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Probiotics are a generally safe treatment option and have been evaluated positively for several conditions by the Cochrane Collaboration. However, they must have adequate compositional quality and be able to persist in the gut to be efficacious and safe.
Probiotics are bacteria with beneficial health effects. Their efficacy and safety have been evaluated positively by the Cochrane Collaboration for several indications such as acute infectious diarrhea [1]. However, the Cochrane Collaboration has also noted that individual preparations can differ and “more research is needed to guide the use of particular probiotic regimens”. As highlighted in two recent review articles [2, 3], the efficacy and safety of probiotic depends not only on the biological properties of specific bacterial species and their strains, but also on the compositional quality of the preparations and their ability to persist in the gut.
Pharmaceuticals licensed as drugs are subject to rigorous quality controls; this applies not only to small molecules and antibodies, but also to probiotics. However, less stringent regulations are generally applied to preparations categorized as dietary supplement or functional foods. A recent review [2] based on 38 evaluations of 31 marketed probiotic drugs found that in 37% (14/38) of the evaluations the included product contained microorganisms other than those listed in the label, with 18% (7/38) found with contaminants. Moreover, only 29 products declared expected amounts on their label, for which 48% (14/29) were found to have differing amounts of bacteria compared to their respective labels. In total, only 29% (9/31) of the drug products consistently satisfied all three criteria in all studies (Tab. 1). The most often tested preparation was a Bacillus clausii product (Enterogermina®) that was found to satisfy all three criteria consistently across five separate studies.
Tab. 1. Compliance with the label claims of probiotic drugs marketed worldwide with focus on microbial composition, amount of living cells and presence of contaminant microorganisms. Reproduced with permission from [2].
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Product
Manufacturer
Country
Compliance (composition)
Compliance (amount)
Contaminants
Reference
Benegut
Abbott
India
No
No
Yes
Kesavelu et al., 2020
Bifilac
Tablets India Ltd
India
No
Yes
Yes
Kesavelu et al., 2020
Bifilac GG
Tablets India Ltd
India
Yes
Yes
No
Kesavelu et al., 2020
Biogermin
Union Health S.r.l.
Italy
Yes
Yes
No
Celandroni et al., 2019
Codex
Zambon
Italy
Yes
Yes
No
De Vecchi et al., 2008
Yes
Yes
No
Vecchione et al., 2018
Combiflora
Medopharm
India
No
No
No
Kesavelu et al., 2020
Cyfolac
Karnataka Antib & Pharm Ltd
India
Yes
Yes
No
Kesavelu et al., 2020
Darolac
Aristo Pharmaceuticals Pvt Ltd
India
No
No
No
Kesavelu et al., 2020
Ecogro
Akum Drugs & Pharma
India
No
Yes
Yes
Patrone et al., 2016
Econorm
Dr. Reddy’s Laboratories Ltd
India
Yes
N.D.
No
Kesavelu et al., 2020
Entero Plus
Glaxo India Ltd
India
Yes
Yes
No
Kesavelu et al., 2020
Enterogermina
Sanofi
Italy
India
Yes
Yes
No
De Vecchi et al., 2008
Yes
Yes
No
Vecchione et al., 2018
Yes
Yes
No
Celandroni et al., 2019
Yes
Yes
No
Patrone et al., 2016
Yes
Yes
No
Kesavelu et al., 2020
Enterol capsules
Biodiphar
Belgium
Yes
Yes
No
Vanhee et al., 2010
Enterol sachets
Biodiphar
Belgium
Yes
Yes
No
Vanhee et al., 2010
Entromax
Mankind Pharma
India
No
Yes
No
Patrone et al., 2016
GNorm
Nouveau Medicament
India
Yes
N.D.
No
Kesavelu et al., 2020
GutPro
Riata Life Sciences Pvt Ltd
India
Yes
No
No
Kesavelu et al., 2020
Infloran
BERNA
Italy
Yes
No
No
Fasoli et al., 2003
Lacidofil
Merck
Poland
No
Yes
No
Zawistowska-Rojek et al., 2016
Yes
Yes
No
Korona-Glowniak et al., 2019
Lakcid
Biomed
Poland
Yes
Yes
No
Zawistowska-Rojek et al., 2016
Yes
Yes
No
Zawistowska-Rojek et al., 2016
Ospor
Matrix Pharma
Pakistan
Yes
No
No
Patrone et al., 2016
Pre Pro Kid
Fourrts India Laboratories
India
No
No
No
Kesavelu et al., 2020
Pre Pro Kid L
Fourrts India Laboratories
India
No
No
Yes
Kesavelu et al., 2020
Reflora Z
Sundyota Numandis
India
No
No
No
Kesavelu et al., 2020
Regutol
Alembic Pharmaceuticals Ltd
India
No
Yes
Yes
Kesavelu et al., 2020
Remune Al
Sundyota Numandis
India
No
No
No
Kesavelu et al., 2020
SPORLAC
Sanzyme Ltd
India
Yes
No
No
Kesavelu et al., 2020
Super Flora GG
Sundyota Numandis
India
Yes
No
No
Kesavelu et al., 2020
Tufpro
Virchow Biotech Pvt. Ltd.
India
No
No
Yes
Patrone et al., 2016
ViBact
USV
India
No
Yes
Yes
Kesavelu et al., 2020
Vizylac
Torrent Pharmaceuticals Ltd
India
Yes
No
No
Kesavelu et al., 2020
A key challenge to orally administered probiotics is that they must survive the passage through the hostile (highly acidic) environment of the stomach to reach the gut in sufficient numbers to become biologically active. This is illustrated by an experimental study in which the survival of several marketed probiotic preparations was tested in three different simulated conditions (two gastric and one intestinal juices) [4]. Among the 10 tested preparations, only three maintained the initial number of microorganisms in two distinct simulated gastric juices and only two in simulated intestinal juice The B. clausii product Enterogermina® was the only product which conserved its biological activity in all three tests (Fig. 1), which can be attributed to its spore-forming capabilities [4].
Figure 1. Viability of probiotic formulation after incubation in one of the two simulated gastric fluids. Data are expressed as logarithm of colony-forming units (CFU) of each product. Reproduced with permission from [4].
A recent systematic review has assessed the survival rate of orally administered probiotic bacteria during gastro-intestinal transit based on clinical studies with 17 studies of single strains and 13 studies of multi-strain products [3]. When the administered dose was higher than 1010 colony-forming units/day, the probiotic could be recovered from stool regardless of the strain used. This was independent of treatment duration.
The B. clausii product Enterogermina®, despite being studied only after a single administration and at a lower dosage (6 billion CFU [colony forming units] versus probiotics administered up to 100 billion CFU), was among the ones with the highest amount recovered [3]. Such a result appears to confirm in a clinical setting the results observed in the preclinical model [4] and suggests that spores are highly resistant to the harsh conditions of gastro-intestinal transit.
The authors in the end concluded that general dosage recommendations for probiotics by regulatory agencies are not high enough for a strain to survive, persist and be efficacious in the gut. Additionally, it was noted that resistance to gastro-intestinal transit is strain specific, with spore-forming bacteria among the ones with higher survivability and persistence. Of interest, among spore formers included in the study, B. clausii appears to have better ability to resist to the gastrointestinal tract [3].
We conclude that greater rigor is required in controlling the pharmaceutical quality of marketed probiotic products and that the same attention should be reserved to fully elucidate the ability of the strain to reach and persists and multiply in the intestine. Such a latter characteristic appears to be strain dependent and poorly affected by the matrix or by the dosage, especially when probiotics are administered in dosages lower that 10 billion CFU. The B. clausii product Enterogermina® appears to be one of the few preparations consistently fulfilling the required criteria on compositional quality, survivability and persistence.
Allen SJ, Martinez EG, Gregorio GV, Dans LF. Probiotics for treating infectious diarrhoea. Cochrane Database of Systematic Reviews 2010;11:CD003048.
Mazzantini D, Calvigioni M, Celandroni F, Lupetti A, Ghelardi E. Spotlight on the compositional quality of probiotic formulations marketed worldwide. Frontiers in Microbiology 2021;12.
Morelli L, Pellegrino P. A critical evaluation of the factors affecting the survival and persistence of beneficial bacteria in healthy adults. Beneficial Microbes 2021;12:321–31.
Vecchione A, Celandroni F, Mazzantini D, Senesi S, et al. Compositional quality and potential gastrointestinal behavior of probiotic products commercialized in Italy. Frontiers in Medicine 2018;5.
Conflict of interest: P. Pellegrino and M. Perez III. are employees of Sanofi.
Disclosures: Medical writing and publication funded by Sanofi.
Aansluiting/Correspondentie: Paolo Pellegrino, MD, Sanofi, Viale Bodio 37/b, 20158 Milan, Italy (paolo.pellegrino@sanofi.com) en Marcos Perez III., MD, Sanofi-Aventis Deutschland GmbH, Industriepark Hoechst, Frankfurt am Main, Germany