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Autoimmune Thrombocytopenic Purpura and Helicobacter pylori Infection
Marc Michel, MD;
Mehdi Khellaf, MD;
Lionel Desforges, MD;
Ketty Lee, MD;
Annette Schaeffer, MD;
Bertrand Godeau, MD;
Philippe Bierling, MD, PhD
Arch Intern Med. 2002;162:1033-1036.
ABSTRACT
Background The mechanisms triggering the production of platelet autoantibodies
in autoimmune thrombocytopenic purpura (AITP) are poorly understood. Recently,
marked improvements in platelet counts have been reported in patients with
AITP and concurrent Helicobacter pylori infection
after eradication of H pylori by a standard antibiotic
regimen. We looked for an association between H pylori
infection and AITP in adults.
Methods Fifty-one adults of white French origin, negative for human immunodeficiency
virus (mean ± SD age, 40 ± 19.8 years), with AITP and a platelet
count of less than 50 x 103/µL at onset were included.
Thirty-five consecutive nonthrombocytopenic patients (mean ± SD age,
43 ± 22 years) of the same origin and with unknown H pylori status served as control subjects. Antibodies against H pylori were detected by means of an agglutination method
in both patients and control subjects. Sex ratio, mean age, hemorrhagic manifestations,
response to corticosteroid therapy, and final outcome were compared in H pylori–negative and H pylori–positive patients with AITP. To test for a possible molecular
mimicry mechanism, we also used an immunoblot assay to look for specific H pylori antibodies in platelet eluates from 3 H pylori–positive patients with AITP.
Results Seroprevalence of H pylori in patients with
AITP (15 [29%]) was not significatively different from that in control subjects
(10 [29%]). The H pylori–positive and H pylori–negative patients with AITP did not differ
in main characteristics at AITP onset, response rate to corticosteroids, and
final outcome. None of the 3 patients investigated had H pylori antibodies in platelet eluates.
Conclusion Although the role of H pylori in a subgroup
of patients with AITP cannot be excluded, we found no evidence of an association
between H pylori infection and AITP.
INTRODUCTION
AUTOIMMUNE thrombocytopenic purpura (AITP) is an acquired bleeding disorder
in which autoantibodies bind to platelet surface, leading to platelet destruction.1 The mechanisms triggering the production of platelet
autoantibodies are poorly understood. In childhood, AITP is usually an acute
self-limited problem; in contrast, AITP in adults is most often chronic, and
up to 25% of cases of chronic AITP are refractory to standard therapy. Recently,
it was suggested that Helicobacter pylori may contribute
to AITP pathogenesis, as partial or even complete remission of thrombocytopenia
has been reported in a few patients after eradication of H pylori.2-6
However, although there is evidence implicating H pylori in some autoimmune disorders,7-9
the link between H pylori infection and AITP remains
speculative.
The aim of our study was to compare the prevalence of H pylori infection in a group of patients with AITP with that in a
group of nonthrombocytopenic control subjects. We also compared the main characteristics
and outcome of AITP between H pylori–positive
and H pylori–negative patients and looked for
cross-reactivity between platelet and H pylori antibodies.
PATIENTS AND METHODS
PATIENTS
Fifty-one unselected adults (older than 18 years) of white French origin
with AITP and whose H pylori infection status was
not known were included in the study. All patients had a definite diagnosis
of AITP according to usual criteria10 and presented
with a platelet count of less than 50 x 103/µL at AITP
onset. Patients infected with the human immunodeficiency virus were not included.
Initial treatment of AITP is standardized in our center. Briefly, all
patients received corticosteroids at a mean dosage of 1 mg/kg per day for
3 weeks as a first-line therapy. Patients with life-threatening hemorrhages
also initially received intravenous immune globulin at a dosage of 1 to 2
g/kg per day.11 Treatment was considered effective
if the platelet count rose to 50 x 103/µL and increased
at least 2-fold. Splenectomy was considered only in patients with a chronic
outcome, ie, when the platelet count remained below 50 x 103/µL
after at least 6 months of follow-up.
Acute AITP was defined by a treatment-free remission of thrombocytopenia
(platelet count >150 x 103/µL) within 6 months of AITP
onset.
The severity of the hemorrhagic syndrome at AITP onset was assessed
by means of a clinical severity scale taking the following items into account:
cutaneous purpura (localized, score of 1; extensive and/or progressive, 3;
associated with large ecchymoses, 4), hemorrhagic oral bullae and/or spontaneous
gingival bleeding (score, 4), epistaxis (unilateral, score of 2; bilateral,
3), macroscopic hematuria (score, 5), gastrointestinal tract hemorrhage (score,
5), major menorrhagia and/or metrorrhagia (score, 5), and bleeding on the
fundus oculi in the absence of other causes (score, 5). The age at onset was
considered as an independent risk factor of bleeding (age >65 years, score
of 1; age >80 years, 3).
CONTROL GROUP
Thirty-five unselected patients older than 18 years, seen consecutively
in our department during a 1-month period (March 1 to April 1, 2000) served
as control subjects. Since the seroepidemiologic characteristics of H pylori infection differ between countries,12
only individuals of white French origin were included. None of them had a
history of thrombocytopenia. Their H pylori infection
status and history were not known.
DETECTION OF H PYLORI ANTIBODIES
An agglutination method (Pyloriset kit TMEIA-G; Orion Diagnostica, Helsinki,
Finland) was used to detect anti– H pylori
antibodies of IgG type in both patients and control subjects. In patients,
tests were performed on serum samples collected and frozen when AITP was diagnosed.
None of the patients had been previously treated with intravenous immune globulin.
All serologic tests in the control group were performed consecutively on fresh
samples.
DETECTION OF PLATELET AUTOANTIBODIES
Patients were screened for circulating and surface-bound IgG and IgM
antiplatelet antibodies by an indirect13 and
a direct suspension immunofluorescence technique on paraformaldehyde-fixed
platelets.14 In patients in whom platelet antibodies
were detected in serum samples by indirect suspension immunofluorescence technique,
the presence of antibodies directed against specific platelet membrane targets
was investigated by a direct and indirect monoclonal antibody–specific
immobilization of platelet antigens assay with the use of a panel of monoclonal
antibodies directed against platelet membrane glycoprotein (Gp) IIb-IIIa,
GpIa-IIa, and GpIb-IX as previously described by Kiefel15
with minor modifications.16
PLATELET ELUATES
To determine whether H pylori antibodies could
cross-react with platelet-membrane antigens, an immunoblot assay (Mikrogen,
Martinsried, Germany) was used to test platelet eluates from 3 H pylori–positive patients with AITP. This immunoassay was used
to detect IgG and IgA antibodies directed against specific H pylori antigens (CagA, VacA, UreB, HspA, HsB, FlaA, and UreA). Platelet
eluates were obtained by an ether-elution method16
and were also tested for the presence of platelet antibodies by means of the
indirect suspension immunofluorescence technique and the indirect monoclonal
antibody–specific immobilization of platelet antigens assay.
STATISTICAL ANALYSIS
Patients were compared with controls and H pylori–positive patients with H pylori–negative
patients for AITP characteristics and outcome. Results are expressed as mean
± SD. A  2 test (or Fisher exact test if necessary)
was used for comparison of categorial data, and the nonparametric Mann-Whitney
test was used for comparison of quantitative data. A P
value of less than .05 was considered significant.
RESULTS
PATIENT CHARACTERISTICS
Fifty-one patients, including 13 men (25%) and 38 women (75%), with
AITP were included. The mean ages of patients (40 ± 19.8 years) and
control subjects (43 ± 22 years) were not significantly different.
The mean platelet count in patients at AITP onset was 21 x 103/µL (range, 1-50 x 103/µL). The course
of AITP was chronic in 42 patients (82%) and acute in 9 (18%). Splenectomy
was required in 14 patients with chronic AITP. All patients were alive after
a median follow-up of 10 months (range, 6 months to 10 years) from AITP onset.
None of the patients had a history of gastric or duodenal ulcer. After AITP
onset, only 2 (4%) of the 51 patients underwent an upper digestive endoscopy,
one for dyspepsia related to a peptic esophagitis and the other for occult
bleeding associated with a duodenal ulcer; H pylori
was present only in the duodenal biopsy specimen of the second patient. At
the time of AITP diagnosis, only 1 patient was being treated by a proton pump
inhibitor for dyspepsia; none of the patients had received antibiotics during
the 4 weeks before AITP onset.
Fifteen (29%) of the 51 patients with AITP and 10 (29%) of the 35 control
subjects (P = .93) were seropositive for H pylori.
CHARACTERISTICS AND OUTCOME OF AITP
The mean age at AITP onset was slightly higher in H pylori–positive patients (47.8 years; range, 19-92 years) than
in H pylori–negative patients (35.5 years;
range, 18-75 years) (P = .05).
Neither the main features of AITP nor the response to corticosteroids
was significantly different between H pylori–positive
and H pylori–negative patients (Table 1).
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Comparison of Patients With Autoimmune Thrombocytopenic Purpura Positive
and Negative for Helicobacter pylori
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H PYLORI IMMUNOBLOT ON PLATELET ELUATES
Helicobacter pylori–specific antibodies
were sought by immunoblotting on platelet eluates in 3 H pylori–positive patients with AITP who had circulating platelet
antibodies detected by indirect suspension immunofluorescence technique and
in whom platelet eluates were available. None of them had detectable anti–H pylori antibodies in platelet eluates. Conversely, platelet-associated
antibodies were detected on platelet eluates in 2 of the 3 patients tested,
specifically directed against GpIIb-IIIa and GpIb-IX, as detected by means
of monoclonal antibody–specific immobilization of platelet antigens
assay in one patient.
COMMENT
Helicobacter pylori is a ubiquitous gram-positive
bacterium involved in the pathogenesis of gastric and duodenal ulcers. Recently,
the involvement of H pylori has also been suggested
in various autoimmune diseases, including megaloblastic anemia17-18
and extraintestinal diseases such as Sjögren syndrome and immune thyroiditis.7, 9 Previous in vitro studies suggested
that H pylori has the potential to initiate autoreactivity
through molecular mimicry, since monoclonal antibodies directed against H pylori may also react with ductal cells of the salivary
glands and renal tubular cells.8 Within the
past 2 years, a role for H pylori in the pathogenesis
of AITP has been suggested because significant and, in some cases, very substantial
improvements in platelet count have been reported after H pylori eradication with a standard antibiotic regimen3-7
from patients with AITP and concurrent H pylori infection.
However, 3 of the relevant reports are anecdotal case reports2, 4-5
and 2 are uncontrolled brief reports.3, 6
Therefore, the implication of H pylori in pathogenesis
of AITP is not backed by strong evidence.
We compared the prevalence of antibodies directed toward H pylori in patients with AITP and in ethnically matched controls.
Although a positive culture obtained from gastric biopsy samples is considered
the gold standard to confirm active H pylori infection
or carriage,19 we used a blood antibody detection
method for the following reasons: (1) Endoscopic methods of H pylori isolation were not feasible in our patients with a platelet
count less than 50 x 103/µL at AITP onset. (2) Nonendoscopic
methods of detection, such as urea breath tests or stool antigen testing,
did not allow retrospective determination of the patients' H pylori carriage or previous infection status. (3) The reliability
(sensitivity of 95.8% and specificity of 95.5%) of the enzyme immunoassay
kit has been validated.20
The observed prevalence of anti–H pylori
antibodies was similar in patients with AITP and control subjects and consistent
with the expected value of 25% to 35%, observed in the French adult population.21
We also compared H pylori–positive and H pylori–negative patients with AITP and found that
neither clinical and biological characteristics of AITP nor the response to
corticosteroids and final outcome were influenced by the serologic H pylori status.
Finally, a molecular mimicry mechanism has been demonstrated in human
immunodeficiency virus–related immune thrombocytopenia,22
and has been suggested by Emilia et al6 as
the possible mechanism for H pylori–associated
AITP. We therefore performed an H pylori immunoblot
assay on platelet eluates obtained in 3 of our H pylori–positive patients, and there was no evidence of cross-reactivity
between platelet and H pylori antibodies.
In conclusion, although the implication of H pylori infection in the pathogenesis of AITP in a particular subgroup of
patients cannot be expressly ruled out by our case-control study, we found
no evidence of an association between these 2 conditions. Moreover, since
spontaneous remissions can occur in chronic AITP,23
controlled trials comparing the effect of an H pylori
eradication therapy with that of a placebo are warranted to determine whether
the subgroup of patients with AITP and active H pylori
infection may benefit from eradication of H pylori.
AUTHOR INFORMATION
Accepted for publication September 18, 2001.
Corresponding author and reprints: Marc Michel, MD, Service de Médecine
Interne, CHU Hôpital Henri-Mondor, 51 Av du Mal de Lattre de Tassigny,
94010 Créteil CEDEX, France (e-mail: Marc.MICHEL8{at}wanadoo.fr).
From the Service de Médecine Interne (Drs Michel, Khellaf, Schaeffer,
and Godeau), Laboratoire de Bactériologie (Dr Desforges), and Laboratoire
d'Immunologie Leuco-plaquettaire, Etablissement Français du Sang (Drs
Lee and Bierling), Hôpital Henri-Mondor, Créteil, France.
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