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Helicobacter pylori

Vivekanandan A
MD General Medicine II year
Institute of Internal Medicine
Madras Medical College
1/8/2014

1
Introduction
▪ Helicobacter pylori (H. pylori) remains one of the most common
worldwide human infections and

▪ It is associated with a number of important upper
gastrointestinal (GI) conditions
– including chronic gastritis,
– peptic ulcer disease,
– gastric malignancy.

1/8/2014

2
Epidemiology
▪ Almost 50% of worlds population is affected by
H.pylori
▪ Genetic studies shows that humans are infected
for more than 58000 years at time they migrated
from Africa

1/8/2014

3
Time of acquisition of
infection
In developing nations

The majority of
children's are
infected before
the age of 10
years

And almost
reaching 80%
in adults
reaching the
age of 50
years

1/8/2014

4
In united states..

Unusual
before the
age of 10
years

Reaches
10% in
adults in the
age between
18 – 30 years

Reaches
almost 50%
in those
older than
60 years

1/8/2014

5
Risk factors
1. Socioeconomic status
•
•
•
•
•

Density of housing
Over crowding
Number of siblings
Sharing the same bed
Lack of running water

2. Consumption of salted food- increases
persistence of infections and also predisposes to
risk of gastric cancer

1/8/2014

6
Hereditary and genetic
factors
▪ Hispanics and African-Americans have a higher
rate of infection than Caucasians.
▪ Monozygotic twins raised in different households
have a greater concordance of H. pylori infection
than do dizygotic twins raised apart

1/8/2014

7
Routes of transmission
▪ Humans are the major reservoir of the H.pylori

▪ Person to person transmission in the form of
1.
2.
3.

Fecal – oral
Oral – oral
Gastric – oral

1/8/2014

8
Risks of transmission
▪ Childrens who consume untreated stream
water, uncooked vegetables
▪ Exposure to diarrheal stools, vomitus of the
infected persons
▪ Dentists and oral hygienists who have exposures to
dental plaques and saliva
▪ Iatrogenic infection in the form of contaminated
endoscopes and other gastric devices

1/8/2014

9
Microbiology
▪ Morphology:
• H. pylori is a spiral shaped,
• microaerophilic, gram negative bacterium
• measuring approximately 3.5 microns in length and 0.5
microns in width
• It has multiple unipolar flagella and it is actively motile
• biochemically characterized as catalyse, oxidise, and
urease positive.

1/8/2014

10
Growth and culture characters
▪ Growth and culture characters
• It’s a slow growing organism
• can be cultured on blood agar
• selective media is Skirrow's media (with
vancomycin, polymyxin B, and trimethoprim, chocolate
medium) incubated at 37ºC in a 5 percent oxygen
atmosphere for three to seven days

• The colonies are translucent and 1–2 mm in diameter.

1/8/2014

11
Pathophysiology

1/8/2014

12
Conditions associated with
H.pylori
▪

Esophagus
1.
2.
3.

GERD
Barrett’s esophagus
adenocarcinoma

▪ Stomach
1.
2.
3.
4.
5.

▪

Acute gastritis ( sometimes self limiting)
Chronic active gastritis
Peptic ulcer disease
Gastric adenocarcinoma
MALT

Duodenum
1.

Peptic ulcer
1/8/2014

13
Non gastrointestinal diseases
associated to H.pylori
▪ Coronary artery disease

▪ Immune thrombocytopenic purpura
▪ Iron deficiency anemia
▪ Reynaud's phenomenon
▪ Scleroderma
▪ Idiopathic urticaria
▪ Acne rosacea
▪ Thyroiditis
▪ GBS
1/8/2014

14
Diagnosis – when to test
ACG recommendations

▪ Testing for H. pylori should be performed only if
the clinician plans to offer treatment for positive
results
▪ Testing is indicated in patients with gastric MALT
lymphoma, active peptic ulcer disease, or a past
history of documented peptic ulcer

1/8/2014

15
Diagnosis – when to test
▪ patients with
uninvestigated
dyspepsia who are
under the age of 55
years and have no
alarm features

alarm features

▪ Deciding which test to use
in which situation relies
heavily upon whether a
patient requires evaluation
with upper endoscopy and
the strengths, weaknesses,
and costs of the individual
tests

▪ unexplained weight loss,

▪ bleeding,
▪ anaemia,
▪ early satiety,
▪ Progressive
▪ dysphagia, odynophagia,
▪ recurrent vomiting,

▪ family history of GI
cancer, previous
esophagogastric
malignancy
1/8/2014

16
Supported by the evidence

Controversial

Indications for testing and
treatment of H.pylori infection
Active peptic ulcer disease (gastric or
Functional dyspepsia
duodenal ulcer)

▪
Confirmed history of peptic ulcer
▪

▪

Gastric MALT-lymphoma (low grade)

▪ Unexplained iron deficiency anaemia
GERD

Persons using NSAIDs or before
starting NSAIDs

or ITP

Following endoscopic resection of early
gastric cancer

▪ Populations at higher risk of gastric
cancer

▪
Uninvestigated dyspepsia (if H. pylori
population prevalence high)

1/8/2014

17
Types of diagnostic test
Non endoscopic tests

Endoscopic tests

1. Serology
(quantitative or
qualitative IgG)

1. Histology

2. Urea breath test (13C
or 14C)

3. Culture

3. Stool antigen test

2. Rapid urease test

4. Polymerase chain
reaction assay

1/8/2014

18
Serology
▪ ELISA technology to detect IgG antibodies is
inexpensive, non-invasive.
▪ high sensitivity (90 to 100%), variable specificity
(76 to 96%) & accuracy( 83 to 98%).
▪ It needs confirmation with another method such
as a stool antigen or urea breath test before
starting treatment
▪ The “serological scar’ may be present even after
successful eradication of organism

1/8/2014

19
Urea breath test (UBT)
▪ detects active H. pylori infection, confirming the
accuracy of serology and documenting successful
treatment.
▪ The specificity is more than 95%, sensitivity of the test
is 88% to 95%
▪ false-negative results reported in patients taking
antisecretory therapy such as PPIs,bismuth, or
antibiotics.
▪ antibiotics should be stopped at least four weeks and
PPIs at least one week before breath testing.

▪ UBT is not accurate in patients who have had gastric
respective surgery.
1/8/2014

20
Urea breath test (UBT)

1/8/2014

21
Stool antigen assay
▪ It is an immunoassay to detect the presence of
h.pylori antigen in stools
▪ The sensitivity and specificity are 94% and
97%, respectively
▪ sensitivity of stool testing is negatively affected by
PPIs, bismuth, and antibiotics which affects the
bacterial load
▪ Its used both for diagnosis and confirm the
eradication .

1/8/2014

22
Endoscopic tests – biopsy
urease testing
Tissue from the antral biopsy is
placed in agar well containing
urea and pH reagent
The urease cleaves the urea to
liberate ammonia
This process changes the
medium alkaline and produces a
color change
1/8/2014

23
Biopsy urease testing
▪ commercially available kits include
CLOtest, PyloriTek, and Hp-fast
▪ The CLOtest may become positive as early as one
hour after collection, but a final reading at 24 hours
is recommended

▪ The sensitivity is 90 to 95% & specificity is 95 to
100%
▪ false positive tests are unusual. False negative
results occur in recent gastrointestinal bleeding or
with the use of PPIs, H2
antagonists, antibiotics, or bismuth-containing
compounds
1/8/2014

24
Rapid urease testing
▪ To know patient's H. pylori status before discharge
from the endoscopy suite.
▪ biopsy specimens are sandwiched between a
reagent strip with a pH indicator and a pad
containing urea.

▪ One hour sensitivity is 89 to 98 percent and
specificity is 89 to 93 percent.

1/8/2014

25
Rapid urease test

1/8/2014

26
Histology
▪ In addition to make diagnosis of H.pylori the biopsy and
histology also reveals intestinal metaplasia, MALT
omas, dysplasia and neoplasia

▪ In addition to biopsying “clinically suspicious”
areas, taking multiple biopsies and sampling lesser and
greater curvatures of gastric antrum and body are
important.
▪ It is gold standard for identifying infection, with
reported sensitivity and specificity as high as 95% and
98%
▪ Limitations…
▪ Brush cytology….
1/8/2014

27
1/8/2014

28
A silver stain (Warthin Starry) of H.pylori
on gastric mucus-secreting epithelial cells
(x1000).
This picture is notorious because it is of
Dr. Marshall's stomach biopsy taken 8
days after he drank a culture of H. pylori.
1/8/2014

29
Culture
▪ Its fastidious and difficult to culture and require
special culture media
▪ Culture is indicated when treating cases not
responding to treatment and suspected antibiotic
resistance

▪ Even though the in vitro sensitivity will not
guarantee the treatment results

1/8/2014

30
This is a 3 day culture of
H.pylori on blood agar
1/8/2014

31
Treatment
▪ Triple therapy

▪ Quadruple therapy
▪ Sequential therapy

1/8/2014

32
Triple therapy
▪ It’s the most commonly
recommended therapy
▪ The duration of therapy must
be 14 days and all drugs in
BD dose

▪ The cure rate is >80%
▪ Metronidazole 500mg can be
substituted for amoxy in
penicillin allergic patients

1/8/2014

33
Quadruple therapy
▪ Dose : 4 times a day

▪ Duration : 14 days
▪ appropriate as initial
therapy in areas in which the
prevalence of resistance
to clarithromycin or
metronidazole is >20%
▪ in patients with recent or
repeated exposure to
clarithromycin or
metronidazole
Eradication rate 70 – 85%

1/8/2014

34
Sequential regimen
Regimen

Days

(PPI + Amoxy 1000 mg) BD 5 + 5
followed by
(PPI+ Clarithromycin 500
mg + Tinidazole 500 mg) BD

Eradication
rate

90%

• It has overall eradication rate better than triple

therapy 90% vs 80%

•Particularly superior if bacteria is clarithromycin
resistant ( 89% Vs 29%)
1/8/2014

35
Eradication confirmation
▪ Eradication may be confirmed by a urea breath test, fecal
antigen test, or upper endoscopy performed four weeks or
more after completion of therapy.
▪ Its indicated in following situations
1.
2.
3.
4.

Patients who have persistent symptoms after H. pylori treatment
for dyspepsia
Patients who had an H. pylori associated ulcer
Patients who had gastric mucosa associated lymphoid tissue
(MALT) lymphoma
Patients who had resection for early gastric cancer.

1/8/2014

36
Treatment failures and
persisitance of H.pylori
▪ The initial treatment results in 25% failures

▪ The reasons for failure are
1.
2.
3.
4.
5.
6.

Resistant organism
Poor compliance with medication
Alcohol consumption
Smoking
Prior antibiotic use
Underlying condition (FD Vs PUD)

1/8/2014

37
Antibiotic resistance
▪ Resistance to metronidazole is 40% in US and 11%
for clarithromycin
▪ Resistace to amox and tetracycline is less than 1%
▪ The resistance to metronidazole is overcome by
increasing doses or combining with bismuth
▪ Macrolide resistance cant overcome by increasing
dose because these are due to alterations in 23S
ribosomal RNA(A2143G, A2142G & A2142C) which
interferes with ribosomal macrolide binding

1/8/2014

38
Rescue therapy

1/8/2014

39
Side effects of treatment
▪ Side effects are reported in up to 50 percent of patients taking one
of the triple therapy regimens .
▪ The adverse effects are usually mild; fewer than 10 percent of
patients stop treatment due to side effects
1. The most common side effect is a metallic taste due
to metronidazole or clarithromycin.
2. Metronidazole can cause a peripheral neuropathy, seizures, and
a disulfiram-like reaction when taken with alcohol.
3. Clarithromycin can cause taste alteration, nausea, vomiting,
abdominal pain, and rarely QT prolongation.
4. Tetracycline can induce a photosensitivity reaction in some
cases. It should also not be administered to pregnant women or
young children.
5. Amoxicillin can cause diarrhea or an allergic reaction with skin
rash.
1/8/2014

40
Take home message
1. H. pylori is a common worldwide infection.

2. Established indications for H. pylori cure include
peptic ulcer,(MALT) and uninvestigated
dyspepsia.
3. Non-endoscopic and endoscopic tests are
available toidentify H. pylori.
4. Proton pump inhibitor (PPI), clarithromycin, and
amoxicillin or metronidazole or a
PPI, bismuth, tetracycline,and metronidazole for
10–14 days are accepted first line treatment
1/8/2014

41
Thank you….

John Robin Warren

Barry James Marshall 42
1/8/2014

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Helicobacter pylori

  • 1. Helicobacter pylori Vivekanandan A MD General Medicine II year Institute of Internal Medicine Madras Medical College 1/8/2014 1
  • 2. Introduction ▪ Helicobacter pylori (H. pylori) remains one of the most common worldwide human infections and ▪ It is associated with a number of important upper gastrointestinal (GI) conditions – including chronic gastritis, – peptic ulcer disease, – gastric malignancy. 1/8/2014 2
  • 3. Epidemiology ▪ Almost 50% of worlds population is affected by H.pylori ▪ Genetic studies shows that humans are infected for more than 58000 years at time they migrated from Africa 1/8/2014 3
  • 4. Time of acquisition of infection In developing nations The majority of children's are infected before the age of 10 years And almost reaching 80% in adults reaching the age of 50 years 1/8/2014 4
  • 5. In united states.. Unusual before the age of 10 years Reaches 10% in adults in the age between 18 – 30 years Reaches almost 50% in those older than 60 years 1/8/2014 5
  • 6. Risk factors 1. Socioeconomic status • • • • • Density of housing Over crowding Number of siblings Sharing the same bed Lack of running water 2. Consumption of salted food- increases persistence of infections and also predisposes to risk of gastric cancer 1/8/2014 6
  • 7. Hereditary and genetic factors ▪ Hispanics and African-Americans have a higher rate of infection than Caucasians. ▪ Monozygotic twins raised in different households have a greater concordance of H. pylori infection than do dizygotic twins raised apart 1/8/2014 7
  • 8. Routes of transmission ▪ Humans are the major reservoir of the H.pylori ▪ Person to person transmission in the form of 1. 2. 3. Fecal – oral Oral – oral Gastric – oral 1/8/2014 8
  • 9. Risks of transmission ▪ Childrens who consume untreated stream water, uncooked vegetables ▪ Exposure to diarrheal stools, vomitus of the infected persons ▪ Dentists and oral hygienists who have exposures to dental plaques and saliva ▪ Iatrogenic infection in the form of contaminated endoscopes and other gastric devices 1/8/2014 9
  • 10. Microbiology ▪ Morphology: • H. pylori is a spiral shaped, • microaerophilic, gram negative bacterium • measuring approximately 3.5 microns in length and 0.5 microns in width • It has multiple unipolar flagella and it is actively motile • biochemically characterized as catalyse, oxidise, and urease positive. 1/8/2014 10
  • 11. Growth and culture characters ▪ Growth and culture characters • It’s a slow growing organism • can be cultured on blood agar • selective media is Skirrow's media (with vancomycin, polymyxin B, and trimethoprim, chocolate medium) incubated at 37ºC in a 5 percent oxygen atmosphere for three to seven days • The colonies are translucent and 1–2 mm in diameter. 1/8/2014 11
  • 13. Conditions associated with H.pylori ▪ Esophagus 1. 2. 3. GERD Barrett’s esophagus adenocarcinoma ▪ Stomach 1. 2. 3. 4. 5. ▪ Acute gastritis ( sometimes self limiting) Chronic active gastritis Peptic ulcer disease Gastric adenocarcinoma MALT Duodenum 1. Peptic ulcer 1/8/2014 13
  • 14. Non gastrointestinal diseases associated to H.pylori ▪ Coronary artery disease ▪ Immune thrombocytopenic purpura ▪ Iron deficiency anemia ▪ Reynaud's phenomenon ▪ Scleroderma ▪ Idiopathic urticaria ▪ Acne rosacea ▪ Thyroiditis ▪ GBS 1/8/2014 14
  • 15. Diagnosis – when to test ACG recommendations ▪ Testing for H. pylori should be performed only if the clinician plans to offer treatment for positive results ▪ Testing is indicated in patients with gastric MALT lymphoma, active peptic ulcer disease, or a past history of documented peptic ulcer 1/8/2014 15
  • 16. Diagnosis – when to test ▪ patients with uninvestigated dyspepsia who are under the age of 55 years and have no alarm features alarm features ▪ Deciding which test to use in which situation relies heavily upon whether a patient requires evaluation with upper endoscopy and the strengths, weaknesses, and costs of the individual tests ▪ unexplained weight loss, ▪ bleeding, ▪ anaemia, ▪ early satiety, ▪ Progressive ▪ dysphagia, odynophagia, ▪ recurrent vomiting, ▪ family history of GI cancer, previous esophagogastric malignancy 1/8/2014 16
  • 17. Supported by the evidence Controversial Indications for testing and treatment of H.pylori infection Active peptic ulcer disease (gastric or Functional dyspepsia duodenal ulcer) ▪ Confirmed history of peptic ulcer ▪ ▪ Gastric MALT-lymphoma (low grade) ▪ Unexplained iron deficiency anaemia GERD Persons using NSAIDs or before starting NSAIDs or ITP Following endoscopic resection of early gastric cancer ▪ Populations at higher risk of gastric cancer ▪ Uninvestigated dyspepsia (if H. pylori population prevalence high) 1/8/2014 17
  • 18. Types of diagnostic test Non endoscopic tests Endoscopic tests 1. Serology (quantitative or qualitative IgG) 1. Histology 2. Urea breath test (13C or 14C) 3. Culture 3. Stool antigen test 2. Rapid urease test 4. Polymerase chain reaction assay 1/8/2014 18
  • 19. Serology ▪ ELISA technology to detect IgG antibodies is inexpensive, non-invasive. ▪ high sensitivity (90 to 100%), variable specificity (76 to 96%) & accuracy( 83 to 98%). ▪ It needs confirmation with another method such as a stool antigen or urea breath test before starting treatment ▪ The “serological scar’ may be present even after successful eradication of organism 1/8/2014 19
  • 20. Urea breath test (UBT) ▪ detects active H. pylori infection, confirming the accuracy of serology and documenting successful treatment. ▪ The specificity is more than 95%, sensitivity of the test is 88% to 95% ▪ false-negative results reported in patients taking antisecretory therapy such as PPIs,bismuth, or antibiotics. ▪ antibiotics should be stopped at least four weeks and PPIs at least one week before breath testing. ▪ UBT is not accurate in patients who have had gastric respective surgery. 1/8/2014 20
  • 21. Urea breath test (UBT) 1/8/2014 21
  • 22. Stool antigen assay ▪ It is an immunoassay to detect the presence of h.pylori antigen in stools ▪ The sensitivity and specificity are 94% and 97%, respectively ▪ sensitivity of stool testing is negatively affected by PPIs, bismuth, and antibiotics which affects the bacterial load ▪ Its used both for diagnosis and confirm the eradication . 1/8/2014 22
  • 23. Endoscopic tests – biopsy urease testing Tissue from the antral biopsy is placed in agar well containing urea and pH reagent The urease cleaves the urea to liberate ammonia This process changes the medium alkaline and produces a color change 1/8/2014 23
  • 24. Biopsy urease testing ▪ commercially available kits include CLOtest, PyloriTek, and Hp-fast ▪ The CLOtest may become positive as early as one hour after collection, but a final reading at 24 hours is recommended ▪ The sensitivity is 90 to 95% & specificity is 95 to 100% ▪ false positive tests are unusual. False negative results occur in recent gastrointestinal bleeding or with the use of PPIs, H2 antagonists, antibiotics, or bismuth-containing compounds 1/8/2014 24
  • 25. Rapid urease testing ▪ To know patient's H. pylori status before discharge from the endoscopy suite. ▪ biopsy specimens are sandwiched between a reagent strip with a pH indicator and a pad containing urea. ▪ One hour sensitivity is 89 to 98 percent and specificity is 89 to 93 percent. 1/8/2014 25
  • 27. Histology ▪ In addition to make diagnosis of H.pylori the biopsy and histology also reveals intestinal metaplasia, MALT omas, dysplasia and neoplasia ▪ In addition to biopsying “clinically suspicious” areas, taking multiple biopsies and sampling lesser and greater curvatures of gastric antrum and body are important. ▪ It is gold standard for identifying infection, with reported sensitivity and specificity as high as 95% and 98% ▪ Limitations… ▪ Brush cytology…. 1/8/2014 27
  • 29. A silver stain (Warthin Starry) of H.pylori on gastric mucus-secreting epithelial cells (x1000). This picture is notorious because it is of Dr. Marshall's stomach biopsy taken 8 days after he drank a culture of H. pylori. 1/8/2014 29
  • 30. Culture ▪ Its fastidious and difficult to culture and require special culture media ▪ Culture is indicated when treating cases not responding to treatment and suspected antibiotic resistance ▪ Even though the in vitro sensitivity will not guarantee the treatment results 1/8/2014 30
  • 31. This is a 3 day culture of H.pylori on blood agar 1/8/2014 31
  • 32. Treatment ▪ Triple therapy ▪ Quadruple therapy ▪ Sequential therapy 1/8/2014 32
  • 33. Triple therapy ▪ It’s the most commonly recommended therapy ▪ The duration of therapy must be 14 days and all drugs in BD dose ▪ The cure rate is >80% ▪ Metronidazole 500mg can be substituted for amoxy in penicillin allergic patients 1/8/2014 33
  • 34. Quadruple therapy ▪ Dose : 4 times a day ▪ Duration : 14 days ▪ appropriate as initial therapy in areas in which the prevalence of resistance to clarithromycin or metronidazole is >20% ▪ in patients with recent or repeated exposure to clarithromycin or metronidazole Eradication rate 70 – 85% 1/8/2014 34
  • 35. Sequential regimen Regimen Days (PPI + Amoxy 1000 mg) BD 5 + 5 followed by (PPI+ Clarithromycin 500 mg + Tinidazole 500 mg) BD Eradication rate 90% • It has overall eradication rate better than triple therapy 90% vs 80% •Particularly superior if bacteria is clarithromycin resistant ( 89% Vs 29%) 1/8/2014 35
  • 36. Eradication confirmation ▪ Eradication may be confirmed by a urea breath test, fecal antigen test, or upper endoscopy performed four weeks or more after completion of therapy. ▪ Its indicated in following situations 1. 2. 3. 4. Patients who have persistent symptoms after H. pylori treatment for dyspepsia Patients who had an H. pylori associated ulcer Patients who had gastric mucosa associated lymphoid tissue (MALT) lymphoma Patients who had resection for early gastric cancer. 1/8/2014 36
  • 37. Treatment failures and persisitance of H.pylori ▪ The initial treatment results in 25% failures ▪ The reasons for failure are 1. 2. 3. 4. 5. 6. Resistant organism Poor compliance with medication Alcohol consumption Smoking Prior antibiotic use Underlying condition (FD Vs PUD) 1/8/2014 37
  • 38. Antibiotic resistance ▪ Resistance to metronidazole is 40% in US and 11% for clarithromycin ▪ Resistace to amox and tetracycline is less than 1% ▪ The resistance to metronidazole is overcome by increasing doses or combining with bismuth ▪ Macrolide resistance cant overcome by increasing dose because these are due to alterations in 23S ribosomal RNA(A2143G, A2142G & A2142C) which interferes with ribosomal macrolide binding 1/8/2014 38
  • 40. Side effects of treatment ▪ Side effects are reported in up to 50 percent of patients taking one of the triple therapy regimens . ▪ The adverse effects are usually mild; fewer than 10 percent of patients stop treatment due to side effects 1. The most common side effect is a metallic taste due to metronidazole or clarithromycin. 2. Metronidazole can cause a peripheral neuropathy, seizures, and a disulfiram-like reaction when taken with alcohol. 3. Clarithromycin can cause taste alteration, nausea, vomiting, abdominal pain, and rarely QT prolongation. 4. Tetracycline can induce a photosensitivity reaction in some cases. It should also not be administered to pregnant women or young children. 5. Amoxicillin can cause diarrhea or an allergic reaction with skin rash. 1/8/2014 40
  • 41. Take home message 1. H. pylori is a common worldwide infection. 2. Established indications for H. pylori cure include peptic ulcer,(MALT) and uninvestigated dyspepsia. 3. Non-endoscopic and endoscopic tests are available toidentify H. pylori. 4. Proton pump inhibitor (PPI), clarithromycin, and amoxicillin or metronidazole or a PPI, bismuth, tetracycline,and metronidazole for 10–14 days are accepted first line treatment 1/8/2014 41
  • 42. Thank you…. John Robin Warren Barry James Marshall 42 1/8/2014