The Inhibitory Effect of Natural Products on Protein Fibrillation May Be Caused by Degradation Products – A Study Using Aloin and Insulin

Lobbens, Eva S.B.; Foderà, Vito; Nyberg, Nils T.; Andersen, Knud Erik; Jäger, Anna K.; Jørgensen, Lene; Weert, Marco van de

doi:10.1371/journal.pone.0149148

Cited by 7 publications

(5 citation statements)

References 28 publications

(39 reference statements)

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“…The MIC values were unable to be determined likely because aloin was metabolized as noted previously (Che et al, 1991; Pogribna et al, 2008). We confirmed this observation by analyzing metabolism of aloin in Eubacterium cultures by HPLC (Lobbens et al, 2016) (Figure 2A). The HPLC analysis revealed disappearance of aloin-A and aloin-B (retention time was 10.30 and 8.50 min, respectively) and appearance of aloe-emodin (retention time was 22.1 min), which provides evidence that Eubacterium sp.…”

Section: Resultssupporting

confidence: 65%

Dose-Dependent Effects of Aloin on the Intestinal Bacterial Community Structure, Short Chain Fatty Acids Metabolism and Intestinal Epithelial Cell Permeability

et al. 2019

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Aloe leaf or purified aloin products possess numerous therapeutic and pharmaceutical properties. It is widely used as ingredients in a variety of food, cosmetic and pharmaceutical products. Animal studies have shown that consumption of aloe or purified aloin cause intestinal goblet cell hyperplasia, and malignancy. Here, we tested antibacterial effects of aloin, against intestinal commensal microbiota. Minimum inhibitory concentration of aloin for several human commensal bacterial species (Gram-positive and Gram-negative) ranged from 1 to 4 mg/ml. Metabolism studies indicated that Enterococcus faecium was capable of degrading aloin into aloe-emodin at a slower-rate compared to Eubacterium spp. As a proof of concept, we incubated 3% rat fecal-slurry (an in vitro model to simulate human colon content) with 0.5, 1, and 2 mg/ml of aloin to test antimicrobial properties. Low aloin concentrations showed minor perturbations to intestinal bacteria, whereas high concentration increased Lactobacillus sp. counts. Aloin also decreased butyrate-production in fecal microbiota in a dose-dependent manner after 24 h exposure. The 16S rRNA sequence-data revealed that aloin decreases the abundance of butyrate-producing bacterial species. Transepithelial resistant result revealed that aloin alters the intestinal barrier-function at higher concentrations (500 μM). In conclusion, aloin exhibits antibacterial property for certain commensal bacteria and decreases butyrate-production in a dose -dependent manner. HIGHLIGHTS –Aloin exhibits antibacterial properties for certain intestinal commensal bacteria. –In rat fecal slurry (an in vitro model to simulate human colon content), longer aloin exposure (24 h) decreases the butyrate production in dose dependent manner. –The 16s rRNA sequencing data show that aloin decreased the abundance of butyrate producing bacterial species. –Rat intestinal commensal bacteria metabolized aloin into aloe-emodin. –Aloin altered the intestinal epithelial cells barrier integrity, however, the metabolic product of aloin - Aloe-emodin did not alter epithelial cells permeability.

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Section: Resultssupporting

confidence: 65%

Dose-Dependent Effects of Aloin on the Intestinal Bacterial Community Structure, Short Chain Fatty Acids Metabolism and Intestinal Epithelial Cell Permeability

et al. 2019

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“…Ascorbic acid (AA) has been shown to have potential therapeutic effects against several neurodegenerative diseases such as AD, PD, Huntington's disease (HD) and ischemic stroke. 54,64,72,73 Furthermore, AA has been shown to interact with Aβ, stefin B, and insulin resulting in inhibition of their aggregation. 30,60 Human semen, which naturally contains SEVI amyloid, also contains a number of vitamins amongst which AA is in the highest concentration (0.4±0.1 mM).…”

Section: Discussionmentioning

confidence: 99%

“…[60][61][62][63][64] In addition to interaction with the β-sheet backbone of amyloids, AA has been shown to exert inhibition of amyloid fibril formation through its degradation products, such as ascorbate anions and dehydroascorbic acid. 72,73 The stability of AA varies with pH and incubation temperature, where self-degradation products are obtained within ~6 hours under physiological pH at 37 ˚C. 60,72 These degradation products were found to inhibit fibrillation and disrupt preformed mature amyloid fibrils of insulin, with an activity positively correlated with the degree of AA degradation.…”

Section: Discussionmentioning

confidence: 99%

“…60,72 These degradation products were found to inhibit fibrillation and disrupt preformed mature amyloid fibrils of insulin, with an activity positively correlated with the degree of AA degradation. 72,73 The metabolites of AA were shown to shield the electrostatic interactions between the β-sheet forming areas of protein monomers prone to form amyloid structures and to disrupt β-sheet stacking. 60 Since in our in vitro assay, effects on fibril formation were seen after 24 hours, we speculate that such degradation products might contribute to the amyloid inhibitory effects observed at concentrations of AA higher than its physiological concentration.…”

Section: Discussionmentioning

confidence: 99%

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Dual concentration-dependent effect of ascorbic acid on PAP(248–286) amyloid formation and SEVI-mediated HIV infection

et al. 2021

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“…In a case study, the inhibitory activity of barbaloin against insulin fibrillation was investigated. The degradation products of barbaloin formed over weeks of storage, in particular oxidation products, were able to significantly inhibit insulin-fibrillation [20] .…”

Section: Immune Modulation By Barbaloin a L O E -E M O D I N A N Dmentioning

confidence: 99%

Prophylactic Aloe Components on Autoimmune Diseases: Barbaloin, Aloe-Emodin, Emodin, and Fermented Butyrate

Yagi¹,

2018

Journal of Gastroenterology and Hepatology Research

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proliferation of RA synoviocytes in a dose-dependent manner under hypoxic condition. Another putative immune modulator we reviewed in this paper is Aloe's butyrate fermented by the dietary Aloe in the gut. Its beneficial effects are based on the host immune metabolism via the activation of intestinal mucosal functions on the suppression of obesity and inflammation. It is hoped that elaboration on butyrate may provide fresh insights as to Aloe's immune modulation and chronic inflammation. Potential efficacious role of barbaloin, Aloeemodin, emodin and fermented butyrate of Aloe vera needs further scrutiny and evidence-based documentation through carefully designed research.

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The Inhibitory Effect of Natural Products on Protein Fibrillation May Be Caused by Degradation Products – A Study Using Aloin and Insulin

Cited by 7 publications

References 28 publications

Dose-Dependent Effects of Aloin on the Intestinal Bacterial Community Structure, Short Chain Fatty Acids Metabolism and Intestinal Epithelial Cell Permeability

Dose-Dependent Effects of Aloin on the Intestinal Bacterial Community Structure, Short Chain Fatty Acids Metabolism and Intestinal Epithelial Cell Permeability

Dual concentration-dependent effect of ascorbic acid on PAP(248–286) amyloid formation and SEVI-mediated HIV infection

Prophylactic Aloe Components on Autoimmune Diseases: Barbaloin, Aloe-Emodin, Emodin, and Fermented Butyrate

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