Autoantibody profile in individuals with chronic hepatitis C

Marconcini, Maíra Luciana; Fayad, Leonardo; Shiozawa, Maria Beatriz Cacese; Dantas-Correa, Esther Buzaglo; Lucca Schiavon, Leonardo de; Narciso-Schiavon, Janaína Luz

doi:10.1590/0037-8682-0039-2013

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Major Articles • Rev. Soc. Bras. Med. Trop. 46 (2) • Mar-Apr 2013 • https://doi.org/10.1590/0037-8682-0039-2013 copy

Autoantibody profile in individuals with chronic hepatitis C

Authorship SCIMAGO INSTITUTIONS RANKINGS

Introduction

Autoantibodies are often produced during infection with chronic hepatitis C virus (HCV), but it remains controversial whether they influence the biochemical profile and histological features of this disease. Therefore, this current study sought to describe these autoantibodies and evaluate their impact on the clinical and histological presentation of hepatitis C.

Methods

This cross-sectional analytical study assessed patients with HCV (RNA+) from October 2011 to July 2012.

Results

This study included 66 patients, with a mean age of 53.2±10.5 years. Of these patients, 60.6% were male, and 54.3% presented with genotype 1. Non-organ-specific autoantibodies (NOSA) were detected in 24% of the patients; of these, 7.6% were anti-mitochondrial antibodies (AMA+), 26.7% were anti-smooth muscle antibodies (SMA+) and 6.8% were liver kidney microsomal type 1 antibodies (LKM1+). With respect to the thyroid autoantibodies, 7.4% were anti-peroxidase (ATPO+) antibodies, and none were anti-thyroglobulin (ATG+) antibodies. Regarding celiac disease autoantibodies, 5.8% were endomysial antibodies (EMA+), and no transglutaminase (TTG+) antibodies were detected. Cryoglobulins were found in 2.1% of patients. When NOSA+ individuals were compared to patients without the presence of NOSAs, they exhibited higher median alkaline phosphatase (0.7 vs. 0.6 xULN; p=0.041), lower median platelet counts (141,500.0 vs. 180,500.0/mm³3. Thein HH, Yi Q, Dore GJ, Krahn MD. Estimation of stage-specific fibrosis progression rates in chronic hepatitis C virus infection: a meta-analysis and meta-regression. Hepatology 2008; 48:418-431.; p=0.036), lower mean prothrombin activity (72.6±11.5% vs. 82.2±16.0%; p=0.012) and an increased prevalence of significant fibrosis (E≥2) (45.5% vs. 18.2%; p=0.012). There was also a tendency for a greater proportion of NOSA+ cases to have marked periportal activity (APP≥3) (44.5% vs. 15.6%; p=0.087).

Conclusions

In addition to the high prevalence of autoantibodies associated with HCV infection, it was observed that NOSA positivity was associated with a more severe histological and biochemical profile of hepatitis C infection.

Hepatitis C; Autoimmunity; Cryoglobulins; Celiac disease

Characteristics	Total	NOSA (+)	NOSA (-)	p
Characteristics	Total	N= 16	N = 50	p
Age (years)^* * mean ± standard deviation;	53.2 ± 10.5	56.3 ± 9.9	52.3 ± 10.6	0.188^t t Student's t test;
Male (%)	60.6	56.3	62.0	0.682^q q chi-square test;
Genotype 1 (%)	54.3	53.8	54.5	0.966^q q chi-square test;
Viral load (x10⁶6. Clifford BD, Donahue D, Smith L, Cable E, Luttig B, Manns M, et al. High prevalence of serological markers of autoimmunity in patients with chronic hepatitis C. Hepatology 1995; 21:613-619. UI/mL)^#	1.10	1.05	1.13	0.696^m m median;
Diabetes mellitus (%)	14.1	6.3	16.7	0.430^f f Fisher's exact test.
Hypertension (%)	21.9	31.3	18.8	0.312^f f Fisher's exact test.
Dyslipidemia (%)	9.5	6.3	10.6	1.000^f f Fisher's exact test.
Hypothyroidism (%)	14.1	6.3	16.7	0.430^f f Fisher's exact test.
HBsAg(+) (%)	1.7	0.0	2.2	1.000^f f Fisher's exact test.
Anti-HBc (+) (%)	21.7	0.0	27.8	0.089^f f Fisher's exact test.
Anti-HIV(+) (%)	3.4	12.5	0.0	0.070^f f Fisher's exact test.
Treatment naïve (%)	54.0	37.5	59.6	0.126^q q chi-square test;
Creatinine (mg/dL)^#	0.9	0.9	0.9	0.705^m m median;
Hemoglobin (g/dL)^* * mean ± standard deviation;	14.0 ± 1.9	13.3 ± 2.1	14.3 ± 1.8	0.064^t t Student's t test;
Platet count (x10³3. Thein HH, Yi Q, Dore GJ, Krahn MD. Estimation of stage-specific fibrosis progression rates in chronic hepatitis C virus infection: a meta-analysis and meta-regression. Hepatology 2008; 48:418-431./mm³3. Thein HH, Yi Q, Dore GJ, Krahn MD. Estimation of stage-specific fibrosis progression rates in chronic hepatitis C virus infection: a meta-analysis and meta-regression. Hepatology 2008; 48:418-431.)^#	165.0	141.5	180.5	0.036^m m median;
Ferritin (ng/mL)^#	326.0	170.0	347.0	0.474^m m median;
Transferrin saturation (%)^* * mean ± standard deviation;	41.2 ± 16.6	35.5 ± 10.7	43.5 ± 18.1	0.113^t t Student's t test;
AST (xULN)^* * mean ± standard deviation;	2.0 ± 1.6	2.4 ± 2.3	1.8 ± 1.2	0.336^t t Student's t test;
ALT (xULN)^#	1.2	1.0	1.4	0.515^m m median;
AP (xULN)^#	0.6	0.7	0.6	0.041^m m median;
GGT (xULN)^#	0.9	0.8	1.0	0.738^m m median;
Direct bilirubin (mg/dL)^#	0.2	0.2	0.2	0.273^m m median;
Albumin (g/dL)^* * mean ± standard deviation;	3.7 ± 0.5	3.6 ± 0.4	3.7 ± 0.5	0.304^t t Student's t test;
Prothrombin activity (%)^* * mean ± standard deviation;	79.9 ± 15.5	72.6 ± 11.5	82.2 ± 16.0	0.012^t t Student's t test;

NOSA			Number	Percentage
ANA (+)	ASM (-)	LKM1 (-)	3	4.5
ANA (+)	ASM (+)	LKM1 (-)	1	1.5
ANA (+)	ASM (+)	LKM1 (+)	1	1.5
ANA (-)	ASM (+)	LKM1 (-)	9	13.6
ANA (-)	ASM (+)	LKM1 (+)	1	1.5
ANA (-)	ASM (-)	LKM1 (+)	1	1.5

Characteristics	Total		NOSA (+)		NOSA (-)		p
Characteristics	n	%	n	%	n	%	p
Significant fibrosis^* * mean ± standard deviation;	17	38.6	8	72.7	9	27.3	0.012^f f Fisher's exact test.
Marked periportal activity^# # periportal activity ≥ 3.	9	22.0	4	44.4	5	15.6	0.087^f f Fisher's exact test.

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