Association of the <i>CHGA</i> gene polymorphism in patients with hemorrhagic stroke and/or aneurysm

Santos Jr, Joanilson C. M; Fratelli, Caroline F; Nóbrega, Alan Cristian F; Rodrigues, Suzana Cristina; Duarte, Ligia Canongia A. C; Silva, Calliandra Maria S; Lima, Jonathan D; Ferreira, Luzitano B; Freire, Daniel O; Cipriano, Vivian Taís F; Silva, Izabel Cristina R; Souza, Hélia Carla

doi:10.5935/1676-2444.20200012

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ORIGINAL ARTICLE • J. Bras. Patol. Med. Lab. 56 • 2020 • https://doi.org/10.5935/1676-2444.20200012 copy

Association of the CHGA gene polymorphism in patients with hemorrhagic stroke and/or aneurysm

Authorship SCIMAGO INSTITUTIONS RANKINGS

ABSTRACT

Introduction:

Cerebrovascular diseases have been associated with several genes. Chromogranin A (CHGA) has been used as maker in cardiovascular disease. Therefore, evaluating the polymorphism and verifying its association with this pathology is very important to better understand this disease.

Objective:

The aim of this study was to identify the association between coding region polymorphism in -264 position of the CHGA gene (Glu264Asp) and hemorrhagic stroke (HS)/aneurysm in the Federal District, Brazil.

Methods:

This is a population-based case-control, involving 45 cases with HS and/or aneurysm. Polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) method is used for genotyping these samples. A significance level of 5% was adopted.

Results:

The absence of the CC genotype the Glu264Asp CHGA polymorphism in the study participants and the significant presence of the GC heterozygote genotype were observed in this study. However, the distribution of genotypes did not differ statistically in the groups.

Conclusion:

The Glu264Asp CHGA polymorphism does not seem to contribute to the genesis of the CHGA protein expression in this patients group, but to understand whether or not there is a possible association of the pathology in question and whether the mutation will contribute in the gene therapy and thus to improve patients’ quality of life.

Key words:
genetic polymorphism; chromogranin A; hemorrhagic stroke

Glu264Asp CHGA	Group
	HS/aneurysm		Control
	n	%	n	%	p	OR	CI
GG	10	22.2	9	17.3
GC	35	77.8	43	82.7	0.543	1.37	0.5-3.73
CC	0	0	0	0
Total	45	100	52	100
G	55	61.1	61	58.7
C	35	38.9	43	41.3	0.729	1.11	0.62-1.97
Total	90	100	104	100

Clinical features		Glu264Asp CHGA
		GG		GC
		n	%	n	%	p
SH	Yes	8	22.9	27	77.1	0.848
SH	No	2	20	8	80
Diabetes	Yes	0	0	3	100	0.338
Diabetes	No	10	23.8	32	76.2
Smoking	Yes	3	20	12	80	0.8
Smoking	No	7	23.3	23	76.7
Alcoholism	Yes	1	14.3	6	85.7	0.583
Alcoholism	No	9	23.7	29	76.3
Glasgow	Intermediate coma	2	33.3	4	66.7	0.482
	Superficial coma	0	0	0	0
	Normality	8	20.5	31	79.5
Rankin	Asymptomatic	0	0	2	100	0.864
	Symptom with no disability	8	23.5	26	76.5
	Slight disability	0	0	1	100
	Moderate disability	0	0	2	100
	Moderately severe disability	1	33.3	2	66.7
	Severe disability	1	33.3	2	66.7
Barthel index	Severe disability	2	33.3	4	66.7	0.371
	Moderate disability	0	0	0	0
	Slight disability	7	25.9	20	74.1
	Functional independence	1	8.3	11	91.7

Laboratory Variables	Glu264Asp CHGA
	GG		GC		Total
	Mean	Standard error of the mean	Mean	Standard error of the mean	Mean	Standard error of the mean	p
Glucose	112	9	109	4	110	4	0.79
Creatinine	0.9	0.1	1.4	0.4	1.3	0.3	0.439
Platelets	321	17	339	12	335	10	0.455

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E-mail: jbpml@sbpc.org.br

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[1] CORRESPONDING AUTHOR: Izabel Cristina Rodrigues da Silva, 0000-0002-6836-3583. e-mail: belbiomedica@gmail.com