ARTICLE
Auteur(s) : Ana C
Hernando-Harder1, Nina Booken2, Sergij
Goerdt2, Manfred V Singer1, Hermann
Harder1
1Department of Medicine II (Gastroenterology,
Hepatology and Infectious Diseases), University Hospital
Mannheim, Mannheim, Germany
2Department of Dermatology, University Hospital
Mannheim, Theodor-Kutzer-Ufer 1-3, D-68167 Mannheim, Germany
accepté le 3 Mai 2009
Two Australian researchers, Barry J. Marshall and Robin Warren,
discovered the curved bacillus Campylobacter pyloridis, which was
later named Helicobacter pylori (H. pylori) in 1982. For this
discovery they were awarded the Nobel Prize of 2005 in Physiology
or Medicine [1, 2]. They had rebutted a long-standing dogma in
medical science that stress and lifestyle factors lead to gastritis
and peptic ulcer disease. Their work and later work by others
established an irrefutable link between the presence of the
gram-negative, flagellate, and microaerophilic bacilli and peptic
ulceration [1, 3], distal gastric adenocarcinoma [2, 4], and
gastric lymphoma [5]. The clinical manifestations of infection with
this bacillus were shown to depend on the host, environmental, and
bacterial factors.
Since then, many reports have emerged describing the
pathogenetic potential of H. pylori. Not only does this pathogen
cause local tissue damage in the gastric mucosa, it also has been
implicated in a variety of diseases that are sometimes not even
related to the gastrointestinal tract. These include, but are not
limited to: mucosa-associated lymphoid tissue lymphomas (MALT
Lymphomas) [6-8], inflammation of the coronaries [9, 10], iron
deficiency anemia [11], rheumatological conditions [12-14],
dermatologic diseases [12, 15-36], as well as a variety of other
disorders (table 1).
Various mechanisms have been proposed in an attempt to explain
the extra intestinal manifestations of H. pylori infections. These
include: atrophic gastritis, an increase in gastric vascular
permeability during infection, release of inflammatory mediators,
molecular mimicry and systemic immune response. As an example,
antigastric autoantibodies have been found in more than 30% of
patients who are infected with H. pylori [39]. An increase in
permeability of the gastric and intestinal mucosa in infected
patients has also been demonstrated [41], and may result in
increased exposure to alimentary antigens. Of note is that it is
well known that the immunological response elicited by H. pylori is
an important determinant of the amount of gastric mucosal damage.
Thus the production of large amounts of various proinflammatory
substances, such as cytokines, eicosanoids, and proteins of the
acute phase, follows gastric colonisation by H pylori [37]. This
inflammatory response may lead to the development of
antigen-antibody complexes or cross-reactive antibodies (by
molecular mimicry) resulting in damage to other organs [40]. It has
been proposed that H. pylori induces a phenomenon similar to that
seen in the molecular mimicry between hemolytic streptococcus group
A antigens and host proteins resulting in both humoral and
cell mediated autoimmune reactions and ultimately causing rheumatic
fever and rheumatic heart disease [38]. Based on these
observations, investigators have examined the role of H. pylori as
a pathogenic determinant for idiopathic extra intestinal diseases,
in which immune dysregulation is implicated. A competing
theory that is also being discussed is that an infection-induced
immune response continues after the pathogen has been eradicated.
This could explain why patients with confirmed eradication therapy
failed to show improvement in short-term observations.
This review aims to provide a brief introduction on the
pathophysiology of gastric H. pylori infection and its diagnosis.
It then reviews current knowledge on the role of H. pylori
infection in the pathogenesis of dermatologic diseases taking into
account the available medical literature between 1988 and 2008.
Gastric Helicobacter pylori infection
H. pylori is one of the most common pathogens affecting humans,
infecting approximately 50% of the world’s population. It is found
more frequently in developing countries than in industrialized
countries, presumably due to poor sanitary conditions [39]. The
outcome of the infection depends on a combination of factors:
bacterial virulence, host factors, and environmental factors (table 2) [40]. Ulceration and carcinogenesis
are mutually exclusive outcomes of this infection. H. pylori
infection is a very persistent infection, and in areas of high
prevalence, repeated infections are common [39, 41]. The bacteria
have been isolated from feces, saliva and dental plaques of
infected patients, which suggests that the fecal-oral route is a
possible transmission mode [42].
The pathogen is a gram-negative spiral shaped bacterium that has
the unique ability to colonize the human gastric mucosa [1]. Some
virulence factors such as urease and flagella are present in all
strains and are necessary for the pathogenesis and colonization of
the gastric mucosa. With its flagella, the bacterium moves through
the gastric lumen and drills into the gastric mucosal layer. The
presence of the flagella, and thus motility, is required for
persistent gastric colonization [43]. The main bacterial factors
associated with pathogenicity comprise outer membrane proteins,
including the vacuolating cytotoxin VacA, and the products of CagA.
An interaction between bacterial factors such as CagA and host
signal transduction pathways seems to be critical for mediating
cell transformation, cell proliferation, invasion,
apoptosis/anti-apoptosis, and angiogenesis [44]. The key
pathophysiological event in H. pylori infection is initiation and
continuance of an inflammatory response. Bacteria or their products
trigger this inflammatory process the main mediators of which are
cytokines [4, 45]. This response is related to the expression of
proinflammatory cytokines, both on the surface epithelium and in
macrophages/monocytes [46-49]. Another putative virulence
determinant is the neutrophil-activating protein (NapA) gene, a
gene that was shown to be induced by contact with the epithelium
(iceA1) [50]. In the last 19 years, Helicobacter-like organisms
like Helicobacter mustelae and Helicobacter hepaticus have been
also detected.
Table 1 Diseases with a proven or suspected
pathophysiological role of Helicobacter pylori.
|
Gastroduodenal diseases [6-8, 12, 50, 180]
|
Gastric cancer
|
|
Gastritis
|
|
MALT lymphoma
|
|
Peptic ulcer
|
|
Cardio- and cerebrovascular diseases [181-185]
|
Coronaritis
|
|
Primary headache
|
|
Primary Raynaud phenomena
|
|
Stroke
|
|
Dermatologic diseases [13-37]
|
Alopecia areata
|
|
Atopic dermatitis
|
|
Behçet’s disease
|
|
Chronic urticaria
|
|
Immune thrombocytopenic purpura
|
|
Lichen planus
|
|
Progressive systemic sclerosis
|
|
Chronic prurigo multiformis
|
|
Nodular prurigo
|
|
Pruritus
|
|
Psoriasis
|
|
Recurrent aphthous stomatitis
|
|
Rosacea
|
|
Schoenlein-Henoch purpura
|
|
Sjögren Syndrome
|
|
Sweet syndrome
|
|
Lung diseases [186]
|
Bronchial asthma
|
|
Chronic obstructive bronchiectasia
|
|
Lung cancer
|
|
Pulmonary disease
|
|
Hepato-biliary diseases [187-190]
|
Cholangiocellular carcinoma
|
|
Gallstones formation
|
|
Hepatocellular carcinoma
|
|
Intestinal diseases [191-194]
|
Enteric diseases
|
|
Inflammatory bowel diseases
|
|
Neurologic diseases [195]
|
Alzheimer disease
|
|
Others [11, 196-198]
|
Extragastric MALT-lymphoma
|
|
Growth retardation
|
|
Iron deficiency anemia
|
Table 2 Clinical outcome of Helicobacter pylori
infection [40].
|
Clinical outcomes
|
|
70% asymptomatic
|
|
10-23% peptic ulcer
|
|
1-3% gastric carcinoma
|
|
< 1% gastric MALT lymphoma
|
Diagnosis of Helicobacter pylori
The available diagnostic methods are summarized in table 3. Carbon 13 or 14 urea breath test (UBT) and
the stool antigen tests are non-invasive tests that can be used for
testing in the clinical setting. Serology kits for the presence of
antibodies in the blood can also be applied with high accuracy. The
commonly used medication proton pump inhibitor leads to false
negative breath and stool antigen tests, but does not affect the
results of serological tests. Proton pump inhibitors should be
stopped at least 2 weeks before performing a breath test or a stool
antigen test. It is recommended to perform a follow-up test in
patients who underwent H. pylori eradication using urea breath
tests. If this diagnostic procedure is not available a
laboratory-based stool antigen test, preferably using monoclonal
antibodies, could be used [50].
Table 3 Diagnostic procedures of Helicobacter pylori
infection.
|
Non-invasive tests
|
|
|
Carbon 13 or 14 urea breath test
|
|
Stool antigen test
|
|
Serology
|
|
Invasive diagnostic tests
|
|
|
Histology
|
|
Rapid urease test
|
|
Molecular methods
|
Helicobacter pylori and chronic urticaria
Chronic urticaria (CU) is a recalcitrant skin disease characterized
by pruritic wheals lasting more than six weeks [51] in the absence
of a physical cause. The pathogenesis of CU has not yet been fully
elucidated and a triggering factor can be indentified in only a
minority of cases. The symptoms of chronic urticaria are caused by
the release of histamine and other vasoactive mediators induced by
the binding of an allergen to a specific receptor on mast cells.
Potential trigger factors include persistent infections and
infestations, pseudoallergic reactions to non-steroidal
anti-inflammatory drugs and food additives and/or autoreactive
mechanisms. These have been proposed as etiological factors for
mast cell degranulation [52-55]. However, in most cases the absence
of an identifiable trigger results in considering the urticaria as
idiopathic.
A possible association between H. pylori infection and chronic
urticaria has been proposed [56-61], and several mechanisms have
been implicated. One proposed mechanism is that an increase in
gastric vascular permeability during infection results in greater
exposure of the host to alimentary allergens [62]. In support of
this suggestion duodenal ulcer patients have a higher incidence of
allergic manifestations than controls. IgE-containing cells in
gastric and duodenal mucosa seem to be the culprits [63], although
there is limited evidence for HP-specific IgE [64, 65]. Thus, the
possibility that patients with urticaria develop specific IgE
against H. pylori is an attractive pathogenic explanation that
unfortunately has not been confirmed yet.
The immunomodulatory role of H. pylori infection in CU is a
subject of intensive debate. This immunomodulation is not only
dependent on the virulence of H. pylori but also on host and
environmental factors. An alternative possibility is that
immunological stimulation by chronic infection may produce, through
mediator release, a non-specific increase in sensitivity of the
cutaneous vasculature to agents that enhance vascular permeability.
Furthermore, IgG and IgA antibodies to 19-kDa H. pylori-associated
lipoprotein were found to play role in the pathogenesis of CU [66,
67]. Moreover, H. pylori causes pronounced complement
consumption due to H. pylori specific antibodies. This contributes
further to the pathogenesis of CU [68, 69]. As recent studies have
demonstrated, IgG autoantibodies against IgE and/or Fc εRi α can be
found in the sera of one-third of patients with CU, and it is
postulated that infection with H. pylori may induce production of
pathogenetic antibodies possibly by molecular mimicry [70].
A growing body of evidence suggests that 30-50% of CU results
from an autoimmune process involving functional histamine-releasing
anti-Fc ε RI α autoantibodies or less commonly,
anti-IgE-autoantibodies [71, 72]. Once this occurs, the production
of antibodies might continue even after the eradication of H.
pylori infection, explaining the lack of clinical improvement after
eradication seen in some studies (table
4). Appelmelk et al. [70] first demonstrated the
molecular mimicry between H. pylori and lipopolysaccharide (LPS)
and anti-Lewis antibodies in autoimmune type-B gastritis. Further
evidence was provided by the highly positive autologous serum skin
test (ASST) results in chronic urticaria patients with H. pylori
IgG antibodies [73].
Conflicting reports have been published. Some suggest that H.
pylori eradication in patients with CU leads to an improvement in
the symptoms of CU [60-74], while others showed no improvement
(table 4).
The study by Magen et al. 2007, uses well-accepted
standardized parameters to evaluate urticaria activity and found a
significant decrease in urticaria activity score in HP-eradicated
but not in non-eradicated CU patients [56].
Yadav et al. conducted a study to assess the prevalence of
HP infection and effect of bacterium eradication on skin lesions in
patients with chronic urticaria. In this study there was a high
prevalence of HP infection, with 48 (70%) of the patients with CU
and 46 (67%) of the controls testing positive for HP. The
prevalence of HP in CU patients does not differ from that in
patients without urticaria. But in infected patients there was a
resolution of urticarial symptoms when HP eradication therapy was
given. Patients of CU with HP-associated gastritis had a mean
pretreatment CU-Q 2 oL score of 70.92 ± 12.59, mean post treatment
score of 40.05 ± 10.35 (mean change 30.87 ± 12.19), which was
statistically significant, P = 0.001, confidence interval at 5%
level of significance [75].
Bakos et al. evaluated 56 patients with urticaria using
gastroduodenoscopy. 33 patients had a positive urea breath test
associated with mild gastritis on histology (score 1.3) [66].
Ojetti et al. studied 33 patients with CU. 57% CU patients and
64% controls (p > 0.05) were found to be infected with H.
pylori. In all patients, endoscopic evaluation showed mild to
moderate gastric hyperemia, and no evidence of peptic ulcer disease
[76]. Wedi et al. assessed 100 patients with chronic
urticaria. 47 of them had serologic evidence of H. pylori exposure.
Twenty seven patients underwent endoscopic gastroduodenal
examination. The presence of antral gastritis (100%) and corpus
gastritis (46%) was confirmed histologically [25]. Thus these three
groups found evidence of gastric inflammation in all patients with
H. pylori positivity, but none had gastric or duodenal ulcers. Caig
et al. studied 88 patients with CU. The 13C urea breath test
was positive in 49 of them (56%). 20 patients underwent an upper
endoscopy, but none had either gastrointestinal symptoms or
endoscopic lesions [74]. To summarize, clinical trials including
large numbers of patients are needed to establish a possible
relationship between endoscopic gastrointestinal findings and
CU.
To cure at least some patients from quality-of-life reducing CU,
it seems worthwhile to eradicate H. pylori in all patients with CU
and H. pylori infection. A positive effect is proposed for the
eradication of H. pylori (grade C recommendation) [77].
Table 4 Studies on the frequency of H. pylori infection
and the effect of eradication therapy in patients with chronic
urticaria. Complete remission (> 90% improvement), partial
remission (50-90% improvement), or no improvement (< 50%
improvement). C: Clarithromycin; A: amoxicillin; M: metronidazole;
L: lanzoprazol (Proton pump inhibitor); UBT: urea breath test.
|
Author Country Year
|
Nr. of CU patients test for H. pylori/% HP (+)
|
Nr. of treated Patients with HP (+)
|
Therapy
|
Complete remission/total eradication/%
|
Partial remission
|
|
Magen et al. Israel, 2007
|
78 58%
|
45
|
OAC
|
Not stated
|
|
|
Vazquez et al. Spain, 2004
|
55
|
Not stated
|
Not stated
|
75%
|
|
|
Fukuda et al. Japan, 2004
|
50 52%
|
19
|
LA and C or M
|
6/17 35%
|
11/17 65%
|
|
Sakurane et al. Japan, 2002
|
50
|
Not stated
|
Not stated
|
Not stated
|
|
|
Gaig et al. Spain, 2002
|
Not stated
|
49
|
OAC
|
> 70%
|
|
|
Dauden et al. Spain, 2000
|
25 68%
|
15
|
OAC
|
8/14 57%
|
|
|
Hook-Nikanne et al. Finland, 2000
|
235 25%
|
53
|
LM and A or T
|
3/5 60%
|
|
|
Erel et al. Turkey, 2000
|
38 76%
|
29
|
OAC
|
1/25 4%
|
|
|
Wustich et al. Germany, 1999
|
30 80%
|
24
|
OA
|
8/24 33%
|
|
|
Schnyder et al. Switerland, 1998
|
46 24%
|
11
|
LA
|
1/3 33%
|
|
|
Valsecchi et al. Italy, 1998
|
125 62%
|
31
|
OCM
|
3/29 10%
|
|
|
Bonamigo et al. Brazil, 1999
|
18 67%
|
18
|
Not stated
|
6/12 50%
|
4/12 33%
|
|
Ozkaya-Bayazit et al. Turkey, 1998
|
35 77%
|
23
|
OAC
|
5/17 29%
|
|
|
Wedi et al. Germany, 1998
|
100 47%
|
39
|
OAC
|
14/21 66%
|
|
|
Di Campli et al. Italy, 1998
|
42 55%
|
18
|
LAC
|
13/16 81%
|
|
|
Tebbe et al. Germany, 1996
|
25 68%
|
17
|
A or C or T and MBO
|
8/17 47%
|
6/17 35%
|
Helicobacter pylori and rosacea
Rosacea is a chronic cutaneous disorder affecting primarily the
convexities of the central face (cheek, nose, chin, and central
forehead), often characterized by remissions and exacerbations
[78]. Although the fundamental pathogenesis of rosacea remains
unknown, inflammation plays a central process in this disorder.
Recent evidence suggests that this inflammation is associated with
the generation of reactive oxygen species (ROS) that are released
by inflammatory cells such as neutrophils. In addition, effective
treatment of the disease with topical [79] or systemic [80] drugs
with antioxidant properties suggests that rosacea may be indeed be
related to increased ROS activity and to deficient function of the
antioxidant system of affected individuals.
Recently, there have been several investigations suggesting a
possible etiological role for H. pylori in rosacea [19, 26, 32, 67,
81-96]. Some of these investigations have shown that the prevalence
of H. pylori infection in patients with rosacea is higher than that
in control subjects [82] or average values, while others have
reported that H. pylori eradication treatment reduces the severity
of rosacea [63, 82-84, 91, 96, 97]. Additionally, it has been shown
that H. pylori can increase serum or tissue levels of nitrous oxide
(NO) [92], a free radical, which is important in a number of
different physiological processes in the skin, including
vasodilatation, inflammation, and immune modulation. Thus, it has
been postulated that NO [92] produced by H. pylori might cause the
flushing and erythema associated with rosacea, or that it may have
a pathogenic role in the inflammation seen in rosacea. Increased
ROS activity [98, 99] and decreased plasma antioxidant compounds,
such as ascorbic acid, have been detected in H. pylori-infected
patients. It has also been reported that the reduced circulating
levels of vitamin C in H. pylori-infected subjects may contribute
to the etiology of some diseases associated with antioxidant
deficiency [100]. Inadequate antioxidant protection or excess
production of ROS creates a condition known as oxidative stress,
which is thought to play an important role in skin cancers,
cutaneous aging, and many inflammatory skin diseases [80, 100].
Bonamigo et al. studied 62 patients with rosacea and 124
controls without rosacea. The data in this study show that: (i)
patients with rosacea do not have a higher frequency of dyspeptic
symptoms or a personal history of proven peptic disease; (ii) there
do not appear to be differences in the frequency of exposure to H.
pylori at different stages in the evolution of rosacea; and (iii) a
weak association was found between exposure to H. pylori and
rosacea, but stratified analysis showed that previous use of
antibiotics modified the relationship between the factor studied
and outcome [88].
Szlachcic and colleagues studied 60 subjects with skin lesions
typical of rosacea. 53 (88.3%) had confirmed H. pylori infections
as compared to only 39 (65%) of the non-ulcer disease controls.
This interesting study showed a beneficial effect of H. pylori
eradication in H. pylori-positive patients with acne rosacea, which
led to a disappearance of the skin manifestations in 51 of 52
treated subjects [19]. The results led the authors to conclude that
H. pylori eradication could be used in patients with rosacea that
is unresponsive to conventional therapy. However, whether this
effect is due to the eradication of H. pylori infection or is
related to the cure of other concomitant infections is still
unclear. In the endoscopic examination, 72% of the rosacea subjects
had chronic active gastritis, predominantly antritis, 10% had
chronic active multifocal inflammation of the stomach, and the
remaining 18% had both antritis and chronic inflammation of the
body of the stomach [19].
Boixeda de Miquel [96] and colleagues studied 44 patients
diagnosed with rosacea. H. pylori infection was found in 84.1%.
This supported a relationship between H. pylori and rosacea, and
suggested that the presence of H. pylori infection should be ruled
out in patients with rosacea because an appreciable percentage of
these patients can benefit from eradication therapy, mainly
patients with the papulopustular subtype. In this study, upper
gastrointestinal endoscopy was performed in 37 patients. The
findings in gastroduodenoscopy were: 5.4% duodenal ulcer; 5.4%
erosive duodenitis; 18.9% chronic gastritis; 2.7% acute gastritis;
and 67.6% of the cases had a normal examination.
Utaş et al. investigated the effect of H. pylori
eradication therapy in 25 patients with rosacea and 87 healthy
controls. The seroprevalence of H. pylori was similar in both
groups. An upper gastrointestinal endoscopy and a rapid urease test
were performed on the 13 patients with rosacea. There was no
statistical difference in seropositivity between both groups. In H.
pylori-positive rosacea patients there was a significant decrease
in the severity of rosacea after eradication. These findings
suggested that H. pylori may be involved in rosacea and that
eradication may be beneficial [82].
However, further evidence from randomized clinical trials is
required to confirm the effect of H. pylori eradication in patients
with rosacea. A relationship between endoscopic
gastrointestinal findings and rosacea could not be established yet.
Prospective trials are necessary to confirm this association. At
this time, and despite the promising data reviewed eradication of
H. pylori in patients with rosacea is not generally
recommended.
Helicobacter pylori and psoriasis
Psoriasis is an inflammatory skin disease that affects 1-3% of
Caucasians and may be persistent, disfiguring and stigmatizing.
There is a wide range of severity, but even when the affected body
surface area is relatively limited the impact on day-to-day
activities and social interactions may be significant [101]. Recent
genetic and immunological advances have greatly increased
understanding of the pathogenesis of psoriasis as a chronic,
immune-mediated inflammatory disorder [102].
It has been suggested that H. pylori infection of gastric mucosa
may be one of the organisms capable of triggering psoriasis [16,
28, 103], but to date this remains controversial. In an
uncontrolled study of 33 patients with psoriasis and without any
history of chronic gastrointestinal tract complaints, the
seroprevalence of H. pylori infection was 27% [24]. Three patients
were treated for H. pylori infection without apparent improvement
in their psoriasis. Daudén et al. studied the CagA
seroprevalence patients with psoriasis and concluded that the more
virulent CagA positive strains of H. pylori did not seem to be
strongly associated with psoriasis [34]. Recently, in another study
in 50 psoriatic patients, the prevalence of H. pylori
sero-positivity was significantly higher than in the control group
[29]. There are contradicting reports on the benefits of H. pylori
eradication in patients with chronic psoriasis [28, 36].
Prospective trials are needed to confirm this association.
Helicobacter pylori and Sjögren’s syndrome
Patients with Sjögren’s syndrome (SS) are more prone to have H.
pylori infection in comparison to patients with other connective
tissue diseases [104]. Serum antibody titers to H. pylori
correlated with an index for clinical disease manifestations, age,
disease duration and C-reactive protein levels. Assessment of H.
pylori infection in older patients suffering from active SS for a
relatively long duration is therefore recommended, especially those
who have been suffering from primary SS for more than 3 years
[105].
The possible relationship between H. pylori and autoimmune
diseases (including Sjögren’s syndrome) has been made particularly
intriguing by a series of studies reporting an autoimmune reaction
in bacterial-induced gastritis [106, 107]. A number of
different autoantibodies in H. pylori infection have been described
in the last few years. Among these, the anticanalicular
autoantibodies seem to be directed against H+K+-ATPase and to
correspond, in part, to the classic antiparietal cell antibodies of
autoimmune gastritis (type A), whereas the antifoveolar antibodies
appear to have less clinical relevance. Patients with
anticanalicular autoantibodies against H+K+-ATPase could develop
corpus atrophy with decreased acid secretion, [108, 109] subsequent
loss of H. pylori and transition to classic autoimmune
gastritis/pernicious anemia [110, 111]. It is not clear whether the
gastritis associated with autoimmunity represents a truly different
type of H. pylori gastritis or whether there are transitions
between one type and the other. What seems likely is that the
autoimmune reaction induced by H. pylori occurs in susceptible
individuals [112]. Susceptibility to develop an autoimmune reaction
following a microbial infection could be linked to the particular
immune background of the host such as that of patients with
Sjögren’s syndrome.
In a Japanese study the mean titers of anti-H. pylori antibodies
was significantly higher (P < 0.05) in 7 patients with Sjögren
syndrome than in 24 age-matched controls with chronic pulmonary
disease [104]. In Finland, Collin et al. [113] studied 32
consecutive patients with primary Sjögren syndrome and 64 age- and
sex-matched controls using upper endoscopy. Although atrophic
gastritis of the antrum was found more frequently in the patients
with Sjögren syndrome (25% vs. 4%; P < 0.01), there was no
significant difference in the prevalence of H. pylori infection
(31% vs. 39%; P > 0.05). In a study by Sorrentino et al.
[114] H. pylori infection was equally prevalent among dyspeptic
Sjögren’s syndrome patients (185 cases) and dyspeptic controls.
Likewise, there were no differences regarding anti CagA prevalence
or antigastric autoantibodies between the two groups. Similarly,
Theander et al. [115] could not find higher H. pylori
seropositivity in 164 Swedish patients with primary SS compared to
controls. Thus good evidence is lacking for an association between
H. pylori infection and Sjögren syndrome.
Helicobacter pylori and Schoenlein-Henoch
purpura
Schoenlein-Henoch purpura (SHP) is a leukocytoclastic vasculitis of
small vessels with deposition of IgA, commonly resulting in skin,
joint, gastrointestinal, and kidney involvement. SHP is
characterized by IgA deposition in the affected tissues [116].
Although the pathogenesis of SHP remains poorly understood, various
factors including infection and drug allergy are considered to be
pathogenic [117, 118]. The disease typically develops after
infections, especially streptococcal infections of the upper
respiratory tract. Recently, single case reports with incomplete
follow-up have described an association between H. pylori infection
and SHP [119-123]. Randomised controlled trials will be necessary
to confirm a relationship between H. pylori and Schoenlein-Henoch
purpura.
Helicobacter pylori and alopecia areata
Alopecia areata affects 1-2% of the population and is hypothesized
to be an autoimmune, organ specific T-cell mediated reaction
directed against the human hair follicle [124]. The potential
pathogenic mechanism involved could be a cross-reaction. However,
in a study in 30 patients Rigopoulos et al. [125] found no
significant difference in the seroprevalence of H. pylori infection
between patients with alopecia areata and healthy controls. In
contrast, Tosti et al. [126] studied a group of 68 consecutive
patients with alopecia areata, and found that the seroprevalence of
H. pylori infection was higher than in age-matched controls.
Randomised controlled trials will be necessary to confirm this
association.
Helicobacter pylori and atopic dermatitis
Atopic dermatitis (AD) is a complex multifactorial disease,
characterized by a chronic pruritic cutaneous inflammation. This
condition occurs predominantly in infancy and childhood, with an
increase in prevalence over the last few years [127].
A positive association between H. pylori antibodies and food
allergy presenting with gastrointestinal symptoms has recently been
reported. A subset of a H. pylori strain possesses an antigen,
CagA, as a virulence factor. Anti H. pylori and anti-CagA IgG titer
have been determined in children with atopic dermatitis as the sole
clinical manifestation of food allergy. Corrado et al.
demonstrated a positive association between H. pylori antibodies
and food allergy in 30 children with gastrointestinal symptoms
[128]. Recently, Galadari et al. studied 20 patients with
atopic dermatitis. The prevalence of H. pylori infection was
significantly higher (p < 0.05) compared to controls. Murakami
et al. reported a case of AD and H. pylori infection in a
14-year-old girl: AD was successfully treated by eradication of H.
pylori without any treatment for the skin lesions [129]. Some data
seem to suggest that the increase in H. pylori antibodies may occur
prior to AD. H. pylori, by damaging gastric mucosa, may trigger a
food allergy reaction [130]. Later, an increase in IgE serum levels
induces the synthesis and release of cytokines, sustaining chronic
allergic inflammation, such as that seen AD. Moreover, it has been
stressed that Staphylococcus aureus may promote AD by an IgE
mediated immune response [131]. It is tempting to hypothesize that
H. pylori may also induce a similar immunological event. Clinical
trials are necessary to confirm these promising preliminary
results.
Helicobacter pylori and Sweet syndrome
Sweet syndrome, or acute febrile neutrophilic dermatosis, is
characterized by the acute onset of fever, leukocytosis, and
erythematous plaques infiltrated with neutrophils. Sweet syndrome
can present in three different forms: classical (or idiopathic),
malignancy-associated, and drug-induced [132]. The etiology of
Sweet syndrome remains unknown, even though it is presumed to be a
hypersensitivity reaction which leads to the production of a
cascade of cytokines that induce neutrophil activation and
infiltration. An association between H. pylori and Sweet syndrome
has been proposed. However, only one case report can be found on
this presumed association [133].
Helicobacter pylori and progressive systemic
sclerosis
Progressive systemic sclerosis (PSS) is a chronic multi systemic
disease characterized by the excess deposition of connective tissue
in the skin and internal organs, and is associated with
microvasculature changes and immunologic abnormalities. The cause
of PSS remains unclear. An increasing body of evidence suggests
that there are many potential environmental triggers for PSS and
that host factors determine the susceptibility of the host to
disease in response to these triggers [134]. Infectious agents,
both bacterial and viral, have long been suspected as a
contributing factor in the development and progression of PSS. The
rationale for this “infection hypothesis” is that many PSS-like
symptoms are transiently elicited by infectious agents in otherwise
healthy individuals. There are two general lines of evidence
implicating bacterial infections in the pathogenesis of PSS. One is
anecdotal evidence that treatment with antibiotics relieves PSS
symptoms in some patients. The other is that graft-versus-host
disease, which is recognized as having many similarities to PSS,
cannot be induced in germ-free animals and is significantly reduced
in children pre-treated with antibiotics to eradicate their normal
bacterial flora [135].
The most recent research on the involvement of bacterial
infections in the pathogenesis of PSS focuses on H. pylori, which
has been implicated in other vascular diseases [10]. Studies have
investigated H. pylori infections for an association with Raynaud’s
phenomenon, Sjögren syndrome, and PSS. In a study of patients with
primary Raynaud’s phenomenon, eradication of H. pylori infection
was associated with complete disappearance of the episodes of
Raynaud’s phenomenon in 17% of treated patients and a reduction in
symptoms in an additional 72% [136]. Although this study was not
double blinded, it is intriguing that symptoms of Raynaud’s
phenomenon did not improve in those patients in whom eradication of
H. pylori failed. A more recent trial of comparable design
reported very similar results [137]. One study identified higher
incidence rates of serological evidence of H. pylori infection in
patients with rheumatological diseases, including PSS [138]. In
contrast, three larger studies found no difference in H. pylori
infection rates between patients with PSS with Raynaud’s phenomenon
compared to healthy controls [139-141]. However, even if it were
true that H. pylori infection rates do not correlate with PSS, this
does not necessarily rule out its involvement in PSS. A recent
study [142] indicated that, despite the absence of a difference in
H. pylori infection rates between PSS patients and control
subjects, 90% of patients with PSS were infected with the virulent
CagA strain compared with only 37% of the infected control
subjects. Therefore, confounding factors such as co-infections,
differences in H. pylori strains, and immunological and genetic
host factors will have to be further identified and controlled in
order to understand the role of H. pylori in Raynaud’s phenomenon,
PSS, and other vascular phenomena. The association between H.
pylori infection and Raynaud’s syndrome [140, 142] has been
attributed to increased levels of cytokines and acute phase
reactants, such as C-reactive protein and fibrinogen, resulting in
vasospasm and platelet aggregation. Kalabay et al. [143], who
found a high prevalence of H. pylori infection in patients with
systemic sclerosis (78%) (n = 55), attempted to explain the
preferential occurrence of H. pylori infection in PSS in two ways.
First, an increased prevalence of H. pylori infection might be
favoured by the disturbed gastrointestinal motility, a clinical
phenomenon well known in patients with PSS. The second explanation
may be that H. pylori infection and the immunological mechanisms
operative in the course of PSS may be related to each other.
Clinical trials are still necessary to define the pathogenesis and
confirm the increase in association between H. pylori and PSS.
Helicobacter pylori and Behçet’s disease
Behçet’s disease (BD) is a systemic vasculitic disorder of unknown
etiology consisting of recurrent aphthous stomatitis, genital
ulcerations, and relapsing uveitis [144]. Involvement of the
intestines, blood vessels, and central nervous system is associated
with poor prognosis. Although the etiology of this disease entity
still remains unknown, various environmental and genetic factors
have been implicated in its pathogenesis. On the one hand, an
enhanced inflammatory response, overexpression of proinflammatory
cytokines, and increased expression of heat shock protein (HSP) 60
are prominent features of BD [144]. On the other hand, an
association between the presence of bacterial heat shock proteins
with positive antibody titers against H. pylori implicates
similarities between BD and H. pylori infection [145].
A genetic susceptibility for both has been implicated by the
fact that H. pylori infection is endemic in most of the countries
in which BD is also highly prevalent. Apan et al. studied 91
patients with BD. The prevalence of H. pylori IgG seropositivity
was slightly but not significantly higher in patients with BD
compared to the controls [146]. However, the prevalence of
cytotoxin-associated gene A positivity was significantly
higher in patients with BD, and the eradication of H. pylori
significantly decreased the clinical manifestations of BD, such as
oral and genital ulcerations, arthritis/arthralgia, and cutaneous
findings of Behçet’s disease. Avci et al. [146] also found
that H. pylori eradication decreased the clinical manifestations of
BD. They observed significant differences in both the number and
diameter of oral and genital ulcers, cutaneous findings, and
arthritis/arthralgia. No significant difference was observed on the
other clinical signs, however. They therefore concluded that
patients with BD should be screened for possible H. pylori
infection in the endemic area and prompt treatment should be
instituted. Ersoy et al. evaluated 45 patients with BD and 40
controls by upper gastrointestinal endoscopy. Endoscopic findings,
prevalence rates and eradication rates of H. pylori were similar
between the two groups [35] (table 5).
More randomised controlled trials will be necessary to confirm this
relationship between H. pylori and Behçet’s disease.
Table 5 Studies on the frequency of H. pylori infection
and the effect of eradication therapy in patients with Behçet
disease (BD). A: amoxicilin; O: omeprazole; M: metronidazole; C:
clarithromycin; UBT: urea breath test; RUT: rapid urease test. (1)
Patients with Behçet disease and any upper gastrointestinal
complaints were included in this study.
|
Country/ Author/Year publication
|
Nr. of BD patients test for H. pylori/Serology (IgG+)
|
Controls/Serology (+)
|
Therapy
|
Control eradication
|
Follow-up Clinical finding
|
|
Turkey/Ersoy/2007
|
45 73.3 %
|
40 75%
|
2 week A-C-L
|
75% UBT 2 month after eradication
|
Not stated
|
|
Apan/Turkey/2007
|
91 79.1% cag-A 64.8%
|
83 67.5 (N.S.) 38.5% (p = 0.002)
|
1 week A-C or M-O
|
76.9% UBT 2 month after eradication
|
Decreased number and/or diameter of oral and genital ulcers,
cutaneous findings, and arthritis or arthralgia
|
|
Avci/Turkey/1999
|
49 83.7%
|
49 71.4% (N.S.)
|
1 week C-M-O
|
65% biopsy +RUT
|
Decreased number and size of oral and genital ulcers
|
Helicobacter pylori and cutaneous pruritus
Pruritus of unknown origin is a common complaint, and systemic
causes must be ruled out. Several case reports have reported that
following resection of gastric cancer pruritus disappeared [20,
147], suggesting an association between the two entities. In this
interesting study patients underwent a diagnostic upper
gastrointestinal endoscopy to screen for gastric carcinoma, but
unfortunately other endoscopic findings were not mentioned. Gastric
cancer was detected in 2/36 (5.6%) patients with cutaneous pruritus
and 3/16 (18.8%) with prurigo chronica multiforme. These results
suggest that patients with both H. pylori infection and pruritic
skin diseases may be at increased risk for development of gastric
cancer. Therefore, endoscopic screening in such patients might be
recommended. In another study, Shiotani et al. found that the
prevalence of H. pylori infection in patients with pruritus
cutaneous was 65%, and 62% of them had a partial remission of the
symptoms after the eradication of H. pylori [63].
In a study by Kandyil et al. [148] 10 patients with severe
pruritus, unresponsive to conventional therapy, were evaluated for
H. pylori infection. Eight had evidence of an active infection. Of
these 88% had some pruritus relief after eradication. It therefore
can be concluded that patients having an H. pylori infection may
experience refractory pruritus that resolves after eradication of
H. pylori (table 6). The evidence for a
causal role of H. pylori in pruritus cutaneous needs further
evaluation, however.
Table 6 The improvement rate in cutaneous pruritus
after H. pylori eradication expressed as Nr. of patients and
percent (%). Complete remission (> 90% improvement), partial
remission (50-90% improvement) or no improvement (< 50%
improvement). C: Clarithromycin; A: amoxicillin; M: metronidazole;
L: lanzoprazol; UBT: urea breath test.
|
Therapy
|
Confirmation of eradication
|
Complete remission
|
Partial remission
|
No change
|
|
Shiotani et al. 2001
|
4 days C-A or M, - proton pump inhibitors.
|
Biopsy + UBT 4-6 weeks after eradication therapy.
|
29 (0%)
|
18 (62.1%)
|
11 (37.9%)
|
|
Sakurane et al. 2002
|
4 days to 2 weeks C-A-L
|
100 % total eradication
|
5/12
|
2/12
|
5/12
|
Chronic prurigo multiformis
Shiotani et al. evaluated 10 patients with chronic prurigo
multiformis. Five patients had complete (30%) or partial (20%)
remission following eradication of H. pylori. The authors therefore
recommend testing for the presence of H. pylori infection in
patients with prurigo chronica multiformis and to eradicate the
infection in those who test positive [63], although prospective
trials are needed to confirm these observations.
Helicobacter pylori and nodular prurigo
Neri and colleagues [149] studied 42 cases of Hide’s nodular
prurigo (NP), a pruritic skin disease of unknown origin (table 7). Evidence for H. pylori infection was
found in 40 out of the 42 patients examined. Eradication of H.
pylori was confirmed in 39/40 cases, in whom pruritus was markedly
diminished. Furthermore, microscopic examination of repeated skin
biopsies revealed improved histological features in patients who
underwent successful eradication of H. pylori. Therefore, it has
been proposed that H. pylori infection may have triggered or
enhanced vasculitis, which, in turn, may have enhanced the clinical
symptoms and signs, and the inflammatory findings on histology.
Future clinical trials will have to confirm these promising
findings.
Table 7 The improvement rate in nodular prurigo after
H. pylori eradication expressed as Nr. of patients and percent (%).
Complete remission (> 90% improvement), partial remission
(50-90% improvement) or no improvement (< 50 improvement). C:
Clarithromycin; A: amoxicillin; O: omeprazol; UBT: urea breath
test.
|
Nr. of patients with nodular prurigo
|
Serology (IgG+)
|
Biosy (+)
|
Therapy
|
Confirmation of eradication
|
Follow-up
|
|
Neri et al. 1999
|
42
|
39
|
40
|
A-C-O
|
After 3 months UBT, Confirmed eradication 39/40
|
Markedly reduced pruritus Improvement with disappearance of
perivascular inflammatory infiltrate, reduced lymphocyte infiltrate
and mild hyperkeratosis
|
Helicobacter pylori and immune thrombocytopenic
purpura
Immune thrombocytopenic purpura (ITP) is an autoimmune disease
mediated by anti-platelet autoantibodies. Accumulating evidence
suggests that eradication of H. pylori is effective in increasing
platelet count in nearly half of ITP patients infected with this
pathogen.
Since the publication of Gasbarrini et al. in 1998 [150],
several investigators, mostly in Japan and Italy, have studied the
efficacy of H. pylori eradication in increasing the platelet count
in ITP patients with evidence of H. pylori infection. In contrast
to the findings by Gasbarrini et al., studies from the United
States [151, 152] have refuted a clinical benefit from eradication
suggesting a geographical difference in the efficacy of H. pylori
eradication on ITP management. The value of H. pylori detection and
eradication in managing ITP patients has therefore not received
universal acceptance. Due to the fact that most studies
demonstrated remarkable therapeutic benefits (i.e., bacterial
eradication rate, platelet response rate, and durability of
response) of antibiotics plus proton-pump inhibitors for adult
patients with chronic ITP and active H. pylori infection [150,
153-171] (table 8), the European
Helicobacter Study Group consensus 2007 [50] has recommended the
eradication of H. pylori infection in patients with chronic
idiopathic thrombocytopenic purpura. However, due to intrinsic
limits in the design of the studies analysed, further evidence from
randomized clinical trials is required to confirm the effect of
eradication treatment on platelet count.
Only few studies in patients with ITP and H. pylori infection
carried out endoscopic evaluations. Although demonstration of H.
pylori in gastric biopsies is the gold standard of H pylori
detection, many authors preferred blood antibody detection and/or
the urea breath test due to the fact that upper endoscopy may
result in unexpected bleeding in thrombocytopenic patients,
especially in those whose platelet counts were less than 50 ×
109/L [152, 158, 161, 162, 164-167, 170-172]. Some
investigators who performed endoscopic evaluation on ITP patients
did not show the data [159, 168]. Emilia et al. studied 10
patients with ITP and H. pylori infection with gastroduodenoscopy.
All (100%) had chronic and/or atrophic gastritis [169]. In a study
by Ando et al., H. pylori infection was found in 17/20 ITP patients
(85%). All of these patients had atrophic gastritis by endoscopic
evaluation [158]. Further studies are needed to establish a
relationship between ITP, H. pylori and endoscopic findings.
Neverthelss, in patients with immune thrombocytopenic purpura and
H. pylori infection, the recommendation for eradication is commonly
accepted.
Table 8 Summary of literature published since 2004 on
the efficacy of H. pylori eradication therapy on idiopathic
thrombocytopenic purpura. HP, Helicobacter pylori; ITP, idiopathic
thrombocytopenic purpura; Plt, platelet; NA, data not available.
|
Author(s) Reference Year Country
|
HP (+)/total ITP patients (%)
|
HP eradicated/total treated (%)
|
Follow-up time (months)
|
Plt response in HP eradicated patients (%)
|
|
Rostami et al. 2008 Iran
|
79/129 (61)
|
62/71 (87)
|
48
|
30/62 (48)
|
|
Emilia et al. 2007 Italy
|
38/75 (51)
|
34/38 (85)
|
60
|
23/34 (64)
|
|
Satake et al. Japan 2007
|
26/38 (68)
|
23/26
|
26
|
13/23 (57)
|
|
Campuzano-Maya et al. 2007 Colombia
|
29/32 (97)
|
26/29
|
2,2
|
21/26 (88)
|
|
Kodama et al. 2007 Japan
|
67/116 (58)
|
44/52 (85)
|
NA (6-NA)
|
27/44 (62)
|
|
Sayan et al. 2006 Turkey
|
20/34 (59)
|
18/20 (90)
|
13 (4-24)
|
8/18 (44)
|
|
Asahi et al. 2006 Japan
|
26/37 (70)
|
26/26 (100)
|
NA (24-56)
|
16/26 (62)
|
|
Suvajdzic et al. 2006 Serbia/Montenegro
|
39/54 (72)
|
23/30 (77)
|
18
|
6/23 (26)
|
|
Ahn et al. 2006 USA
|
15/NA
|
14/15 (93)
|
NA (6-24)
|
1/15 (7)
|
|
Veneri et al. 2005 Italy
|
43/NA
|
41/43 (95)
|
31 (3-65)
|
20/41 (49)
|
|
Suzuki et al. 2005 Japan
|
25/36 (69)
|
11/13 (85)
|
NA (6-12)
|
6/13 (46)
|
|
Fujimura et al. 2005 Japan
|
300/435 (69)
|
161/207 (78)
|
NA (3-12)
|
101/163 (63)
|
|
Stasi et al. 2005 Italy
|
64/137 (47)
|
52/52 (100)
|
25 (7-42)
|
17/52 (33)
|
|
Inaba et al. 2005 Japan
|
25/35 (71)
|
25/25 (100)
|
20 (10-28)
|
11/25 (44)
|
|
Sato et al. 2004 Japan
|
39/53 (74)
|
27/32 (84)
|
6
|
15/27 (56)
|
|
Ando et al. 2004 Japan
|
17/20 (85)
|
15/17 (88)
|
24
|
10/15 (67)
|
|
Takahashi et al. 2004 Japan
|
15/20 (75)
|
13/15 (87)
|
4
|
7/13 (54)
|
|
Michel et al. 2004 USA
|
16/74 (22)
|
14/15 (93)
|
11.5 (3-18)
|
1/14 (7)
|
Helicobacter pylori and lichen planus
Lichen planus (LP) is a skin disorder easily diagnosed by means of
its characteristic clinical picture of polygonal, violaceous
papules and plaques with white lines on their surface. The
incidence of LP varies based on the geographic location, and
cutaneous LP has been reported to affect 0.2-1% of the adult
population in western countries. Although its etiology and
pathogenesis are not fully understood, LP has been associated with
multiple disease processes and agents, such as viral and bacterial
infections, autoimmune diseases, medications, vaccinations and
dental restorative materials. Infections and stress are suspected
to be the most common triggering factors (table
9).
A case-control study was conducted in 78 patients with LP. The
prevalence of H. pylori infection in patients with
chronic/refractory LP and transient LP was not significantly
different from that in patients with other skin diseases [173].
Dauden et al. [27] found that eradication of H. pylori in 10
patients resulted in partial remission in three patients, no change
in four patients and aggravation in the remaining three patients.
Later, Dauden et al. investigated the seroprevalence of CagA
in 14 patients with LP and evidence of H. pylori infection, but
could not find a strong association between CagA and LP [174]. In
conclusion, there is no clear evidence of a causal association
between H. pylori infection and LP and further studies are
needed.
Table 9 Prevalence of H. pylori in patients with lichen
planus expressed as Nr. of patients and percent (%). C:
Clarithromycin; A: amoxicillin; O: omeprazol.
|
Nr. of patients with lichen/ (Serology IgG+)
|
Control
|
Therapy
|
Eradication
|
Follow-up
|
|
Daudén et al. 2000
|
61 (75.4%)
|
58 (74.1%)
|
In 15 patients 1 week A-C-O
|
In 10 patients
|
Partial remission: 3; no change: 4; and aggravation: 3.
|
|
Daudén et al. 2003
|
14 (57.1%) (anti CagA IgG)
|
28 (64.2%) (N.S.)
|
Not stated
|
Not stated
|
Not stated
|
Helicobacter pylori and aphthous stomatitis
Recurrent aphthous stomatitis (RAS) is a disorder characterized by
painful ulcers restricted to the oral mucosa. Patients with the
recalcitrant type of this disorder have difficulties speaking,
eating, and even attending to daily activities [175]. Most experts
in dental issues do not consider RAS as a single disease entity
because there are several conditions that have clinical features
similar to RAS, such as immunological disorders, hematological
defects, allergy [176].
Several issues led investigators to study the association
between RAS and H. pylori infection. These include the association
of both with MALT (mucosa-associated lymphoid tissue), the
histological similarities between RAS and peptic ulcers [177], and
the response of RAS to the broad-spectrum antibiotics such as
tetracycline used to eradicate H. pylori infection. Therefore, a
possible role for H. pylori in the development of RAS lesions has
been proposed [50, 178], and the oral environment has been
suggested to be one of the many potential routes for transmission.
The studies of Elsheikh and colleagues [179] of 146 patients with
recurrent multiple aphthous ulcers of the oral cavity and pharynx,
support a possible causative role for H. pylori in recurrent
aphthous ulcerations with a characteristic distribution and
affinity to mucosa-associated lymphoid tissues (MALT) of the
pharynx. Mansour-Ghanaei et al. [175] studied 50 patients with
RAS. Twenty-six patients (52%) had evidence of H. pylori infection
by serological IgG antibody tests, but H. pylori DNA could only be
identified in one patient (2%). This suggests that this pathogen is
not involved in recurrent oral aphthous ulcers.
Conclusion
In the European Helicobacter Study Group consensus 2007,
eradication of H. pylori infection in patients with chronic
idiopathic thrombocytopenic purpura was recommended. Evidence for a
potential link of H. pylori infection exists for chronic urticaria,
and promising data have been reported for pruritus cutaneous,
Behçet’s disease, nodular prurigo and lichen planus, although some
of these data are still conflicting. An association between H.
pylori and other dermatological diseases such as rosacea, aphtous
stomatitis, atopic dermatitis, alopecia areata and Sjögren syndrome
has been reported in single cases, small patient series and
non-randomized trials. Still missing are randomized, double-blind,
placebo-controlled studies, with adequate diagnostic procedures and
evidence of effective eradication to support the observations.
The diagnosis of H. pylori infection was predominantly carried
out using evidence of the presence of circulating antibodies by
serological tests and/or urea breath tests. In the limited number
of studies in which endoscopic evaluation was followed by
subsequent H. pylori tests, the description of the findings was
incomplete at best. A relationship between dermatological
diseases, H. pylori infection and endoscopic findings in the upper
gastrointestinal tract cannot be definitively confirmed, and
further studies are necessary. No data are available evaluating
differences between developing and developed countries in the
prevalence of H. pylori in skin diseases, which could be a key
issue and seems to be an interesting topic for future trials.
Acknowledgments
The authors thank Dr. Inaam Nakchbandi, University of Heidelberg,
Germany, for her thoughtful input. Grant support: Research Fund of
the Mannheim Faculty of Clinical Medicine. Nr. 098200/99-245,
University of Heidelberg, Germany. Conflict of interest: none.
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