Two-locus Involvement in the Association of Human
Leukocyte Antigen with the Extrahepatic Manifestations of
Autoimmune Chronic Active Hepatitis
YANINA MARCOS,’ HUGOA. FAINBOIM,3 MONICACAPUCCHIO,l JORGEFINDOR,’JORGE DARUICH,~
RE YES,^ MARCEL0 PANDO,’ GRACIELA
BEATRIZ NORA MENDEZ,3 M. LEONARDO
DEL c . THEILER,~
LEONARDO FAINBOIM~
‘Laboratorio de Inmunogenktica and 2Division Gastroenterologia, Seccidn Hepatologia, Hospital de Clinicas, Universidad
de Buenos Aires, and “Hepatopatias Infecciosas, Hospital F.J. Muiiiz, Buenos Aires, Argentina
We investigated the association of human leukocyte
antigen antigens and type 1 chronic active “autoim-
mune” hepatitis in a population of 66 white Argen-
tinian patients, taking into account the different
manifestations of the disease. Standard microlympho-
cytotoxicitywas used for human leukocyte antigen A,
B, C, DR and DQ typing. Human leukocyte antigen class
2 alleles were also typed on genomic DNA by means of
polymerase chain reaction amplification and hybrid-
ization to sequence specific oligonucleotides. A pri-
mary association with human leukocyte antigen DR4
was present (human leukocyte antigen DR4: 44% in
patients vs. 29% in controls; 9, 6.6; p = 0.02, relative
risk, 2.1). However, a novel association was observed
with human leukocyte antigen A l l (31%in patients vs.
6%in the contmk $,26.3; corrected p = 0.001: relative
risk, 6.8). Moreover, of the 20 human leukocyte antigen
A l l patients, 18 had extrahepatic manifestations asso-
ciated with autoimmune chronic active hepatitis. This
represented 60% of the patients bearing this form of
the diae~ar3e(n = 30), conferring a relative risk of 22.2
($,46.3; corrected p = 0.00008). In this group, human
leukocyte antigen DR3 and DR4 had a weak asso-
ciation. When present together, human leukocyte an-
tigen DR4 and human leukocyte antigen A l l had a
synergistic a e c t , yielding an odds ratio of 367. Statis-
tical anal* and family segregation studies suggest
that the two loci products may represent independent
risk factorsfor this form of autoimmune chronic active
hepatitis. This synergistic effect was not evident with
A l l @US DR3. In autoimmune chronic active hepatitis
patients without extrahepatic manifestations, a weak
association with human leukocyte antigen DR6 was
found. Interestingly, in autoimmune chronic active
hepatitis of childhood (in which extrahepatic manifes-
tations a m seldom observed) a strong association with
Received August 30, 1993;accepted January 18, 1994.
L.Fainboim and M.L.Satz are members of CONICET. M.L.Satz is a recipient
of a Biotechnologg Career Fellowship from the Rockefeller Foundation.
Addreas reprint requests to: Dr. L. Fainboim, Hospital de Clinicas, Av.
C6rdoba 2351,pis0 3 (1120)Buenos Aires, Argentina.
Copyright 0 1994 by the American Association for the Study of Liver
Diseases.
0270-9139194$3.00 + 0 3111/54878
1371
SATZ’ AND
human leukocyte antigen DR6 was recently observed
in patients from the same ethnic group and geographic
region. The clinical and genetic heterogeneity ob-
served in this study may explain the weak human
leukocyte antigen associations reported previously for
autoimmune chronic active hepatitis and suggest that
the extrahepatic forms in patients with autoimmune
chronic active hepatitis represents a separate clinical
entity. (HEPATOLOGY 1994;19:1371-1374.)
Autoimmune CAH (A-CAH) is a progressive liver
disease characterized by piecemeal necrosis accom-
panied by hyperglobulinemia,circulating autoantibodies
and marked female prevalence. In up to 48% of these
patients extrahepatic manifestations are also observed
( 1).Since the first report by Mackay and Morris, several
studies have demonstrated the association of A-CAH
with human leukocyte antigens (HLAs) (2-4). These
studies, performed in an Anglo-Saxon population,
showed a primary association with HLA-B8 and HLA-
DR3 antigens. Donaldson et al. ( 5 )described a secondary
association with HLA-DR4 and revised all the conflicting
results obtained when the association of HLA with
A-CAH was analyzed in different ethnic groups. In this
study, we investigated the association of HLA with
A-CAH in Argentina, taking into account the different
manifestations of the disease. Only patients with clas-
sical or “lupoid type 1” A-CAH, characterized by the
presence of antinuclear antibody (ANA),smooth muscle
antibody (SMA) or both were selected for this work. A
new association of A-CAH with two HLA locus products
was found in patients with extrahepatic manifestations
of this disease.
PATIENTS AND METHODS
Patients. Sixty-fivewhite Argentinian patients (52females)
with the diagnosis of type 1 A-CAH were referred from two
different liver units for the HLA study. All were seronegative
for HBV and hepatitis C virus. None had history of drug or
alcohol abuse. All were positive for ANA, SMA or both, with
titers of 1 :80 or greater, aU had the histopathological picture
of CAH and all were negative for liver-kidney microsomal
1372 MARCOS ET AL. HEPATOLOGY
June 1994

1. Frequency of selected HLA markers in A-CAH patients

TABLE
Marker Patients (%) Controls n (%) RR P p Value p, Value
~~~ ~~ ~~ ~~~ ~~ ~ ~

AU A-CAH patients
HLA-A11 20 (31) 14 (6) 6.8 25.3 0.00002 0.001
HLA-DR3 16 (25) 37 (19) 1.6 1.6 NS NS
HLA-DR4 28 (44) 57 (29) 2.1 5.6 0.02 NS
HLA-DR6 16 (25) 34 (17) 1.7 2.3 NS NS
A-CAH patients with extrahepatic autoimmunity
HLA-A11 18 (60) 14 (6) 22.2 46.3 0.000001 0.00008
HLA-DR3 10 (36) 37 (19) 2.4 4.3 0.036 NS
HLA-DR4 14 (50) 57 (29) 2.4 4.9 0.025 NS
HLA-DR6 3 (11) 34 (17) 0.65 0.5 NS NS
A-CAH patients without extrahepatic autoimmunity
HLA-A11 2 (6) 14 (6) 1.1 0.025 NS NS
HLA-DR3 6 (18) 37 (19) 1.0 0.003 NS NS
HLA-DR4 14 (41) 57 (29) 1.7 2.1 NS NS
HLA-DR6 13 (38) 34 (17) 3.0 7.64 0.006 NS

All A-CAH patients: n = 65 (HLA-A,B,C), and n = 62 (HLA-DR,DQ); A-CAH patients with extrahepatic autoimmune diseases: n = 30
(HLA-A,B,C),and n = 28 (HLA-DR,DQ); A-CAH patients without extrahepatic manifestations, n = 35 (HLA-A,B,C) and n = 34 (HLA-DR,DQ).
Controls: n = 231 (HLA-A,B,C); n = 197 (HLA-DR,DQ).

antibodies. Autoantibodies were tested by means of indirect
immunofluorescenceusing appropriate rat tissues. At presen-
tation of the disease, all but two patients (one with acute liver
failure and one who had previously received corticosteroids)
were carefully studied for the presence of associated au-
toimmune diseases as follows. Patients were referred to the
rheumatology department for evaluation of joint diseases.
Thyroid involvement was assessed on the basis of the levels of
TSH, triiodothyronine and thyroxine (by RIA) and the
presence of antibodies to thyroglobulin, thyroid epithelial
microsomal antigens or both (by means of indirect immuno-
fluorescence).Coomb’s tests were performed in three patients
with anemia. The diagnosis of Sjogren’s syndrome in a patient
with subjective dryness of mouth and eyes was based on the
Schirmer test. Patients with abnormal urinary sediment were
further studied for immunological renal disease. Special care
was taken in the diagnosis of skin-associated diseases and type
1diabetes.
Extrahepatic manifestations were present in 30 patients (28
females; mean age, 43.0 yr; range, 16 to 68 yr). These included
Coomb’s positive hemolytic anemia (3 patients), pericarditis
and pleuritis (1 patient), Sjogren’s syndrome (1 patient),
thyroid disease with thyroid autoantibodies (7 patients),
membranoproliferative glomerulonephritis (1patient), photo-
sensitivity (1 patient), psoriasis vulgaris (1 patient) and
arthritis (18 patients). In this group, three patients had more
than one extrahepatic disease. A second group of 35 A-CAH
patients (24 females; mean age, 38.6 yr; range, 17 to 73 yr)
showed only chronic liver disease without any detectable
extrahepatic manifestations.
At this writing, the patients have been followed in the clinic
for periods between 3 mo and 15yr (mean, 10 yr), during which
time all but one has been treated with various combinations of
prednisolone and azathioprine or prednisolone alone. All but
one have had sustained remission on this therapy throughout.
One patient first seen with cirrhosis died as a consequence of
portal hypertension during the follow-up period. A similar
response to this standard therapy was observed in patients
with or without extrahepatic manifestations.
TiSam Icsping. HLA-ABC (65 patients) and DR,DQ (62
patients) phenotyping was performed by means of standard
complement-dependent microcytotoxicity assay using sera
from the X and XI International Histocompatibility Work-
shops supplemented with local sera. HLA-DR typing was
performed with DR-positive cells isolated by use of immuno-
magnetic beads (Dynabeads; Dynal Inc., Great Neck, NY).
Antigen frequencies were compared against those of a panel
comprising 231 (HLA-ABC)and 197 (HLA-DR)normal indi-
viduals of the same ethnic group.
HLA C i b s ZZ DNA Icsping. HLA class I1 DNA typing was
performed in accordancewith protocols of the XI International
Histocompatibility Workshop (XI-IHW). Polymorphic do-
mains of DRB, DQB and DQA loci were amplified from genomic
DNA with the set of primers designed for the XI-IHW.
Amplified DNA was dotted onto nylon membranes and
hybridized to 32P-labeledoligonucleotides probes distributed
for the XI-IHW studies. Frequencies in patients were com-
pared with those from a panel of 55 normal individuals of the
same ethnic group.
Statistics. HLA antigen frequencies in A-CAH and control
panels were compared for significant differences by means of
x2 analysis. We estimated the strength of association by
calculating odds ratios and expressed these values as relative
risks (RRs). The method of Woolf-Haldanewas used for these
calculations (6). For the previously reported associations
between A-CAH with DR3, DR4 (2-5), and DR6 (Fainboim L,
et al., Human Immunol 1994: in press), the p values derived
from x2 statistics were taken as significant without further
correction. For the new associations found here, we corrected
p values (P,) by multiplying for the total number of com-
parisons involved (77 antigens). Analysis of the combined
effect of two different loci on susceptibility to A-CAH was
performed by an analysis similar to that described by Svejgaard
et al. (7, 8).
RESULTS AND DISCUSSION
The analysis of the frequencies of HLA-A, B, C, DR
and DQ antigens in the 65 A-CAH patients studied
confirmed the previously described increased frequency
of HLA-DR4 in other populations (Table 1).However, no
association with HLA-DR3 and only a very weak
 Vol. 19, No. 6, 1994
HEPATOLOGY MARCOS ET AL. 1373

TABLE
2. Odds ratios for the effects of MA-A11 with MA-DR4 or DR3 in the extrahepatic manifestation of A-CAB
Combination No. of patients No. of controls Odds ratio Xp Value p. Value

HLA-A11AUA-DR4
+I+ 10 0 357.0 15.4 0.0003
+I- 7 13 9.4 14.5 0.0004
-/+ 4 57 1.3 0.2 NS
-I- 7 127 - - -
HLA-A1lkILA-DR3
+I+ 7 5 24.5 23.3 0.00003
+/- 10 8 22.2 28.5 0.00001
-I+ 3 32 1.9 1.0 NS
-I- 8 152 - - -

“Patients” refers to patients with A-CAH showing extrahepatic manifestations. HLA-DR typing was not available for two patients (one with
HLA-All); therefore this analysis was performed in 28 patients. A total of 13 HLA-A11 controls was included. (DR,DQ typing was not available
in one additional A l l control.)
Odds ratios and x2 and p, values were calculated by comparison of the combination in question with a - I - combination.

association with DR4 was present in our population. A
new primary association with HLA-A11 was found (31%
in patients vs. 6% in controls; RR, 6.8; P, = 0.001).
Interestingly, 18 of the 30 patients (60%) with extrahe-
patic manifestations had HLA-A11 (x2, 46.3; p, =
0.00008; RR, 22.2). In this clinically different group, a
weak association with HLA-DR3 was also observed, and
the frequency of HLA-DR4 remained significantly in-
creased (Table 1). In the group of A-CAH patients
without any detectable extrahepatic manifestations,
only a sigdicant association with HLA-DR6 was found.
Interestingly, a recent study of our laboratory in a group
of 52 pediatric A-CAH patients showed a strong asso-
ciation with HLA-DR6 (DRB1*1301 haplotype), with an
RR of 16.2 (Fainboim L, et al., Human Immunol 1994:
in press). It is worth mentioning that in this group of
children, only two patients had extrahepatic manifesta-
tions. Taken together, all the data support the idea that
A-CAH patients with extrahepatic manifestations may
define a separate clinical entity with a different genetic
predisposition.
As mentioned above, A-CAH patients with extrahe-
patic manifestations had increased frequencies of HLA-
A l l , DR3 and DR4. To assess a possible synergistic
effect of the class I and class I1 HLA loci in determining
susceptibility to this form of the disease, we followed the
approach described by Svejgaard et al. and Morling et al.
(6,7) (Table 2). Whereas HLA-A11 alone (in the absence
of DR4) conferred high susceptibility (odds ratio, 9.41,
HLA-DR4 alone (in the absence of HLA-All) was not a
risk factor for the extrahepatic forms of A-CAH (odds
ratio, 1.3). The joint expression of HLA-A11 and
HLA-DR4 showed a dramatic synergistic effect in
conferring susceptibility to extrahepatic A-CAH. Indi-
viduals positive for HLA-A11 and HLA-DR4 were highly
predisposed to extrahepatic A-CAH, with an odds ratio
of 357, a value si&cantly higher than that obtained by
multiplying the independent risk factors obtained with
HLA-A11 and DR4. This synergistic effect was not
observed for HLA-AllLHLA-DR3 (Table 2).
It was possible for us to study segregation of HLA
antigens in one family, and our study showed that
HLA-A11 and DR4 were present in separate haplotypes,
suggesting that the increased risk provided by these two
antigens would not involve extended haplotypes.
To analyze whether a particular HLA-DR4 allelic
variant was involved in this association, DR4 subtypes
were studied by means of DNA amplification and
oligotyping in 14 DR4 patients with A-CAH, including
patients with and without extrahepatic manifestations.
On comparing patient data with a panel of 19 DR4
normal individuals of the same ethnic group, no sig-
nificant differences were found between patients and
controls (DRB1*0401, 14% patients vs. 5% controls;
0402,0% vs. 16%; 0403,7% vs. 16%; 0404,21% vs. 26%;
0405,29% vs. 10%; 0406,0% vs. 5%;0407,14% vs. 21%;
041 1,14%vs. 0%).This finding is in agreement with the
DR4 association reported in A-CAH patients of Japanese
origin (9, 10). Also, the DQA and DQB alleles were
investigated in this group of DR4 patients so that we
might analyze their extended haplotypes. The results
showed that DQB1*0301 was present in 5 of 15 normal
DR4 individuals and in 1 of 13 DR4 A-CAH patients.
HLA-DQB1*0302 was present in 10 of 13 patients (vs. 9
of 15 controls). These differences were not statistically
different.
In conclusion, a new and strong association of
HLA-A11was present in A-CAH patients with extrahe-
patic manifestations. Although HLA-DR4 was asso-
ciated with A-CAH, this class I1 product was a weak
primary risk factor for this form of the disease; however
it showed a strong synergistic effect when present with
A l l . This observation may reflect the fact that extra-
hepatic forms of disease in patients with A-CAH rep-
resent a separate clinical entity. On the other hand, it is
evident that in different ethnic groups A-CAH is
associated with various HLA antigens: DR3 in Anglo-
Saxon patients, DR4 in Japanese patients and A l l in
Latin American Caucasian individuals. It would be
interesting to reevaluate the data obtained in other
ethnic groups to see whether the HLA-DR3 and DR4
associations are restricted to either group of patients
(with or without extrahepatic disease). This is relevant
when one takes into account the fact that all the relative
1374 MARCOS ET AL. HEPATOLOGY
June 1994

risks obtained with these alleles reported in the lit- 3. Opelz G, Vogten AJ, Summerskill WH, Schalm SW, Terasaki PI.
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reported preliminary findings also showing an increase 5. Donaldson PT, Doherty DG, Hayllar KM, McFarlane IG, Johnson
of HLA-A11 in A-CAH patients with multiple extrahe- PJ, Williams R. Susceptibility to autoimmune chronic active
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