A case with α-thalassemia caused by novel start codon variant in conjunct with right deletion variant of α2-globin gene / 中华医学遗传学杂志

OBJECTIVE@#The explore the genetic basis for a patient with microcytic hypochromic anemia and iron deficiency anemia.@*METHODS@#Common deletions and variants of the globin genes were detected by Gap-PCR and next generation sequencing (NGS). Suspected mutations were verified by Sanger sequencing.@*RESULTS@#Gap-PCR and NGS showed that the proband has carried a αα/-α @*CONCLUSION@#Patients with α HBA2 c.2T>A(p.Met1Lys) α/-α

[Molecular analysis of alpha globin gene deletions among patients with microcytic hypochromic anemia in Kermanshah-Iran]

The majority of alpha-thalassemi mutations are deletions of one or both alpha- globin genes. Since the Iranian populaion is a mixture of different ethnic groups, frequency and distribution of globin mutations in various regions of the country need to be clarified. The aim of this study was to determine the common alpha globin gene deletions among individuals with hypochromic microcytic anemia in Kermanshah province. Following the initial evaluation, 92 patients [47 women and 45 men] were found as microcytic hypochromic [MCV < 80 fl and MCH< 27 pg] anemia and selected for this study. All samples were analyzed for detection of four alpha-gene deletions [-alpha3.7,-alpha4.2,- [alpha] 20.5 and --MED] by GAP-PCR technique. After amplification, 10microl of PCR product was electrophoresed through 1.2% agarose gel and bands were visualized by staining gel in ethidium bromide solution and photographed under a UV transilluminater. 45 patients had -alpha 3.7 single gene deletion. In patients with -alpha3.7 deletion, in both homozygous and heterozygous states, MCH was lower than normal ranges. However, the percent of HbA2 was in normal range. In this study, other common deletional mutations, including - [alpha]20.5, -alpha4.2 and --MED were not found. The results of persent study showed that the frequency of -alpha3.7 single gene deletion among patients with microcytic hypochromic anemia in Kermanshah province was 48.9%

Microcytic hypochromic anemia patients with thalassemia: genotyping approach.

BACKGROUND: Microcytic hypochromic anemia is a common condition in clinical practice, and alpha-thalassemia has to be considered as a differential diagnosis. AIMS: This study was conducted to evaluate the frequency of alpha-gene, beta-gene and hemoglobin variant numbers in subjects with microcytic hypochromic anemia. SETTING AND DESIGNS: Population-based case-control study in the Iranian population. MATERIALS AND METHODS: A total of 340 subjects from southwest part of Iran were studied in the Research Center of Thalassemia and Hemoglobinopathies (RCTH), Iran. Genotyping for known alpha- and beta-gene mutations was done with gap-PCR and ARMS. In cases of some rare mutations, the genotyping was done with the help of other techniques such as RFLP and ARMS-PCR. STATISTICAL ANALYSIS: Statistical analysis was carried out by SPSS 11.5 and an independent-sample t test. RESULTS: Out of the total 340 individuals, 325 individuals were evaluated to have microcytic hypochromic anemia based on initial hematological parameters such as MCV<80 fl; MCH<27 pg; the remaining 15 patients were diagnosed with no definite etiology. The overall frequency of -alpha3.7 deletion in 325 individuals was 20.3%. The most frequent mutations were IVS II-I, CD 36/37 and IVS I-110 with frequencies of 6.31%, 5.27% and 1.64%, respectively. Only, there was a significant difference between beta-thalassemia trait and beta-thalassemia major with regard to MCV (P<0.05) and MCH (P<0.05) indices, and also MCH index between beta-thalassemia trait and Hb variants (P<0.05). CONCLUSION: Molecular genotyping provides a rapid and reliable method for identification of common, rare and unknown alpha- and beta-gene mutations, which help to diagnose unexplained microcytosis and thus prevent unnecessary iron supplementation.

Genotyping of thalassemia in microcytic hypochromic anemia patients from southwest region of Iran

To evaluate the frequency of -gene, beta-gene, and hemoglobin variant numbers in subjects with Microcytic hypochromic anemia. In total out of 850, 340 subjects with microcytic hypochromic anemia [MCV<80fl; MCH<27pg] from Southwest part of Iran, were studied in Research Center of Thalassemia and Hemoglobinopathies [RCTH] which is the only center working on hematology and oncology in Southwest [Khuzestan] region of Iran. These include 325 individuals: 171 with Beta-thalassemia trait, 88 with Alpha-thalassemia trait, 13 with thalassemia major, 11 with hemoglobin variants [HbS, HbC, and HbD Punjab] and 42 with iron-deficiency anemia. The rest 15 patients diagnosed with no definite etiology. Genotyping for - alpha[3.7], - alpha[4.2], - alpha[PA], - alpha[5NT] and - - [MED] was done with gap-PCR. The overall frequency of - alpha[3.7] deletion in 325 individuals is 20%. Genotyping for 23 most known beta-gene mutations was done with direct mutation analysis by Amplification Refractory Mutation System [ARMS]. The most frequent mutations were CD 36/37, IVS II-I, and IVS I-110 with 9.7%, 11.7%, and 3.5% respected frequencies in 340 patients. There was statistically significant difference between Beta-thalassemia trait and Beta-thalassemia Major in case of MCV [p- value = 0.25] and MCH [P-value =0.23] indices, and also MCH index between Beta-thalassemia trait and Hb Variants [P-value = 0.04]. The - alpha gene and beta-gene mutation is quite common in the Southwest part of Iran. Molecular genotyping of - alpha thalassemia and beta-thalassemia help to diagnose unexplained microcytosis, and thus prevent unnecessary iron supplementation