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Low serum concentrations of 25-hydroxyvitamin D in older persons and the risk of nursing home admission^1,2,3

¹ From the Institute of Health Sciences, Faculty of Earth and Life Sciences, Vrije University, Amsterdam, Netherlands (MV and JCS), and the Institute for Research in Extramural Medicine (MV, DJHD, MTEP, and PL) and the Department of Endocrinology (PL), Vrije University Medical Center, Amsterdam, Netherlands.

² Supported by the Dutch Ministry of Public Health, Welfare, and Sports.

³ Reprints not available. Address correspondence to M Visser, Faculty of Earth and Life Sciences, Institute of Health Sciences, Vrije University, De Boelelaan 1085, 1081 HV Amsterdam, Netherlands. E-mail: marjolein.visser{at}falw.vu.nl.

See corresponding editorial on page 471.

See corresponding CME exam on page 671.

	ABSTRACT

TOP ABSTRACT INTRODUCTION SUBJECTS AND METHODS RESULTS DISCUSSION REFERENCES

 
Background: The prevalence of vitamin D deficiency in nursing home patients is high.

Objective: We aimed to ascertain whether lower serum 25-hydroxyvitamin D [25(OH)D] concentrations increase the risk of future nursing home admission and early death.

Design: We included 1260 independent, community-dwelling persons aged 65 y who were participating in the Longitudinal Aging Study Amsterdam (1995–1996). Study outcomes were time to nursing home admission during 6 y of follow-up and time to death until 1 April 2003.

Results: Vitamin D deficiency [25(OH)D < 25 nmol/L] and insufficiency [25(OH)D = 25–49.9 nmol/L] were present in 127 (10.1%) and 462 (36.7%) subjects, respectively. During follow-up, 138 subjects (11.0%) were admitted to nursing homes, and 380 subjects (30.2%) died. The risk of nursing home admission for participants with 25(OH)D deficiency was 53 cases per 1000 person-years higher than that for those with high 25(OH)D (75 nmol/L) concentrations (58 compared with 5 cases). After adjustment for potential confounders, the hazard ratio (95% CI) of nursing home admission was 3.48 (1.39, 8.75) for vitamin D–deficient, 2.77 (1.17, 6.55) for vitamin D–insufficient, and 1.92 (0.79, 4.66) for vitamin D–borderline persons as compared with persons with high 25(OH)D (P for trend = 0.002). The results remained after additional adjustment for frailty indicators. Lower 25(OH)D was associated with higher mortality risk, but this association was not significant after adjustment for frailty indicators.

Conclusion: Lower serum 25(OH)D concentrations in older persons are associated with a greater risk of future nursing home admission and may be associated with mortality.

Key Words: Vitamin D deficiency • nursing home admission • mortality • nutrition • prospective study • elderly

	INTRODUCTION

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Vitamin D deficiency is common in older persons; it has a reported prevalence of 30% to 90%, depending on the definition used (1, 2). This frequency in older persons is partly due to their lower sunshine exposure and the reduced capacity of older skin to synthesize vitamin D₃ under the influence of ultraviolet light (3). A poor nutritional intake also contributes to a lower vitamin D status in older persons (4). The high prevalence of vitamin D deficiency in nursing home patients may thus be the consequence of their poor physical health and functioning. However, a reverse pathway could also be hypothesized.

It is well known that low 25-hydroxyvitamin D [25(OH)D] concentrations and low 1,25-hydroxyvitamin D [1,25(OH)D] concentrations accelerate bone loss with aging and increase the risk of falling (5) and, possibly, of fractures (1, 6, 7). Several cross-sectional studies have shown that low 25(OH)D is also related to lower muscle strength and poorer physical performance in older persons (8-11), and a prospective study by our group reported that low 25(OH)D concentrations in older men and women were associated with greater loss of muscle strength (12). Although not all intervention studies support these findings (13, 14), several intervention studies have shown improvements of muscle strength, body sway, fall risk, and physical performance after vitamin D supplementation in older persons (15-19).

The results of most of the studies referenced above suggest that low vitamin D concentrations may accelerate the age-related decline in physical health and functioning. We therefore hypothesized that low vitamin D concentrations increase the risk of nursing home admission. To our knowledge, this hypothesis has never been tested. Even among community-dwelling older persons, vitamin D deficiency is common (1, 2), which shows the dramatic effect of a potential association on chronic care of older persons. Thus, the aim of this prospective, population-based study was to investigate whether lower 25(OH)D concentrations increase the risk of nursing home admission and mortality in independent, community-dwelling older men and women.

	SUBJECTS AND METHODS

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Study participants
Data for this study were collected in the Longitudinal Aging Study Amsterdam (LASA), a prospective study of persons aged 55–85 y. The sampling and data collection procedures and the response rate were described in detail elsewhere (20). In summary, a random sample stratified by age, sex, and expected 5-y mortality was drawn from the population registers of 11 municipalities in 3 areas—the western, northeastern, and southern parts of the Netherlands. In total, 3107 subjects were enrolled in the baseline examination (1992–1993), and they were representative of the Dutch older population. Examinations, which were repeated after 3, 6, and 9 y of follow-up, consisted of general and medical interviews, conducted in each participant's home. The medical interviews were performed by trained nurses, and all interviews were recorded so that their quality could be monitored.

The sample for the current study comprised 1509 participants who participated in the medical interview at the first LASA follow-up (1995–1996) and who were born in or before 1930 (ie, were aged 65 y as of 1 January 1996). This follow-up examination was selected as the baseline of our study because of blood sample availability. We excluded participants who were not living independently at baseline (n = 88), who did not provide a blood sample or had no measurement of serum 25(OH)D (n = 153), or who had missing contact information during the 6-y follow-up (n = 8); these exclusions left a total of 1260 participants with complete data for the statistical analyses.

Compared with those who were included in the statistical analyses, those excluded (n = 249) were older, less educated, less physically active, and less likely to have a household partner; had poorer mobility performance, lower serum total cholesterol concentrations, poorer cognitive function, more depressive symptoms, and more diabetes mellitus, incontinence, and stroke; used less alcohol; and were more likely to smoke. Those excluded with available serum 25(OH)D concentrations (n = 60) had a lower median (interquartile range) concentration (28.3 nmol/L; 20.3–43.8 nmol/L) than did those included (51.8 nmol/L; 37.2–68.8 nmol/L; P < 0.0001). Finally, those excluded were more likely (59.4%) than were those included (30.2%) to die during follow-up.

Written informed consent was obtained from all participants. The study was approved by the Medical Ethics Committee of the Vrije University Medical Center.

Serum 25-hydroxyvitamin D
During an additional visit in a nearby hospital or health care center, fasting blood samples were obtained. The blood samples were collected in the morning and centrifuged at 1800 x g for 5 min at room temperature, and the serum samples were stored at –20° until hormone measurement in 1997–1998. Serum 25(OH)D was measured by using a competitive protein–binding assay (Nichols Diagnostics, San Juan Capistrano, CA). The lower limit of functional detection was 10 nmol/L, and the interassay CV was <15%. The analyses were carried out at the Endocrine Laboratory of the Vrije University Medical Center. To investigate the effect of storage at –20° on the 25(OH)D concentration, 25 serum samples were remeasured in 2004 by using a radioimmunoassay (DiaSorin SpA, Saluggia, Italy); the correlation between the 2 measurements was 0.94 (P Lips, unpublished observations, March 2006).

Serum 25(OH)D was categorized into 4 groups on the basis of published cutoffs: <25 nmol/L for deficiency, 25–49.9 nmol/L for insufficiency, 50–74.9 nmol/L for borderline status, and 75 nmol/L for normal status (ie, reference group) (1). Because the lowest serum 25(OH)D concentration that allows optimal skeletal health varies between 50 and 80 nmol/L (21), the category of 50–74.9 nmol/L was labeled as "borderline."

Nursing home admission
A nursing home was defined as a chronic care facility, mainly for older persons. In the Netherlands, admission to a nursing home is based on the level of care requested by a regional Center of Care Assessment, and expenses are covered by the Exceptional Medical Expenses Act (Dutch national insurance) so that long-term care is accessible for all citizens.

Time to nursing home admission was ascertained through the general interviews of the participant (69.2% of the study sample) or a proxy (3.0% of the study sample), information from the death certificate (24.4% of the study sample), and information obtained during the last study contact (3.3% of the study sample).

If the participant had moved to a nursing home, person-time (in this case, the time that elapsed during the study before a person moved to a nursing home) was set at the midpoint between the previous (pre-nursing home) interview and the next interview that took place after he or she went to the nursing home. For participants who died during follow-up, the last known residence, stated on the death certificate, was used to ascertain nursing home admission. If the deceased participant had moved to a nursing home before death, person-time was set at the midpoint between the last interview and the date of death. If the participant was contacted for a planned interview but refused or was physically or cognitively ineligible to participate further, information obtained from the participant (or a proxy) during this last study contact was used to assess nursing home admission. If the participant had moved to a nursing home, person-time was set at the midpoint between the last interview and the date of this final study contact. If no nursing home admission took place, person-time for each participant was calculated as the time between the date of the baseline interview (1995–1996) and the date of the follow-up interview 6 y later (2002–2003), the date of death, or the date of final study contact, whichever came first.

Mortality
Death certificates were traced through the registries of the municipalities in which the participants were living. Vital status ascertainment was 100% complete. All deaths that occurred between the baseline of our study (1995–1996) and 1 April 2003 were recorded. Survival time was calculated as the time between the date of the baseline interview and the date of death or 1 April 2003, whichever came first.

Potential confounders and effect modifiers
The following potential confounders measured at baseline were included in the statistical analyses: sex, age, education, household partner status (for nursing home admission outcome only), chronic diseases, the serum creatinine concentration, cognitive status, depressive symptoms, smoking status, alcohol consumption, body mass index, physical activity level, mobility performance, a low serum albumin concentration, and a low serum total cholesterol concentration. These confounders are known to be associated with 25(OH)D and the study outcomes nursing home admission, mortality, or both, and therefore they may confound the associations under study. Level of education was categorized as low (elementary school or less), moderate, and high (higher vocational school, college, or university). A household partner was defined as a person whom the participant considered as a partner (spouse or other person) and with whom the participant was living and sharing a household. Participants were asked (yes or no) whether they currently had or had had any of the following conditions: chronic obstructive pulmonary disease (ie, asthma, chronic bronchitis, or pulmonary emphysema), cardiac disease, peripheral atherosclerosis, stroke, diabetes mellitus, arthritis (ie, rheumatoid arthritis and osteoarthritis), cancer, and incontinence. The serum creatinine concentration (µmol/L) was used as an indicator of renal function, which is known to influence 25(OH)D concentrations (22).

A Dutch version of the Center for Epidemiologic Studies Depression (CES-D) scale, a 20-item self-report scale, was used to measure depressive symptoms; a score 16 points was used to identify clinically relevant depression (23, 24). Cognitive function was measured with the Mini-Mental State Examination; and a score <24 was used to identify poor cognitive function (25). Smoking (never, former, or current) and alcohol consumption (none, <7 drinks/wk, or 7 drinks/wk) were based on self-report. Measured body weight and height were used to calculate the body mass index (BMI; in kg/m²), which was categorized as <25, 25–29.9, or 30. Information on physical activity in the previous 2 wk was obtained by using a validated interviewer-administered questionnaire (26). The total time spent in walking outdoors, bicycling, heavy household activities, and sports activities was categorized as <30, 30–59, or 60 min/d. Mobility performance was objectively assessed by using a timed walking test and a repeated chair stands test. Those completing a test were assigned scores of 1 to 4, corresponding to the quartiles of time needed to complete the test; the fastest times were scored as 4 (27). Those who could not complete a test were assigned a score of 0. Mobility performance scores could range from 0 (unable to perform both tests) to 8 (performance time in the fastest quartile for both tests). Serum albumin concentrations (g/L) were measured by using the bromcresol purple method. Low serum albumin was defined as a concentration < 38 g/L (28). Serum total cholesterol concentrations (mmol/L) were measured by using an enzymatic colorimetry assay with a Hitachi 747 analyzer (Roche Diagnostics, Basel, Switzerland). Low serum cholesterol was defined as a concentration < 5.2 mmol/L (<200 mg/dL) (29).

Statistical analysis
All analyses were conducted by using SAS software (version 9.1.3; SAS Institute Inc, Cary, NC). Potential differences between 25(OH)D categories in continuous variables were tested by using linear regression analyses, and differences between those in categorical variables were tested by using the chi-square test. P values were based on 2-sided tests and were considered significant if P < 0.05. Kaplan-Meier curves were generated to investigate the associations of 25(OH)D categories with time to nursing home admission and mortality, which were tested by using the log-rank test. Cox proportional hazards analysis was used to investigate the association between 25(OH)D category (independent variable) and time to nursing home admission or time to death (dependent variables). In the first model, adjustment for age, sex, and education (and household partner status for nursing home admission outcome) was made. The second model added adjustment for chronic disease, serum creatinine concentrations, cognitive status, and depressive symptoms. The third model further added adjustment for lifestyle variables including smoking status, alcohol consumption, BMI, and physical activity level. Poor mobility performance, a low serum albumin concentration, and a low serum total cholesterol concentration are known indicators of frailty and have been associated with nursing home admission and mortality (27, 30, 31) and with lower vitamin D concentrations (8-10, 32). These indicators may confound the associations but may also act as potential mediators. Therefore, the frailty indicators were adjusted for in a separate, final model (model 4). Results are presented as hazard ratios (HRs) with 95% CIs. Because of the controversy regarding cutoffs for 25(OH)D categories, we also used the 25(OH)D concentration as a continuous variable and expressed the HRs per 1-SD increase in 25(OH)D. Log(-log) plots and time interaction terms were used to check the proportional hazards model assumption, which was not violated in any of the models. Potential sex and age group differences in the relation of serum 25(OH)D to nursing home admission and mortality were tested by using product terms in additional analyses.

	RESULTS

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Vitamin D deficiency and insufficiency were present in 127 (10.1%) and 462 (36.7%) persons, respectively (Table 1). Persons with lower 25(OH)D concentrations were more likely to be female, older, less educated, obese, physically inactive, and never smokers; more likely to abstain from alcohol; and less likely to live with a partner. They were also more likely to be incontinent and cognitively impaired or depressed, to report arthritis, and to have a lower serum creatinine concentration. Finally, they had a poorer performance on the mobility performance tests and were more likely to have low serum albumin and total cholesterol concentrations.

Figure 1

Table 2

View larger version (19K): [in this window] [in a new window]   FIGURE 1. Kaplan-Meier curves for nursing home admission according to categories of serum 25-hydroxyvitamin D [25(OH)D] concentration from the Longitudinal Aging Study Amsterdam.

Figure 2

Table 3

View larger version (20K): [in this window] [in a new window]   FIGURE 2. Kaplan-Meier curves for mortality according to categories of serum 25-hydroxyvitamin D [25(OH)D] concentration from the Longitudinal Aging Study Amsterdam.

	DISCUSSION

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An association between lower 25(OH)D concentrations and higher mortality risk was also observed. However, this association was no longer significant after adjustment for the frailty indicators. Because the frailty indicators may act as mediators of the association between lower 25(OH)D and mortality risk, adjustment for these indicators could be considered overadjustment.

The results are even more striking when considering the high prevalence (46.7%) of vitamin D deficiency and insufficiency in our sample of independently living men and women, which is comparable to that reported in other studies (33, 34). This high prevalence and the results of our study could indicate that poor vitamin D status may have a large effect on nursing home admission in the general population and may lead to additional health care costs.

The higher risk of nursing home admission in those with deficient and insufficient 25(OH)D concentrations may be explained by their greater risk of sarcopenia and falls (5, 12). Vitamin D concentrations have also been associated with physical performance in cross-sectional and intervention studies (8-11, 15-19). The only available prospective study reported no greater risk of new disability in disabled women with low vitamin D concentration than in those with higher vitamin D concentrations (35), although selection bias may have caused this result (36). The greater risk of nursing home admission may also be explained by the higher risk of osteoporosis, and possibly fracture, which subsequently leads to a decline in functional status, an increase in pain, and an impaired quality of life (37-39). More recently, low vitamin D concentrations have been associated with obesity, diabetes, and cardiovascular disease (40-43). These associations offer an additional explanation for the association between lower vitamin D concentrations and nursing home admission, because these diseases increase the risk of functional limitation, disability, and cognitive impairment in old age (44-47). Finally, we cannot exclude that low vitamin D concentration may act as a marker for something else related to nursing home admission. Future studies are needed to elucidate the pathways through which vitamin D deficiency may increase the risk of nursing home admission.

It is known that vitamin D supplementation in older persons increases 25(OH)D and 1,25-hydroxyvitamin D concentrations (48, 49), and supplementation could be appropriate in settings of nutritional adequacy and frailty. However, spending more time outdoors will also improve vitamin D status (50, 51). The latter option seems preferable for older persons when it is combined with physical activity, because physical activity will increase muscle strength, slow down bone loss, and lower the risks of falls, of a decline in functional performance, and of disability with aging (52-54). Regular outdoor walking has already been shown to reduce the risk of mobility decline (54, 55). Furthermore, beneficial effects of physical activity on cognitive functioning and chronic disease in older persons have been reported (56, 57).

Some of the weaknesses of the current study should be discussed. No exact date of nursing home admission was available in the study. Almost 70% of the information on nursing home admission was obtained directly from the participant at 3-y intervals. When a participant was reported to have moved to a nursing home, the date of admission was conservatively set at the midpoint of 2 follow-up examinations, in imitation of other studies (58). This nondifferential bias may have resulted in an underestimation of the reported associations and less precise estimates. Another weakness is that those excluded from the study had a poorer health status, had more frailty indicators, had lower serum vitamin D concentrations, and were more likely to die during follow-up than were those included in the study. This selection bias may also have contributed to an underestimation of the reported associations. Finally, our results may not be generalizable to other countries because of differences in the health care systems in various countries.

In conclusion, lower serum 25(OH)D concentrations in older men and women are associated with a greater risk of future nursing home admission and may be associated with a greater mortality risk. These results could indicate that lower vitamin D concentrations may specifically affect the level of independence in old age.

	ACKNOWLEDGMENTS

 
MV, DJHD, and PL contributed to the study design. MV was responsible for the statistical analysis of the data and for drafting the manuscript. All authors were responsible for critical revision of the manuscript. PL has received funds for research, fees for consulting, or both from Nycomed, Lilly, MSD, Wyeth, Servier, Aventis, and Procter & Gamble. None of the other authors had a personal or financial conflict of interest.

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