Background &amp; Aims: Antibiotic resistance is the main reason for failure of Helicobacter pylori (H. pylori) treatment. Currently, guidelines recommend a treatment guided by antimicrobial susceptibility testing after two failures. However, microbial culture is not feasible everywhere, and the limited number of effective antibiotics against the bacterium narrows the options; thus a rescue therapy combining antibiotics with a low resistance may be fitting.

Methods: Patients who have failed a first-line treatment (either prolonged triple or sequential regimens) and, successively, a levofoxacin-based triple therapy were considered for the study. Subjects underwent urea breath test (UBT), stool antigen test (ST) and endoscopy/histology to confirm the diagnosis. Cytopenia and impaired liver and kidney function were exclusion criteria. Fify-four subjects were randomized 1:1 to two regimens: RMB abeprazole/Rifabutin/Minocycline/Bismuth sub-citrate or MTB Rabeprazole/Tinidazole/ Minocycline/Bismuth sub-citrate both for 10 days. Te results were checked 6 weeks afer the end of therapy with ST/UBT plus endoscopy when indicated.

Results: RMB eradicated the bacterium in 21 patients. Two subjects dropped out. Te eradication rate was 77.7% (CI 62.0-93.4%) at intention-to-treat and 84.0% (CI 69.6-98.4%) at per-protocol analysis. MTB was successful in 14 patients (51.9%, CI 33.1-70.7%). No patient withdrew from the treatment for adverse events. Drug-related side effects were reported only in 3 subjects, but in all cases the treatment was carried on. Conclusions: Te association minocycline/rifabutin seems to have a synergic effect and a good therapeutic outcome in patients who have failed at least two previous regimens, although a trial on a large population is needed

AMORUSO, Annacinzia

De Francesco V

DI LEO, Alfredo

Giangaspero A

Giorgio F

Ierardi E

Losurdo G

PRINCIPI, MARIABEATRICE

English

Archivio istituzionale della ricerca - Università di Bari

J Gastrointestin Liver Dis,December 2014 Vol. 23 No 4: 367-3701) Section of Gastroenterology, Department of Emergency and Organ Transplantation, University of Bari, Bari2) Ospedali Riuniti, Gastroenterology Unit, Foggia, ItalyAddress for correspondence: Prof. Enzo IerardiSection of Gastroenterology, Department of Emergency and Organ Transplantation, University of Bari, 70124 Bari, Italyierardi.enzo@gmail.com  Received: 02.10.2014 Accepted: 27.11.2014Quadruple Rescue erapy aer First and Second Line Failure for Helicobacter pylori Treatment: Comparison between Two Tetracycline-Based Regimens Enzo Ierardi1, Antonio Giangaspero1, Giuseppe Losurdo1, Floriana Giorgio1, Annacinzia Amoruso1, Vincenzo De Francesco1,2, Alfredo Di Leo1, Mariabeatrice Principi1INTRODUCTIONThe increasing antibiotic resistance is the main reason for Helicobacter pylori  (H. pylori) treatment failure [1]. After an unsuccessful first-line regimen (usually triple or sequential/concomitant/hybrid therapies), guidelines recommend a triple therapy with levooxacin or a bismuth/tetracycline/metronidazole quadruple regimen [2]. When a second-line treatment fails, the possible options are very ORIGINAL PAPERABSTRACTBackground & Aims: Antibiotic resistance is the main reason for failure of Helicobacter pylori (H. pylori) treatment. Currently, guidelines recommend a treatment guided by antimicrobial susceptibility testing aer two failures. However, microbial culture is not feasible everywhere, and the limited number of eective antibiotics against the bacterium narrows the options; thus a rescue therapy combining antibiotics with a low resistance may be tting.Methods: Patients who have failed a rst-line treatment (either prolonged triple or sequential regimens) and, successively, a levooxacin-based triple therapy were considered for the study. Subjects underwent urea breath test (UBT), stool antigen test (ST) and endoscopy/histology to conrm the diagnosis. Cytopenia and impaired liver and kidney function were exclusion criteria. Fiy-four subjects were randomized 1:1 to two regimens: RMB Rabeprazole/Rifabutin/Minocycline/Bismuth sub-citrate or MTB Rabeprazole/Tinidazole/Minocycline/Bismuth sub-citrate both for 10 days. e results were checked 6 weeks aer the end of therapy with ST/UBT plus endoscopy when indicated.Results: RMB eradicated the bacterium in 21 patients. Two subjects dropped out. e eradication rate was 77.7% (CI 62.0-93.4%) at intention-to-treat and 84.0% (CI 69.6-98.4%) at per-protocol analysis. MTB was successful in 14 patients (51.9%, CI 33.1-70.7%). No patient withdrew from the treatment for adverse events. Drug-related side eects were reported only in 3 subjects, but in all cases the treatment was carried on.Conclusions: e association minocycline/rifabutin seems to have a synergic eect and a good therapeutic outcome in patients who have failed at least two previous regimens, although a trial on a large population is needed.Key words: Helicobacter pylori – antibiotic resistance – rescue therapy – rifabutin – minocycline. Available from: URL: http://www.jgld.ro/2014/3/6DOI:  http://dx.doi.org/10.15403/jgld.2014.1121.234.qrthlimited [3]. In this case, Maastricht-IV Consensus advises a treatment guided by antimicrobial susceptibility testing, i.e. culture [2]. However, despite the fact that this technique may permit the achievement of good eradication rates [4], culture is not feasible everywhere and dicult to perform even in expert hands. Moreover, the limited number of effective antibiotics against the bacterium narrows the eld of options. On the other hand, Italian guidelines [5] suggest a rifabutin based triple therapy as a third line. e possibility of using an empiric third-line regimen when culture is not available or most antibiotics have failed is essential, and rifabutin has been investigated in many studies, with a success rate ranging from 44 to 95% [6]. In a recent meta-analysis, the mean percentage of success of a rifabutin-based triple therapy (rifabutin, amoxicillin and a proton pump inhibitor - PPI) was 66% when used in third line [6].368 Ierardi et alJ Gastrointestin Liver Dis, December 2014 Vol. 23 No 4: 367-370 Tetracycline is a class of antibiotics that is largely used in second and third line therapy [7], usually in association with bismuth and metronidazole, the so called “quadruple therapy”. However, in Italy the commercial package of tetracycline contains tablets with a dose of 250 mg. erefore, for an eective treatment, the patient is requested to assume 8 pills/day of tetracycline in addition to the other drugs with a total number of 16 tablets/day for at least 10 days. It may be argued that relevant consequences on the compliance are very common. Minocycline belongs to the tetracycline class. It is used at a dose of 100 mg (one tablet) twice daily, and this could push the patient to a complete adherence to the therapeutic regimen.erefore, herein we describe a preliminary experience with a novel quadruple regimen containing rifabutin, minocycline and bismuth (RMB) as a rescue therapy in patients who had failed at least two previous regimens, compared to a classical quadruple therapy which comprised minocycline, tinidazole and bismuth (MTB).PATIENTS AND METHODSPatients who failed a rst-line regimen (either prolonged triple or sequential therapy) and successively a levooxacin-based triple therapy were considered for the study. Before starting the treatment, all eligible patients underwent a full blood count and evaluation of renal (creatinine, blood urea nitrogen) and hepatic function (transaminases, bilirubin, alkaline phosphatase and gamma-glutamyl transpeptidase). All subjects with cytopenia (dened as white blood cells < 4,000/μL, hemoglobin < 10g/dL and platelets < 150,000/μL), impaired renal function and liver cytolysis/cholestasis were excluded. All subjects had H. pylori infection diagnosed by the concordance of the urea breath test (UBT) and stool test antigen (ST). e diagnosis was conrmed by upper endoscopy with histology before starting the therapy. e patients were randomized 1:1 to the rifabutin-based quadruple therapy (RMB) or to the modied conventional quadruple therapy (MTB). Both treatments lasted 10 days.The RMB eradication regimen was given as follows: Rabeprazole 20mg b.i.d, Rifabutin 150 mg b.i.d, Minocycline 100 mg b.i.d and Bismuth sub-citrate 120 mg four times/day. e MTB regimen consisted of Rabeprazole 20 mg b.i.d, Tinidazole 500 mg b.i.d, Minocycline 100 mg b.i.d and Bismuth sub-citrate 120mg four times/day. e patients had PPI 30 minutes before meals and antibiotics 30 minutes aer meals. Bismuth administration was independent by meals. Informed consent was obtained from each patient.e result of the eradication treatment was checked by UBT and ST 6 weeks aer its cessation, and therapy was considered successful only when both tests conrmed H. pylori negativity. When necessary (ulcer or low grade MALT lymphoma) a second endoscopy/histology was performed. At the 5th day and the end of therapy, the side eects were investigated by a personal interview.e χ2 test or the Fisher’s exact probability test were used, as appropriate, to compare the percentages and nominal variables. For continuous variables, dierences between the patients in the two treatment arms were compared using the Student t-test for unpaired samples. e eradication rates were expressed both as intention-to-treat (ITT) and per-protocol (PP) analysis, and 95% condence interval (95% CI) was provided. e statistical analysis was performed using the statistical soware GraphPad Prism version 5.00 for Windows, GraphPad Soware, San Diego California USA.RESULTSFiy-four patients (32 females, 22 males) fullled inclusion criteria and received the rescue regimen in the period July 2013-July 2014. The mean age was 53.3 years (range 23-80, standard deviation 13.3, median 54). All patients were referred to endoscopy for long-lasting dyspeptic and/or ulcer-like symptoms. Endoscopy revealed peptic ulcer in 9 cases. Histology and immunohistochemistry revealed in three patients a low grade MALT lymphoma. Diuse antral incomplete intestinal metaplasia was observed in 6 patients.In the rst line, 22 patients (40.7%) had failed sequential regimen, while 32 (59.3%) a 10-day triple therapy. All patients had successively failed a second line levooxacin-amoxicillin 10-day triple therapy.In the RMB group, 21 patients eradicated the bacterium. Two subjects dropped out, so no data regarding their therapy results are available. e eradication rate was 77.7% (CI 62.0-93.4%) at ITT and 84.0% (CI 69.6-98.4%) at PP analysis.In the MTB group, 14 patients eradicated H. pylori. We did not record any drop out. e eradication rate was 51.9% (CI 33.1-70.7%) at both PP and ITT analysis.H. pylori related disorders and therapeutic outcome of enrolled patients are described in Table I.No patient withdrew from the treatment for adverse events. Main drug-related side eects were reported only in 3 subjects (5.6%): diarrhea in two cases (one in RMB and one in MTB) and severe asthenia in the other one (RMB). However, in both cases the treatment was not halted and in the rst case a probiotic supplementation was given.DISCUSSIONH. pylori is a well-known cause of gastritis, peptic ulcer and malignant diseases of the stomach [8, 9]. Since its eradication is able to avoid the evolution of gastric lesions into severe gastric malignancies, such as adenocarcinoma or lymphoma, eective eradication regimens are required. However, antibiotic resistances are a frequent cause of therapy failure; therefore, rescue therapies are of strong relevance. Rifabutin is an anti-tuberculosis agent used in patients aected by acquired immune-deciency syndrome. Its use in H. pylori eradication regimens is indicated today only for the rescue therapy given the low rates of antibiotic resistance [10], the high economic costs and the potential severe side eects, such as neutropenia or anemia [11]. A recent meta-analysis showed a mean percentage of success of a third-line rifabutin-based triple therapy (rifabutin, amoxicillin and a PPI) of 66% [6].e second antibiotic used in our regimens, minocycline, belongs to the tetracycline drug class, which has been associated with low rates of antibiotic resistance in Italy [12]. A single trial with minocycline and amoxicillin is available and H. pylori rescue quadruple therapy 369J Gastrointestin Liver Dis, December 2014 Vol. 23 No 4: 367-370shows a disappointing eectiveness (38.5%) [13]. However, the case of a multi-resistant H. pylori strain successfully treated with minocycline/amoxicillin/bismuth has been described [14]. Tetracycline has been employed in third line regimens, enclosed in classical bismuth-containing quadruple therapy, with results varying from 65% in a recent Spanish trial [15] to 36% in another study conducted in the year 2000 in the same country [16].e data of the present preliminary report demonstrated that the association minocycline/rifabutin has a satisfactory eradication rate (PP: 84%; ITT: 77.7%) when compared to previous studies using tetracycline or rifabutin alone. is eect could be explained by two main reasons: i) two dierent antibiotics with low resistance rates were combined, and ii) these antibiotics had not been used in precedent eradication regimens in our patients. On the other hand, a conventional bismuth based quadruple therapy, although with minocycline instead of tetracycline, did not reach a satisfactory eradication rate (51.9%). e use of tinidazole, which was already employed in first line by some patients, could explain this result. Nevertheless, the dierent outcomes of the two regimens could not have been aected by the previous tinidazole assumption, as clearly shown in Table I.Based on this hypothesis, the association rifabutin-minocycline could have a synergic action and fulfills its maximal potential therapeutic eect when compared with other third line schemes. e possibility of the combination of these two drugs is secondary to the approval of local pharmaceutical agencies. Both drugs were approved by the Food and Drug Administration (FDA) [17] and by the European Medicines Agency (EMA), so they are available both in Europe and the United States [18]. Studies related to their use in Asian and African countries are also available [19-22].Of relevance, H. pylori eradication was obtained in two patients with low grade MALT lymphoma.In our study, no patient developed severe drug reactions. Possible explanations may be : i) the short duration of the treatment (rifabutin side eects are common in a 14-day lasting regimen [23] or when the dose is 600mg/day for mycobacterial infection [24]), and ii) the exclusion criteria that did not allow the enrolling of patients at high risk of severe reactions to both antibiotics.Despite the encouraging results, this is a preliminary study and the present data come from a small-size group of subjects. is last aspect is due to the rarity of multiple failures, since the patients were recruited during a period of one year. In conclusion, further investigations are required to conrm our results and to denitively ascertain the eectiveness and safety of the combination rifabutin-minocycline in H. pylori multi-resistant infection.Conicts of interests: none declared.Authors’ contribution: E.I. and A.D.L. designed the study. G.L., A.A., A.G. and V.D.F. collected the data. M.P. performed the endoscopies. F.G. and G.L. extracted and performed statistical analysis. E.I. and G.L. wrote the manuscript. All authors revised the nal version before approval.REFERENCES 1. Ierardi E, Giorgio F, Losurdo G, Di Leo A, Principi M. How antibiotic resistances could change Helicobacter pylori treatment: A matter of geography? World J Gastroenterol 2013;19:8168-8180. 2. Malfertheiner P, Megraud F, O‘Morain CA, et al. Management of Helicobacter pylori infection--the Maastricht IV/ Florence Consensus Report. Gut 2012;61:646-664. 3. Song M, Ang TL. Second and third line treatment options for Helicobacter pylori eradication. World J Gastroenterol 2014;20:1517-1528. 4. Fiorini G, Vakil N, Zullo A, et al. Culture-based selection therapy for patients who did not respond to previous treatment for Helicobacter pylori infection. Clin Gastroenterol Hepatol 2013;11:507-510. Table I. Demographic, clinical, endoscopic and histological characteristics of enrolled patients and the related therapeutic outcome.RMB MTB p* p**Features Number (%) Eradicated patients n(%)Number (%) Eradicated patients n (%)Total 27 21 (77.7) 27 14 (51.9%) - 0.02Age (mean ± SD) 53.8 ± 12.6 51.6 ± 12.1 52.6 ± 14.5 50.4 ± 13.3 0.45 0.43Sex (female) 15 (55.5) 12 (80.0) 14 (51.9) 10 (71.4) 1 0.68Dyspepsia                 17 (62.9) 13 (76.5) 19 (70.4) 10 (52.6) 0.77 0.18Peptic ulcer 5 (18.5) 5 (100) 4 (14.8) 2 (50) 1 0.17Duodenal 4(14.8) 4 (100) 4 (14.8) 2 (50)Gastric  1 (3.7) 1 (100) 0 (0) -Antral diuse intestinal metaplasia 3 (11.1) 1 (33.3) 3 (11.1) 1 (33.3) 1 1Low grade MALT lymphoma 2 (7.4) 2 (100) 1 (3.7) 1 (100) 1 1Side eects 2 (7.4) - 1 (3.7) - 1 -* t-test or Fisher exact text/χ2 test where needed. e comparision was performed between the total number of patients enrolled in each group. ** t-test or Fisher exact text/χ2 test where needed. e comparision was performed between the number of patients who eradicated H. pylori between the two groups. RMB = rifabutin, minocycline, bismuth; MTB = minocycline, tinidazole, bismuth.  370 Ierardi et alJ Gastrointestin Liver Dis, December 2014 Vol. 23 No 4: 367-370  5. Caselli M, Zullo A, Maconi G, et al. „Cervia II Working Group Report 2006”: guidelines on diagnosis and treatment of Helicobacter pylori infection in Italy. Dig Liver Dis 2007;39:782-789. 6. Gisbert JP, Calvet X. Review article: rifabutin in the treatment of refractory Helicobacter pylori infection. Aliment Pharmacol er 2012;35:209-221. 7. Cianci R, Montalto M, Pandol F, Gasbarrini GB, Cammarota G. ird-line rescue therapy for Helicobacter pylori infection. World J Gastroenterol 2006;12:2313-2319. 8. Ierardi E, Goni E, Losurdo G, Di Mario F. Helicobacter pylori and nonmalignant diseases. Helicobacter 2014;19 Suppl 1:27-31. 9. Venerito M, Nardone G, Selgrad M, Rokkas T, Malfertheiner P. Gastric cancer--epidemiologic and clinical aspects. Helicobacter 2014;19 Suppl 1:32-37. 10. O‘Connor A, Taneike I, Nami A, et al. Helicobacter pylori resistance rates for levooxacin, tetracycline and rifabutin among Irish isolates at a reference centre. Ir J Med Sci 2013;182:693-695.  11. Brogden RN, Fitton A. Rifabutin. A review of its antimicrobial activity, pharmacokinetic properties and therapeutic ecacy. Drugs 1994;47:983-1009. 12. De Francesco V, Giorgio F, Hassan C, et al. Worldwide H. pylori antibiotic resistance: a systematic review. J Gastrointestin Liver Dis 2010;19:409-414. 13. Murakami K, Sato R, Okimoto T, et al. Eectiveness of minocycline-based triple therapy for eradication of Helicobacter pylori infection. J Gastroenterol Hepatol 2006;21:262-267. 14. Nakajima S, Inoue H, Inoue T, Maruoka Y. Multiple-antibiotic-resistant Helicobacter pylori infection eradicated with a tailor-made quadruple therapy. J Gastroenterol Hepatol 2012;27 Suppl 3:108-111.  15. Gisbert JP, Perez-Aisa A, Rodrigo L, et al ird-line rescue therapy with bismuth-containing quadruple regimen aer failure of two treatments (with clarithromycin and levooxacin) for H. pylori infection. Dig Dis Sci 2014;59:383-389. 16. Gomollón F, Sicilia B, Ducóns JA, Sierra E, Revillo MJ, Ferrero M. ird line treatment for Helicobacter pylori: a prospective, culture-guided study in peptic ulcer patients. Aliment Pharmacol er 2000;14:1335-1338. 17. U S Food and Drug Administration. www.fda.gov/ 18. European Medicines Agency. www.ema.europa.eu/ 19. Seo JH, Jun JS, Yeom JS, et al. Changing pattern of antibiotic resistance of Helicobacter pylori in children during 20 years in Jinju, South Korea. Pediatr Int 2013;55:332-336.  20. Tan Y, Hu Z, Zhao Y, et al. e beginning of the rpoB gene in addition to the rifampin resistance determination region might be needed for identifying rifampin/rifabutin cross-resistance in multidrug-resistant Mycobacterium tuberculosis isolates from Southern China. J Clin Microbiol 2012;50:81-85. 21. Miyazaki M, Nagata N, Matsuo K, Takata T, Tanihara S, Kamimura H. Trends and antimicrobial susceptibilities of clinical methicillin-resistant Staphylococcus aureus isolates in Fukuoka University Chikushi Hospital 2008-2012. Yakugaku Zasshi 2014;134:269-276. 22. Kanj SS, Whitelaw A, Dowzicky MJ. In vitro activity of tigecycline and comparators against Gram-positive and Gram-negative isolates collected from the Middle East and Africa between 2004 and 2011. Int J Antimicrob Agents 2014;43:170-178. 23. Miehlke S, Hansky K, Schneider-Brachert W, et al. Randomized trial of rifabutin-based triple therapy and high-dose dual therapy for rescue treatment of Helicobacter pylori resistant to both metronidazole and clarithromycin.  Aliment Pharmacol er 2006;24:395-403. 24. Grith DE, Brown BA, Girard WM, Wallace RJ Jr. Adverse events associated with high-dose rifabutin in macrolide-containing regimens for the treatment of Mycobacterium avium complex lung disease. Clin Infect Dis 1995;21:594-598.

QUADRUPLE RESCUE THERAPY AFTER FIRST AND SECOND LINE FAILURE FOR HELICOBACTER PYLORI TREATMENT: COMPARISON BETWEEN TWO TETRACYCLINE-BASED REGIMENS

https://ricerca.uniba.it/bitstream/11586/66801.3/2/rescue%20therapy-JGLD.pdf

QUADRUPLE RESCUE THERAPY AFTER FIRST AND SECOND LINE FAILURE FOR HELICOBACTER PYLORI TREATMENT: COMPARISON BETWEEN TWO TETRACYCLINE-BASED REGIMENS

Abstract

Similar works

Full text

Available Versions

Archivio istituzionale della ricerca - Università di Bari