Wine: An Aspiring Agent in Promoting Longevity and Preventing Chronic Diseases
Abstract
:1. Introduction
2. Methods
3. Results
3.1. Association between Wine Consumption and Cardiovascular Disease
3.2. Association between Wine Consumption and Blood Pressure
3.3. Association between Wine Consumption and Metabolic Syndrome
3.4. Association between Wine Consumption and Weight
3.5. Association between Wine Consumption and Cancer
3.6. Association between Wine Consumption and Mental Health
3.7. Association between Wine Consumption and Gut Flora
4. Discussion
5. Conclusions
Author Contributions
Funding
Acknowledgments
Conflicts of Interest
References
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Clinical Sample | Dose | Duration-Experimental Models | Main Results | References |
---|---|---|---|---|
1248 patients | Wine ≤ 500 mL/day | 3.5 years of follow-up | Lower risk of cardiovascular (CV) events and mortality | Levantesi G., et al., 2013 |
6973 patients | 1 glass of wine per day | Kansas City Cardiomyopathy Questionnaire | Better health status, lower depressive symptoms and vascular inflammation | Cosmi F., et al., 2015 |
449 older, U.S. male physicians with prevalent heart failure | 1–2 drinks per day (beer, wine, or liquor) | 7 years | Lowest mortality, independent of alcoholic drink type | Petrone A.B., et al., 2014 |
11,470 patients with type 2 diabetes aged at least 55 years in 20 countries | 0.28 L of beer, 125 mL of wine, and 25 mL of spirits. | 5 years of follow-up, self-report | Reduced risks of CV events and all-cause mortality | Blomster J.I., et al., 2014 |
40 otherwise healthy individuals with high cholesterol | RW, 125 mL for women and 250 mL for men/daily | 1 month | Better cholesterol levels and LDL/HDL ratio | Apostolidou C., et al., 2015 |
23 hypercholesteraemic participants | 250 mL daily of RW or WW or RO | 10 weeks | Both RW and RO improved LDL oxidation lag time. | Chiu H.F., et al., 2016 |
12 healthy men, aged 25–39 years | 4 mL/kg body weight WW or RW or ethanol solution | 2 weeks | Cardioprotective effect of moderate wine consumption, independently of ethanol. | Xanthopoulou M.N., et al., 2017 |
157 healthy participants | RW and WW | 12 months | Both RW and RO improve LDL. RW suppressed the total cholesterol | Taborsky M., et al., 2017 |
122 patients, aged >30 years | RW, women: 100 mL, men: 200 mL, with rich Med. | 20 weeks | No changes on peak systolic, end-diastolic or mean cerebral blood flow velocity | Droste D.W., et al., 2014 |
122 patients, aged >30 years | RW (100 mL for women and 200 mL for men) | 20 weeks | Improved the LDL/HDL ratio of the participants | Droste D.W., et al., 2013 |
Clinical Sample | Dose | Duration-Experimental Models | Main Results | References |
---|---|---|---|---|
24 premenopausal women, aged 25–49 years | 200 to 300 mL red wine (RW)/day | 4 weeks | Increased the 24-h systolic and diastolic BP. | Mori T.A., et al., 2015 |
24 patients with well-controlled T2DM | Women: 230 mL RW/day, Men: 300 mL/day or DRW | 4 weeks | RW, increased heart rate (HR), awake and asleep (24 h) | Mori T.A., et al., 2016 |
54 participants (age = 57 years; 85% men) with T2DM | 150 mL RW at dinner/daily, with Med. diet | 6 months | Reductions in BP were observed in the red wine group at midnight (3–4 h after ingestion) | Gepner Y., et al., 2016 |
224 patients with T2DM | 150 mL of mineral water, WW, or RW with dinner | 2 years | No differences were identified in blood pressure | Gepner Y., et al., 2015 |
18 healthy subjects, aged 25–53 years) | 2 glasses of RW | 24 h | Higher heart rate during the consumption and lowered after consumption | Fantin F., et al., 2016 |
25 normotensive men, aged 20–65 years | 375 mL RW or 375 mL non-alcoholic wine or water | 3 different days | A decrease in BP in the first 4 h and an increase after 20 h | Barden A.E., et al., 2013 |
60 untreated, hypertensive participants | 2 grape extracts (grape-RW and grape alone) | 4 weeks | Systolic and diastolic BP were significantly lower during the day. | Draijer R., et al., 2015 |
Clinical Sample | Dose | Duration-Experimental Models | Main Results | References |
---|---|---|---|---|
15,905 Hispanics/Latinos, aged 18–74 years | RW, WW, beer, liquor | Self-report questionnaire | Low levels of wine, related with lower odds of MetS | Vidot D.C., et al., 2016 |
64,046 participants aged 18–80 years | Beer, wine or spirits/mixed drinks group | Self-report questionnaire | Protective effect against MetS, and low HDL cholesterol | Slagter S.N., et al., 2014 |
14,375 active or retired civil servants, aged 35–74 years | Beer (350 mL), wine (120–150 mL) or spirits (40 mL). | Standard questionnaire | Consumption of wine in lesser quantities with meals was generally more protective than when taken outside of meals | Vieira B.A., et al., 2016 |
8103 participants (men = 2687 and women = 5416) | Red or other wines (100 mL), beer (330 mL), and spirits (50 mL) | Questionnaire consumption | Higher risk of developing specific MetS after at least 6 years of follow-up with 7 alcoholic drinks/week | Barrio-Lopez M.T., et al., 2013 |
5801 elderly participants at a high cardiovascular risk | 100 mL of wine, 250 mL of beer, 65 mL of liquors and 32 mL of spirits | 137-item FF Questionnaire | Lower prevalence of the MetS in an elderly Mediterranean population at a high cardiovascular risk | Tresserra-Rimbau A., et al., 2015 |
66,485 women from the French prospective E3N-EPIC cohort | 150 mL wine, 250 mL beer, 70 mL fortified wine, 40 mL spirits | Questionnaires, every 2–3 years, for 14 years | Wine, associated with T2D risk, only in overweight women. | Fagherazzi G., et al., 2014 |
67 men at high cardiovascular risk, after a run-in period | RW (30 g alcohol/day) or gin (30 g alcohol/day) | 4 weeks | Beneficial effect of the non-alcoholic fraction of RW on insulin resistance and cardiovascular disease | Chiva-Blanch G., et al., 2013 |
224 patients with T2DM | 150 mL of mineral water, WW, or RW with dinner | 2 years | Both ethanol and RW non-alcoholic constituents can be beneficial to the cardio-metabolic risk in well controlled T2D patients. | Gepner Y., et al., 2015 |
Clinical Sample | Dose/Type | Duration | Main Results | References |
---|---|---|---|---|
224 patients with T2DM | 150 mL of mineral water, WW, or RW with dinner | 2 years | No weight change in patients with T2DM | Gepner Y., et al., 2015 |
48 participants | 150 mL of mineral water, WW or RW with dinner | 2 years | Without changes to ratio of abdominal fat | Golan R., et al., 2017 |
14,971 from 51,529 men in the USA, aged 40–75 years | FFQ | 4 years | Dose-dependent relationship | Downer M.K., et al., 2017 |
5879 Australian-born individuals aged 40–69 years | 121-item FFQ | 8 years | Greater waist circumference and body weight | MacInnis R.J., et al., 2014 |
7855 men aged 50–59 years | FFQ | 2 years | Associated with BMI and waist circumference | Dumesnil C., et al., 2013 |
Clinical Sample | Dose/Type/Experimental Models | Main Results | References |
---|---|---|---|
2513 cases of ovarian cancer | Beer, RW and WW and spirits/questionnaire | Wine consumption was associated with a lower risk of cancer | Cook L.S., et al., 2016 |
476,160 individuals aged 35–70 years from 10 countries | Beer, wine, sweet liquor, distilled spirits/13.9 year | No association between alcohol and UCC | Botteri E., et al., 2017 |
301,051 women from 10 countries | Different types of alcoholic beverages/questionnaires | No associations between alcohol consumption and endometrial cancer risk. | Fedirko, V., et al., 2013 |
66,481 women aged 40–65 years from the French | 150 mL wine, 250 mL beer, 70 mL fortified wine, 40 mL spirits/questionnaires | >2 glasses of wine/day in postmenopausal period increased the risk of breast cancer by 33% | Fagherazzi G., et al., 2015 |
167,765 women from the NHS and 43,697 men | Beer, RW, WW, liquor/FFQ | Alcohol consumption is associated with increased risk of cutaneous BCC | Wu S., et al., 2015 |
380 BCC and 390 controls with benign skin conditions | Wine, beer, hard liquor or mixed drinks/saliva sample and questionnaires | No association between lifetime alcohol intake and early-onset BCC | Zhang Y., et al., 2014. |
59,575 white postmenopausal women | Beer, wine, liquor and gin, brandy and whisky/FFQ | Increased hazard of melanoma (MM) and risk of non-melanoma skin cancer | Kubo J.T., et al., 2014 |
210,252 participants from the USA | Beer, RW, WW, liquor/FFQ | Alcohol intake was associated with a modest increase in the risk of melanoma | Rivera A., et al., 2016 |
120,852 participants aged 55–69 years from Holland | Beer, RW, WW, liquor/FFQ | Wine consumption was inversely associated with overall risk of HNC, and HNC-subtypes | Maasland D.H.E., et al., 2014 |
24,068 men and women aged 39–79 years | Beer, wine and spirits/FFQ | Wine drinking associated inversely with lower risk of oesophageal adenocarcinoma | Yates M., et al., 2014. |
3397 patients | Beer, wine and liquor/FFQ | RW, associated with longer overall survival and disease-free survival | Phipps A.I., et al., 2016 |
4966 cases of incident invasive colorectal cancer (CRC) | Beer, hard cider, wine, fortified wines, hard liquor/FFQ | Wine consumption modestly associated with more favourable survival after colorectal cancer (CRC) | Phipps A.I., et al., 2017 |
3146 patients with CRC from southwest of Germany | Beer, wine and liquor/questionnaires | Alcohol abstinence and heavy drinking behaviour were associated with poorer survival after CRC | Walter V., et al., 2016 |
141 patients with incurable invasive cancer | Wine arm and nutritional supplement arm/questionnaires and diaries | Wine does not improve appetite or weight in advanced cancer patients. | Jatoi A., et al., 2016 |
Clinical Sample | Dose/Type/Experimental Models | Main Results | References |
---|---|---|---|
12,326 individuals from the Swedish Twin Registry | Beer, wine, or 6 cL of 80-proof spirits/questionnaire | >12 g of alcohol per day may increase risk of dementia. | Handing E.P., et al., 2015 |
589 multi-ethnic community residents of New York aged ≥65 years | Beer, wine, or liquor/FFQ | Protective effect of wine on brain | Gu Y., et al., 2014 |
2613 participants, aged 43–70 years | Beer, wine (red, white and rosé), fortified wine and spirits/FFQ | Only moderate red wine consumption, associated with less strong cognitive decline | Nooyens A.C., et al., 2014 |
360 patients with early AD in New York, Boston, Baltimore and Paris | Alcohol intake/FFQ | Wine did not affect the rate of cognitive decline | Heymann D., et al., 2016 |
5505 high-risk middle aged and elderly men and women | Beer, wine, spirits/FFQ | 2–7 units of wine per week, associated with 32% lower risk of depression, yet heavy drinking can increase the risk of depression | Gea A., et al., 2013 |
1572 adults living in southern Italy | Dietary intakes of polyphenols/questionnaire | Higher dietary intake of flavonoid may be inversely associated with depressive symptoms. | Godos J., et al., 2018 |
Clinical Sample | Dose/Type | Duration | Main Results | References |
---|---|---|---|---|
41 volunteers, aged 20−65 years | 250 mL/day RW | 4 weeks | The microbial metabolic profile of faeces is significantly modified after moderate intake of red wine polyphenols | Munoz-Gonzalez I., et al., 2013 |
60 microbial phenolic metabolites in faecal samples | DRW: 272 mL, RW: 272 mL/, Gin: 100 mL/day | 3 months | The microbial metabolic profile of faeces is significantly modified after moderate intake of red wine polyphenols | Jimenez-Giron A., et al., 2013 |
10 male volunteers, aged 45–50 years | RW (272 mL/day), DRW (272 mL/day), or gin (100 mL/day) | 20 days | Chronic RW consumption increases Bifidobacterium and Prevotella amounts, which may have beneficial effects by leading to lower plasma lipopolysaccharide (LPS) concentrations. | Clemente-Postigo M., et al., 2013 |
10 patients with metabolic syndrome and 10 healthy subjects | RW & DRW | 30 days | Modulation of the gut microbiota by using red wine could be an effective strategy for managing metabolic diseases associated with obesity. | Moreno-Indias I., et al., 2016 |
38 volunteers, 55–67 years | 100 mL per day RW/FFQ | Regular consumption of RW appears to be associated with a reduced serum lipoperoxidation in which the intestinal microbiota may be involved | Cuervo A., et al., 2015 | |
41 healthy volunteers | 250 mL of red wine per day | 28 days | Consumption of red wine increased the global faecal microbial diversity | Barroso E., et al., 2017 |
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Pavlidou, E.; Mantzorou, M.; Fasoulas, A.; Tryfonos, C.; Petridis, D.; Giaginis, C. Wine: An Aspiring Agent in Promoting Longevity and Preventing Chronic Diseases. Diseases 2018, 6, 73. https://doi.org/10.3390/diseases6030073
Pavlidou E, Mantzorou M, Fasoulas A, Tryfonos C, Petridis D, Giaginis C. Wine: An Aspiring Agent in Promoting Longevity and Preventing Chronic Diseases. Diseases. 2018; 6(3):73. https://doi.org/10.3390/diseases6030073
Chicago/Turabian StylePavlidou, Eleni, Maria Mantzorou, Aristeidis Fasoulas, Christina Tryfonos, Dimitris Petridis, and Constantinos Giaginis. 2018. "Wine: An Aspiring Agent in Promoting Longevity and Preventing Chronic Diseases" Diseases 6, no. 3: 73. https://doi.org/10.3390/diseases6030073
APA StylePavlidou, E., Mantzorou, M., Fasoulas, A., Tryfonos, C., Petridis, D., & Giaginis, C. (2018). Wine: An Aspiring Agent in Promoting Longevity and Preventing Chronic Diseases. Diseases, 6(3), 73. https://doi.org/10.3390/diseases6030073