Your search keyword '"HEMOGLOBINOPATHY diagnosis"' showing total 127 results

1. Hb Bart's immunochromatographic test result and Hb F level in normal cord blood and in selected haemoglobinopathy cases.

Author

Chan, George, Wong, Jenna, and Sami, Viraj

Subjects

*ALPHA-Thalassemia, *BLOOD testing, *ERYTHROCYTES, *DIAGNOSTIC errors, *CLINICAL pathology, *MONOCLONAL antibodies, *CAPILLARY electrophoresis, *IMMUNOASSAY, *SENSITIVITY & specificity (Statistics), *MOLECULAR diagnosis, HEMOGLOBINOPATHY diagnosis

Published

2024

2. A high level of Hb F unmasks a new case of Hb Wanjiang (β (F3‐F4) Ala87_Thr88delinsSer_Gln (HBB:c.255_264 delinsTTTTTCTCAG)) in a pregnant woman of African ancestry.

Author

Pissard, Serge, Moyrand, Claire Bobrie, Peron, Anne, Bodereau, Virginie, Bichr, Allaf, El Osta, Marven, Gouriou, Yann, Ducoroy, Patrick, and Wajcman, Henri

Subjects

*HYPERTENSION, *AFRICANS, *HEMOGLOBINS, *SINGLE nucleotide polymorphisms, *KIDNEY diseases, *MOLECULAR biology, *PREGNANCY, HEMOGLOBINOPATHY diagnosis

Published

2023

3. Comparison of Capillary Zone Electrophoresis with High-pressure Liquid Chromatography in the Evaluation of Hemoglobinopathies.

Author

Madenci, Özlem Çakır, Hürmeydan, Özlem, Orçun, Asuman, and Erdoğmuş, Fatma

Subjects

*HIGH performance liquid chromatography, *CONFIDENCE intervals, *GENETIC mutation, *HEMOGLOBINS, *MEDICAL screening, *CAPILLARY electrophoresis, *COMPARATIVE studies, *DESCRIPTIVE statistics, *ANEMIA, *THALASSEMIA, *LONGITUDINAL method, HEMOGLOBINOPATHY diagnosis

Abstract

Objective: The capillary zone electrophoresis (CZE) and highperformance liquid chromatography (HPLC) methods were compared in terms of HbA2 measurement for the assessment of hemoglobinopathies. Materials and Methods: CZE was compared with HPLC for the evaluation of patients without hemoglobinopathy (n=321), with β-thalassemia trait (n=113), and with common (HbD-Punjab, E, C, S/A, and S/S) and rare (HbS/D, O-Arap, Lepore, G-Coushata, Setif, Hamadan, Q-Iran, and H) variants (n=21). The reference range for HbA2 was determined by CZE. Results: Among patients without hemoglobinopathy, the median (2.5th-97.5th percentiles) values were 97.4% (97.0-98.0%) and 97.5% (96.6-98.4%) for HbA (p=0.060) and 2.4% (1.6-3.0%) and 2.5% (1.6-3.1%) for HbA2 (p<0.001) by HPLC and CZE, respectively. The reference range for HbA2 was 1.6-3.1% by CZE. In the comparison of methods for HbA2, there was a constant error of 0.255 (confidence interval: 0.062-0.448) and bias of 0.10% (limit of agreement: 0.33- 0.53), and higher values were obtained with CZE. A strong correlation was observed between the methods (r=0.782). Interrater agreement was almost perfect for clinical diagnosis (=0.911). The two methods detected and identified the common variants similarly. All rare variants, except HbH by HPLC and HbS/D by CZE, were detected as separate peaks by both methods. Conclusion: The two methods were in agreement regarding the preliminary identification of β-thalassemia patients. Different Hb variants were detected by both methods but with possible methodological interference for HbA2 measurements. CZE is a reliable and simple alternative for the evaluation of hemoglobinopathies. The standardization of HbA2 measurements should be prioritized as more techniques become available in routine laboratory practice [ABSTRACT FROM AUTHOR]

Published

2023

4. The role of molecular diagnostic testing for hemoglobinopathies and thalassemias.

Author

Sabath, Daniel E.

Subjects

*GENETICS of thalassemia, *THALASSEMIA diagnosis, *HEMOGLOBINOPATHY genetics, *MOLECULAR diagnosis, *ELECTROPHORESIS, *INFERTILITY, *HEMOGLOBINOPATHY, *CHROMATOGRAPHIC analysis, *GENETIC counseling, *THALASSEMIA, *DISEASE risk factors, HEMOGLOBINOPATHY diagnosis

Abstract

Hemoglobin disorders are among the most common genetic diseases worldwide. Molecular diagnosis is helpful in cases where the diagnosis is uncertain and for genetic counseling. Protein‐based diagnostic techniques are frequently adequate for initial diagnosis. Molecular genetic testing is pursued in some cases, particularly when a definitive diagnosis is not possible and especially for the purpose of assessing genetic risk for couples wanting to have children. The expertise available in the clinical hematology laboratory is essential for the diagnosis of patients with hemoglobin abnormalities. Initial diagnoses are made using protein‐based techniques such as electrophoresis and chromatography. Based on these findings, genetic risk to an individual's offspring can be assessed. In the setting of β‐thalassemia and other β‐globin disorders, coincident α‐thalassemia may be difficult to diagnose, which can have potentially serious consequences. In addition, unusual forms of β‐thalassemia caused by deletions in the β‐globin locus cannot be definitively characterized using standard techniques. Molecular diagnostic testing has an important role in the diagnosis of hemoglobin disorders and is important in the setting of genetic counseling. Molecular testing also has a role in prenatal diagnosis to identify fetuses affected by severe hemoglobinopathies and thalassemias. [ABSTRACT FROM AUTHOR]

Published

2023

5. Diagnostic Workup of Microcytic Anemia: An Evaluation of Underuse or Misuse of Laboratory Testing in a Hospital Setting Using the AlinIQ System.

Author

Cadamuro, Janne, Simundic, Ana-Maria, von Meyer, Alexander, Haschke-Becher, Elisabeth, Keppel, Martin H., Oberkofler, Hannes, Felder, Thomas K., and Mrazek, Cornelia

Subjects

*THALASSEMIA diagnosis, *ANEMIA diagnosis, *CLINICAL pathology, *PATIENT aftercare, *C-reactive protein, *HEMOGLOBINS, *TRANSFERRIN, *FERRITIN, *IRON, *IRON in the body, *MEDICAL care use, *DESCRIPTIVE statistics, *QUALITY assurance, *ERYTHROCYTES, HEMOGLOBINOPATHY diagnosis

Abstract

* Context.--Underuse of laboratory testing has been previously investigated in preselected populations, such as documented malpractice claims. However, these numbers might not reflect real-life situations. Objective.--To evaluate the underuse and misuse of laboratory follow-up testing in a real-life hospital patient population with microcytic anemia, using laboratory results ordered during routine patient care. Design.--From all patients in whom a microcytic anemia was detected during routine diagnostics in 2018, all available laboratory data were collected and screened for appropriateness of diagnostic workup of iron deficiency and thalassemia. Subgroup analysis was performed for patient groups with mean corpuscular volume values 75 to 79 µm³ (group 1), 65 to 74 µm³ (group 2), and <65 µm³ (group 3). Results.--A total of 2244 patients with microcytic anemia were identified. Follow-up testing for iron deficiency was not performed in 761 cases (34%). For inconclusive ferritin levels due to elevated C-reactive protein results (n = 336), reticulocyte hemoglobin content or soluble transferrin receptor levels were missing in 86 cases (26%). In patients with suspected thalassemia (n = 127), follow-up testing for hemoglobin variants was not performed in 70 cases (55%). Subgroup analysis showed that the frequency of underuse of iron status as well as thalassemia/hemoglobinopathy testing decreased from group 1 to group 3. When considering relevant preexisting anemia diagnoses, laboratory tests were underused in 904 cases (40.3%). Conclusions.--Because 40% (n = 904) of the patients with microcytic anemia were potentially not followed up correctly, laboratory specialists are advised to act by implementing demand management strategies in collaboration with clinicians to overcome underuse of laboratory tests and to improve patient safety. [ABSTRACT FROM AUTHOR]

Published

2023

6. Newborn screening for abnormal haemoglobins in Jamaica: Practical issues in an island programme.

Author

Serjeant, Graham R, Serjeant, Beryl E, Mason, Karlene P, Gibson, Felicea, Gardner, Ruth-Ann, Warren, Lansford, Hambleton, Ian R, Thein, Swee L, Happich, Margit, and Kulozik, Andreas E

Subjects

*HEMOGLOBINS, *HIGH performance liquid chromatography, *SEQUENCE analysis, *MEDICAL screening, *HEMOGLOBINOPATHY, *GENOTYPES, *DESCRIPTIVE statistics, *PHENOTYPES, *BETA-Thalassemia, *SICKLE cell anemia, *CHILDREN, HEMOGLOBINOPATHY diagnosis

Abstract

Objective: To report the diagnostic challenges of newborn screening for abnormal haemoglobins. Setting: Cord blood samples from 13 hospitals in southwest Jamaica taken in 2008–2019. Methods: Blood spots, collected from the umbilical cord, were analysed by high pressure liquid chromatography (HPLC) to reveal phenotypes for HbSS and HbCC, but genotype confirmation may require parental studies or gene sequencing. Such cases that were successfully traced were analysed in this follow-up study. Results: HPLC screening of 121,306 samples detected HbAS in 11,846 (9.8%), HbAC in 4508 (3.7%) and other electrophoretic abnormalities in 1090 babies. Among 101 previously unconfirmed cases, 34/90 (38%) with HPLC evidence of a HbSS phenotype had other genotypes, and 7/11 (64%) with a HbCC phenotype had other genotypes. Syndromes from the interaction of β thalassaemia occurred in 112 babies (85 with HbS, 27 with HbC) and of genes for hereditary persistence of fetal haemoglobin (HPFH) in 18 (12 with HbS, 6 with HbC). Variants other than HbS and HbC occurred in 270 babies, 16 in combination with either HbS or HbC, and 254 as traits. Most variants are benign even when inherited with HbS, although HbO Arab, HbD Punjab, or Hb Lepore Washington, which occurred in 6 cases, may cause sickle cell disease. Conclusions: Genes for β thalassaemia and HPFH are common in western Jamaica and when associated with HbS may present diagnostic challenges in newborns, as HbF and HbA2 have not reached diagnostic levels. Family and DNA studies may be necessary for genotype confirmation. [ABSTRACT FROM AUTHOR]

Published

2022

7. A practical approach for your lab's A1c testing & why your methodology matters.

Author

Wagner, Matthew C.

Subjects

*EDUCATION of medical technologists, *GLYCOSYLATED hemoglobin, *CLINICAL pathology, *PATHOLOGICAL laboratories, *REFERENCE values, *GENETIC mutation, *GLYCEMIC control, *MEDICAL practice, *ANALYTICAL chemistry, HEMOGLOBINOPATHY diagnosis

Abstract

The article discusses the challenges and complexities of hemoglobin A1c (HbA1c) testing, particularly in patients with abnormal hemoglobin due to hemoglobinopathies. Topics include the importance of choosing appropriate HbA1c testing methodologies, highlights the impact of hemoglobin variants, and suggests strategies for laboratories to mitigate the risk of incorrect results in diabetes diagnosis.

Published

2023

8. The hemoglobinopathies, molecular disease mechanisms and diagnostics.

Author

Harteveld, Cornelis L., Achour, Ahlem, Arkesteijn, Sandra J. G., ter Huurne, Jeanet, Verschuren, Maaike, Bhagwandien‐Bisoen, Sharda, Schaap, Rianne, Vijfhuizen, Linda, el Idrissi, Hakima, and Koopmann, Tamara T.

Subjects

*HEMOGLOBINOPATHY genetics, *TISSUE arrays, *CHROMOSOMES, *MOLECULAR diagnosis, *SEQUENCE analysis, *HEMOGLOBINS, *GENETIC testing, *MOLECULAR biology, *SEVERITY of illness index, *GENOTYPES, *GENETIC techniques, *BETA-Thalassemia, *PHENOTYPES, HEMOGLOBINOPATHY diagnosis

Abstract

Hemoglobinopathies are the most common monogenic disorders in the world with an ever increasing global disease burden each year. As most hemoglobinopathies show recessive inheritance carriers are usually clinically silent. Programmes for preconception and antenatal carrier screening, with the option of prenatal diagnosis are considered beneficial in many endemic countries. With the development of genetic tools such as Array analysis and Next Generation Sequencing in addition to state of the art screening at the hematologic, biochemic and genetic level, have contributed to the discovery of an increasing number of rare rearrangements and novel factors influencing the disease severity over the recent years. This review summarizes the basic requirements for adequate carrier screening analysis, the importance of genotype–phenotype correlation and how this may lead to the unrevealing exceptional interactions causing a clinically more severe phenotype in otherwise asymptomatic carriers. A special group of patients are β‐thalassemia carriers presenting with features of β‐thalassemia intermedia of various clinical severity. The disease mechanisms may involve duplicated α‐globin genes, mosaic partial Uniparental Isodisomy of chromosome 11p15.4 where the HBB gene is located or haplo‐insufficiency of a non‐linked gene SUPT5H on chromosome 19q, first described in two Dutch families with β‐thalassemia trait without variants in the HBB gene. [ABSTRACT FROM AUTHOR]

Published

2022

9. Generation of a single‐tube quality control material for hemoglobin and DNA analyses of hemoglobinopathies.

Author

Pansuwan, Anupong, Changtrakul, Duangrudee, Chaibunruang, Attawut, Yamsri, Supawadee, Sanchaisuriya, Kanokwan, Fucharoen, Goonnapa, and Fucharoen, Supan

Subjects

*DNA analysis, *CLINICAL pathology, *HEMOGLOBINS, *GENETIC mutation, *BLOOD collection, *MEDICAL laboratories, *QUALITY control, *QUALITY assurance, *THALASSEMIA, HEMOGLOBINOPATHY diagnosis

Abstract

Introduction: Hemoglobinopathies are major public health problems worldwide. Accurate laboratory diagnosis of the carrier is essential, which includes initial screening, Hb analysis, and DNA analysis. For the first time, we have developed a single‐tube quality control (QC) sample for these laboratory tests. Methods: The QC sample was made from a lyophilized mixture of the stabilized hemolysate with carbon monoxide saturation and the white blood cells of known thalassemia mutations. Homogeneity and stability were examined by Hb and DNA analyses on day 0 and every month for 12 months, at room temperature, 4°C, and −20°C. A preliminary proficiency testing (PT) program for hemoglobinopathies using this single QC material was developed. Results: Hemoglobin (Hb) and DNA analyses of a single‐tube QC sample demonstrated satisfactory results of Hb analysis for at least five months and DNA analysis for at least one year of storage at −20°C. The results obtained from a preliminary PT program on five expert laboratories confirmed that a single tube QC sample prepared could be used as a PT item with various Hb and DNA analyses methods. Conclusion: A single lyophilized control sample has been generated for use in hemoglobinopathies' internal and external quality control program. Unlike other available control materials, which are used for individual testing, a single‐tube QC sample generated can be used to control the pre‐analytical and analytical processes of both Hb and DNA analyses and is suitable for use in the PT program of hemoglobinopathies. [ABSTRACT FROM AUTHOR]

Published

2022

10. The management of haemoglobinopathies in pregnancy and childbirth.

Author

Jackson, Lucy A, Hill, Quentin A, and Ciantar, Etienne

Subjects

*HEMOGLOBINOPATHY genetics, *CHILDBIRTH, *HEMOGLOBINOPATHY, *PREGNANCY, HEMOGLOBINOPATHY diagnosis

Abstract

Key Content: The haemoglobinopathies encompass a complex collection of red blood cell disorders that are responsible for considerable morbidity and mortality in women and their unborn children.Sickle cell disease and the thalassaemias are the commonest haemoglobinopathies encountered in UK clinical practice.A consistent standard of care will enable women with haemoglobinopathies to have a pregnancy that is as safe as possible, with good outcomes and minimal long‐term effects on their health and the health of their babies.The most effective way to deliver a consistent standard of care for these women is via the multidisciplinary team (MDT). The MDT should include a haematologist, cardiologist, maternal medicine obstetrician, specialist midwife, reproductive medicine specialist and a nurse specialist.The care of these women, within the MDT, should start with pre‐conception advice and continue through their antenatal care, intrapartum support and finally, provide postnatal considerations including contraception advice. Learning Objectives: To understand the inheritance, incidence, detection and pathophysiology of the commonest haemoglobinopathies.To appreciate the role of pre‐conception advice and prenatal diagnosis in the management of women with a haemoglobinopathy.To appreciate the multidisciplinary team approach in managing women with these conditions. Ethical Issues: Prenatal diagnostic techniques can be used to diagnose an affected pregnancy; however, diagnosis after conception means families must address the option of terminating the pregnancy. This requires expert counselling to minimise long‐term sequelae.The definitive prenatal tests – chorionic villus sampling and amniocentesis – are both associated with a small risk of miscarriage.Non‐invasive free fetal DNA (ffDNA) tests that will minimise the risk of testing to the developing fetus are being developed, but use of these tests will still require expert counselling both before and after a test is taken. [ABSTRACT FROM AUTHOR]

Published

2022

11. The effect of Voxelotor on quantitation of HbS levels by high‐performance liquid chromatography in a patient with sickle cell disease.

Author

Giacomini, Luca, Puricelli, Chiara, Sacchetti, Sara, Zanotti, Valentina, and Rolla, Roberta

Subjects

*DRUG therapy for sickle cell anemia, *DRUG efficacy, *ANTISICKLING agents, *HEMOGLOBINS, *HIGH performance liquid chromatography, *BILE pigments, *PHLEBOTOMY, *BLOOD transfusion, *TRANSFERASES, *OXIDOREDUCTASES, *PHARMACODYNAMICS, HEMOGLOBINOPATHY diagnosis

Abstract

The article focuses on the impact of Voxelotor, an oral sickle hemoglobin inhibitor, on the quantitation of HbS levels in a patient with sickle cell disease. Topics include the patient's clinical presentation, the challenges in accurately quantifying HbS levels using high-performance liquid chromatography (HPLC) due to Voxelotor treatment, and the importance of providing information about the patient's drug treatment to ensure proper laboratory test interpretation.

Published

2023

12. The association of -related significant hemoglobinopathies and low fetal fraction on noninvasive prenatal screening for fetal aneuploidy.

Author

Putra, Manesha, Idler, Jay, Patek, Kara, Contos, George, Walker, Christopher, Olson, Danielle, Hicks, Melissa A., Chaperon, Jessica, Korzeniewski, Steven J., Patwardhan, Sanjay C., and Sokol, Robert J.

Subjects

*ANEUPLOIDY, *PRENATAL diagnosis, *RETROSPECTIVE studies, *CASE-control method, HEMOGLOBINOPATHY diagnosis

Abstract

Objectives: HBB-related significant hemoglobinopathies have been anecdotally associated with low fetal fraction on noninvasive prenatal screening (NIPS). We sought to compare the difference in fetal fraction using NIPS in women with HBB-related significant hemoglobinopathies (HSH) and women with normal hemoglobin.Study Design: This is a retrospective case-control study. Cases were women with a diagnosis of HSH using NIPS from a commercial laboratory. The comparison group was women with hemoglobin AA from a tertiary care center database. We tested for differences in median fetal fraction using quantile regression analysis, adjusting for maternal body weight and gestational age.Results: This study includes 35 women with clinically significant HSH and a comparison group of 636 women with hemoglobin AA. Adjusting for gestational age and body weight, the median fetal fraction was 4.1 point lower in the HSH than in the comparison group (β - 4.1; 95% -5.7 to -2.5, p < .05). The rate of no-calls due to low fetal fraction was significantly higher in the clinically significant HSH group than in the comparison group [HSH: n = 9/35, 25.7% versus comparison: n = 32/636, 5.0% (p < .001)].Conclusion: Women with HSH were more likely to have a lower fetal fraction and ultimately a five-fold higher no-call rate. What's already known about this topic?Low fetal fraction is one of the most common causes of no-call result in noninvasive prenatal screeningHigh maternal weight, early gestational age and fetal aneuploidies are associated with low fetal fraction What does this study add?HBB-related significant hemoglobinopathies are associated with low fetal fractionReduction in fetal fraction due to HBB-related significant hemoglobinopathies may also result in higher no-call rate. [ABSTRACT FROM AUTHOR]

Published

2021

13. Sky High or Undetectable? A Patient with Discordant Hemoglobin A1c.

Author

Lee, Patricia, Chambliss, Allison B, and Marin, Maximo J

Subjects

*GLYCOSYLATED hemoglobin, *ION exchange chromatography, *CLINICAL pathology, *HIGH performance liquid chromatography, *HEMOGLOBINS, *GLYCEMIC control, *BLOOD sugar monitoring, *BLOOD sugar, *IMMUNOASSAY, *HEMOGLOBINOPATHY, *DYSPNEA, *FACE, *DIAGNOSTIC errors, *MOLECULAR structure, HEMOGLOBINOPATHY diagnosis

Abstract

A female patient aged 47 years presented with a hemoglobin A1c (HbA1c) level of 54.6%, as measured by ion-exchange high-performance liquid chromatography (HPLC), and a glucose level of 106 mg/dL. The HbA1c was re-evaluated using a turbidimetric inhibition immunoassay and found below the level of detection. Hemoglobinopathy testing led to the identification of a hemoglobin variant consistent with Hb Raleigh, in which a valine → alanine substitution on the beta chain effects a charge difference, resulting in coelution with HbA1c on HPLC and a spuriously high reading. Many Hb variants may interfere with HbA1c measurement and generate misleading results. The unique properties of Hb Raleigh may give rise to analytical errors when evaluating HbA1c using 2 different methods—molecular charge–based (eg, HPLC) and molecular structure–based (eg, immunoassay)—yielding diametrically opposed results. Consequently, recognition and diagnosis of this entity are essential in patients with Hb Raleigh, especially when monitoring long-term glucose control. [ABSTRACT FROM AUTHOR]

Published

2021

14. Results from 8 years of the proficiency testing program for diagnosis of hemoglobinopathies under the prevention and control program of thalassemia in Thailand.

Author

Pansuwan, Anupong, Yamsri, Supawadee, Changtrakul, Duangrudee, Fucharoen, Goonnapa, and Fucharoen, Supan

Subjects

*PREVENTIVE health services, *MEDICAL laboratories, *CAPILLARY electrophoresis, *SEVERITY of illness index, *QUALITY assurance, *DESCRIPTIVE statistics, *THALASSEMIA, HEMOGLOBINOPATHY diagnosis

Abstract

Introduction: Hemoglobin (Hb) analysis is a key testing for diagnosis of hemoglobinopathies. Accurate analysis, interpretation of results, and genetic risk assessment are important. We report on 8 years of the proficiency testing (PT) program for hemoglobinopathies in Thailand. Methods: Laboratory participants were required to test two simulated PT items in each cycle using capillary electrophoresis, one was a husband and another was his pregnant wife. Related hematological parameters were provided. The participants also provide interpretation and evaluate the risk of having three severe thalassemia diseases in an expected fetus. Three cycles were operated per year in accordance with the ISO17043 and ISO13528 guidelines. A total of 84 laboratories throughout Thailand were participated. Results: A total of 24 PT cycles were performed during 2012‐2019. Most participants had Excellent performance for the PT items with normal, β‐thalassemia trait, hemoglobin E trait, hemoglobin E trait with α‐thalassemia, and Hb H disease. However, when the PT items with homozygous Hb E and Hb E‐β‐thalassemia were tested, an increase in a Needs improvement performance was noted. From 24 PT cycles, the performance with Excellent, Good, Fair, and Needs improvement was ranging from 10.5%‐95.8%, 0%‐11.3%, 0%‐77.2%, and 2.3%‐37.0%, respectively. Conclusion: Most participants have proven their performance to be reliable and demonstrated their abilities to provide interpretation and genetic risk assessment on most of the PT items. For complex thalassemia however, a need to improve the interpretation and risk assessment skills is required which is essential for effective prevention and control of severe thalassemia diseases in Thailand. [ABSTRACT FROM AUTHOR]

Published

2021

15. Antenatal haemoglobinopathy screening – Experiences of a large Australian Centre.

Author

Ai, Sylvia, Cliffe, Corrina, and Kidson-Gerber, Giselle

Subjects

*BLOOD testing, *DELAYED diagnosis, *PRENATAL diagnosis, *ACQUISITION of data methodology, *HIGH performance liquid chromatography, *HEMOGLOBINS, *ELECTROPHORESIS, *MEDICAL screening, *RETROSPECTIVE studies, *GENETIC testing, *GESTATIONAL age, *HEMOGLOBINOPATHY, *PREGNANCY complications, *BLOOD diseases, *MEDICAL records, HEMOGLOBINOPATHY diagnosis

Abstract

Background: Antenatal screening is vital to identifying couples at risk of having children with a clinically significant haemoglobinopathy. In Australia, immigration is increasing carrier incidence. Methods: A retrospective analysis was performed of full blood count, high-performance liquid chromatography and haemoglobin electrophoresis of women and their partners who underwent antenatal haemoglobinopathy screening over three years at a major NSW laboratory. Genetic testing results were included where available. Results: One thousand six hundred and twenty-eight women and 729 male partners were screened at a median gestation of 14 weeks. 8.2% of women had a clinically significant result, with a median 16-day interval to partner testing. In 35% of couples screened simultaneously, the partner did not require testing. Genetic confirmatory testing was performed in 65% of high risk couples. Conclusion: There was a significant delay to antenatal haemoglobinopathy screening for mothers, limiting time for genetic diagnosis, prenatal diagnosis and management of affected pregnancies. Screening should be performed earlier. Simultaneous couple testing is not cost-effective. [ABSTRACT FROM AUTHOR]

Published

2021

16. Diagnosis of Hemoglobin M Disease in a Toddler Presenting With Hypoxemia and Hemolysis.

Author

Picca, Andrew, Ruthford, Mason, Ghanim, Majd T., Sims, Morgan, and Kanter, Julie

Subjects

*REACTIVE oxygen species, *ANEMIA, *HYPOXEMIA, *BODY temperature, *HEMOLYSIS & hemolysins, *INBORN errors of metabolism, *METHEMOGLOBINEMIA, *OXYGEN in the body, *TACHYCARDIA, HEMOGLOBINOPATHY diagnosis

Abstract

The article present case study of a 20-month-old male with complaints of 1 day of fever in the setting of 2 weeks of upper respiratory symptoms. Further discusses finding of hypoxemia, severe anemia and hemolysis; and Hemoglobin electrophoresis performed by Mayo Clinic later confirmed Hemoglobin M-Hyde Park.

Published

2019

17. Hemoglobinopathies in the North of Morocco: Consanguinity Pilot Study.

Author

Laghmich, Achraf, Alaoui Ismaili, Fatima Zahra, Zian, Zeineb, Barakat, Amina, Ghailani Nourouti, Naima, and Bennani Mechita, Mohcine

Subjects

*HEMOGLOBINOPATHY genetics, *CONSANGUINITY, *HEMOGLOBINOPATHY, *MARRIAGE, *RISK assessment, *PILOT projects, *DISEASE incidence, *DISEASE risk factors, HEMOGLOBINOPATHY diagnosis

Abstract

Consanguinity is a social behavior characterized by the arrangement of marriages between relatives. It coincides generally with the geographic distribution of recessive genetic diseases as it increases the likelihood of homozygosis and, consequently, the incidence of their pathologies in the population. In this pilot study, we assess the effect of inbreeding on the burden of hemoglobinopathies in Northern Morocco. From January 2016 to December 2018, 197 children born in the studied region to three ancestral generations and diagnosed with hemoglobinopathies were subject to investigation. The rate of consanguinity in the parents' generation of children with hemoglobinopathies was 50.25%, with first cousin marriages accounting for 68.69% of consanguineous unions (FI = 0.02). The corresponding rates in the general population, based on a sample of N = 900, were 29.67% and 82.02%, respectively. The marriages between first cousins are the most common among the other types of consanguineous unions. Our study propounds that consanguinity substantially contributes to the hemoglobinopathy burden in the studied region and has changed little over time. Refraining from consanguineous marriages and detecting couples at risk could contribute to the reduction of the incidence of genetic diseases in our country. [ABSTRACT FROM AUTHOR]

Published

2019

18. Early prenatal diagnosis of hemoglobinopathies by celocentesis is ready for use in routine clinical practice.

Author

Giambona, Antonino, Leto, Filippo, Cassarà, Filippo, Tartaglia, Viviana, Marchese, Giuseppe, Orlandi, Emanuela, Cigna, Valentina, Picciotto, Francesco, Maggio, Aurelio, and Vinciguerra, Margherita

Subjects

*PRENATAL diagnosis, *MEDICAL practice, HEMOGLOBINOPATHY diagnosis

Published

2023

19. Severe Anemia in the Newborn Nursery.

Author

Miller, Jennifer J. and Seske, Laura M.

Subjects

*ACUTE kidney failure, *ATRIAL septal defects, *NEONATAL jaundice, *VITAMIN K, *CEFOTAXIME, *AMPICILLIN, *ERYTHROCYTES, *ALANINE, *ANEMIA, *ARTIFICIAL respiration, *ASPARTATE aminotransferase, *BLOOD, *BLOOD cell count, *BLOOD coagulation disorders, *BLOOD platelet transfusion, *CELL culture, *CHEST X rays, *CREATININE, *CRYOPRESERVATION of organs, tissues, etc., *CUTANEOUS manifestations of general diseases, *ECHOCARDIOGRAPHY, *RED blood cell transfusion, *HEART murmurs, *HEMODYNAMICS, *HEMOGLOBINS, *NEWBORN screening, *NEONATAL intensive care, *PHOTOTHERAPY, *RARE diseases, *SHOCK (Pathology), *URINALYSIS, *NEONATAL intensive care units, *BLOOD urea nitrogen, *UMBILICAL cord clamping, *CONGENITAL hemolytic anemia, *SPLENIC rupture, *DISEASE complications, *CHILDREN, *DIAGNOSIS, *THERAPEUTICS, *VITAMIN therapy, *DISEASE risk factors, HEMOGLOBINOPATHY diagnosis, ULTRASONIC imaging of the abdomen

Abstract

The article presents a case study of a female infant with splenic rupture with multiple etiologies. It notes the complete blood count (CBC) and echocardiogram for atrial septal defect, transferred to the neonatal intensive care unit and low hemoglobin, with the examination of a had ultrasound and abdominal ultrasound.

Published

2019

20. The phenotypic and molecular diversity of hemoglobinopathies in India: A review of 15 years at a referral center.

Author

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.

Subjects

*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

21. Prenatal and preimplantation diagnosis of hemoglobinopathies.

Author

Vrettou, C., Kakourou, G., Mamas, T., and Traeger‐Synodinos, J.

Subjects

*BIOPSY, *CLINICAL pathology, *FERTILIZATION in vitro, *HEMATOPOIETIC stem cell transplantation, *HUMAN reproductive technology, *LEUCOCYTES, *GENETIC mutation, *OVUM, *PREIMPLANTATION genetic diagnosis, *PRENATAL diagnosis, *ZYGOTES, *EMBRYOS, HEMOGLOBINOPATHY diagnosis

Abstract

Abstract: The hemoglobinopathies, as a group, are one of the most common serious monogenic diseases in the world. An accepted and widely adopted approach to reduce the number of new cases involves carrier‐screening programs, with the option of prenatal diagnosis (PND) or preimplantation diagnosis (preimplantation genetic testing for monogenic disease, PGT‐M) for carrier couples. The aim of PND is to provide an accurate result as early in pregnancy as possible, which necessitates prior identification of the parental disease‐causing mutations, as well as safe and timely biopsy of fetal material. PGT‐M aims to characterize the genetic status of in vitro fertilized embryos during assisted reproductive technology (ART), in a few cells biopsied from oocytes/zygotes or embryos, in order to initiate an unaffected pregnancy. Another application of PGT‐M is preimplantation genetic diagnosis for human leukocyte antigen (PGD‐HLA), which, in addition to identifying unaffected embryos, also characterizes the embryos that are HLA compatible with an existing affected child requiring a hemopoietic stem cell transplantation (HSCT). This review outlines the current practices related to these procedures, with emphasis on the aspects related to laboratory techniques. Finally, future prospects related to developments in noninvasive prenatal diagnosis are discussed. [ABSTRACT FROM AUTHOR]

Published

2018

22. Haemoglobin Titusville: A case study and review of the literature.

Author

Mina, Mina, James, Radhika, and Gandhi, Salil

Subjects

*HEMOGLOBINOPATHY, *HEMOGLOBIN genetics, *HEMOGLOBIN polymorphisms, *BLOOD diseases, *PHYSIOLOGICAL effects of nucleotides, *BLOOD gases analysis, *HEMOGLOBINS, *OXYGEN, HEMOGLOBINOPATHY diagnosis

Abstract

The article presents a case study that involves an asymptomatic neonate with reduced peripheral oxygen saturations (SpO2), whereby the patient's father has a confirmed rare haemoglobinopathy, haemoglobin Titusville. It reports that Haemoglobin Titusville is a low-oxygen affinity haemoglobinopathy involving a single nucleotide change from G to A at codon 94 of the alpha globin gene.

Published

2018

23. A Healthy Infant Incidentally Presenting With Low SpO2: The Pitfalls of Pulse Oximetry.

Author

Vanner, Robert, Cho, Romy, and Weinstein, Michael

Subjects

*PULSE oximeters, *ACTIVE oxygen in the body, *CONSTIPATION, *DIFFERENTIAL diagnosis, *ELECTROCARDIOGRAPHY, *HOSPITAL emergency services, *OXIMETRY, *WHITE people, HEMOGLOBINOPATHY diagnosis

Abstract

The article presents a case of 7-month-old white female infant with parental concerns of constipation. The infant was placed on supplemental oxygen by nasal cannula with no improvement. She presented mild anemia and trace carboxyhemoglobin in blood. Bubble-contrast echocardiogram suggested a right-to-left shunt or a patent formane ovale. Chest computed tomography and abdominal ultrasound were normal.

Published

2018

24. New challenges in diagnosis of haemoglobinopathies: Migration of populations.

Author

Old, John, Timbs, Adele, McCarthy, Janice, Gallienne, Alice, Proven, Melanie, Rugless, Michelle, Lopez, Herminio, Eglinton, Jennifer, Dziedzic, Dariusz, Beardsall, Matthew, Khalila, Mohamed S. M., and Henderson, Shirley

Subjects

*HEALTH of immigrants, *GENETIC mutation, HEMOGLOBINOPATHY diagnosis

Abstract

The current influx of economic migrants and asylum seekers from countries with a high prevalence of haemoglobinopathies creates new challenges for health care systems and diagnostic laboratories. The migration of carriers introduces new and novel haemoglobinopathy mutations to the diagnostic repertoire of a laboratory, often creating new pressures to improve and update the carrier screening technology and diagnostic scope. For antenatal screening programmes, the marriage of partners from different ethnic groups can lead to the risk of compound heterozygote children being born novel mutation combinations, creating problems in the provision of accurate advice regarding the expected phenotype of the thalassaemia or haemoglobinopathy disorder. In the UK, the impact of immigration required the National Haemoglobinopathy Reference laboratory to change the strategy and techniques used for the molecular diagnosis of thalassaemia and the haemoglobinopathies. In 2005, due to the increasingly large range of β-thalassaemia mutations that needed to be diagnosed, the laboratory switched from a three-step screening procedure using ARMS-PCR to a simpler but more expensive one-step strategy of DNA sequencing of the beta and alpha globin genes for all referrals. After ten years of employing this strategy, a further 57 novel thalassaemia and haemoglobionpopthy alleles were discovered (11 new β-chain variants, 15 α-chain variants, 19 β-thalassaemia mutations and 12 α+-thalassaemia mutations), increasing further the extremely heterogeneous spectrum of globin gene mutations in the UK population. [ABSTRACT FROM AUTHOR]

Published

2018

25. Co-inheritance of α0-thalassemia elevates Hb A2 level in homozygous Hb E: Diagnostic implications.

Author

Singha, K., Srivorakun, H., Fucharoen, G., and Fucharoen, S.

Subjects

*HEMOGLOBINOPATHY genetics, *DNA analysis, *ALPHA-Thalassemia, *BIOMARKERS, *CAPILLARY electrophoresis, *DIFFERENTIAL diagnosis, *HEMOGLOBINS, *GENETIC mutation, *POLYMERASE chain reaction, *PROBABILITY theory, *RESEARCH funding, *T-test (Statistics), *DATA analysis software, *DESCRIPTIVE statistics, *IN vitro studies, *GENOTYPES, *GENETICS, *DIAGNOSIS, HEMOGLOBINOPATHY diagnosis

Abstract

Introduction Differentiation of homozygous hemoglobin (Hb) E with and without α0-thalassemia is subtle on routine hematological ground. We examined in a large cohort of homozygous Hb E if the level of Hb A2 is helpful. Methods A total of 592 subjects with homozygous Hb E were recruited from ongoing thalassemia screening program. Additionally, five couples at risk of having fetuses with Hb Bart's hydrops fetalis who were homozygous Hb E were also investigated. Hb analysis was performed using capillary electrophoresis system. Globin genotypes were defined by DNA analysis. Results Subjects were classified into four groups including pure homozygous Hb E (n=532), homozygous Hb E/α0-thalassemia (n=48), Hb Constant Spring EE Bart's disease (n=8), and Hb EE Bart's disease (n=4). The levels of Hb A2 were found, respectively, to be 4.97±0.69, 6.64±1.02, 4.86±0.87, and 7.60±1.04%. Among five couples at risk, α0-thalassemia was identified in three subjects with Hb A2>6.0%. Conclusions Increased Hb A2 level is a useful marker for differentiation of homozygous Hb E with and without α0-thalassemia. This should lead to a significant reduction in number of referral cases of homozygous Hb E for molecular testing of α0-thalassemia in routine practice. [ABSTRACT FROM AUTHOR]

Published

2017

26. HBB : c.316-125A>G and HBB : c.316-42delC: Phenotypic Evaluations of Two Rare Changes in the Second Intron of the HBB Gene.

Author

Vinciguerra, Margherita, Cannata, Monica, Cassarà, Filippo, Passarello, Cristina, Leto, Filippo, Calvaruso, Giuseppina, Renda, Disma, Maggio, Aurelio, and Giambona, Antonino

Subjects

*PRENATAL diagnosis, *POINT mutation (Biology), *GLOBIN genes, *PHENOTYPES, HEMOGLOBINOPATHY diagnosis

Abstract

We report two very rare changes in the second intron of theHBBgene, a substitution at nucleotide (nt) 726 [IVS-II-726 (A>G) (β+), NM_000518,HBB: c.316-125A>G] and a deletion of a cytosine at nt 809 [IVS-II-809 (–C) (β), NM_000518,HBB: c.316-42delC] identified during the screening program for hemoglobinopathies in the resident Sicilian population. The purpose of this study was to evaluate the clinical implication of these rare changes, particularly in coinheritance with known mutations in the globin clusters, in order to conduct an appropriate genetic counseling for at-risk couples. Molecular analysis detected the first rare nt substitution in two cases in simple heterozygosity and in two cases in association with other known mutations on globin genes, while the deletion was identified in a pregnant woman, carrier of β-thal, and in her fetus at prenatal diagnosis (PND) for hemoglobinopathies. The present study emphasizes the importance of sharing the observed changes in the globin gene cluster, especially in the case of new or rare undefined mutations, in order to facilitate the determination of their phenotypic expression and possible interactions with known molecular defects. [ABSTRACT FROM AUTHOR]

Published

2017

27. The epidemiologic transition of thalassemia and associated hemoglobinopathies in southern Taiwan.

Author

Wang, Hui-Ching, Hsieh, Li-Ling, Liu, Yi-Chang, Hsiao, Hui-Hua, Lin, Shu-Kai, Tsai, Wen-Chan, and Liu, Ta-Chih

Subjects

*THALASSEMIA diagnosis, *EPIDEMIOLOGY, *HEMOGLOBINOPATHY, *INTERRACIAL marriage, *EMIGRATION & immigration, *NUCLEOTIDE sequencing, *GENETIC mutation, *THALASSEMIA, *ALPHA-Thalassemia, *BETA-Thalassemia, *SEQUENCE analysis, *GENOTYPES, HEMOGLOBINOPATHY diagnosis

Abstract

Since 1993, following the National Thalassemia Major Prevention Program and an increase in immigration and interracial marriages, especially in southern Taiwan, the distribution of hemoglobinopathies may have changed. This study investigates the epidemiologic transition of hemoglobinopathies. We analyzed 1870 specimens collected between 2003 and 2012 in southern Taiwan, used gap-polymerase chain reaction and PCR-restriction fragment length polymorphism-based methods, and confirmed genotypes of hemoglobinopathies by DNA sequencing. We found a 91% reduction in the incidence of thalassemia major compared with samples from between 1986 and 1995. The most common genotypes of α-thalassemia and α Hb variants were the SEA type (69.4%) and Hb Quong Sze (1.54%). The most common genotypes of β-thalassemia and β Hb variants were IVS-II-654 (46.2%) and Hb E (2.2%), respectively. Compared with studies performed in different areas of and time intervals in Taiwan, a higher prevalence of -α3.7, Hb Quong Sze, and Hb E and a lower prevalence of the SEA type were found in this study. However, the SEA type remained the most common genotype observed. In addition, an increasing number of cases with an -α3.7 type carrier, Hb Quong Sze carrier, and Gγ(Aγδβ)° were identified following a peak of interracial marriages between 2003 and 2005, reflecting a regional difference and the impact of interracial marriage. In conclusion, global migration and international marriage have changed the distribution of hemoglobinopathies in Taiwan. A more comprehensive prenatal screening for new immigrants with a longer follow-up is warranted. [ABSTRACT FROM AUTHOR]

Published

2017

28. Mass Spectrometry-Based Diagnosis of Hemoglobinopathies: A Potential Tool for the Screening of Genetic Disorder.

Author

Das, Rajdeep, Mitra, Gopa, Mathew, Boby, Bhat, Vijay, Ross, Cecil, Pal, Debnath, and Mandal, Amit

Subjects

*GENETIC disorders, *MEDICAL screening, *HEMOGLOBINS, *GEL electrophoresis, HEMOGLOBINOPATHY diagnosis

Abstract

Hemoglobinopathies are caused by point mutation in globin gene that results in structural variant of hemoglobin. While 7 % of world populations are carrier of hemoglobinopathies, the prevalence of the disease varies between 3 to 17 % across different population groups in India. In a diagnostic laboratory, alkaline gel electrophoresis and cation exchange-based HPLC (CE-HPLC) are most widely used techniques for characterization of hemoglobin variants. In the above methods, the differential surface charge of hemoglobin molecule in variants is exploited for their characterization. Sometime, co-migration of variants in gel electrophoresis and co-elution or elution with unknown retention time in automated CE-HPLC might lead to ambiguity in the analysis of hemoglobinopathies. Under such circumstances, it is necessary to use other analytical methods that provide unambiguous results. Mass spectrometry-based proteomics approach and DNA sequence analysis are examples of such alternative methods. In the present study, liquid chromatography coupled to mass spectrometry has been used for three commonly observed variants in India, e.g., HbE, HbQ India and HbD Punjab that appeared with inappropriate results in the conventional analysis. A customized hemoglobin variant database has been used in the mass spectrometry-based analysis of those three variants. Mass spectrometry-based proteomics approach was used to analyze above variant sample accurately. [ABSTRACT FROM AUTHOR]

Published

2016

29. CT abdominal imaging findings in patients with sickle cell disease: acute vaso-occlusive crisis, complications, and chronic sequelae.

Author

Gardner, Carly, Boll, Daniel, Bhosale, Priya, and Jaffe, Tracy

Subjects

*SICKLE cell anemia diagnosis, *COMPUTED tomography, *DIAGNOSIS of abdominal pain, *HEPATIC veno-occlusive disease, *MICROCIRCULATION disorders, *SICKLE cell anemia, *PATIENTS, HEMOGLOBINOPATHY diagnosis

Abstract

Sickle cell disease (SCD) is the most prevalent hemoglobinopathy. Survival in patients with SCD has improved over the past few decades. These patients experience a lifetime of repeated acute pain crises, which are thought to result from sickling and microvascular occlusions; acute abdominal pain is common. Moreover, repeated crises often lead to organ dysfunction, such as asplenia, hepatic failure, and renal failure. The spleen, liver, biliary system, kidneys, and gastrointestinal tract can all be affected. Patients may undergo CT to further direct clinical management. We review the spectrum of CT imaging findings of abdominal manifestations in patients with SCD, from the acute microvascular occlusive pain crisis to the potential complications and chronic sequelae. [ABSTRACT FROM AUTHOR]

Published

2016

30. Type and frequency of hemoglobinopathies, diagnosed in the area of Karachi, in Pakistan.

Author

Shabbir, Shaista, Nadeem, Muhammad, Sattar, Abdul, Ara, Iffat, Ansari, Saqib, Farzana, Tassneem, Taj, Mehwish, Borhany, Munira, Manzir, Saima, Zaidi, Uzma, Hassan, Jawad, Naz, Arshi, Shamsi, Tahir, and Schumacher, Udo

Subjects

*BLOOD sampling, *BONE marrow transplantation, *HEMOGLOBINS, *ELECTROPHORESIS, *HIGH performance liquid chromatography, *DISEASE prevalence, HEMOGLOBINOPATHY diagnosis

Abstract

Hemoglobinopathies are one of the major problems in Pakistan. A retrospective analysis of blood samples of 2731 patients from 2010 to 2014 was done at National Institute of Blood Disease & Bone Marrow Transplantation for the workup of anemia or other blood-related disorders. Whole blood samples in EDTA were collected; complete blood counts with peripheral smears were prepared. Hemoglobin (Hb) electrophoresis on Genio was performed at alkaline pH. Samples showing borderline results were further tested by high-performance liquid chromatography or for specific mutation analysis by ARMS-PCR. Out of total 2731, 935 (34.2%) patients had hemoglobinopathies. Out of these 935 patients who had hemoglobinopathies, beta thalassemia minor 51.8%, beta thalassemia major 24.1%, HbD trait 6.7, sickle/ beta thalassemia 4.5%, sickle cell disease 3.9%, HbE trait 1.9%, and sickle cell trait 1.7% were most common hemoglobinopathies. Less prevalent were delta/beta thalassemia, HbE homozygous, HbD homozygous, and HbH disease. [ABSTRACT FROM AUTHOR]

Published

2016

31. Oxygen Saturation of 75%, but No Symptoms!

Author

Guler, Sabina, Brunner-agten, Saskia, Bartenstein, Sophia, Bettschen, Hans Ueli, Geiser, Thomas, Keller, Peter, and Funke, Manuela

Subjects

*ACTIVE oxygen in the body, *GENETIC mutation, *SPECTROPHOTOMETRY, HEMOGLOBINOPATHY diagnosis

Published

2016

32. Erroneous HbA1c results in a patient with elevated HbC and HbF.

Author

Adekanmbi, Joy, Higgins, Trefor, Rodriguez-Capote, Karina, Thomas, Dylan, Winterstein, Jeffrey, Dixon, Tara, Gifford, Jessica L., Krause, Richard, Venner, Allison A., Clarke, Gwen, and Estey, Mathew P.

Subjects

*DIABETES, *HEMOGLOBINS, *MOLECULAR biology, *ELECTROPHORESIS, *CRYSTALLOGRAPHY, HEMOGLOBINOPATHY diagnosis

Abstract

Background HbA1c is used in the diagnosis and monitoring of diabetes mellitus (DM). Interference from hemoglobin variants is a well-described phenomenon, particularly with HPLC-based methods. While immunoassays may generate more reliable HbA1c results in the presence of some variants, these methods are susceptible to negative interference from high concentrations of HbF. We report a case where an accurate HbA1c result could not be obtained by any available method due to the presence of a compound hemoglobinopathy. Methods HbA1c was measured by HPLC, immunoassay, and capillary electrophoresis. Hemoglobinopathy investigation consisted of a CBC, hemoglobin fractionation by HPLC and electrophoresis, and molecular analysis. Results HbA1c analysis by HPLC and capillary electrophoresis gave no result. Analysis by immunoassay yielded HbA1c results of 5.9% (Siemens DCA 2000 +) and 5.1% (Roche Integra), which were inconsistent with other markers of glycemic control. Hemoglobinopathy investigation showed HbC with the hereditary persistence of fetal hemoglobin-2 Ghana deletion. Conclusion Reliable HbA1c results may be unobtainable in the presence of some hemoglobinopathies. HPLC and capillary electrophoresis alerted the laboratory to the presence of an unusual hemoglobinopathy. Immunoassays generated falsely low results without warning, which could lead to missed diagnoses and under treatment of patients with DM. [ABSTRACT FROM AUTHOR]

Published

2016

33. Real-life experience with liver iron concentration R2 MRI measurement in patients with hemoglobinopathies: baseline data from LICNET.

Author

Vitrano, Angela, Calvaruso, Giuseppina, Tesé, Lorenzo, Gioia, Francesco, Cassarà, Filippo, Campisi, Saveria, Butera, Franco, Commendatore, Valeria, Rizzo, Michele, Santoro, Vincenzo, Cigna, Valeria, Quota, Alessandra, Bagnato, Sabrina, Argento, Crocetta, Fidone, Carmelo, Schembari, Dario, Gerardi, Calogera, Barbiera, Filippo, Bellisssima, Giuseppe, and Giugno, Giovanni

Subjects

*MAGNETIC resonance imaging, *FERRITIN genetics, *CROSS-sectional method, *SICKLE cell anemia, HEMOGLOBINOPATHY diagnosis

Abstract

Background Real-life data on the use of R2 MRI for the assessment of liver iron concentration ( LIC) remain limited. Methods We conducted a cross-sectional analysis on 363 patients (mean age 35.6 yr, 44.1% men) with hemoglobinopathies (204 β-thalassemia major [ TM], 102 β-thalassemia intermedia [ TI], and 57 sickle cell disease [ SCD]) that were evaluated with R2 MRI as part of LICNET, an MRI network of 13 Italian treatment centers. Results The mean LIC was 7.8 mg/g (median: 4.0), with high LIC (>7 mg/g) noted in both transfused ( TM, TI 37%; SCD 38%) and non-transfused ( TI 20%) patients. Ferritin levels correlated with LIC in both transfused ( TM, TI, SCD) and non-transfused ( TI) patients ( P < 0.001), although lower values predicted high LIC in non-transfused patients (1900 vs. 650 ng/mL in TM vs. non-transfused TI). A correlation between LIC and ALT levels was only noted in HCV-negative patients (rs = 0.316, P < 0.001). The proportion of patients with high LIC was significantly different between iron chelators used ( P = 0.023), with the lowest proportion in deferasirox (30%) and highest in deferiprone (53%)-treated patients. Conclusions High LIC values persist in subgroups of patients with hemoglobinopathy, warranting closer monitoring and management optimization, even for non-transfused patients with relatively low ferritin levels. [ABSTRACT FROM AUTHOR]

Published

2016

34. Hb A1c Separation by High Performance Liquid Chromatography in Hemoglobinopathies.

Author

Chandrashekar, Vani

Subjects

*HIGH performance liquid chromatography, *GLYCOSYLATED hemoglobin, *HEMOGLOBINOPATHY, *CHROMATOGRAMS, *BETA-Thalassemia, *PATIENTS, HEMOGLOBINOPATHY diagnosis

Abstract

Hb A1c measurement is subject to interference by hemoglobin traits and this is dependent on the method used for determination. In this paper we studied the difference between Hb A1c measured by HPLC in hemoglobin traits and normal chromatograms. We also studied the correlation of Hb A1c with age. Hemoglobin analysis was carried out by high performance liquid chromatography. Spearman’s rank correlation was used to study correlation between A1c levels and age. Mann-Whitney U test was used to study the difference in Hb A1c between patients with normal hemoglobin and hemoglobin traits. A total of 431 patients were studied. There was positive correlation with age in patients with normal chromatograms only. No correlation was seen in Hb E trait or beta thalassemia trait. No significant difference in Hb A1c of patients with normal chromatograms and patients with hemoglobin traits was seen. There is no interference by abnormal hemoglobin in the detection of A1c by high performance liquid chromatography. This method cannot be used for detection of A1c in compound heterozygous and homozygous disorders. [ABSTRACT FROM AUTHOR]

Published

2016

35. Effectiveness of Prenatal Screening for Hemoglobinopathies in a Developing Country.

Author

Choudhuri, Soumita, Sen, Aditi, Ghosh, Malay Kumar, Misra, Sanjay, and Bhattacharyya, Maitreyee

Subjects

*MEDICAL screening, *PRENATAL diagnosis, *HEMOGLOBINOPATHY, *THALASSEMIA in children, *PATIENTS, *DIAGNOSIS, HEMOGLOBINOPATHY diagnosis

Abstract

The thalassemias are among the most common monogenic diseases worldwide, a national health burden in India. There are estimated 7500–12,000 babies born with β-thalassemia major (β-TM) every year in this country. Couples who are at-risk of having children with hemoglobin (Hb) disorders desired to have the option of avoiding the birth of an affected child by prenatal diagnosis (PND). Thus, the prenatal women are a highly important target group for carrier screening and preventing the birth of thalassemic children in the country. The present study was conducted among 20,883 pregnant women, irrespective of gravida and duration of pregnancy, from the prenatal clinic of Nilratan Sarkar (NRS) Medical College & Hospital, Kolkata, West Bengal, India, from February 2009 to November 2012. Thalassemia carrier status was assessed by high performance liquid chromatography (HPLC) along with red blood cell (RBC) indices. Husbands of all thalassemia carrier women were advised and persuaded to undergo screening for hemoglobinopathies. The couples were counseled to undergo PND if both of them were detected to be thalassemia carriers. The data were statistically analyzed to evaluate the efficacy of this procedure. [ABSTRACT FROM AUTHOR]

Published

2015

36. Identification of Hb Wayne and its effects on HbA1c measurement by 5 methods.

Author

Rodríguez-Capote, Karina, Estey, Mathew P., Barakauskas, Vilte E., Burton, Teralee, Holmes, Deborah, Krause, Richard, and Higgins, Trefor N.

Subjects

*TYPE 2 diabetes diagnosis, *DIAGNOSTIC errors, *ELECTROPHORESIS, *HIGH performance liquid chromatography, HEMOGLOBINOPATHY diagnosis

Abstract

Background The World Health Organization and the American and Canadian Diabetes Associations approved HbA1c > 6.5% as diagnostic for type 2 diabetes mellitus (T2DM). Hb variants and/or their chemically modified species can interfere with HbA1c measurements. We recently described a patient with Hb Wayne trait who was misdiagnosed with T2DM based on falsely elevated HbA1c. Hb Wayne is a clinically silent variant that exists as two isoforms: Hb Wayne I (Asn 139) and Hb Wayne II (Asp 139). Methods Hemoglobinopathy investigation was performed by HPLC (Bio-Rad VARIANT-II), alkaline and acid electrophoresis (Sebia Hydrasis2), capillary zone electrophoresis (Sebia CAPILLARYS2™) and DNA sequencing. HbA1c was measured by five methods. Results Hb Wayne eluted as two small fractions with retention times of 1.0 and 1.46 min on the HPLC (Bio-Rad VARIANT-II). Alkaline gel and capillary electrophoresis showed two small bands migrating faster than HbA. Hb Wayne generated spuriously high results on the Bio-Rad VARIANT-II Turbo 2.0, no results on the Tosoh G8, and did not interfere with either the Sebia CAPILLARYS2™ or immunoassays from Roche (tinaquant) and Siemens (Bayer DCA2000 +). Based on the Hb Wayne HPLC profile of 3 patients, an algorithm was developed to facilitate its detection, which identified 9 additional patients with Hb Wayne trait. Conclusions We characterize Hb Wayne by chromatographic and electrophoretic techniques and show the effect of Hb Wayne on five common HbA1c methodologies. We developed a quality assurance tool to assist in detecting Hb Wayne trait during HbA1c analysis on the Bio-Rad VARIANT-II™ Turbo 2.0. [ABSTRACT FROM AUTHOR]

Published

2015

37. Prevalence of hemoglobinopathies in different regions and castes of Uttar Pradesh, India - A hospital based study.

Author

Verma, Pratima, Ghildiyal, Archna, Verma, Dileep, Krishna, Akhilesh, Singh, Shraddha, Kumar, Ashutosh, and Tiwari, Sunita

Subjects

*DISEASE prevalence, HEMOGLOBINOPATHY diagnosis

Abstract

Background: Thalasemia and other hemoglobinopathies are found in all the states of India and their prevalence is quite variable. In Uttar Pradesh very few studies are found which explore the spectrum of hemoglobinopathies. There is no such study which identifies the geographic distribution of high-risk communities with frequencies of hemoglobinopathies. Aim: Present study was carried out to determine the prevalence of hemoglobinopathies in different regions and castes of Uttar-Pradesh (UP) state. Materials and Methods: This is a preliminary community based cross-sectional, hospital based study, conducted at King George's Medical University, Lucknow, Uttar-Pradesh. Subjects aged between 18 to 65 years were enrolled for sampling. The anticoagulated blood was used for performing CBC (complete blood count), and hemoglobin electrophoresis to measure hemoglobinopathies. Results: The present study revealed higher(28/194;19.5%,p<0.05) prevalence of hemoglobinopathies in Lucknow district as compared to other districts of Uttar-Pradesh and Brahmin caste having high frequency (33/112;29.5%) followed by Jaiswal (3/13;23.1%) and Arora (2/9;22.2%). Conclusion: The data regarding prevalence and distribution can be useful in prevention and management of various hemoglobinopathies which play a vital role in the hospital blood bank as well as in the formulation of transfusion policies. [ABSTRACT FROM AUTHOR]

Published

2015

38. Diagnostic strategies in hemoglobinopathy testing, the role of a reference laboratory in the USA.

Author

Oliveira, Jennifer L.

Subjects

*MEDICAL care, *GENETIC mutation, HEMOGLOBINOPATHY diagnosis

Abstract

Although commonly assessed in the context of microcytosis or sickling syndrome screening, hemoglobin mutations may not be as readily considered as a cause of other symptoms. These include macrocytosis with or without anemia, chronic or episodic hemolysis, neonatal anemia, erythrocytosis, cyanosis/hypoxia and methemoglobinemia/sulfhemoglobinemia. Hemoglobin disorders commonly interfere with the reliability of Hb A1c measurement. Because the clinical presentation can be varied and the differential diagnosis broad, a systematic evaluation guided by signs and symptoms can be effective. A tertiary care reference laboratory is particularly challenged by the absence of pertinent clinical history and relevant laboratory findings, and appropriate use of resources in a data vacuum can be problematic. To address these issues, our laboratory has constructed testing panels with a tiered strategy utilizing screening assays that detect the most common causes and reflexing additional assays that assess less common etiologies. See Figure 1. Our testing algorithm panels include a rapid hemoglobin fraction monitoring test, a generic diagnostic hemoglobin electrophoresis profile, and more specific diagnostic evaluations for microcytic anemia, hereditary hemolytic anemia, methemoglobinemia and sufhemoglobinemia and erythrocytosis. Use of these testing strategies has facilitated the identification of rare and complex hemoglobin disorders from a wide variety of ethnic groups, including over 500 distinct named alpha, beta and gamma variants (of which 60+ were novel variants at the time of first detection), 99 beta thalassemia mutations and greater than 20 large deletional beta globin cluster deletion subtypes. [ABSTRACT FROM AUTHOR]

Published

2018

39. Evaluation of the Sebia Minicap Flex Piercing capillary electrophoresis for hemoglobinopathy testing.

Author

Oyaert, M., Van Laer, C., Claerhout, H., Vermeersch, P., Desmet, K., Pauwels, S., and Kieffer, D.

Subjects

*ELECTROPHORESIS equipment, *CONFIDENCE intervals, *ELECTROPHORESIS, *HEMOGLOBINS, *HIGH performance liquid chromatography, *PROBABILITY theory, *REGRESSION analysis, *STATISTICS, *EVALUATION research, *INTER-observer reliability, *MEDICAL equipment reliability, *DATA analysis software, HEMOGLOBINOPATHY diagnosis

Abstract

Introduction Capillary zone electrophoresis (CZE) at alkaline pH is one of the techniques used for hemoglobinopathy screening. In this study, an evaluation of the performance of a lower throughput CZE instrument, the Sebia Minicap Flex Piercing system, for this purpose is reported for the first time. Methods The analytical performance of the Sebia Minicap Flex Piercing system was evaluated. Furthermore, a method comparison between the Sebia Minicap Flex Piercing and two HPLC methods, that is, the Bio-Rad Variant Classic™ and the Bio-Rad D-10™ systems was performed by measuring samples with and without clinically relevant hemoglobin disorders. Results The analytical performance was acceptable for the determination of HbA, HbA2, HbS, and HbF, with an imprecision ≤2.0%. Method comparison showed a linear correlation for HbA2, HbF, and HbS measurements. Clinical concordance was acceptable when comparing CZE and HPLC. Conclusions Lower throughput CZE using the Sebia Minicap Flex Piercing can be used for precise and accurate first line screening and follow-up of hemoglobinopathies. [ABSTRACT FROM AUTHOR]

Published

2015

40. Improvements in phenotype studies of hemoglobin disorders brought by advances in reversed-phase chromatography of globin chains.

Author

Riou, J., Pissard, S., Goossens, M., and Wajcman, H.

Subjects

*IMMUNOGLOBULIN analysis, *DIFFERENTIAL diagnosis, *HIGH performance liquid chromatography, *PHENOTYPES, *IN vitro studies, HEMOGLOBINOPATHY diagnosis

Abstract

Introduction: Phenotype studies still occupy a key position in the diagnosis of hemoglobin (Hb) disorders. Material and Methods: In addition to the conventional methods for diagnosis of Hb disorders which are mostly based on differences in charge of the Hb molecules, some progresses have been brought by studying other properties of the globin chains. Among those, difference in hydrophobicity that may be investigated by reversed-phase HPLC (RP-HPLC) discriminates between variants displaying identical charges. Results: In this study, we show how an update of this method allows to recognize an α-chain variant from a γ-chain variant, a problem frequently during neonatal screening. We illustrate that RP-HPLC may also unravel unclear phenotypes which are modified by the presence of an additional variant not detected by the conventional methods, and help to characterize rare mutants. Also we show that it allows a clear distinction between variants with identical electrophoretical charges as exemplified by Hb Lepore Boston-Washington and Lepore Baltimore. Conclusions: In view of our results, RP-HPLC is a technique that needs to be used as a second step in the general strategy for a correct characterization of Hb variants. [ABSTRACT FROM AUTHOR]

Published

2015

41. Molecular diagnostics of the HBB gene in an Omani cohort using bench-top DNA Ion Torrent PGM technology.

Author

Hassan, S. M., Vossen, R. H. A. M., Chessa, R., den Dunnen, J. T., Bakker, E., Giordano, P. C., and Harteveld, C. L.

Subjects

*MOLECULAR diagnosis, *EARLY diagnosis, *BETA globin, *COHORT analysis, *NUCLEOTIDE sequencing, *BETA-Thalassemia, HEMOGLOBINOPATHY diagnosis

Abstract

Hemoglobinopathies, such as sickle cell disease (SCD) and beta-thalassemia major (TM), are severe diseases and the most common autosomal recessive condition worldwide and in particular in Oman. Early screening and diagnosis of carriers are the key for primary prevention. Once a country-wide population screening program is mandated by law, a sequencing technology that can rapidly confirm or identify disease-causing mutations for a large number of patients in a short period of time will be necessary. While Sanger sequencing is the standard protocol for molecular diagnosis, next generation sequencing starts to become available to reference laboratories. Using the Ion Torrent PGM sequencer, we have analyzed a cohort of 297 unrelated Omani cases and reliably identified mutations in the beta-globin (HBB) gene. Our model study has shown that Ion Torrent PGM can rapidly sequence such a small gene in a large number of samples using a barcoded uni-directional or bi-directional sequence methodology, reducing cost, workload and providing accurate diagnosis. Based on our results we believe that the Ion Torrent PGM sequencing platform, able to analyze hundreds of patients simultaneously for a single disease gene can be a valid molecular screening alternative to ABI sequencing in the diagnosis of hemoglobinopathies and other genetic disorders in the near future. [ABSTRACT FROM AUTHOR]

Published

2014

42. Potential pitfalls in the diagnosis of Hb Handsworth in areas with high prevalence of Hb S.

Author

Al Zadjali, S., Al‐Riyami, A. Z., Gravell, D., Al Haddabi, H., Al Rawahi, M., Al Falahi, K., and Daar, S.

Subjects

*AGAR, *DIFFERENTIAL diagnosis, *ELECTROPHORESIS, *HEMOGLOBINS, *HIGH performance liquid chromatography, HEMOGLOBINOPATHY diagnosis

Abstract

Hb Handsworth is a rare α-globin structural variant caused by a missense mutation either on the α2 or α1-globin gene ( HBA2 or HBA1: c.55G>C, p.Gly18Arg). This variant might be erroneously diagnosed as Hb S unless secondary confirmative tests are carried out. We encountered a child with a prominent peak eluting in the ' S' window on high-performance liquid chromatography ( HPLC). Sickle solubility test, gel electrophoresis, and selective direct nucleotide sequencing of α1, α2, and β globin genes were performed on the patient's sample. In addition, previous HPLC results on a cord blood sample were retrieved. Sickle solubility test was negative. Gel electrophoresis revealed a band migrating at the S region with an extra faint band seen on acid gel electrophoresis. Molecular analysis of α2 globin gene revealed heterozygous state of Hb Handsworth. Hb Handsworth is a rare variant that can mimic Hb S on HPLC. Failure to recognize this rare variant in regions where Hb S is highly prevalent may result in serious misdiagnosis and subsequent incorrect genetic counseling. [ABSTRACT FROM AUTHOR]

Published

2014

43. α-Thalassemia Does Not Seem to Influence Erythrocyte Deformability in Sickle Cell Trait Carriers.

Author

Vayá, Amparo, Collado, Susana, Alis, Rafael, Vera, Belen, Romagnoli, Marco, and Barragán, Eva

Subjects

*SICKLE cell anemia diagnosis, *BETA-Thalassemia, *HEMOGLOBIN polymorphisms, *GENETIC polymorphisms, *ERYTHROCYTES, *HEMORHEOLOGY, *DIAGNOSIS, HEMOGLOBINOPATHY diagnosis

Abstract

Studies dealing with rheological red blood cell (RBC) behavior in sickle cell trait carriers are scarce. Moreover, the association with α-thalassemia (α-thal), which also modifies erythrocyte behavior, has not always been taken into account. We analyzed erythrocyte deformability by means of a shear stress diffractometer, along with hematological and biochemical parameters (glucose and plasma lipids), given their possible influence on erythrocyte deformability, in 14 sickle cell trait carriers and 23 healthy controls. Nine patients were also α-thal carriers and five were not. Among the thalassemia carriers, eight were heterozygous and one was homozygous. When compared with controls, sickle cell trait carriers showed no differences for any of the biochemical parameters analyzed ( p > 0.05), but significantly lower hemoglobin (Hb) ( p = 0.003), mean corpuscular volume (MCV) and mean corpuscular Hb (MCH) ( p < 0.001) levels, although no differences in erythrocyte deformability were observed at any of the shear stresses tested ( p > 0.05). When comparing sickle cell trait carriers, with and without α-thal, no differences in erythrocyte deformability were observed ( p > 0.05), in spite of the former showing lower MCV and MCH ( p < 0.05) levels. Carriers of α-thal had lower Hb S [β6(A3)Glu → Val; HBB: c.20A > T] levels ( p = 0.013) than non carriers. The existence of a compensating mechanism seems reasonable because, despite presenting lower erythrocyte indices, which could worsen erythrocyte deformability, this rheological property improves when the percentage of Hb S is lower. [ABSTRACT FROM AUTHOR]

Published

2014

44. Prenatal diagnosis of hemoglobinopathies: from fetoscopy to coelocentesis.

Author

Damiani, Gianfranca, Vinciguerra, Margherita, Jakil, Cristina, Cannata, Monica, Cassarà, Filippo, Picciotto, Francesco, Schillaci, Giovanna, Cigna, Valentina, Renda, Disma, Volpes, Aldo, Sammartano, Francesca, Milone, Samuela, Allegra, Adolfo, Passarello, Cristina, Leto, Filippo, and Giambona, Antonino

Subjects

*PRENATAL diagnosis, *HEMOGLOBINOPATHY in children, *NEWBORN screening, *FETOSCOPY, HEMOGLOBINOPATHY diagnosis

Abstract

Prenatal diagnosis of hemoglobinopathies involves the study of fetal material from blood, amniocytes, trophoblast coelomatic cells and fetal DNA in maternal circulation. Its first application dates back to the 70s and it involves globin chain synthesis analysis on fetal blood. In the 1980s molecular analysis was introduced as well as amniocentesis and chorionic villi sampling under high-resolution ultrasound imaging. The application of direct sequencing and polymerase chain reaction-based methodologies improved the DNA analysis procedures and reduced the sampling age for invasive prenatal diagnosis from 18 to 16- 11 weeks allowing fetal genotyping within the first trimester of pregnancy. In the last years, fetal material obtained at 7-8 weeks of gestation by coelocentesis and isolation of fetal cells has provided new platforms on which to develop diagnostic capabilities while non-invasive technologies using fetal DNA in maternal circulation are starting to develop. [ABSTRACT FROM AUTHOR]

Published

2014

45. Control of thalassemia in India.

Author

Colah, Roshan B. and Gorakshakar, Ajit

Subjects

*BETA-Thalassemia, *SICKLE cell anemia treatment, *PUBLIC health, *PRENATAL diagnosis, *EPIDEMIOLOGY, *HEALTH education, *PREVENTION, HEMOGLOBINOPATHY diagnosis

Abstract

The β-thalassemias and sickle cell disorders pose a major health burden in the large and diverse Indian population. Education programs for awareness generation are being done by National Institutions, non-governmental organizations and Thalassemia Societies in different states. Several extensive epidemiological studies have shown that there are many non-tribal and tribal communities where the prevalence of β-thalassemia carriers is much higher (5.3 to 17.0%) than the average of 3 to 4% projected for the entire country. These variations have also been shown within small geographic regions in some states, emphasizing the need for micro mapping to estimate the true burden of disease. There are 10 to 12 centers where prenatal diagnosis for hemoglobinopathies is done and the Indian Council of Medical Research is establishing additional regional centers in states where they are most needed. Sixty-eight β-thalassemia mutations have been described so far among Indians and the knowledge on their prevalence and regional distribution has helped to undertake prenatal diagnosis in a cost effective way. [ABSTRACT FROM AUTHOR]

Published

2014

46. Providing appropriate genetic information to healthy multi-ethnic carriers of hemoglobinopathy in The Netherlands.

Author

Giordano, Piero C., Binda, Natasha B. N., Amato, Antonio, Bakker, Engbert, and Harteveld, Cornelis L.

Subjects

*HEMOGLOBINOPATHY in children, *SICKLE cell anemia in children, *PREGNANCY complications, *BETA-Thalassemia, *DIAGNOSIS, HEMOGLOBINOPATHY diagnosis

Abstract

The aims of this study are: i) to enquire whether informing healthy hemoglobinopathy carriers about their condition is a welcome initiative in The Netherlands; ii) to study whether using information letters and thorough explanation is associated with presence or absence of undesired feelings or emotions. We have approached 100 multi-ethnic carriers previously diagnosed in our lab. All subjects had previously received our information letter through their physician who was supposed to have provided an explanation of the letter if required. We have enquired whether the subjects had experienced negative or positive emotions after receiving our diagnosis and explanation and to which degree, if they were sufficiently informed and satisfied and if they would have considered prevention in case of risk. The rate negative versus positive feelings was calculated using a numerical distribution. We have registered negative feelings in a rate that was directly proportional to the lack of information. While the number of registered negative feelings in well-informed carriers was very low it was more present in badly informed. Nevertheless, all participants found carrier information a welcome initiative and over 80% of them declared to be in favor of prenatal diagnosis in case of risk._Carrier information is essential for an informed reproductive choice and is welcome in a multi-ethnic society. Unfortunately, information is not always consequently provided and should therefore be imbedded in the ongoing national screening for Rhesus and infectious diseases available to all women in early pregnancy. [ABSTRACT FROM AUTHOR]

Published

2014

47. State of the art and new developments in molecular diagnostics for hemoglobinopathies in multiethnic societies.

Author

Harteveld, C. L.

Subjects

*HEMOGLOBINOPATHY genetics, *CAPILLARY electrophoresis, *GENE amplification, *HEMOGLOBINOPATHY, *HIGH performance liquid chromatography, *MOLECULAR diagnosis, *POLYMERASE chain reaction, *GENETIC carriers, *MICROARRAY technology, *SEQUENCE analysis, HEMOGLOBINOPATHY diagnosis

Abstract

For detecting carriers of thalassemia traits, the basic part of diagnostics consists of measurement of the hematological indices followed by mostly automatic separation and measurement of the Hb fractions, while direct Hb separation either on high pressure liquid chromatography or capillary electrophoresis is sufficient to putatively identify carriers of the common Hb variants like Hb S, C, E, D, and O- Arab. A putative positive result is reported together with an advice for parents, partner, or family analysis. For couples, presumed at-risk confirmation at the DNA level is essential. In general, this part of diagnostics is done in specialized centers provided with sufficient experience and the technical tools needed to combine hematological and biochemical interpretation with identification of the mutations at the molecular level. State-of-the-art tools are usually available in centers that also provide prenatal diagnosis and should consist of gap- PCR for the common deletions, direct DNA sequencing for all kind of point-mutations and the capacity to uncover novel or rare mutations or disease mechanisms. New developments are MLPA for large and eventually unknown deletion defects and microarray technology for fine mapping and primer design for breakpoint analysis. Gap- PCR primers designed in the region flanking the deletion breakpoints can subsequently be used to facilitate carrier detection of uncommon deletions in family members or isolated populations in laboratories where no microarray technology or MLPA is available. [ABSTRACT FROM AUTHOR]

Published

2014

48. Hemoglobin Variant (Hemoglobin Aalborg) Mimicking Interstitial Pulmonary Disease.

Author

Panou, Vasiliki, Mathias Jensen, Peter-Diedrich, Pedersen, Jan Freddy, Thomsen, Lars Pilegaard, and Weinreich, Ulla Møller

Subjects

*HEMOGLOBIN polymorphisms, *INTERSTITIAL lung diseases, *BLOOD diseases, *ADULT respiratory distress syndrome, *CHOLECYSTECTOMY, *WOMEN'S health, HEMOGLOBINOPATHY diagnosis

Abstract

Hemoglobin Aalborg is a moderately unstable hemoglobin variant with no affiliation to serious hematological abnormality or major clinical symptoms under normal circumstances. Our index person was a healthy woman of 58, not previously diagnosed with hemoglobinopathy Aalborg, who developed acute respiratory failure after a routine cholecystectomy. Initially she was suspected of idiopathic interstitial lung disease, yet a series of tests uncovered various abnormal physiological parameters and set the diagnosis of hemoglobinopathy Aalborg. This led us to examine a group of the index person's relatives known with hemoglobinopathy Aalborg in order to study whether the same physiological abnormalities would be reencountered. They were all subjected to spirometry and body plethysmography, six-minute walking test, pulse oximetry, and arterial blood gas samples before and after the walking test. The entire study population presented the same physiological anomalies: reduction in diffusion capacity, and abnormalities in PaO2 and p50 values; the latter could not be presented by the arterial blood gas analyzer; furthermore there was concordance between pulse oximetry and arterial blood gas samples regarding saturation. These data suggest that, based upon the above mentioned anomalies in physiological parameters, the diagnosis of hemoglobinopathy Aalborg should be considered. [ABSTRACT FROM AUTHOR]

Published

2014

49. Diagnostic utility of isoelectric focusing and high performance liquid chromatography in neonatal cord blood screening for thalassemia and non-sickling hemoglobinopathies.

Author

Uaprasert, Noppacharn, Settapiboon, Rung, Amornsiriwat, Supaporn, Sarnthammakul, Patsita, Thanapat, Tassanee, Rojnuckarin, Ponlapat, and Sutcharitchan, Pranee

Subjects

*ISOELECTRIC focusing, *HIGH performance liquid chromatography, *CORD blood, *BLOOD testing, *THALASSEMIA diagnosis, *MEDICAL screening, HEMOGLOBINOPATHY diagnosis

Abstract

Abstract: Background: Thalassemia syndromes are highly prevalent in Southeast Asia. In Thailand, high performance liquid chromatography (HPLC) is the most common technique routinely performed in diagnosis of thalassemia and hemoglobinopathies, while isoelectric focusing (IEF) is rarely employed. We compared the diagnostic utility of IEF and HPLC in neonatal screening for thalassemia and non-sickling hemoglobinopathies. Methods: Two-hundred and forty-one cord blood samples were analyzed using IEF and HPLC, β-thalassemia short program. The results were correlated with red cell indices and molecular analyses. Hemoglobin (Hb) Bart's was quantified only on IEF. Results: Of 241 newborns, IEF and HPLC yielded 85.4% and 76.4% sensitivity to identify α-thalassemia syndrome, respectively. HbBart's≥2% yielded 100% sensitivity to identify 2 α-globin gene deletions and/or mutations, while MCV≤95fl and MCH≤30pg yielded 100% sensitivity to identify 2 α-globin gene deletions. DNA analysis revealed HbE mutation in all 61 subjects with HbA2 >1% on both IEF and HPLC. Conclusion: IEF is an effective method in neonatal screening for thalassemia and non-sickling hemoglobinopathies. The HbBart's level, MCV and MCH are helpful for identifying α-thalassemia. The presence of HbA2 higher than 1% in cord blood indicates HbE carriers in Southeast Asian newborns. [Copyright &y& Elsevier]

Published

2014

50. Preimplantation genetic diagnosis, an alternative to conventional prenatal diagnosis of the hemoglobinopathies.

Author

Traeger‐Synodinos, J.

Subjects

*PREIMPLANTATION genetic diagnosis, *PRENATAL genetic testing, *HEMOGLOBINOPATHY genetics, *HISTOCOMPATIBILITY testing, *GENETIC mutation, *POLYMERASE chain reaction, *HLA-B27 antigen, HEMOGLOBINOPATHY diagnosis

Abstract

Prenatal diagnosis ( PND) and preimplantation genetic diagnosis ( PGD) both represent highly important reproductive choices for couples with a high risk of transmitting a severe disease, such as a severe hemoglobinopathy. Conventional PND for hemoglobinopathies based on molecular analysis of trophoblast or amniocyte DNA has been applied for around 30 years, but the major disadvantages with this approach include 'invasive' fetal sampling, and the potential involvement of pregnancy termination when affected. In comparison, the major advantage of PGD over conventional PND is that it supports the initiation of unaffected pregnancies, avoiding the need to terminate affected pregnancies. However, it is a multistep technically demanding procedure requiring the close collaboration of experts from several fields. PGD is also limited by the need to involve assisted reproduction, even in couples without fertility problems. Furthermore, even for fertile couples, pregnancy rates rarely surpass 30-35%. Both PND and PGD have advantages and drawbacks. Before embarking on either procedure, couples should be carefully counseled by experts so that they can select the option most appropriate for them. Finally, whatever their choice, it is paramount that both prenatal and PGD be applied with the highest standards of clinical, laboratory, and ethical practice. [ABSTRACT FROM AUTHOR]

Published

2013