Case–Control Research Study of Auto-Brewery Syndrome

Cordell, Barbara; Kanodia, Anup K.; Miller, Gregory K.

doi:10.1177/2164956119837566

Cited by 24 publications

(44 citation statements)

References 37 publications

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“…The human body is well prepared to get rid of the consumed alcohol in order to prevent its accumulation and more serious acute health problems. Alcohol removal proceeds preferentially through enzymatic degradation [20,23,24].…”

Section: Alcohol and Acetaldehyde Metabolismmentioning

confidence: 99%

“…Although present also in the gastrointestinal tract [35,36,37,38,39,40,41], MEOS is predominantly found in the liver, when it was first described in 1968 [42] and 1970 [43]. Based on these early investigations and various other studies [42,43,44,45,46], and as summarized recently [20,23], MEOS can now be characterized as follows: the reaction converts ethanol to acetaldehyde, MEOS depends on reduced nicotinamide adenine dinucleotide phosphate (NADPH + H + ) or a NADPH regenerating system, and requires molecular oxygen [31,42,43,44,45,46,47,48,49]; key components of MEOS are several form of cytochrome P450 (CYP) with preference of its CYP 2E1 isoform, the NADPH-dependent cytochrome P450 reductase, and phospholipids [45,47,50,51]; MEOS is most active at a physiological pH, has a Michaelis–Menten constant of 7–11 mM and thereby active at intermediate and high alcohol concentrations, and is inducible in its activity following prolonged alcohol consumption [42,43]. Apart from ethanol, other aliphatic alcohols and various chemicals are known substrates of this special enzyme system [20,23].…”

Section: Alcohol and Acetaldehyde Metabolismmentioning

confidence: 99%

“…It has also been suggested that when corrected for microsomal losses during preparation, half to two thirds of the increase in the rate of ethanol oxidation after chronic alcohol use can be accounted for by MEOS [33]. Conservatively speaking and considering variable results, MEOS may contribute >25% of overall hepatic alcohol metabolism at high alcohol concentrations and after prolonged alcohol abuse considering mostly kinetic characteristics and also, rarely, inhibitory studies [55], with details outlined recently [23].…”

Section: Alcohol and Acetaldehyde Metabolismmentioning

confidence: 99%

“…This has a major impact on hepatic intermediary pathways, which require NAD + or are inhibited by excess NAD + H + [34]. Certainly, part of the redox changes can be attenuated by reducing equivalents in the form of NADPH + H + required for ethanol oxidation via MEOS [23].…”

Section: Alcohol and Acetaldehyde Metabolismmentioning

confidence: 99%

“…For understanding the pathogenesis of ALD the occurrence and action of ROS is of pivotal importance [7,23,58,59,60,61]. Along the NADPH dependent MEOS reaction also involving CYP 2E1, acetaldehyde and a variety of ROS are generated from incomplete split of molecular oxygen [7,23]: ethoxy radical CH 3 CH 2 O • , hydroxyethyl radical CH 3 C( • )HOH, acetyl radical CH 3 CHO • , singlet radical 1 O 2, superoxide radical HO • 2 , hydrogen peroxide H 2 O 2 , hydroxyl radical HO • , alkoxyl radical RO • , and peroxyl radical ROO • . ROS undergoes covalent bonding to macromolecules within the liver cells including those present in membranes of subcellular organelles like mitochondria with their structural proteins and phospholipids.…”

Section: Reactive Oxygen Speciesmentioning

confidence: 99%

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Alcoholic Liver Disease: Current Mechanistic Aspects with Focus on Their Clinical Relevance

Teschke

2019

Biomedicines

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The spectrum of alcoholic liver disease (ALD) is broad and includes alcoholic fatty liver, alcoholic steatohepatitis, alcoholic hepatitis, alcoholic fibrosis, alcoholic cirrhosis, and alcoholic hepatocellular carcinoma, best explained as a five-hit sequelae of injurious steps. ALD is not primarily the result of malnutrition as assumed for many decades but due to the ingested alcohol and its metabolic consequences although malnutrition may marginally contribute to disease aggravation. Ethanol is metabolized in the liver to the heavily reactive acetaldehyde via the alcohol dehydrogenase (ADH) and the cytochrome P450 isoform 2E1 of the microsomal ethanol-oxidizing system (MEOS). The resulting disturbances modify not only the liver parenchymal cells but also non-parenchymal cells such as Kupffer cells (KCs), hepatic stellate cells (HSCs), and liver sinusoidal endothelial cells (LSECs). These are activated by acetaldehyde, reactive oxygen species (ROS), and endotoxins, which are produced from bacteria in the gut and reach the liver due to gut leakage. A variety of intrahepatic signaling pathways and innate or acquired immune reactions are under discussion contributing to the pathogenesis of ALD via the five injurious hits responsible for disease aggravation. As some of the mechanistic steps are based on studies with in vitro cell systems or animal models, respective proposals for humans may be considered as tentative. However, sufficient evidence is provided for clinical risk factors that include the amount of alcohol used daily for more than a decade, gender differences with higher susceptibility of women, genetic predisposition, and preexisting liver disease. In essence, efforts within the last years were devoted to shed more light in the pathogenesis of ALD, much has been achieved but issues remain to what extent results obtained from experimental studies can be transferred to humans.

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Section: Alcohol and Acetaldehyde Metabolismmentioning

confidence: 99%

Section: Alcohol and Acetaldehyde Metabolismmentioning

confidence: 99%

Section: Alcohol and Acetaldehyde Metabolismmentioning

confidence: 99%

Section: Alcohol and Acetaldehyde Metabolismmentioning

confidence: 99%

Section: Reactive Oxygen Speciesmentioning

confidence: 99%

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Alcoholic Liver Disease: Current Mechanistic Aspects with Focus on Their Clinical Relevance

Teschke

2019

Biomedicines

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Auto‐brewery syndrome caused by oral fungi and periodontal disease bacteria

Takahashi

Hoshikawa

Kan

et al. 2021

Acute Medicine & Surgery

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Background Auto‐brewery syndrome (ABS) is often caused by fungi in the intestinal tract. We describe a rare case of alcohol production by Candida albicans and periodontal disease bacteria in the oral cavity. Case Presentation A man aged in his 60s had a car accident, and alcohol was detected on his breath. At the time, he exhibited alcohol overdose seizures with no alcohol consumption. We carried out a gastrointestinal endoscopy, detected esophageal candidiasis, and diagnosed ABS. His seizures continued despite using miconazole oral gel. Significant tooth decay, periodontal disease, and high C. albicans levels were observed in his oral cavity. Alcohol production was confirmed from periodontal bacteria and C. albicans cultures and alcohol‐degrading enzyme functions were poor. Dental treatment and antifungal drugs reduced seizures, and improved his fatty liver. Conclusion Alcohol can be produced by microorganisms in healthy individuals. Therefore, blood alcohol levels and alcohol‐degrading enzyme functions should be examined in patients with unexplained liver dysfunction.

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Gut fermentation syndrome: A systematic review of case reports

et al. 2021

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Background:The gut fermentation syndrome (GFS), also known as the endogenous alcohol fermentation syndrome or auto brewery syndrome, is a rare and underdiagnosed medical condition where consumed carbohydrates are converted to alcohol by the microbiota in the gastrointestinal or urinary tract. The symptoms of GFS can have severe impact on patients' wellbeing and can have social and legal consequences. Unfortunately, not much is reported about GFS. The aim of this systematic review was to assess the evidence for GFS, causal micro-organisms, diagnostics, and possible treatments.Methods: A protocol was developed prior to initiation of the systematic review (PROSPERO 207182).We performed a literature search for clinical studies on 1 September 2020 using PubMed and Embase. We included all clinical studies, including case reports that described the GFS. Results:In total, 17 case reports were included, consisting of 20 patients diagnosed with GFS. The species that caused the GFS included Klebsiella pneumoniae, Candida albicans, C. glabrata, Saccharomyces cerevisiae, C. intermedia, C. parapsilosis, and C. kefyr.Conclusions: GFS is a rare but underdiagnosed disease in daily practice. The disease is mostly reported by Saccharomyces and Candida genera, and some cases were previously treated with antibiotics. Studies in Nonalcoholic Fatty Liver disease suggest a bacterial origin of endogenous alcohol-production, which might also be causal micro-organisms in GFS. Current treatments for GFS include antibiotics, antifungal medication, low carbohydrate diet, and probiotics. There might be a potential role of fecal microbiota transplant in the treatment of GFS.

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Case–Control Research Study of Auto-Brewery Syndrome

Cited by 24 publications

References 37 publications

Alcoholic Liver Disease: Current Mechanistic Aspects with Focus on Their Clinical Relevance

Alcoholic Liver Disease: Current Mechanistic Aspects with Focus on Their Clinical Relevance

Auto‐brewery syndrome caused by oral fungi and periodontal disease bacteria

Gut fermentation syndrome: A systematic review of case reports

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