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Alcohol consumption and bone mineral density in elderly women

Published online by Cambridge University Press:  17 July 2012

Isolde Sommer*
Affiliation:
Institute of Public Health and Clinical Nutrition, University of Eastern Finland, Kuopio, Finland
Arja T Erkkilä
Affiliation:
Institute of Public Health and Clinical Nutrition, University of Eastern Finland, Kuopio, Finland
Ritva Järvinen
Affiliation:
Institute of Public Health and Clinical Nutrition, University of Eastern Finland, Kuopio, Finland
Jaakko Mursu
Affiliation:
Institute of Public Health and Clinical Nutrition, University of Eastern Finland, Kuopio, Finland
Joonas Sirola
Affiliation:
Bone and Cartilage Research Unit, Clinical Research Center, University of Eastern Finland, Kuopio, Finland Departments of Orthopedics and Traumatology and Handsurgery, Kuopio University Hospital, Kuopio, Finland
Jukka S Jurvelin
Affiliation:
Department of Clinical Physiology, Nuclear Medicine, Kuopio University Hospital, Kuopio, Finland Department of Applied Physics, University of Eastern Finland, Kuopio, Finland
Heikki Kröger
Affiliation:
Bone and Cartilage Research Unit, Clinical Research Center, University of Eastern Finland, Kuopio, Finland Departments of Orthopedics and Traumatology and Handsurgery, Kuopio University Hospital, Kuopio, Finland
Marjo Tuppurainen
Affiliation:
Bone and Cartilage Research Unit, Clinical Research Center, University of Eastern Finland, Kuopio, Finland Department of Obstetrics and Gynecology, Kuopio University Hospital, Kuopio, Finland
*
*Corresponding author: Email [email protected]
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Abstract

Objective

Findings regarding alcohol consumption and bone mineral density (BMD) in elderly women have been inconsistent. The objective of the present study was to explore the association of alcohol intake with BMD in elderly women.

Design

This cohort study included women from the population-based Kuopio Osteoporosis Risk Factor and Prevention – Fracture Prevention Study (OSTPRE-FPS). Alcohol intake and potential confounders were assessed at baseline and after 3 years of follow-up using a lifestyle questionnaire. In addition, an FFQ was distributed in the third year to measure dietary intake, including alcohol. Women underwent BMD measurements at the femoral neck and lumbar spine at baseline and after 3 years of follow-up.

Setting

Kuopio Province, Finland.

Subjects

Three hundred elderly women (mean age 67·8 years) who provided both BMD measurements and FFQ data.

Results

Alcohol consumption estimated from the FFQ and lifestyle questionnaire was significantly associated with BMD at both measurement sites after adjustment for potential confounders, including lifestyle and dietary factors (P < 0·05). Using the FFQ, women drinking >3 alcoholic drinks/week had significantly higher BMD than abstainers, 12·0 % at the femoral neck and 9·2 % at the lumbar spine. Results based on the lifestyle questionnaire showed higher BMD values for all alcohol-consuming women at the femoral neck and for women drinking 1–3 alcoholic beverages/week at the lumbar spine, compared with non-users.

Conclusions

The results from OSTPRE-FPS suggest that low to moderate alcohol intake may exert protective effects on bone health in elderly women.

Type
Nutrition and health
Copyright
Copyright © The Authors 2012

Osteoporosis and related fractures have major consequences for the health of elderly women worldwide. Low bone mineral density (BMD) has been shown to be a strong predictor of an enhanced fracture risk(Reference Johnell, Kanis and Oden1, Reference Cauley, Hochberg and Lui2). In addition to unmodifiable risk factors such as age and sex, several nutritional and lifestyle factors including low Ca intake and low physical activity are recognized as important risk factors for the development of osteoporosis(Reference Kröger, Tuppurainen and Honkanen3). Alcohol intake as a potential contributing factor to osteoporosis and osteoporotic fractures was first described in 1965(Reference Saville4). Since then, the negative impact of chronic heavy alcohol consumption on bone health has been recognized(Reference Peris, Parés and Guañabenes5). Long-term alcohol use has been shown to exert direct and indirect effects on bone turnover and remodelling, leading to decreased BMD and increased risk of fractures(Reference Sampson6). Alcohol may directly worsen bone health by impairing proliferation and function of osteoblasts(Reference Klein7), causing malabsorption, increased renal excretion and disruption of Ca-regulating hormones such as parathyroid hormone, calcitonin and vitamin D metabolites. Also, insufficient dietary intake related to alcohol may indirectly interfere with bone homeostasis(Reference Sampson8, Reference Turner9). In contrast to these harmful effects of alcohol abuse, several studies have reported that moderate alcohol use may decrease fracture rates and increase bone density, mostly in postmenopausal women(Reference Angus, Sambrook and Pocock10Reference Tucker, Jugdaohsingh and Powell23). However, others showed no significant association between alcohol intake and BMD(Reference Stevenson, Lees and Devenport24Reference Tivis and Tivis28), and one reported a negative relationship between BMD at the lumbar spine and lifetime beer consumption(Reference Grainge, Coupland and Cliffe29).

As with CVD, the relationship between alcohol intake and bone health may be U-shaped(Reference Klatsky30). Moderate alcohol consumption has been suggested to increase oestrogen levels in postmenopausal women and subsequently prevent the development of osteoporosis. Studies, especially more recent ones(Reference Onland-Moret, Peeters and van der Schouw31, Reference Gavaler32), have suggested that moderate alcohol intake may be associated with increased oestrogen levels in postmenopausal women. However, the findings regarding the effect of alcohol intake on BMD in elderly women are inconclusive and more studies with extensive adjustments for potential confounders are needed. To continue this line of investigation, the present study examined the association between alcohol intake and BMD at the lumbar spine and proximal femur in a subsample of the Kuopio Osteoporosis Risk Factor and Prevention Study (OSTPRE) population.

Materials and methods

Study design and participants

The present study was based on the Kuopio Osteoporosis Risk Factor and Prevention – Fracture Prevention Study (OSTPRE-FPS) which began in 2003 in Kuopio, Finland(Reference Kärkkäinen, Tuppurainen and Salovaara33). The primary aim of the study was to determine whether vitamin D and Ca supplementation would prevent bone loss in postmenopausal women in a non-placebo-controlled, parallel-group trial. The ethics committee of Kuopio University Hospital approved the OSTPRE-FPS in October 2001. The trial was registered at Clinictrials.gov under identifier NCT00592917 (registration date: 2 January 2008). Written informed consent was obtained from the study participants at baseline enquiry. The OSTPRE-FPS population (n 5407) was selected from the population-based OSTPRE cohort of 13 100 peri- and postmenopausal women born in 1932–1941(Reference Honkanen, Alhava and Saarikoski34). The inclusion criteria for OSTPRE-FPS were: being a minimum of 65 years of age at the end of November 2002; living in Kuopio Province at the onset of the trial; and not having been included in the OSTPRE sample in which BMD measurements were conducted. Willingness to participate in a vitamin D and Ca supplementation trial was enquired via mail. A response rate of 63·5 % led to a study population of 3432 women, which was randomized into two groups of equal size. From this study population, a subsample of 750 women was randomly selected to take part in a clinical trial. Of these, a total of 606 participants started the trial.

The baseline measurements took place between February 2003 and May 2004 and the follow-up measurements between January 2006 and May 2007 (mean follow-up time 2·8 (sd 0·4) years). In both examinations, lifestyle, health status and use of drugs were assessed using questionnaires, and BMD measurements were undertaken. The supplementation group received daily cholecalciferol 20 μg (800 IU)+Ca 1000 mg via prescription, while the control group received neither supplementation nor placebo. A total of 593 participants completed the study. Of them, 544 women underwent BMD measurements at the femoral neck and 480 women at the lumbar spine. Additionally, an FFQ was distributed at the follow-up examination. However, not all women were willing to complete the FFQ. This left a total of 341 women who underwent both baseline and 3-year BMD measurements and returned the FFQ. Thereof, fifteen women were excluded because of implausible energy intake (>14644 kJ (>3500 kcal)) and twenty-six were excluded due to incomplete data, leaving 300 women to be included in the final analysis (Fig. 1).

Fig. 1 Flowchart of the subsample of the Kuopio Osteoporosis Risk Factor and Prevention – Fracture Prevention Study (OSTPRE-FPS) trial (BMD, bone mineral density)

Questionnaires

The OSTPRE-FPS questionnaire (lifestyle questionnaire) was used to collect information on lifestyle, health status and medications at baseline and alcohol consumption at baseline and follow-up. Although it has not been validated to measure alcohol consumption, it was successfully used to demonstrate the association between alcohol intake and spinal BMD in an earlier study(Reference Kröger, Tuppurainen and Honkanen3). In the lifestyle questionnaire, participants were asked questions about age, current and past hormone therapy (HT), current smoking status, mobility, diseases and medications, and use of non-prescribed Ca and/or vitamin D supplements. Non-prescribed Ca and/or vitamin D supplements included those available over the counter, which were consumed in addition to the prescribed Ca and vitamin D intervention of the trial. The mean duration of HT use in years (10·9 years) was substituted for fifty participants who reported that they had used HT but did not remember its exact duration. Criteria for restricted mobility were: (i) not able to walk more than 1 km; (ii) not able to walk more than 100m; (iii) only able to move indoors; and (iv) immobile. To assess alcohol consumption, participants were asked to quantify their intake of beer/cider (bottles), wine (glasses) or spirits/strong alcohol (portions) during the last 4 weeks. A ‘drink’ referred to a bottle of beer/cider, a glass of wine or one portion of spirits/strong alcohol. In Finland, the average portion size for a bottle of beer/cider is 330 ml, for a glass of wine is 120 ml and for a shot of spirits/strong alcohol 40 ml.

The FFQ assessed the usual dietary intake at follow-up. Participants were asked to report their usual consumption of beer/cider (1 bottle = 330 ml), red or white wine (120 ml) or spirits (40 ml) by selecting one of nine frequency categories: ‘never or very seldom’, ‘1–3 times per month’, ‘once per week’, ‘2–4 times per week’, ‘5–6 times per week’, ‘once per day’, ‘2–3 times per day’, ‘4–5 times per day’ or ‘more than 5 times per day’. For analysis, average alcohol intakes per week were calculated. Total dietary intakes of energy, protein, K, Ca and vitamin D, out of all questioned food items, were computed. These are considered potential confounders and were therefore used as covariates in the statistical models. The FFQ was validated with food records for energy and nutrient intakes, and agreement between the two measurement tools was moderate(Reference Erkkilä, Järvinen and Karvonen35).

Anthropometric measurements

Weight of the participant was measured with a digital calibrated scale (Philips, type HF 351/00) and height with a calibrated wall meter during the baseline research visit. BMI (kg/m2) was computed by dividing the weight (in kilograms) by the square of height (in metres).

Measurements of bone mineral density

BMD measurements were performed at the lumbar spine (L2–L4) and left femoral neck with dual-energy X-ray absorptiometry (DXA; Lunar DPX, Madison, WI, USA) at baseline and year 3 examinations. The quality control of the DXA measurements was run daily. The in vitro long-term reproducibility (CV) for the total femur region was 0·3 %. Measurements were carried out by following the guidelines of the instrument's manufacturer. The technical quality of each DXA measurement and analysis was carefully checked and those with measurement errors were not included in the statistical analyses(Reference Kärkkäinen, Rikkonen and Kröger36).

Statistical analyses

Average alcohol consumption derived from the lifestyle questionnaires or the FFQ was divided into four categories: no use; <1 drink/week; 1–3 drinks/week; and >3 drinks/week. These cut-offs produced categories with sufficient numbers of participants to be able to generate more stable estimates. Since the number of participants in the highest category was relatively small, more detailed analysis to detect potential differences between moderate v. heavy drinkers was not possible due to limited statistical power. Associations between alcohol intake and other variables potentially affecting BMD were analysed using one-way ANOVA for continuous variables and the χ 2 test for categorical variables. These potential confounders were identified through literature review. Linear mixed-effects modelling was used to examine the relationship between alcohol consumption (added as the mean of two measurement time points using the lifestyle questionnaire, or added as one measurement time point at year 3 using the FFQ) and BMD changes over time (added as a time-varying covariate with two measurement time points). No significant changes in alcohol consumption were found and therefore alcohol was entered into the model as the mean of baseline and follow-up. The possibility of an interaction between alcohol intake and the effect of the vitamin D and Ca intervention (study group) on BMD was also tested using the likelihood ratio test, and showed no significance. Therefore, results are presented for all women.

Models were run unadjusted in the first step (accounting for study group only; Model 1); then run adjusted for confounding factors assessed at baseline including age (years), BMI (kg/m2), whether a current smoker (yes/no), HT use current or past (yes/no), duration of HT use (years), use of non-prescribed Ca and vitamin D supplement in addition to intervention (yes/no), study group (intervention/control), restricted mobility (yes/no), disease or medication decreasing BMD (yes/no; Model 2); and finally dietary factors including total energy intake (kJ/d), dietary protein intake (g/d), dietary K intake (mg/d), dietary Ca intake (mg/d) and dietary vitamin D (μg/d) were added to the list of covariates (Model 3). The diseases potentially affecting bone metabolism included hyperthyroidism, disease of the parathyroid gland, chronic liver disease, chronic intestinal disease, coeliac disease, ventricle operation, chronic nephropathy, arthritis, osteoporosis and lactose intolerance. Medications affecting bone metabolism included loop-diuretics, insulin, anti-epileptics, glucocorticoids and cancer chemotherapy. Results are shown as estimated marginal means. Analyses were conducted separately for alcohol consumption from the lifestyle questionnaire and for alcohol consumption from the FFQ. Statistical analyses were carried out with the statistical software packages SPSS for Windows version 15·0 (SPSS Inc.) and STATA version 9·0 (StataCorp). The level of significance was set at 0·05.

Results

Generally, alcohol consumption among the elderly women was low. The majority of the women were non-drinkers (lifestyle questionnaire (n 118), 39·9 %; FFQ (n 169), 56·3 %) or consumed <1 drink/week (lifestyle questionnaire (n 103), 34·8 %; FFQ (n 69), 23·0 %). A total of 18·9 % of women based on the lifestyle questionnaire (n 56) and 11·0 % of women based on the FFQ (n 33) reported intake of 1–3 drinks/week. Only a very few participants consumed >3 drinks/week (lifestyle questionnaire (n 19), 6·4 %; FFQ (n 29), 9·7 %).

Mean alcohol intake measured by the lifestyle questionnaire at baseline and follow-up was 0·82 drinks/week, which was slightly lower than the mean alcohol intake that was obtained from the FFQ (0·93 drinks/week) at the follow-up measurement (Table 1). The mean BMD at the lumbar spine was increased at follow-up (1·097 g/cm3) compared with baseline (1·087 g/cm3). About half of the women (54·5 %) currently used or had used HT at some time in their life. Only 4·8 % of the women were current smokers.

Table 1 Characteristics of the study participants: elderly Finnish women (n 300), Kuopio Osteoporosis Risk Factor and Prevention – Fracture Prevention Study (OSTPRE-FPS)

HT, hormone therapy; BMD, bone mineral density.

According to their alcohol consumption categories assessed through the lifestyle questionnaire at baseline and follow-up, women in the higher categories of alcohol intake were more likely to be smokers (Table 2).

Table 2 Characteristics of the study participants according to alcohol intake assessed using the lifestyle questionnaire: elderly Finnish women (n 300), Kuopio Osteoporosis Risk Factor and Prevention – Fracture Prevention Study (OSTPRE-FPS)

HT, hormone therapy; BMD, bone mineral density.

*The difference between categorical variables was analysed using the χ 2 test, and that between continuous variables using ANOVA.

Alcohol use was significantly associated with BMD (Tables 3 and 4). Using the FFQ, women in the highest category of alcohol intake had significantly higher BMD than non-consumers at both measurement sites (Table 3). At the femoral neck, the P value for the unadjusted model was 0·020 (Model 1). The strongest association between alcohol intake and BMD was observed after adjustment for both lifestyle and dietary factors (P = 0·014). In this model, women consuming >3 alcoholic drinks/week had 12·0 % higher BMD values than abstainers (Model 3). Similar results were found for the lumbar spine, where the association between alcohol intake and BMD was strongest in the unadjusted model (P = 0·002; Model 1). After adjustment for lifestyle and dietary factors, women in the highest category of alcohol intake had 9·2 % higher BMD compared with non-users (P = 0·006; Model 3).

Table 3 Estimated marginal means derived from the linear mixed model predicting BMD change over time by category of alcohol intake assessed using the FFQ at follow-up: elderly Finnish women (n 300), Kuopio Osteoporosis Risk Factor and Prevention – Fracture Prevention Study (OSTPRE-FPS)

BMD, bone mineral density; HT, hormone therapy.

*Adjusted for study group (intervention v. control).

†Adjusted for age, BMI, HT use, duration of HT use, current smoking, use of Ca and vitamin D supplements, restricted mobility, disease or medication decreasing BMD, study group (intervention v. control).

‡Adjusted for age, BMI, HT use, duration of HT use, current smoking, use of Ca and vitamin D supplements, restricted mobility, disease or medication decreasing BMD, study group (intervention v. control), energy intake, dietary protein, dietary Ca, dietary vitamin D, dietary K.

§The difference between category no use v. other categories is statistically significant at the 0·05 level.

Table 4 Estimated marginal means derived from the linear mixed model predicting BMD change over time by category of alcohol intake assessed using the lifestyle questionnaire at baseline and follow-up (mean): elderly Finnish women (n 300), Kuopio Osteoporosis Risk Factor and Prevention – Fracture Prevention Study (OSTPRE-FPS)

HT, hormone therapy; BMD, bone mineral density.

*Adjusted for study group (intervention v. control).

†Adjusted for age, BMI, HT use, duration of HT use, current smoking, use of Ca and vitamin D supplements, restricted mobility, disease or medication decreasing BMD, study group (intervention v. control).

‡Adjusted for age, BMI, HT use, duration of HT use, current smoking, use of Ca and vitamin D supplements, restricted mobility, disease or medication decreasing BMD, study group (intervention v. control), energy intake, dietary protein, dietary Ca, dietary vitamin D, dietary K.

§The difference between category no use v. other categories is statistically significant at the 0·05 level.

Using the lifestyle questionnaire to assess alcohol intake, significant associations between alcohol intake and BMD at both bone sites were found in unadjusted and adjusted models (Table 4). At the femoral neck, the P value in the unadjusted model was 0·008 (Model 1). Women who consumed any amount of alcohol (from <1 to >3 drinks/week) had significantly higher BMD than women who abstained from alcohol after adjustment for lifestyle and dietary factors (Model 3). Women drinking >3 alcoholic drinks/week had 7·7 % higher BMD than non-drinkers after adjustment for both lifestyle and dietary factors (P = 0·025; Model 3). Analysis at the lumbar spine showed that women consuming 1–3 and >3 alcoholic drinks/week had significantly higher BMD than non-drinkers in the unadjusted model (P = 0·008 and P = 0·039, respectively; Model 1). After adjustment for lifestyle and dietary factors, only women drinking 1–3 alcoholic drinks/week had significantly higher BMD (6·4 %) than abstainers (P = 0·019; Model 3).

Discussion

The findings of the present study suggest that low alcohol consumption may be beneficially related to bone health in elderly women. Depending on the alcohol assessment method, alcohol consumption of >3 drinks/week (FFQ) or 1–3 and >3 drinks/week (lifestyle questionnaire) was positively associated with BMD at the femoral neck and lumbar spine. All associations between alcohol use and BMD at both measurement sites remained significant after adjustment for lifestyle and dietary factors (Model 3). Depending on measurement site, dietary factors, including total energy intake and dietary intakes of protein, Ca, vitamin D and K, strengthened or attenuated the association between alcohol and BMD. The latter have been identified as the most evident dietary factors affecting BMD in the literature(Reference Darling, Millward and Torgerson37Reference Zhu, Devine and Prentice41) and were therefore added to the analysis. These findings suggest that low alcohol consumption has an independent effect on BMD. However, other dietary issues and many other factors contribute to bone health.

Although earlier observations suggested a potential protective effect of moderate alcohol consumption on BMD at the femoral neck and/or lumbar spine in postmenopausal women(Reference Angus, Sambrook and Pocock10Reference Holbrook and Barrett-Connor12, Reference Felson, Zhang and Hannan14Reference Feskanich, Willet and Stampfer16, Reference Rapuri, Gallagher and Balhorn18, Reference Wosje and Kalkwarf20Reference Tucker, Jugdaohsingh and Powell23), highest BMD values were mostly found in women who consumed at least one drink daily. Among a group of peri- and postmenopausal women, alcohol consumption (mean intake of consumers was 125 g/week) was a positive predictor for spine BMD(Reference Kröger, Tuppurainen and Honkanen3). The women participating in the present study consumed at most 1–3 drinks/week or >3 drinks/week, respectively, which corresponds to weekly alcohol intake of 10–30 g or more. Laitinen et al.(Reference Laitinen, Välimäki and Keto11) and Rapuri et al.(Reference Rapuri, Gallagher and Balhorn18) have previously reported a beneficial effect of low alcohol consumption on BMD. Laitinen et al.(Reference Laitinen, Välimäki and Keto11) found higher BMD for postmenopausal women consuming 11–77 g alcohol/week than for abstainers at all measurement sites (femoral neck, Ward's triangle, trochanter and lumbar spine). Similar results were found in the study conducted by Rapuri et al.(Reference Rapuri, Gallagher and Balhorn18) where women with an alcohol consumption of 28·7–57·2 g/week had the highest lumbar spine, total body and mid-radius BMD compared with non-users. Therefore, alcohol consumption may already be beneficial for bone health at lower doses than previously assumed.

The average alcohol consumption of elderly women in the present study, 0·8–0·9 drinks/week, was relatively low, but comparable to previous estimates found for Finnish elderly(Reference Halme, Seppä and Alho42). Using an FFQ to measure alcohol intake, 37·7 % of women aged 65–69 years reported to abstain from alcohol and 35·3 % reported to consume less than one alcoholic drink per week(Reference Halme, Seppä and Alho42). The present study found 39·3 % of elderly women to abstain from alcohol when using the lifestyle questionnaire and 56·3 % when using the FFQ data. Likewise, 34·8 % (lifestyle questionnaire) and 23·0 % (FFQ) of elderly women consumed less than one alcoholic drink weekly in the present study. It has recently been reported(Reference MacDonald43) that under-reporting of alcohol consumption most likely occurs when data are collected from an FFQ. Additionally, drinking behaviour and beliefs about alcohol differ between cultures and age groups. Studies assessing alcohol use among the elderly (>74 years) in Finland found that alcohol use was less likely to be under-reported if it was in the context of medicinal use(Reference Aira, Hartikainen and Sulkava44). We cannot rule out the possibility that some women may have been misclassified and if so, the association between alcohol intake and BMD would be underestimated.

In line with the findings from the original OSTPRE-FPS trial(Reference Kärkkäinen, Tuppurainen and Salovaara33) where BMD measurements at the lumbar spine had increased after 3 years irrespective of the intervention, results at the lumbar spine were also higher at the follow-up assessment in the present study. This observation has been made in earlier studies(Reference Jones, Nguyen and Sambrook45, Reference Greenspan, Maitland and Myers46) and could be explained by age-related degenerative changes, such as osteoarthritis, that have been shown to confound DXA measurements(Reference Muraki, Yamamoto and Ishibashi47). Since our analysis was adjusted for current and past HT use, duration of HT use and medications affecting BMD, we can rule out the potential impact of these on the BMD increase.

As reported in previous studies(Reference Holbrook and Barrett-Connor12, Reference Felson, Zhang and Hannan14, Reference Rapuri, Gallagher and Balhorn18, Reference Williams, Cherkas and Spector19, Reference Mukamal, Robbins and Cauley21, Reference Hansen, Overgaard and Riis25) smoking and drinking habits tend to be strongly associated. Although the percentage of smokers in the current study population was low (4·8 %), the proportion of smokers was higher among those consuming 1–3 or >3 alcoholic drinks/week than among non-drinkers (12·7 % or 10·5 % v. 2·6 %). Additionally, low body weight or low BMI, which are strong predictors of osteoporotic fractures(Reference Ricci, Hdeymsfield and Pierson48), frequently occur in alcohol-drinking elderly women(Reference Holbrook and Barrett-Connor12, Reference Felson, Zhang and Hannan14, Reference Feskanich, Willet and Stampfer16, Reference Rapuri, Gallagher and Balhorn18, Reference Wosje and Kalkwarf20, Reference Mukamal, Robbins and Cauley21, Reference Hansen, Overgaard and Riis25). However, in our sample there were no statistically significant differences in BMI across the categories of alcohol intake. There seemed to be an association between HT use and alcohol consumption in our study. A total of 73·7 % women in the highest category of alcohol intake currently used or had used HT for some time during their life.

Mobility is another factor with positive impact on BMD. All elderly women consuming >3 drinks/week had normal mobility, whereas 9·6 % of the abstaining women had restricted mobility. Higher physical activity among alcohol-consuming women was reported by Ganry et al.(Reference Ganry, Baudoin and Fardellone17) and Mukamal et al.(Reference Mukamal, Robbins and Cauley21). Alcohol-drinking women participating in the study conducted by Felson et al.(Reference Felson, Zhang and Hannan14) were exercising less than non-drinking women. Based on the findings from this and previous studies, elderly women who drink alcohol seem to have a certain lifestyle pattern. They are more likely to smoke and exercise, have lower BMI and are more likely to use HT than alcohol-abstaining elderly women.

The present study sought to investigate the impact of alcohol consumption on BMD at the femoral neck and lumbar spine in a homogeneous study population. There was repeated longitudinal information on alcohol consumption using the lifestyle questionnaire and BMD measurements, and the analytical approach selected allowed the correlation between repeated BMD measurements on the same participants to be taken into account. Strengths of the study also include the ability to control for well-established confounders, including lifestyle factors and dietary factors. However, limitations of our study are also recognized. Although data on alcohol consumption using the lifestyle questionnaire were collected from baseline and 3-year follow-up, the FFQ was distributed only at the follow-up examination. One of the drawbacks was also the relatively small sample size. Since data on dietary intake were available from only about half the women initially enrolled in the trial, we cannot rule out the possibility of attrition bias. However, the women participating in the study showed no differences in terms of main characteristics (age, BMI, HT use, duration of HT use and smoking) compared with those who did not participate. The proportions of women with restricted mobility (9·3 %), non-prescribed use of Ca and vitamin D supplements (18·5 %) and disease or medication decreasing BMD (41·6 %) were higher in non-participating women. The study was part of a non-placebo-controlled, parallel-group trial, where half of the sample received vitamin D and Ca supplementation. To rule out the possibility of an independent effect between alcohol intake and the Ca and vitamin D intervention (study group) on BMD, its interaction was tested prior to analysis and showed no significance. Additionally, the study group was added as a covariate to all models of analysis.

Ideally, the effect of alcohol consumption on BMD needs to be studied over a long period of time. The follow-up period of our study was 3 years, and therefore cannot fully address this issue. Another limitation was the fact that physical activity was not directly measured. However we did assess mobility, which reflects the ability to perform physical exercise. Also, the possibility of other unmeasured confounding factors cannot be ruled out.

Conclusion

The results from the OSTPRE-FPS cohort suggest that low alcohol intake may exert protective effects on bone health in elderly women. Further studies are needed to confirm these findings.

Acknowledgements

The OSTPRE-FPS was supported by the Finnish Cultural Foundation (Hulda Tossavainen Foundation), the Sigrid Juselius Foundation, the Academy of Finland and a Kuopio University Hospital EVO grant. The authors declare that they have no conflicts of interest. I.S. conducted data analysis, data interpretation and the writing of the first manuscript draft. A.T.E. and R.J. were responsible for the FFQ data and contributed to data interpretation. J.M. contributed to the data interpretation. J.S. performed BMD measurements. H.K., J.S.J. and M.T.T. were responsible for the original OSTPRE-FPS study design. All of the authors contributed to revising the manuscript and approved the final version. The authors thank Ms Seija Oinonen for technical support.

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Figure 0

Fig. 1 Flowchart of the subsample of the Kuopio Osteoporosis Risk Factor and Prevention – Fracture Prevention Study (OSTPRE-FPS) trial (BMD, bone mineral density)

Figure 1

Table 1 Characteristics of the study participants: elderly Finnish women (n 300), Kuopio Osteoporosis Risk Factor and Prevention – Fracture Prevention Study (OSTPRE-FPS)

Figure 2

Table 2 Characteristics of the study participants according to alcohol intake assessed using the lifestyle questionnaire: elderly Finnish women (n 300), Kuopio Osteoporosis Risk Factor and Prevention – Fracture Prevention Study (OSTPRE-FPS)

Figure 3

Table 3 Estimated marginal means derived from the linear mixed model predicting BMD change over time by category of alcohol intake assessed using the FFQ at follow-up: elderly Finnish women (n 300), Kuopio Osteoporosis Risk Factor and Prevention – Fracture Prevention Study (OSTPRE-FPS)

Figure 4

Table 4 Estimated marginal means derived from the linear mixed model predicting BMD change over time by category of alcohol intake assessed using the lifestyle questionnaire at baseline and follow-up (mean): elderly Finnish women (n 300), Kuopio Osteoporosis Risk Factor and Prevention – Fracture Prevention Study (OSTPRE-FPS)