TY - JOUR
T1 - Molecular diagnosis of α-thalassemia in a multiethnic population
AU - Gilad, Oded
AU - Shemer, Orna Steinberg
AU - Dgany, Orly
AU - Krasnov, Tanya
AU - Nevo, Michal
AU - Noy-Lotan, Sharon
AU - Rabinowicz, Ron
AU - Amitai, Nofar
AU - Ben-Dor, Shifra
AU - Yaniv, Isaac
AU - Yacobovich, Joanne
AU - Tamary, Hannah
N1 - Publisher Copyright: © 2017 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd
PY - 2017/6/1
Y1 - 2017/6/1
N2 - Objective: α-Thalassemia, one of the most common genetic diseases, is caused by deletions or point mutations affecting one to four α-globin genes. Molecular diagnosis is important to prevent the most severe forms of the disease. However, the diagnosis of α-thalassemia is complex due to a high variability of the genetic defects involved, with over 250 described mutations. We summarize herein the findings of genetic analyses of DNA samples referred to our laboratory for the molecular diagnosis of α-thalassemia, along with a detailed clinical description. Methods: We utilized a diagnostic algorithm including Gap-PCR, to detect known deletions, followed by sequencing of the α-globin gene, to identify known and novel point mutations, and multiplex ligation-dependent probe amplification (MLPA) for the diagnosis of rare or novel deletions. Results: α-Thalassemia was diagnosed in 662 of 975 samples referred to our laboratory. Most commonly found were deletions (75.3%, including two novel deletions previously described by us); point mutations comprised 25.4% of the cases, including five novel mutations. Our population included mostly Jews (of Ashkenazi and Sephardic origin) and Muslim Arabs, who presented with a higher rate of point mutations and hemoglobin H disease. Overall, we detected 53 different genotype combinations causing a spectrum of clinical phenotypes, from asymptomatic to severe anemia. Conclusion: Our work constitutes the largest group of patients with α-thalassemia originating in the Mediterranean whose clinical characteristics and molecular basis have been determined. We suggest a diagnostic algorithm that leads to an accurate molecular diagnosis in multiethnic populations.
AB - Objective: α-Thalassemia, one of the most common genetic diseases, is caused by deletions or point mutations affecting one to four α-globin genes. Molecular diagnosis is important to prevent the most severe forms of the disease. However, the diagnosis of α-thalassemia is complex due to a high variability of the genetic defects involved, with over 250 described mutations. We summarize herein the findings of genetic analyses of DNA samples referred to our laboratory for the molecular diagnosis of α-thalassemia, along with a detailed clinical description. Methods: We utilized a diagnostic algorithm including Gap-PCR, to detect known deletions, followed by sequencing of the α-globin gene, to identify known and novel point mutations, and multiplex ligation-dependent probe amplification (MLPA) for the diagnosis of rare or novel deletions. Results: α-Thalassemia was diagnosed in 662 of 975 samples referred to our laboratory. Most commonly found were deletions (75.3%, including two novel deletions previously described by us); point mutations comprised 25.4% of the cases, including five novel mutations. Our population included mostly Jews (of Ashkenazi and Sephardic origin) and Muslim Arabs, who presented with a higher rate of point mutations and hemoglobin H disease. Overall, we detected 53 different genotype combinations causing a spectrum of clinical phenotypes, from asymptomatic to severe anemia. Conclusion: Our work constitutes the largest group of patients with α-thalassemia originating in the Mediterranean whose clinical characteristics and molecular basis have been determined. We suggest a diagnostic algorithm that leads to an accurate molecular diagnosis in multiethnic populations.
KW - microcytic anemia
KW - molecular diagnosis
KW - α-thalassemia
UR - http://www.scopus.com/inward/record.url?scp=85017354729&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=85017354729&partnerID=8YFLogxK
U2 - https://doi.org/10.1111/ejh.12866
DO - https://doi.org/10.1111/ejh.12866
M3 - مقالة
C2 - 28160324
SN - 0902-4441
VL - 98
SP - 553
EP - 562
JO - European Journal of Haematology
JF - European Journal of Haematology
IS - 6
ER -