Vitamin D status in chronic dialysis patients with depression: a prospective study

Depression ranks fourth on the World Health Organization (WHO) global disease burden list. Depression is the most widely acknowledged psychological problem among end-stage renal disease (ESRD) patients [1, 2]. About 28% of chronic kidney disease patients facing impending dialysis undergo major depression, and even a larger proportion of dialyzed patients suffer from depression [3]. Inflammation in the body is a common manifestation to many diseases, including high blood pressure, coronary artery disease, diabetes as well as chronic kidney disease [4, 5]. Recently, many authors have tried to reveal the connection between depression and inflammatory status in ESRD patients [6, 7]. Depression is also linked to an inflammation marker in blood called C-reactive protein (CRP). Proinflammatory cytokines were proven very important in the pathogenesis of depression in the general population and the levels of the same cytokines elevated in ESRD patients [8]. However, repeated episodes of depression contribute to inflammation in the body, which highlights a potentially important role for untreated depression as a contributor to a series of serious medical problems [9]. The causality between depression and inflammation is still unclear.

Vitamin D (VD) is an essential nutrient for bone health, and has other physiological functions. There are plausible reasons for investigating the curative effects of VD for depressive disorders. Depression may be associated with VD deficiency [10‐12]. Hypovitaminosis D and secondary hyperparathyroidism commonly occur in the dialyzed population for several reasons [13, 14]. Therefore, Calcitriol supplementation is popular among dialyzed patients. However, spontaneous 25(OH)D levels > 20 ng/mL seem sufficient to control serum intact parathyroid hormone (iPTH) in chronic kidney disease (CKD) patients [15]. These findings reinforce the guidelines to supplement VD only if less than 30 ng/mL. In China, Calcitriol is used as a form of VD to treat hypovitaminosis D and secondary hyperparathyroidism in patients whose kidneys or parathyroid glands are not working normally.

However, it is unknown whether serum VD content is associated with depression in the dialyzed population and whether calcitriol supplementation is efficient for treatment of depression. The intentions of this study were to (a) investigate the prospective association between HsCRP, VD contents and depressive symptoms in the dialyzed population, and (b) find the efficacy of calcitriol supplementation on depression in dialyzed patients.

This prospective study provided a comprehensive and detailed description of the incidence of depression and the effect of calcitriol supplementation on treatment of depression in dialyzed patients. The overall incidence of depression was (44%, 95% CI: −0.137-0.027) in the dialyzed patients, which was consistent with previous reports [30‐32]. The high occurrence of depression may be partly due to anemia and poor nutritional status in the dialyzed population [33]. Moreover, employment status, health insurance mode, marital status, and constipation status can all affect the incidence of depression. In our study, anemia (hemoglobin level) and nutritional status (albumin) were also evaluated, and there was difference in mean hemoglobin level, but not in mean albumin level. Thus, we thought depression for dialysis patients was multifactorial apart from poor nutritional status.

The depressive patients have higher serum HsCRP level than the non- depressive patients, and thus CRP may be as a new risk factor of depression in the dialyzed population. Also HsCRP level can be used to predict the outcome in HD patients. After one-year follow up, calcitriol supplementation slightly improved the level of mean serum HsCRP, which was not accompanied by the improvement of depressive symptoms. The causality between depression and inflammation is not well clear. Depression was linked to worse nutritional status in ESRD patients, [34] indicating that repeated episodes of depression contribute to inflammation, rather than inflammation contribute to depression in the body [9].

We did find an association between depressive symptoms and serum VD (VD2+ VD3) levels in the dialyzed population. The patients with higher serum VD levels at baseline tended to have fewer depressive symptoms. Recently, the possible link between depression and VD status has been investigated in several small studies, but the findings are inconsistent because of differences in races, study populations, geographic locations and methodologies [35‐39]. In particular, the depressive state may be a cause rather than a consequence of VD deficiency, because if depression caused VD deficiency owing to lack of sunlight exposure, then the association between VD levels and depressive symptoms would be stronger in the summer months when VD levels are most strongly influenced, which was not evident in this sample. Serum VD level is related to physical activity (time spent outdoors), body mass index (BMI), chronic diseases, social status and nutritional status. Luigi Ferrucci et al. explored whether low VD levels and depression in older people were related [40]. They did not find that low vitamin D levels can cause depression, and thus they thought other characteristics might predispose people with low nutrient levels to depression [40]. Also the most important one probably is that people with low VD are likely to have all these pathological problems associated with low VD and these problems can cause depression. Therefore, prospective research is required to clarify the direction of cause and effect [40].

The effect of VD in the brain is not well understood. VD is considered as a neurosteroid across the blood–brain barrier. The VD receptors widespread in the brain include the hippocampus, which is associated with the development of depression. In our intervention, we did not find a significant effect of calcitriol supplementation on enhancing the depressive symptoms in the dialyzed population, since the effects are also conflicting [41‐43]. There are some reasons for this result. First, calcitriol supplementation did not significantly enhance the depressive symptoms in the dialyzed population since we did not find the correct cause-and-effect relationship between VD and depression. Second, some causes lead to the opposite result: (1) The tested dose of VD (0.5 μg/day) might be insufficient to affect the occurrence of depression, and the VD intake from food sources was ignored. (2) One year was a rather short time frame for investigation of depression, since depression may develop slowly and last for several years. (3) BDI scores reflect the self-report of depressive symptoms, but it was controversial that a cut-off value of 16 was set to include the patients with depression (Some study chosen BDI score ≥ 20 as moderate to severe depression) [44]. It stressed that calcitriol supplementation can improve cardiovascular symptoms, [45, 46] and reduce vascular depression, but many reasons may induce the occurrence of depression in dialyzed population. Additionally, we use the dialyzed patients as objects for the first time.

A few limitations in the current study should be noted. Specifically, although we assessed a broad range of depressive disorders, it is difficult to ascertain the specific causes of depression within the sample. Second, We did not subdivide the patients with depression: one group treated with the active compound and one treated with placebo. It was not a randomized double-blind trial study. Thirdly, the dose of 0.5 μg calcitriol for dialyzed patients is far enough for curing depression. Moreover, the sample in our study is far smaller than enough.

Even though people with low levels of serum VD were more depressed, Calcitriol supplementation did not significantly enhance the depressive symptoms in our dialysis population. More prospective randomized controlled trials are necessary to find the exact cause-and-effect relationship between VD status and depressive symptoms or VD status related to some specific subtypes in dialyzed patients.