Society of Nuclear Medicine Procedure Guideline for C-14 Urea Breath Test version 3.0, approved June 23, 2001 Authors: Helena R. Balon, MD (William Beaumont Hospital, Royal Oak, MI); Eileen Roff, RN, MSA, (William BeaumontHospital, Royal Oak, MI); John E. Freitas, MD (St. Joseph Mercy Hospital, Ann Arbor, MI); Vanessa Gates, MS (WilliamBeaumont Hospital, Royal Oak, MI); and Howard J. Dworkin, MD (William Beaumont Hospital, Royal Oak, MI).
istration of C-14 urea, followed by sampling of the ex-haled breath at timed intervals. The breath samples
The purpose of this guideline is to assist nuclear
are then analyzed in a liquid scintillation counter.
medicine practitioners in recommending, perform-ing, interpreting and reporting the results of the C-14 urea breath test.
III. Common Indications
Detection of the presence of H. pylori in the stomach. II. Background Information and Definitions
A. Given the very high probability of patients w i t h
duodenal ulcers being infected with H. pylori, t h e
The discovery of the Gram-negative spiral rod, Heli-
C-14 urea breath test has not been routinely
cobacter pylori, in the 1980s radically changed the ap-
recommended for initial diagnosis, but has
proach to treatment of peptic ulcer disease (PUD).
been recommended to document H. pylori e r a d-
The causal relationship between H. pylori infection
ication following anti-H. pylori therapy. Eradi-
and chronic gastritis is well established. Althoughonly a small fraction of H. pylori-positive patients de-
cation should be confirmed no sooner than 1
velop PUD, essentially all patients with duodenal ul-
month, and preferably longer, after completion
cers and about 80% of patients with other than non-
steroidal anti-inflammatory drug (NSAID)-induced
B. Since the prevalence of H. pylori in gastric ulcer
gastric ulcers are infected with H. pylori. Eradication
patients (non-NSAID-induced gastric ulcers) is
of H. pylori markedly reduces ulcer recurrence to
about 80%, the C-14 urea breath test may be used
<10% in 1 yr vs. 60-100% recurrence rate in 1 yr with
for initial diagnosis as well as follow-up in this
There is also evidence that H. pylori infection is as-
s o c i a t e d with adenocarcinoma and lymphoma of the
IV. Procedure
stomach, although in the United States fewer than 1%of H. pylori-infected people will develop gastric cancer.
Further research is needed to determine the role of
1. Patients should be off the following medica-
H. pylori eradication in gastric cancer prevention.
The presence of active H. pylori infection can be di-
a. Antibiotics and bismuth compounds for 30
agnosed non-invasively with the C-14 urea breath
test. This test is based on the detection of the enzyme
urease produced by H. pylori. Since urease is not pre-
(e.g., omeprazole, esomeprazole, lansopra-
sent in normal human tissues, and since other ure-
zole, rabeprazole, pantoprazole) for 2 wk
ase-producing bacteria do not colonize the stomach,
the presence of urease in the stomach can be equated
2. Patients should be NPO for at least 6 hr before
In the presence of urease, orally administered C-
B. Information Pertinent to Performing the Procedure
14 urea will be hydrolyzed into ammonia and
A relevant history should be obtained; particu-
1 4C O2. 1 4C O2 is absorbed into the circulation and ex-
larly, a list of relevant medications and the time
haled by the lungs. The presence of a significant
of their most recent administration should be
amount of 1 4C O2 in the exhaled breath indicates ac-
tive H. pylori i n f e c t i o n .
The C-14 urea breath test consists of the oral admin-
Radiation Dosimetry for C-14 Urea* Administered Activity Organ Receiving the Effective Dose L a r g e s t Radiation Dose Equivalent+ ( r a d / m C i ) (rem/mCi)
*from Stubbs JB, Marshall BJ. Radiation dose estimates for the C-14 labeled urea breath test.
tion fluid (e.g., BCST M, Econo-SafeT M) is
C-14 urea in a capsule form containing 1 mg urea
labeled with 37 kBq (1 mCi) C-14. This prepara-
breath collection and mixed thoroughly.
tion is currently available as PYTestT M f r o m
Kimberly-Clark/Ballard Medical Products.
C-14 is a pure beta-emitter with a physical half
life of 5730 yr and maximum energy of 160 keV.
known activity is stated on the vial) to a
To measure beta emissions, C-14 is counted in a
blank breath sample (a breath sample con-
taining no C-14). The same volume of scin-
tillation fluid that is used for patient sam-
At time zero, the patient swallows the capsule
containing 37 kBq (1 mCi) C-14 urea with 20
ml lukewarm water. At 3 min post-dose, the
breath sample from a person not receiving
patient drinks another 20 ml lukewarm water.
At 10 min post-dose, the patient is asked to
d. All timed breath samples, the blank sample
take a deep breath, hold it for approximately
and the C-14 standard are counted for 5–20
5–10 sec and then exhale through a straw into
min in a liquid scintillation counter (LSC),
sample (into another balloon) can be obtained
a. For each balloon, 2.5 ml trapping solution is
pipetted into a scintillation vial. The trap-
ping solution (collection fluid) is availablefrom the manufacturer and contains 1
thalein. The air from the balloons is trans-
ferred into the scintillation vials using an
change of the collection fluid (from blue to
colorless) indicates the end point of trans-
counter for the specific procedure and the
specific scintillation cocktail can then be
trapped. Ten milliliters of suitable scintilla-
SOCIETY OF NUCLEAR MEDICINE PROCEDURE GUIDELINES MANUAL JUNE 2002
Efficiency = (standard cpm – blank cpm)
2. Causes of potential false-positive results:
a. Resective gastric surgery with potential re-
sultant bacterial overgrowth (non- H. pylori
shipped to another institution/laboratory, if
a liquid scintillation counter is not available
If a value of 50–300 dpm is obtained immedi-
ately after the addition of the scintillation
fluid, the sample should be recounted in 1–2
hr or the next day, to exclude falsely elevated
Reference values recommended by the manufac-
V. Issues Requiring Further Clarification VI. Concise Bibliography
≥ 200 dpm at 10 min Positive for H. pylori
Friedman LS. Helicobacter pylori and nonulcer dyspep-
sia (editorial). New Engl J Med. 1998;339: 1928–1930.
Aside from patient demographics, the report
NIH Consensus Statement. Helicobacter pylori in peptic
should include the following information:
ulcer disease. JAMA. 1994;272:65–69.
1. Indication for the study (e.g., suspected H. py-
P Y T e s tTM package insert. Ballard Medical Products,
l o r i infection, follow-up after anti-H. pylori
Soll AH. Consensus Statement. Medical treatment of
2. Procedure (i.e., radiopharmaceutical and
peptic ulcer disease - practice guidelines. J A M A.
dosage, number and timing of breath samples
Stubbs JB, Marshall BJ. Radiation dose estimates for the
3. Result (i.e., net dpm in the 10 min sample)
C-14 labeled urea breath test. J Nucl Med.
5. Study limitations, confounding factors6. Interpretation (i.e., positive, negative, indeter-
Disclaimer
minate for the presence of active H. pylori in-fection)
The Society of Nuclear Medicine has written and
approved guidelines to promote the cost-effective
use of high quality nuclear medicine procedures.
Proper calibration and QC of the LSC should
These generic recommendations cannot be applied
be performed as per facility procedure.
to all patients in all practice settings. The guidelines
should not be deemed inclusive of all proper proce-
1. Causes of potential false-negative results:
dures or exclusive of other procedures reasonably
a. Antibiotics (if administered within 30 days
directed to obtaining the same results. The spec-
trum of patients seen in a specialized practice set-
b. Bismuth (if administered within 30 days of
ting may be quite different than the spectrum of pa-
tients seen in a more general practice setting. The
c. Sucralfate (if administered within 14 days
appropriateness of a procedure will depend in
part on the prevalence of disease in the patient
d. Proton pump inhibitors (see examples in
population. In addition, the resources available to
section IV.A.b.) if administered within 14
care for patients may vary greatly from one med-
ical facility to another. For these reasons, guide-
Advances in medicine occur at a rapid rate. The
g. Difficulty with swallowing test capsule
date of a guideline should always be considered in
(additional breath samples collected at 15
determining its current applicability.
Chemical Descriptions for Marcellus Shale Wells The purpose of this document is to allow a better understanding of the chemistry that is commonly used in stimulating a Marcellus shale well. An explanation of the entire completion process is needed to understand the closed system in which the chemicals are injected into the fluid system and enter an isolated and specific formation. Additional doc
Social Movements: Challenging the State Paper for Harold Wolpe Memorial Seminar, 4 May 2005 Mark Heywood I’d like to thank the organisers for the chance to make this presentation this evening – I thought for a minute I might have Trevor’s time as well because he was late coming in but he’s here now. I want to start just by saying that I think the Treatment Action Campaign (
Radiation Dosimetry for C-14 Urea*
SOCIETY OF NUCLEAR MEDICINE PROCEDURE GUIDELINES MANUAL JUNE 2002
Efficiency = (standard cpm – blank cpm)
2. Causes of potential false-positive results:
a. Resective gastric surgery with potential re-
sultant bacterial overgrowth (non- H. pylori
shipped to another institution/laboratory, if
a liquid scintillation counter is not available
If a value of 50–300 dpm is obtained immedi-
ately after the addition of the scintillation
fluid, the sample should be recounted in 1–2
hr or the next day, to exclude falsely elevated
Reference values recommended by the manufac-
V. Issues Requiring Further Clarification