<i>HFE</i> MUTATIONS AND IRON OVERLOAD IN PATIENTS WITH ALCOHOLIC LIVER DISEASE

COSTA-MATOS, Luís; BATISTA, Paulo; MONTEIRO, Nuno; HENRIQUES, Pedro; GIRÃO, Fernando; CARVALHO, Armando

doi:10.1590/S0004-28032013000100008

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ORIGINAL ARTICLES • Arq. Gastroenterol. 50 (1) • Jan-Mar 2013 • https://doi.org/10.1590/S0004-28032013000100008 copy

HFE MUTATIONS AND IRON OVERLOAD IN PATIENTS WITH ALCOHOLIC LIVER DISEASE

Authorship SCIMAGO INSTITUTIONS RANKINGS

Context

Alcoholic liver disease (ALD) is generally associated with iron overload, which may contribute to its pathogenesis, through increased oxidative stress and cellular damage. There are conflicting reports in literature about hemochromatosis (HFE) gene mutations and the severity of liver disease in alcoholic patients.

Objectives

To compare the prevalence of mutations in the hemochromatosis (HFE) gene between patients with ALD and healthy controls; to assess the relation of HFE mutations with liver iron stores and liver disease severity.

Methods

Liver biopsy specimens were obtained from 63 ALD patients (during routine treatment) and 52 healthy controls (during elective cholecystectomy). All individuals underwent routine liver function tests and HFE genotyping (to detect wild-type sequences and C282Y, H63D, S65C, E168Q, E168X, V59M, H63H, P160delC, Q127H, Q283P, V53M and W164X mutations). Associations between HFE mutations and risk of excessive liver iron stores, abnormal serum ferritin, liver fibrosis, or necroinflammatory activity were assessed by multivariate logistic regression analysis.

Results

ALD patients had significantly higher serum ferritin and transferrin saturation than controls (both P<0.05), but the distribution of HFE mutations was similar between the two groups. For ALD patients, the odds ratio for having at least one HFE mutation and excessive liver iron stores was 17.23 (95% confidence interval (CI): 2.09-142.34, P = 0.008). However, the presence of at least one HFE mutation was not associated with an increased risk of liver fibrosis or necroinflammatory activity. Active alcohol ingestion showed the strongest association to increased serum ferritin (OR = 8.87, 95% CI: 2.11-34.78, P = 0.003).

Conclusions

ALD patients do not present with a differential profile of HFE mutations from healthy controls. In ALD patients, however, the presence of at least one HFE mutation increases the risk of having excessive liver iron stores but has no detectable effects on liver disease activity or severity.

Alcoholic liver disease; Membrane proteins; Iron; Hemochromatosis

	ALD (n = 63)	Controls (n = 52)	P
Age, years	53.17 ± 10.74	48.35 ± 15.38	NS
Males, %	84.1	28.8	<0.0001
Active alcoholism, %	61.9	-	-
Daily consumption, g	164.76 ± 55.37	-	-
Lifetime total consumption, kg	2227.63 ± 1044.30	-	-
Significant fibrosis^* * perisinusoidal and portal/periportal fibrosis, bridging fibrosis, or cirrhosis , %	65.1	-	-
Cirrhosis, %	41.3	-	-
MELD	7.63 ± 4.55	-	-
WBC, x10⁹/L	6.02 ± 2.08	6.35 ± 1.66	NS
Hemoglobin, g/L	13.47 ± 1.12	13.92 ± 1.12	NS
Creatinine, mg/dL	0.89 ± 0.27	0.79 ± 0.15	0.036
Serum iron, µg/dL	115.59 ± 58.38	97.10 ± 37.10	NS
Serum ferritin, ng/mL	450.24 ± 404,62	160.64 ± 131.23	<0.0001
Transferrin saturation, %	39.40 ± 19.91	30.12 ± 11.78	0.035
CRP, mg/dL	0.96 ± 1.55	0.50 ± 0.65	NS

	ALD (n = 63)	Controls (n = 52)	P
WT/WT	61.9	65.4	NS
WT/C282Y	1.6	0	NS
C282Y/H63D	3.2	0	NS
WT/H63D	27.0	26.9	NS
H63D/H63D	3.2	1.9	NS
WT/S65C	1.6	5.8	NS
H63D/S65C	1.6	0	NS
At least one HFE mutation	38.1	32.7	NS

	At least one HFE mutation (n = 24)	WT/WT HFE (n = 39)	P
Age, years	52.04 ± 10.81	53.87 ± 10.80	NS
Males, %	79.2	87.2	NS
BMI	26.62 ± 3.04	26.75 ± 3.44	NS
Active alcoholism, %	54.2	66.7	NS
Daily consumption, g	172.0 ± 50,64	160.31 ± 58.28	NS
Lifetime total consumption, kg	2277.58 ± 1127.48	2196.90 ± 1003.84	NS
Significant fibrosis^* * perisinusoidal and portal/periportal fibrosis, bridging fibrosis or cirrhosis , %	58.3	69.2	NS
Necroinflammatory activity, %	20.8	30.8	NS
Significant iron liver stores^ Iron stores Perls grade 2 or higher , %	37.5	12.8	0.031
Serum iron, µg/dL	118.54 ± 57.98	113.80 ± 59.30	NS
Serum ferritin, ng/mL	512.25 ± 469.47	412.08 ± 360.26	NS
Transferrin saturation, %	41.12 ± 22.33	38.35 ± 18.50	NS
MELD	7.13 ± 4.36	7.95 ± 4.69	NS
WBC, x10⁹/L	6.18 ± 2.08	5.92 ± 2.07	NS
Neutrophils, x10⁹/L	3.88 ± 1.79	3.73 ± 1.62	NS
Lymphocytes, x10⁹/L	1.55 ± 0.54	1.50 ± 0.56	NS
Haemoglobin, g/L	13.86 ± 1.99	13.23 ± 1.98	NS
Platelets, x10⁹/L	148.71 ± 74.24	152.36 ± 94.69	NS
MCV, fL	98.60 ± 7.49	96.74 ± 6.25	NS
INR	1.15 ± 0.20	1.22 ± 0.25	NS
Albumin, g/dL	3.95 ± 0.58	3.61 ± 0.89	NS
Alkaline phosphatase, UI/L	104.89 ± 45.99	128.74 ± 70.01	NS
GGT, UI/L	172.15 ± 164.81	252.57 ± 271.38	NS
ALT, UI/L	38.75 ± 14,65	44.13 ± 35.99	NS
AST, UI/L	58.83 ± 46.26	60.05 ± 33.38	NS
Total bilirubin, mg/dL	1.96 ± 3.81	1.58 ± 1.28	NS
Creatinine, mg/dL	0.90 ± 0.23	0.89 ± 0.3	NS
CRP, mg/dL	1.25 ± 2.31	0.78 ± 0.80	NS

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[1] Correspondence: Dr. Luís Costa Matos - Serviço de Medicina Interna I, Centro Hospitalar Tondela-Viseu E.P.E. - 3504-509, Portugal. E-mail: costamatos.luis@gmail.com