Frequencies of CD39, IVS1-1, IVS1-6 and IVS1-110 mutations in beta-thalassemia carriers and their influence on hematimetric indices

Gomes, Willian R.; Santos, Raquel A.; Cominal, Juçara G.; Tavares, Cristiane F. F.

doi:10.5935/1676-2444.20170058

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LABORATORY MEDICINE, ORIGINAL ARTICLE • J. Bras. Patol. Med. Lab. 53 (6) • Nov-Dec 2017 • https://doi.org/10.5935/1676-2444.20170058 copy

Frequencies of CD39, IVS1-1, IVS1-6 and IVS1-110 mutations in beta-thalassemia carriers and their influence on hematimetric indices

Frequências de mutações CD39, IVS1-1, IVS1-6 e IVS1-110 em portadores de betatalassemia e suas influências nos valores hematimétricos

Authorship SCIMAGO INSTITUTIONS RANKINGS

ABSTRACT

Introduction:

Beta-thalassemia is caused by a deficient synthesis of the ß-chain of hemoglobin, which leads to a chronic, microcytic and hypochromic anemia. More than 200 mutations have already been associated with this type of thalassemia, and their frequencies may vary according to the population.

Objectives:

The objectives of this study were to determine the frequencies of CD39, IVS1-1, IVS1-6 and IVS1-110 mutations in people with beta-thalassemia from the city of Franca, São Paulo, and to evaluate the influence of the genotypes on hematological alterations.

Methods:

Venous blood samples were collected from 25 volunteers previously diagnosed with beta-thalassemia. Complete blood counts (CBC) were performed, and the identification of the mutations was carried out using the polymerase chain reaction (PCR).

Results:

The CD39 mutation was found in 11 (44%) individuals, followed by IVS1-6 (9; 36%) and IVS1-110 (4; 16%). One patient (4%) did not present any of these mutations. IVS1-6 mutation was inversely correlated to red cell distribution width (RDW) (r_s = -0.44; p = 0.034), and CD39 was correlated to lower mean corpuscular volume (MCV) (r_s = -0.44; p = 0.034). Multivariable linear regression models showed that the CD39 mutation carriers have lower levels for hemoglobin (ß = -0.61; p = 0.044) and hematocrit (ß = -2.1; p = 0.018).

Conclusion:

The results showed a high frequency of the CD39 mutation in the city of Franca, and the correlations observed between the presence of CD39 mutation and the hematological alterations suggest a genotype influence on the phenotype of beta-thalassemia, which would contribute to the clinical variations of this hemoglobinopathy.

Key words:
beta-thalassemia; hemoglobinopathies; genotype

X ± SD
		Women	Men	p ^a a Student's t-test to compare the differences between genders.
		X ± SD	X ± SD
Hb (g/dl)	11.5 ± 1.17	11.1 ± 0.875	12.4 ± 1.43	0.016^* * p ≤ 0.050;
Erythrocytes (mi/mm³)	5.43 ± 0.774	5.19 ± 0.759	6.04 ± 0.389	0.01^ p ≤ 0.010
Ht (%)	36.0 ± 3.57	34.9 ± 2.69	39.0± 4.02	0.006^ p ≤ 0.010
MCV (fl)	67.7 ± 7.7	68.4 ± 8.87	65.8 ± 2.91	0.454
MCH (pg)	21.2 ± 2.83	21.8 ± 3.02	19.9 ± 1.78	0.14
MCHC (%)	31.8 ± 0.923	31.9 ± 0.803	31.5 ± 1.22	0.415
RDW (%)	15.0 ± 1.58	14.6 ± 1.33	15.8 ± 1.93	0.17

Mutation	Frequency
CD39 (C>T)	11 (44%)
IVS1-6 (T>C)	9 (36%)
IVS1-110 (G>A)	4 (16%)
IVS1-1 (G>A)	0 (0%)
Other	1 (4%)
Total	25 (100%)

Genotype	Hb^a a Hb = α + β1 × gender + β2 × erythrocytes + β3 × genotype;	Erythrocytes^b b erythrocytes = α + β1 × gender + β2 × genotype;	Ht^c c Ht = α + β1 × gender + β2 × erythrocytes + β3 × genotype	RDW^d d RDW = α + β1 × genotype;	MCV^e e MCV = α + β1 × genotype;	MCH^f f MCH = α + β1 × genotype;	MCHC^g g MCHC = α + β1 × gender + β2 × genotype. Hb: hemoglobin; Ht: hematocrit; RDW: red cell distribution width; MCV: mean corpuscular volume; MCH: mean corpuscular hemoglobin; MCHC: mean corpuscular hemoglobin concentration.
CD39	-0.61^* * p ≤ 0.050.	0.034	-2.1^* * p ≤ 0.050.	0.065	-2.8	-0.99	0.002
IVS1-6	0.42	-0.094	1.4	-0.071	2.3	0.61	-0.002
IVS1-110	0.35	0.097	1.2	0.005	1.1	0.67	0.001

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E-mail: jbpml@sbpc.org.br

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[1] CORRESPONDING AUTHOR Willian Robert Gomes, Faculdade de Ciências Farmacêuticas de Ribeirão Preto; Universidade de São Paulo; Avenida do Café, s/n; Monte Alegre; CEP: 14040-903; Ribeirão Preto-SP, Brasil; e-mail: williangomes@usp.br.