Aliphatic alcohols in spirits inhibit phagocytosis by human monocytes

Pajor, László; Árnyas, Ervin; Bujdosó, Orsolya; Baranyi, Gergő; Rácz, Gábor; Ádány, Róza; Szűcs, Sándor

doi:10.3109/08923973.2015.1009998

Cited by 5 publications

(7 citation statements)

References 44 publications

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“…Some previous research does show that 1‐propanol, 1‐butanol, and 1‐pentanol can be incorporated into the phospholipid bilayer, just like ethanol, thereby altering the membrane fluidity and migration of granulocytes (Tomonaga, Hirota & Snyderman, ; Yuli, Tomonaga & Synderman, ). However, the concentrations of OAAs (9.1–27.3 mM) used in these experiments significantly exceeded the blood levels expected in alcohol abusers (Pál et al, ; Tomonaga, Hirota & Snyderman, ; Yuli, Tomonaga & Synderman, 1982). Consequently, we now ask whether membrane fluidity and migration of granulocytes are affected when cells are treated separately with ethanol, methanol, mixture of OAAs, and mixture of OAAs combined with ethanol at biologically relevant concentrations.…”

Section: Introductionmentioning

confidence: 56%

“…Some previous research does show that 1-propanol, 1-butanol, and 1-pentanol can be incorporated into the phospholipid bilayer, just like ethanol, thereby altering the membrane fluidity and migration of granulocytes (Tomonaga, Hirota & Snyderman, 1983;Yuli, Tomonaga & Synderman, 1982). However, the concentrations of OAAs (9.1-27.3 mM) used in these experiments significantly exceeded the blood levels expected in alcohol abusers (Pál et al, 2015;Tomonaga, Hirota & Snyderman, 1983;Yuli, Tomonaga & Synderman, 1982).…”

Section: Introductionmentioning

confidence: 65%

“…It was also shown that 0.04–80.0 mM concentrations of OAAs can be detected in spirits from commercial and noncommercial sources (Lachenmeier & Musshoff, ; Rehm et al, ). As have been described previously, consumption of 71.3 ml spirits containing 40% ethanol and OAAs at concentrations of 0.04–80.0 mM can produce biologically relevant levels of OAAs in blood, in the range of 0.0001–0.116 mM (Pál et al, ). Could these also affect membrane fluidity and granulocyte migration, possibly to an even greater extent than ethanol alone?…”

Section: Introductionmentioning

confidence: 82%

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How do methanol and higher alcohols found in alcoholic beverages affect membrane fluidity and migration of granulocytes?

et al. 2018

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Ethanol‐induced changes in membrane fluidity and migration of granulocytes has been suggested to contribute to development of alcoholic hepatitis. Besides ethanol other aliphatic alcohols (OAAs) have been detected in alcoholic beverages. We examined the effects of OAAs alone and in combination with ethanol on these processes. Granulocytes isolated from human blood were treated separately with methanol, ethanol, and a mixture of OAAs including methanol, 1‐propanol, 2‐propanol, 1‐butanol, 2‐butanol, isobutanol, and isoamyl alcohol at biologically relevant concentrations. The membrane fluidity and migration activity of granulocytes was examined by fluorescence anisotropy method and migration chambers, respectively. Our findings showed that OAAs increased membrane fluidity and migration activity of granulocytes in a concentration‐dependent manner and when combined with ethanol they caused a further increase in the migration activity of granulocytes. It is possible that OAAs consumed with alcoholic beverages may further enhance migration of granulocytes in heavy drinkers and contribute to ethanol‐induced liver damage. Practical applications The consumption of OAAs in alcoholic beverages has been hypothesized as an additional risk factor for the development of alcoholic liver diseases. To confirm this suggestion, the potentially adverse effects of exposure to OAAs should be further examined. Our investigation provides new toxicological data on the effects of OAAs found in alcoholic beverages. The results of this study can be used for more precise toxicological evaluations to clarify whether OAAs may pose an additional risk factor for the development of alcoholic liver diseases. Furthermore, information on the harmful effects of OAAs could enable health policy makers to make evidence‐based decisions when implementing new regulations on alcoholic beverages.

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Section: Introductionmentioning

confidence: 56%

Section: Introductionmentioning

confidence: 65%

Section: Introductionmentioning

confidence: 82%

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How do methanol and higher alcohols found in alcoholic beverages affect membrane fluidity and migration of granulocytes?

et al. 2018

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“…We have previously shown that AAs can decrease superoxideanion production by human granulocytes and inhibit phagocytosis by human granulocytes and monocytes in a concentration dependent manner and, when combined with ethanol, they caused a further decrease in phagocytic activity (22)(23)(24). We have found similar effects when granulocytes and monocytes were exposed to metabolites of AAs including formaldehyde, 1-propanal, acetone, 1-butanal, and 2-butanone (25).…”

Section: Short-chain Alcohols Upregulate Gilz Gene Expression and Attmentioning

confidence: 64%

“…We have found similar effects when granulocytes and monocytes were exposed to metabolites of AAs including formaldehyde, 1-propanal, acetone, 1-butanal, and 2-butanone (25). We have also calculated that blood concentrations of AAs and their metabolites could reach levels sufficient to decrease phagocytosis by granulocytes and monocytes in a clinically meaningful way in heavy users of distilled spirits (24,25). Thus, AAs and their metabolites may contribute to increased susceptibility to infectious diseases (22)(23)(24)(25).…”

Section: Short-chain Alcohols Upregulate Gilz Gene Expression and Attmentioning

confidence: 67%