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Abstract

Background: Functional probiotics may prevent Helicobacter pylori infection, and some evidence suggests that they also possess antitumor properties. Lactobacillus brevis (CD2) is a functional Lactobacillus strain with peculiar biochemical features, essentially related to the activity of arginine deiminase. This enzyme catalyzes the catabolism of arginine and affects the biosynthesis of polyamines (putrescine, spermidine, and spermine). Polyamines are polycations found in high concentrations in both normal and neoplastic cells. Our aims were: 1, to assess whether oral administration of L. brevis (CD2) affects H. pylori survival in the human gastric mucosa; 2, to evaluate the effects of L. brevis (CD2) on polyamine biosynthesis in gastric biopsies from H. pylori-positive patients.

Materials and methods: For 3 weeks before endoscopy, 22 H. pylori-positive dyspeptic patients randomly received (ratio 1 : 1) high oral doses of L. brevis (CD2) or placebo. Before and after treatment, H. pylori infection was determined by urea breath test (UBT). In gastric biopsies, ornithine decarboxylase activity and polyamine levels were, respectively, evaluated by a radiometric technique and high-pressure liquid chromatography (HPLC).

Results: L. brevis (CD2) treatment did not eradicate H. pylori. However, a reduction in the UBT delta values occurred, suggesting a decrease in intragastric bacterial load. Significantly, L. brevis (CD2) induced a decrease in gastric ornithine decarboxylase activity and polyamine levels.

Conclusions: Our data support the hypothesis that L. brevis (CD2) treatment decreases H. pylori colonization, thus reducing polyamine biosynthesis. Alternatively, the arginine deiminase activity following L. brevis (CD2) administration might cause arginine deficiency, preventing polyamine generation from gastric cells.

Research Insights

SupplementHealth OutcomeEffect TypeEffect Size
Lactobacillus brevisReduced Gastric Polyamine LevelsBeneficial
Moderate
Lactobacillus brevisReduced Helicobacter pylori ColonizationBeneficial
Moderate
Lactobacillus brevis HA-112Reduced Gastric Ornithine Decarboxylase ActivityBeneficial
Moderate
Lactobacillus brevis HA-112Reduced Helicobacter pylori ColonizationBeneficial
Moderate
Lactobacillus brevis HA-112Reduced Polyamine LevelsBeneficial
Moderate
Lactobacillus brevis LB01Reduced Gastric Ornithine Decarboxylase ActivityBeneficial
Moderate
Lactobacillus brevis LB01Reduced Helicobacter pylori ColonizationBeneficial
Moderate
Lactobacillus brevis LB01Reduced Polyamine LevelsBeneficial
Moderate
Lactobacillus brevis Lbr-35Reduced Gastric Ornithine Decarboxylase ActivityBeneficial
Moderate
Lactobacillus brevis Lbr-35Reduced Helicobacter pylori ColonizationBeneficial
Moderate
Lactobacillus brevis Lbr-35Reduced Polyamine LevelsBeneficial
Moderate
Lactobacillus brevis MAK11L82BReduced Helicobacter pylori ColonizationBeneficial
Moderate
Lactobacillus brevis MAK11L82BReduced Polyamine LevelsBeneficial
Moderate
Lactobacillus brevis SBC8803Reduced Gastric Ornithine Decarboxylase ActivityBeneficial
Moderate
Lactobacillus brevis SBC8803Reduced Helicobacter pylori ColonizationBeneficial
Moderate
Lactobacillus brevis SBC8803Reduced Polyamine LevelsBeneficial
Moderate
Lactobacillus brevis SD-5214Reduced Gastric Ornithine Decarboxylase ActivityBeneficial
Moderate
Lactobacillus brevis SD-5214Reduced Intragastric Bacterial LoadBeneficial
Moderate
Lactobacillus brevis SD-5214Reduced Polyamine LevelsBeneficial
Moderate
Lactobacillus brevis UALbr-02Reduced Helicobacter pylori ColonizationBeneficial
Moderate
Lactobacillus brevis UALbr-02Reduced Polyamine LevelsBeneficial
Moderate
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