A Critical Evaluation of In Vitro Hesperidin 2S Bioavailability in a Model Combining Luminal (Microbial) Digestion and Caco‐2 Cell Absorption in Comparison to a Randomized Controlled Human Trial

Rymenant, Evelien Van; Salden, Bouke; Voorspoels, Stefan; Jacobs, Griet; Noten, Bart; Pitart, Judit; Possemiers, Sam; Smagghe, Guy; Grootaert, Charlotte; Camp, John Van

doi:10.1002/mnfr.201700881

Cited by 21 publications

(22 citation statements)

References 34 publications

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“…Data from in vitro studies using various GI digestion models have provided additional information. In vitro digestion of hesperidin, naringin, and their aglycones has been carried out either in batch-like settings using incubations with fecal slurries or isolated bacteria [37,40,41], or in more comprehensive models, such as the TNO in vitro model of the colon (TIM-2) and the simulator of the human intestinal microbial ecosystem (SHIME) [42,43]. These in vitro studies, listed in Table 1, show quite consistently that during colonic microbial fermentation, hesperidin and naringin are first metabolized into their aglycones hesperetin and naringenin and subsequently into various phenolics, including dihydrocaffeic acid, isoferulic acid, 4-hydroxyphenylacetic acid, dihydroferulic acid, ferulic acid, resorcinol, phloroglucinol, 2,4-dihydroxyphenylacetic acid, 4-hydroxybenzoic acid, phloretic acid, phloroglucinic acid, hydrocinnamic acid, 3-(3′-hydroxyphenyl)propionic acid, protocatechuic acid, and hippuric acid.…”

Section: Intestinal Fate and Bioavailabilitymentioning

confidence: 99%

“…In addition to the type of metabolites formed, a recent study by Van Rymenant et al provided information about the location of citrus flavanone metabolism. Using a digestion model comprising compartments representing the ascending, transverse, and descending colon (SHIME) inoculated with a fecal sample from a healthy volunteer, the metabolites formed upon hesperidin conversion were found at the highest concentrations in the compartments representing the ascending and transverse colon, while lower concentrations were measured in the descending colon [42]. These in vitro results suggest that microbial metabolism predominantly takes place in the more proximal parts of the colon.…”

Section: Intestinal Fate and Bioavailabilitymentioning

confidence: 99%

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The Intestinal Fate of Citrus Flavanones and Their Effects on Gastrointestinal Health

et al. 2019

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Citrus flavanones, with hesperidin and naringin as the most abundant representatives, have various beneficial effects, including anti-oxidative and anti-inflammatory activities. Evidence also indicates that they may impact the intestinal microbiome and are metabolized by the microbiota as well, thereby affecting their bioavailability. In this review, we provide an overview on the current evidence on the intestinal fate of hesperidin and naringin, their interaction with the gut microbiota, and their effects on intestinal barrier function and intestinal inflammation. These topics will be discussed as they may contribute to gastrointestinal health in various diseases. Evidence shows that hesperidin and naringin are metabolized by intestinal bacteria, mainly in the (proximal) colon, resulting in the formation of their aglycones hesperetin and naringenin and various smaller phenolics. Studies have also shown that citrus flavanones and their metabolites are able to influence the microbiota composition and activity and exert beneficial effects on intestinal barrier function and gastrointestinal inflammation. Although the exact underlying mechanisms of action are not completely clear and more research in human subjects is needed, evidence so far suggests that citrus flavanones as well as their metabolites have the potential to contribute to improved gastrointestinal function and health.

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Section: Intestinal Fate and Bioavailabilitymentioning

confidence: 99%

Section: Intestinal Fate and Bioavailabilitymentioning

confidence: 99%

The Intestinal Fate of Citrus Flavanones and Their Effects on Gastrointestinal Health

et al. 2019

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“…In future experiments, bioavailability can therefore be addressed by using a transwell system that combines intestinal and hepatic cells. Moreover, by using the Simulator of the Human Intestinal Microbial Ecosystem (SHIME), the in vivo situation could be better mimicked (Van Rymenant et al, ). Also, more structural derivatives of the main structures that were presented could be tested.…”

Section: Discussionmentioning

confidence: 99%

Search for Natural Compounds That Increase Apolipoprotein A‐I Transcription in HepG2 Cells: Specific Attention for BRD4 Inhibitors

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Pijl

Lin

et al. 2019

Lipids

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Although increasing apolipoprotein A‐I (apoA‐I) might lower the cardiovascular disease risk, knowledge on natural compounds that elevate apoA‐I transcription is limited. Therefore, the aim of this study was to discover natural compounds that increase apoA‐I transcription in HepG2 cells. Since BRD4 inhibition is known to elevate apoA‐I transcription, we focused on natural BRD4 inhibitors. For this, the literature was screened for compounds that might increase apoA‐I and or inhibit BRD4. This resulted in list A, (apoA‐I increasers with unknown BRD4 inhibitor capacity), list B (known BRD4 inhibitors that increase apoA‐I), and list C (BRD4 inhibitors with unknown effect on apoA‐I). These compounds were compared with the compounds in two natural compound databases. This resulted in (1) a common substructure (ethyl‐benzene) in 60% of selected BRD4‐inhibitors, and (2) four compounds that increased ApoA‐I: hesperetin, equilenin, 9(S)‐HOTrE, and cymarin. Whether these increases are regulated via BRD4 inhibition and the ethyl‐benzene structure inhibits BRD4 requires further study.

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“…Similarly, olive oil polyphenol glycosides, including oleuropein (glycoside of elenolic acid linked to hydroxytyrosol) underwent rapid and time-dependent hydrolysis, yielding appreciable amounts of free hydroxytyrosol and tyrosol, probably through nucleophilic attack [ 66 ]. On the contrary, other studies, using the same in vitro model, along with oral administration of polyphenols to humans, showed stability of a variety of polyphenols in the acidic milieu [ 67 , 68 , 69 , 70 , 71 , 72 , 73 ]. Interestingly, the incubation of apple phloretin and quercetin for 5 min with native saliva resulted in the production of the respective aglycones, likely by oral bacterial flora as the process was blocked by antibiotics [ 68 ].…”

Section: Polyphenols: Classification Structure and Bioavailabilimentioning

confidence: 92%

“…Although valuable for screening polyphenol bioavailability, caution should be used when interpreting the data obtained from the Caco-2 cellular model in terms of predictability. Indeed, even if in vitro smaller phenolic derivatives of hesperidin 2S were absorbed, hesperidin conjugates were the main bioavailable moieties in a randomized human controlled study [ 69 ].…”

Section: Polyphenols: Classification Structure and Bioavailabilimentioning

confidence: 99%

Insight into Polyphenol and Gut Microbiota Crosstalk: Are Their Metabolites the Key to Understand Protective Effects against Metabolic Disorders?

et al. 2020

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Lifestyle factors, especially diet and nutrition, are currently regarded as essential avenues to decrease modern-day cardiometabolic disorders (CMD), including obesity, metabolic syndrome, type 2 diabetes, and atherosclerosis. Many groups around the world attribute these trends, at least partially, to bioactive plant polyphenols given their anti-oxidant and anti-inflammatory actions. In fact, polyphenols can prevent or reverse the progression of disease processes through many distinct mechanisms. In particular, the crosstalk between polyphenols and gut microbiota, recently unveiled thanks to DNA-based tools and next generation sequencing, unravelled the central regulatory role of dietary polyphenols and their intestinal micro-ecology metabolites on the host energy metabolism and related illnesses. The objectives of this review are to: (1) provide an understanding of classification, structure, and bioavailability of dietary polyphenols; (2) underline their metabolism by gut microbiota; (3) highlight their prebiotic effects on microflora; (4) discuss the multifaceted roles of their metabolites in CMD while shedding light on the mechanisms of action; and (5) underscore their ability to initiate host epigenetic regulation. In sum, the review clearly documents whether dietary polyphenols and micro-ecology favorably interact to promote multiple physiological functions on human organism.

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A Critical Evaluation of In Vitro Hesperidin 2S Bioavailability in a Model Combining Luminal (Microbial) Digestion and Caco‐2 Cell Absorption in Comparison to a Randomized Controlled Human Trial

Cited by 21 publications

References 34 publications

The Intestinal Fate of Citrus Flavanones and Their Effects on Gastrointestinal Health

The Intestinal Fate of Citrus Flavanones and Their Effects on Gastrointestinal Health

Search for Natural Compounds That Increase Apolipoprotein A‐I Transcription in HepG2 Cells: Specific Attention for BRD4 Inhibitors

Insight into Polyphenol and Gut Microbiota Crosstalk: Are Their Metabolites the Key to Understand Protective Effects against Metabolic Disorders?

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