , *PREMARITAL examinations , *DIAGNOSTIC use of polymerase chain reaction - Abstract
α-Thalassemia (α-thal) is one of the most common inherited hemoglobin (Hb) disorders in the world. In addition to large deletions, over 50 different α-thal point mutations were detected around the world, thus, patients showed different phenotypes with regard to genotype. This study evaluated the genetic frequency of α-thal in Khuzestan Province, Southwest Iran, to help implement premarital and prenatal screening programs. The study was conducted on couples proposing to get married and parents who were referred to the genetic center of Shafa Hospital, Ahvaz, Iran, for prenatal diagnosis (PND) in 2012. Genomic DNA was purified by the salting-out method and tested using multiplex gap-polymerase chain reaction (gap-PCR), amplification refractory mutation system-PCR (ARMS-PCR), reverse hybridization test strips and DNA sequencing. Overall, 11 mutations were found on the α-globin genes. Based on gene frequency, the most common mutant allele was –α3.7 (rightward) (71.3%) followed by the two gene deletion – –MED (9.7%). Other common mutations were αcodon 19α (GCG>GC–, α2) (8.4%), the polyadenylation (polyA1) site αpolyA1α (AATAAA>AATAAG) (2.8%), and α–5 ntα (–TGAGG) (2.0%). In addition, an extremely rare mutation at αcodon 21α [Hb Fontainebleau, HBA2: c.64G > C (or HBA1)] was also found. The results of this study are critical for correct diagnosis of α-thal carriers, premarriage counseling and PND. This study suggests that the distribution of mutations on the α-globin genes differs among the ethnic groups in Khuzestan Province as well as in other provinces. [ABSTRACT FROM AUTHOR]
- Published
- 2016
- Full Text
- View/download PDF
43. Investigation of molecular heterogeneity of β-thalassemia disorder in District Charsadda of Pakistan.
- Author
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Shakeel, Muhammad, Arif, Muhammad, Ur Rehman, Shoaib, and Yaseen, Tabassum
- Subjects
- *
BETA-Thalassemia , *POLYMERASE chain reaction , *GENETIC mutation , *BLOOD sampling , *PRENATAL diagnosis - Abstract
Objective: Thalassemia is blood related disease which arises from the reduced level of hemoglobin in red blood cells (RBC), a protein responsible for carrying oxygen inside the body. Considering its widespread occurrence in developing countries like Pakistan, this study aims to investigate the common molecular anomalies of the beta thalassemia disease in district Charsadda, Khyber Pakhtunkhwa. Methods: This work was done at Abdul Wali Khan University (AWKU) Mardan, Khyber Pakhtunkhwa, Pakistan. The work was performed on the blood samples collected from the patients and their families with beta thalassemia major (n = 13 families) belonged to District Charsadda. The collected blood samples were analyzed for presence of six known mutations with the help of polymerase chain reaction technique i.e. amplification of refractory mutation system. Results: Our Study reports six known mutations (IVS-1-5, FSC 8/9, CD 41/42, IVS-1-1, CD 15 and FSC-5) accounting for about 90% of total beta thalassemia genes in this country. Among the reported mutations, IVS 1-5 was the most prevalent beta thalassemia gene in patients belonging to District Charsadda. Conclusion: The results and findings of the current study may help in accessing the frequency of these common mutations and in initiating pre-natal diagnosis programme in Pakistan. [ABSTRACT FROM AUTHOR]
- Published
- 2016
- Full Text
- View/download PDF
44. Category D: Oral Presentations: Fetal Medicine.
- Subjects
- *
OBSTETRICS , *FETAL heart rate , *BETA-Thalassemia , *FETAL ultrasonic imaging , *PRENATAL diagnosis , *FETAL development - Published
- 2018
- Full Text
- View/download PDF
45. The Reproductive Behavior of Families with Thalassemic Children in Hormozgan.
- Author
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Moradabadi, Ali Safari, Alavi, Azin, Eftekhaari, Tasnim Eqbal, and Dadipoor, Sakineh
- Subjects
- *
BETA-Thalassemia , *CHORIONIC villus sampling , *CONCEPTION , *GENETIC counseling , *RESEARCH methodology , *MOTHERS , *PRENATAL diagnosis , *QUESTIONNAIRES , *RESEARCH funding , *REPRODUCTIVE health , *SOCIOECONOMIC factors , *ATTITUDES of mothers , *FAMILY planning , *GENETICS , *PREVENTION - Abstract
Background: Thalassemic disorders are the most prevalent monogenic hereditary diseases around the world caused by decreased and altered synthesis or agenesis in one or more globin chains. Families who have a child with thalassemia major face a myriad of significant problems. Hormozgan province ranks second with thalassemic patients in Iran. Therefore, current research is aimed to analyze the reproductive behavior of such families in the southern province of Iran. Methods: In this descriptive study 190 mothers of patients suffering from thalassemia major were included. The reproductive behavior of mothers was investigated by a questionnaire regarding the number of thalassemic infants born after their first child with thalassemia major. Results: About 23% of these mothers had more than 1 child with major thalassemia. The findings showed that the reasons for conception among these mothers were to have a healthy child (64.2%) and to have a boy (20%). In about 92.6% of mothers CVS test was not performed. Conclusion: This study showed that awaring mothers and families regarding the prevention of birth of afflicted infants and provision of accessible diagnostic facilities can reduce the number of children with thalassemia major. [ABSTRACT FROM AUTHOR]
- Published
- 2015
46. Pre-natal diagnosis of thalassaemia in Sri Lanka: A ten year review.
- Author
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Nanayakkara, Kalinga Khemal, Rodrigo, Undugodage Ganganath, Perera, Kuda Liyanage Nandika, and Nanayakkara, Chinthani Deepthi
- Subjects
- *
AMNIOCENTESIS , *GENETIC disorder diagnosis , *PRENATAL diagnosis , *AMNIOTIC liquid , *MISCARRIAGE , *GENEALOGY , *GENETIC techniques , *GENETIC mutation , *GENETIC testing , *DISEASE prevalence , *GENETIC carriers , *BETA-Thalassemia , *DIAGNOSIS - Abstract
Thalassaemia is the commonest monogenic disease in Sri Lanka, affecting over 3500 children and half-a-million thalassaemia carriers. This is a review of 82 amniocenteses performed from 2006 to 2016, in the largest prenatal diagnoses study for thalassaemia carried out in Sri Lanka. Amniocenteses were performed between 11 and 12 weeks of ultrasonically confirmed gestation, on mothers with previous thalassaemia major children pregnant for the second time and nulliparous thalassaemia trait women married to trait partners. The Consultant Radiologist, using local analgesia, under ultrasound cover, performed these as an outpatient procedure, at the Teaching Hospital Kandy & Suwasevana Hospital Kandy. The amniotic fluid was analysed by the team of Senior Geneticists, at the Genetech Molecular Diagnostics and School of Gene Technology, Colombo, via the polymerase-chain-reaction based ARMS (Amplification Refractory Mutation Systems) assay. The genetic results indicated the presence of 21% thalassaemia major foetuses, 53% thalassaemia traits and 26% foetuses without thalassaemia mutations. The predominance of the IVS1-5(G-C) mutation in the Sri Lankan population is exemplified, with a low prevalence of HbE thalassaemia. Impact statement Thalassaemia is the commonest monogenic disease in Sri Lanka affecting over 3500 children and half-a-million thalassaemia carriers. Although pre-natal diagnosis by amniocentesis was practised universally for many years, this could not be performed in Sri Lanka as genetic diagnostic facilities were not available until 2005. Therefore, parents with a thalassaemia major child limited their families to one child, by choice or by termination. The results of this study point to a 21% probability of thalassaemia major in the next child, giving the parents a guarded optimism to conceive another child without thalassaemia disease. With siblings being the highest HLA compatibility for Bone Marrow Transplant, that is now being established in Sri Lanka as a permanent cure for thalassaemia, this will bring a ray of hope for these desperate parents to finally cure their previous sick child. Although, 95% of the Sri Lankan mutated genetic sites for thalassaemia are known, more research will be needed to identify the other rare sites. The publication of this paper, with its novelty for pre-natal diagnosis, would encourage clinicians to practice it in other centres and to extend it to families with other genetic disorders. [ABSTRACT FROM AUTHOR]
- Published
- 2017
- Full Text
- View/download PDF
47. Evaluation of the National Prevention Program in Iran, 2007-2009: the Accomplishments and Challenges with Reflections on the Path Ahead.
- Author
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Hadipour Dehshal, Mahmoud, Tabrizi Namini, Mehdi, Ahmadvand, Alireza, Manshadi, Mohsen, Sadeghian Varnosfaderani, Forouzan, and Abolghasemi, Hassan
- Subjects
- *
BETA-Thalassemia , *PRENATAL diagnosis , *BIRTH rate , *BLOOD transfusion , *PREVENTION - Abstract
β-Thalassemia major (β-TM) is an inherited disease and efforts have been made in several countries to reduce the number of affected births. In the present study, we aimed to evaluate the Iranian thalassemia prevention program, considered to be an important program in the region. The time period of the present study ranges from 2007-2009, during which new thalassemic births and the relevant causes were evaluated throughout the country. A cross-sectional analytical study was conducted at the Iranian Blood Transfusion Organization (IBTO), Tehran, Iran. A questionnaire was forwarded to all blood centers of the IBTO so as to obtain information about the new cases of thalassemia and the causes of these thalassemic births. Provincial thalassemia societies also received the questionnaires so that screening and prenatal diagnosis (PND) errors would be recorded. The results showed that 755 new thalassemia cases were born during 2007-2009 with the average fall in affected thalassemia births of 80.82%. The main cause of the new births was attributed to unregistered 'timeless religious marriages' based on the conventions of the Sunni community which accounted for 43.17% of all new cases mainly having occurred in Sistan & Baluchestan Province. Not using PND was evaluated to be another main cause. Although the prevention program has led to a great reduction in thalassemic births, new measures are required, including research on how to make the program compatible with social and economic conventions and norms of Sistan & Baluchestan Province. The province of Kohgiluyeh Boyer Ahmad also needs to be revisited in terms of the program efficacy. [ABSTRACT FROM AUTHOR]
- Published
- 2014
- Full Text
- View/download PDF
48. α-Globin Gene Mutations in Isfahan Province, Iran.
- Author
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Karamzade, Arezo, Mirzapour, Hadi, Hoseinzade, Majid, Asadi, Sara, Gholamrezapour, Tahere, Tavakoli, Parvaneh, and Selebi, Mansoor
- Subjects
- *
GLOBIN genes , *GENETIC mutation , *BETA-Thalassemia , *PRENATAL diagnosis , *MEDICAL care costs , *DIAGNOSIS - Abstract
α-Thalassemia (α-thal) encompasses a spectrum of mutations including deletion and point mutations on the α-globin chains that is characterized by a reduction or complete absence of α-globin genes. Most of the α-thal cases are deletions involving one (α+) or both (α0) α-globin genes, although point mutations (αTα or ααT) are found as well. In this study, 314 individuals with low hematological values, normal Hb A2 who were not affected with β-thal or iron deficiency, were investigated for the presence of α-thal mutations. The most common deletion was −α3.7 (rightward) with a frequency of 70.7%, followed by α−5 nt (-TGAGG) (8.7%), −α4.2 (leftward) (4.7%), the polyadenylation signal (polyA2) site (AAT AAA > AAT GAA) (4.2%), −(α)20.5 (3.8%), Hb Constant Spring [Hb CS, α142, Stop→Gln; HBA2: c.427T > C] (2.9%), polyA1 (AATAA A > AATAA G) and αcodon 19 (GCG > GC-, α2) (16%), and - -MED (0.9%). The results of this study may be valuable for designing a plan for carrier screening, premarital genetic counseling, prenatal diagnosis (PND) and reducing excessive health care costs to an affordable level in Isfahan Province, Iran. [ABSTRACT FROM AUTHOR]
- Published
- 2014
- Full Text
- View/download PDF
49. Characterizing a Cohort of α-Thalassemia Couples Collected During Screening for Hemoglobinopathies: 14 Years of an Iranian Experience.
- Author
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Hafezi-Nejad, Nima, Khosravi, Mohsen, Bayat, Nooshin, Kariminejad, Ariana, Hadavi, Valeh, Oberkanins, Christian, Azarkeivan, Azita, and Najmabadi, Hossein
- Subjects
- *
BETA-Thalassemia , *ALPHA-Thalassemia , *HEMOGLOBIN polymorphisms , *GENETIC polymorphisms , *PRENATAL diagnosis , *GENETIC testing , *DIAGNOSIS - Abstract
Our study aimed to determine the number of couples with normal hemoglobin (Hb) electrophoresis and low-borderline hematological values, which may come up with a clinically critical status in their offspring. The number of couples at risk for severe α-thalassemia (α-thal) needed to be estimated before recommending genetic counseling and prenatal diagnosis (PND). During the past 14 years, from at least 7000 referrals, 754 couples were investigated for α-thal by direct mutation detection methods followed by reverse strip assay and α-globin gene sequencing for inconclusive cases. Detection of silent β-thalassemia (β-thal) mutations was done in suspected cases by complete β-globin gene sequencing. We were able to provide a molecular diagnosis in 87.3% (658/754) of couples. A total of 9.1% (60/658) may have a clinically significant hemoglobinopathy in their offspring. Significant conditions included hydrops fetalis (20.0%; 12/60), certain Hb H (β4) genotypes (78.3%; 47/60) and β-thal intermedia (β-TI) (1.7%; 1/60). The diagnostic flowchart for couples with microcytic hypochromic anemia in countries with a high prevalence of hemoglobinopathies should include α and β gene sequencing. As our results indicate, every nine out of 100 of these couples will face significant hemoglobinopathies and every two out of 100 can carry Hb Bart's (γ4) hydrops fetalis in their pregnancies. For such cases, PND should be utilized to allow the carrier couples to decide whether or not to abort the fetus. [ABSTRACT FROM AUTHOR]
- Published
- 2014
- Full Text
- View/download PDF
50. Case Report: Prenatal Diagnosis of Hb Hammersmith [β42(CD1)Phe→Ser; HBB: c.128T > C] in a Family with an Adult Male Patient.
- Author
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Li, Ru, Wang, Ting, Xie, Xing-Mei, and Li, Dong-Zhi
- Subjects
- *
PRENATAL diagnosis , *BETA-Thalassemia , *HEMOGLOBIN polymorphisms , *HEMOGLOBINOPATHY , *HEMOLYTIC anemia , *CYANOSIS , *DIAGNOSIS - Abstract
Hb Hammersmith [β42(CD1)Phe → Ser; HBB: c.128T > C] is a rare, unstable hemoglobin (Hb) variant. In this case report, we describe another male case of Hb Hammersmith. A 39-year-old male had hemolytic anemia, cyanosis and splenomegaly since 6 months after birth. He passed the disease allele to his daughter, a 3-year-old girl, who also had hemolytic anemia and splenomegaly. This mutation was not identified in the parents and two brothers of the father. Early prenatal diagnosis was performed in the second pregnancy in this family. This is the first case of Hb Hammersmith in an adult male patient. [ABSTRACT FROM AUTHOR]
- Published
- 2014
- Full Text
- View/download PDF
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