Hypovitaminosis D, Low Bone Mineral Density, and Diabetes Mellitus as Probable Risk Factors for Benign Paroxysmal Positional Vertigo in the Elderly

Bazoni, Jessica Aparecida; Ciquinato, Daiane Soares Almeida; Marquez, Audrey de Souza; Costa, Viviane de Souza Pinho; Marchiori, Glória de Moraes; Marchiori, Luciana Lozza de Moraes

doi:10.1055/s-0039-1700583

Abstract

Introduction

Studies have found that elderly patients with benign paroxysmal positional vertigo (BPPV) may present low levels of vitamin D (25 (OH) D), changes in bone mineral density, and diabetes mellitus (DM).

Objective

To investigate the possible association between BPPV, bone mineral density, hypovitaminosis D, 25 (OH) D and DM.

Methods

The sample consisted of 109 elderly subjects. The BPPV was verified by a standardized questionnaire and the Dix-Hallpike maneuver. Blood samples were collected for the investigation of 25 (OH) D serum levels. The bone mineral density was evaluated by means of a densitometer. Diabetes mellitus verification was performed using a self-reported questionnaire.

Results

Of the 109 participants, 17 had BPPV. There was a statistically significant difference between BPPV and gender (p = 0.027, phi = 0.222), with female representing 88.2% of those with BPPV. In the group with BPPV, there was a statistically significant difference for the amount of vitamin D found (p = 0.001) and for age (p = 0.001). In the elderly group with DM and BPPV, a difference was found for the standard deviation of the femur (p = 0.022) with posthoc Dunn, identifying the difference between diabetics with and without BPPV (p = 0.047).

Conclusion

Although no association was found (25 (OH) D levels) with BPPV in the general population of this study, it was observed that there was an association with bone mineral density in the elderly group with DM and BPPV, and, in the group with BPPV, there was an association between the amount of vitamin D and age.

Keywords
vitamin D; bone mineral density; benign paroxysmal positional vertigo; elderly

Introduction

Benign paroxysmal positional vertigo (BPPV) is defined as a vestibular dysfunction of peripheral origin and unilateral predominance, characterized by episodes of vertigo that are usually intense, short in duration, and typically triggered by certain postural changes in the head.¹1 von Brevern M, Bertholon P, Brandt T, et al. Benign paroxysmal positional vertigo: Diagnostic criteria. J Vestib Res 2015;25(3-4):105-117

2 Burlamaqui JC, Campos CAH, Mesquita Neto O. Manobra de Epley para Vertigem Postural Paroxistica Benigna: revisão sistemática. Acta Otorrinolaringol. 2006;24:38-45^-³3 Dix MR, Hallpike CS. The pathology, symptomatology and diagnosis of certain common disorders of the vestibular system. Ann Otol Rhinol Laryngol 1952;61(04):987-1016 Benign paroxysmal positional vertigo represents ∼ 20 to 30% of dizziness diagnoses in specialized clinics, with an incidence of 0.6% per year, and its prevalence rate increases to 3.4% in individuals over 60.2 years of age. It is the most common cause of vertigo in adults, affecting women twice as much and constituting in most cases of the idiopathic BPPV.⁴4 von Brevern M, Radtke A, Lezius F, et al. Epidemiology of benign paroxysmal positional vertigo: a population based study. J Neurol Neurosurg Psychiatry 2007;78(07):710-715

5 Silva C, Amorim AM, Paiva A. Benign paroxysmal positional vertigo-a review of 101 cases. Acta Otorrinolaringol Esp 2015;66(04):205-209^-⁶6 Cho EI, White JA. Positional vertigo: as occurs across all age groups. Otolaryngol Clin North Am 2011;44(02):347-360, viii

Low levels of vitamin D have been associated with the development and recurrence of BPPV, with a possible level of disturbance attributed to vestibular endolymph Ca²⁺, which results in the formation of abnormal otoconia. Calcium is the main component of these otoconia that are generated by the same mechanism of calcium absorption that occurs in bones, which, in turn, has many important biological functions, including the regulation of homeostasis of calcium.⁷7 Marom T, Oron Y, Watad W, Levy D, Roth Y. Revisiting benign paroxysmal positional vertigo pathophysiology. Am J Otolaryngol 2009;30(04):250-255

8 Jeong SH, Kim JS, Shin JW, et al. Decreased serum vitamin D in idiopathic benign paroxysmal positional vertigo. J Neurol 2013;260(03):832-838^-⁹9 Gans R. Benign paroxysmal positional vertigo: a common dizziness sensation. Audiology online serial on the internet. 2002. Disponivel em: URL: http://www.audiologyonline.com/articles/article_detail.asp?article_id1/486. Acesso em 14 junho 2018.
http://www.audiologyonline.com/articles/...

All people have several free otoconia in the semicircular canals; however, the body is able to absorb calcium usually within hours or days without triggering symptoms.⁹9 Gans R. Benign paroxysmal positional vertigo: a common dizziness sensation. Audiology online serial on the internet. 2002. Disponivel em: URL: http://www.audiologyonline.com/articles/article_detail.asp?article_id1/486. Acesso em 14 junho 2018.
http://www.audiologyonline.com/articles/... Epidemiological studies have found that a significant portion of the world population, regardless of age, ethnicity, and geographic location, has a prevalence of osteoporosis and low serum vitamin D levels in patients with BPPV.⁸8 Jeong SH, Kim JS, Shin JW, et al. Decreased serum vitamin D in idiopathic benign paroxysmal positional vertigo. J Neurol 2013;260(03):832-838

9 Gans R. Benign paroxysmal positional vertigo: a common dizziness sensation. Audiology online serial on the internet. 2002. Disponivel em: URL: http://www.audiologyonline.com/articles/article_detail.asp?article_id1/486. Acesso em 14 junho 2018.
http://www.audiologyonline.com/articles/...

10 Talaat HS, Abuhadied G, Talaat AS, Abdelaal MS. Lowbone mineral density and vitamin D deficiency in patients with benign positional paroxysmal vertigo. Eur Arch Otorhinolaryngol 2015;272(09):2249-2253

11 Mikulec AA, Kowalczyk KA, Pfitzinger ME, Harris DA, Jackson LE. Negative association between treated osteoporosis and benign paroxysmal positional vertigo in women. J Laryngol Otol 2010;124(04):374-376

12 Yu S, Liu F, Cheng Z, Wang Q; K Yu S. Association between osteoporosis and benign paroxysmal positional vertigo: a systematic review. BMC Neurol 2014;14:110^-¹³13 Parham K, Leonard G, Feinn RS, Lafreniere D, Kenny AM. Prospective clinical investigation of the relationship between idiopathic benign paroxysmal positional vertigo and bone turnover: a pilot study. Laryngoscope 2013;123(11):2834-2839 Bone mineral density (BMD) and serum 25-hydroxyvitamin D (25 (OH) D) levels may be affected by several factors, such as age; gender; preexisting metabolic disorders, such as diabetes mellitus (DM), and lifestyle.¹⁴14 Tuzun S, Eskiyurt N, Akarirmak U, et al; Turkish Osteoporosis Society. The impact of a FRAX-based intervention threshold in Turkey: the FRAX-TURK study. Arch Osteoporos 2012;7:229-235^,¹⁵15 Lee JH, O'Keefe JH, Bell D, Hensrud DD, Holick MF. Vitamin D deficiency an important, common, and easily treatable cardiovascular risk factor? J Am Coll Cardiol 2008;52(24):1949-1956

Since there is a scarcity of studies that provide evidence of such associations, which may lead to better prevention and treatment options for BPPV in the elderly, this research aimed to investigate a possible association between BPPV, bone mineral density, hypovitaminosis D, levels of 25 (OH) D, and DM in this population.

Methods

Study Design

The present study is a cross-sectional analysis. The sample consisted of a population of 43,610 elderly enrolled in the 38 Basic Health Units of the urban area of the municipality of Londrina, Parana, Brazil. The sample selection of individuals was randomly stratified, taking into consideration the five regions of the city; They are 15% of the central region, 27% of the northern region, 23% in the southern region, 19% in the eastern region, and 16% in the western region. This study is part of the ELLO Project (Study on Aging and Longevity).

Part of this sample was selected to perform the bone densitometry test. The selection criteria for bone densitometry were: to be physically independent according to the functional classification proposed by Spirduso: 3 (physically independent) and 4 (physically active).¹⁶16 Spirdurso WW. Dimensoes Fisicas do Envelhecimento. Barueri, Manole2005 Of the 323 elderly individuals who were invited to perform bone densitometry, 42 were not found, 28 refused to participate, 135 were excluded because they had one of more of the exclusion criteria, and 9 died. The final sample consisted of 109 elderly subjects. For this part of the study, the following inclusion criteria were used: age ≥ 60 years; both genders; voluntarily agree to participate in the study. The exclusion criteria were: present unilateral and/or bilateral conductive or mixed hearing loss; present otorrhea, surgery in the vestibular system, and not agreeing to perform one of the study evaluations. The study was approved by the ethics committee of the institution, and all subjects participated voluntarily after signing the free and informed consent term to comply with resolution 466/12.¹⁷17 Brasil (2012). Resolução 466, de 12 de dezembro de 2012. In Uniao DOd (ed).

Clinical Evaluation

Benign paroxysmal positional vertigo diagnosis was verified by vertigo complaint, an audiological anamnesis,¹⁸18 Miller MH. A integração dos achados audiológicos. In: Katz J (Org). Tratado de audiologia clínica. São Paulo: Manole; 1999; 3:268-70 and the Dix-Hallpike diagnostic maneuver.¹⁹19 Bhattacharyya N, Baugh RF, Orvidas L, et al; American Academy of Otolaryngology-Head and Neck Surgery Foundation. Clinical practice guideline: benign paroxysmal positional vertigo. Otolaryngol Head Neck Surg 2008;139(05, Suppl 4):S47-S81 The diagnosis of BPPV includes a greater caution regarding the history of dizziness associated with changes in head position, confirmed by the Dix-Hallpike maneuver, and the patient who presented nystagmus was considered with BPPV.

The 25-OH-vitamin D dosages were performed in serum samples by fully automated chemiluminescent method (Architect iSR2000-Abbott). They were adopted according to 25-OH vitamin D serum with the following criteria: Vitamin D deficiency was defined as a 25(OH)D below 20 ng/ml (50 nmol/liter), vitamin insufficiency D as a 25(OH)D of 21 to 29 ng/ml, normal or sufficient as a 25(OH)D ≥ 30 ng/ml and hypovitaminosis D as a 25(OH)D ≤ 29 ng / ml.²⁰20 Holick MF, Binkley NC, Bischoff-Ferrari HA, et al; Endocrine Society. Evaluation, treatment, and prevention of vitamin D deficiency: an Endocrine Society clinical practice guideline. J Clin Endocrinol Metab 2011;96(07):1911-1930^,²¹21 Souberbielle JC, Body JJ, Lappe JM, et al. Vitamin D and musculoskeletal health, cardiovascular disease, autoimmunity and cancer: Recommendations for clinical practice. Autoimmun Rev 2010;9(11):709-715

The BMD was evaluated with the QDR 4500 duo-energy densitometer (Hologic Inc., Bedford, MA, USA) in the lumbar spine (L1-L4), femoral neck and total femur regions. For the analysis, we used the criteria of the World Health Organization,²²22 OMS. World Health Report. Suica: WHO; 2010 normal BMD with T-score up to −1.0 ± standard deviation (SD), osteopenia with T-score between −1.0 to −2.4 ± SD, and osteoporosis with T-score ≤ −2.5 ± SD at any bone site.

Specific data on vertigo complaint and comorbidities²³23 Lapenna R, Faralli M, Del Zompo MR, Cipriani L, Mobaraki PD, Ricci G. Reliability of an anamnestic questionnaire for the diagnosis of benign paroxysmal positional vertigo in the elderly. Aging Clin Exp Res 2016;28(05):881-888 were also verified with self-reported responses.

The Statistical Package of Social Science (SPSS) 20.0 for Windows (SPSS Inc., Chicago, IL, USA) was used for the statistical analysis. The normality of the data was verified with the Kolmogorov-Smirnov test, but as the assumption was not met, the Mann-Whitney and Kruskal-Wallis test with Dunn posthoc were selected to analyze the quantitative variables in the comparison between the groups. For analysis of subgroups, normality was also verified. The t-test for a sample selected for the BPPV subgroup. The Kolmogorov-Smirnov test for a sample was selected for the control group. The Chi-square test was selected to verify the association between BPPV and other categorical variables. A 95% confidence interval and a significance level of 5% (p < 0.05) were established for all tests.

Results

The variables analyzed were: serum levels of vitamin D, vitamin D classification (deficiency, insufficiency, normal), hypovitaminosis, BMD, diabetes (DM). In addition to the covariates related to personal data (sex and age), symptoms (tinnitus and headache), lifestyle (physical activity), and comorbidity (hypertension and diabetes mellitus). Of the 109 participants, 17 had BPPV confirmed by the Dix-Hallpike maneuver. The general characteristics of the sample are presented in Table 1. (view Table 1).

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Table 1
Descriptive data of the sample (N = 109)

There was a significant association between BPPV and gender (p = 0.027; phi = 0.222), as shown in Table 2. The female gender represented 88.2% of those with BPPV. There was also an association between hypovitaminosis and gender (p = 0.038; phi = 0.199); of the female group, 68.7% were classified as hypovitaminosis D.

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Table 2
Comparative analyses between groups (n = 109)

Although no statistical difference was found between BPPV and bone mineral density (p = 0.125), lumbar spine densitometry was the variable that most approached a significant value. Only 23.5% of the elderly with BPPV diagnosed with normal densitometry, 47.1% with osteopenia, and 29.4% with osteoporosis. That is, the elderly with BPPV presented worse results than their healthy controls.

Subgroup analysis showed that, in the group with BPPV, there was a statistically significant difference for the amount of vitamin D found (p = 0.001) and for age (p = 0.001) when compared with its healthy controls, as shown in Table 3. Adjusted analyzes for BPPV and comorbidities, such as arterial hypertension and DM, were also performed. The Kruskal-Wallis test identified a difference for the elderly group with DM and BPPV for the femur SD (p = 0.022) with Dunn posthoc identifying the difference between the groups with BPPV and with DM, and the group without BPPV and with DM (p = 0.047). The other analyzed variables presented p > 0.05.

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Table 3
Comparative analyses subgroups

Discussion

In this study, no association was found between low levels of BMD, hypovitaminosis D and levels of 25 (OH) D and DM with BPPV in the general population. However, it was observed that in the elderly group with DM and BPPV, a statistically significant difference was found for BMD with the SD of the femur. In the group with BPPV, there was a statistically significant difference for the variables amount of 25 (OH) D found and age. These findings contribute to group information on this controversial aspect of human health.

The effect of low levels of BMD, hypovitaminosis D and levels of 25 (OH) D, and DM on the health of the older population has been largely studied; however, their effects on BPPV is less known. Previous studies have found an association between changes in BPPV hypovitaminosis D.⁸8 Jeong SH, Kim JS, Shin JW, et al. Decreased serum vitamin D in idiopathic benign paroxysmal positional vertigo. J Neurol 2013;260(03):832-838^,²⁴24 Ding J, Liu L, Kong WK, Chen XB, Liu X. Serum levels of 25-hydroxy vitamin D correlate with idiopathic benign paroxysmal positional vertigo. Biosci Rep 2019;39(04):BSR20190142

Regarding the prospective relation between low levels of BMD, hypovitaminosis D and levels of 25 (OH) D, and DM with BPPV, other studies diverge on the associations found.

For instance, in a study to investigate the relationship between BMD and 25-hydroxyvitamin D with the occurrence and recurrence of BPPV, evaluted the records of 130 idiopathic BPPV. The records of 130 idiopathic BPPV patients (55 ± 12 years old, 30 men and 100 women) and 130 age- and gender-matched controls who underwent bone mineral densitometry. Was compared the BMD and serum 25-hydroxyvitamin D between the patients and controls, and also compared the BMD between recurrent and non-recurrent BPPV groups. Among the female subjects, the BPPV group showed significantly decreased BMD compared with the controls (p < 0.05). The men in the control group had significantly higher 25-hydroxyvitamin D levels than the men with BPPV (p < 0.05). Sixty-three patients (48%) reported recurrent attacks of BPPV. The women with recurrent BPPV were significantly older and showed a significantly lower BMD than non-recurrent women (p < 0.001). However, multiple regression analysis revealed that age alone was significantly associated with the recurrence of BPPV in women. Bone mineral density in women and serum 25-hydroxyvitamin D levels in men are associated with the occurrence of BPPV. Only age is an independent predictor of recurrence, although a low BMD and age correlate with the recurrence of BPPV.²⁵25 Yang CJ, Kim Y, Lee HS, Park HJ. Bone mineral density and serum 25-hydroxyvitamin D in patients with idiopathic benign paroxysmal positional vertigo. J Vestib Res 2018;27(5-6):287-294 Similar findings regarding gender and age were observed in our study, since there was a statistically significant difference in the amount of vitamin D, age, and gender in the BPPV group.

We also found that in the elderly group with DM and BPPV, there was a significant difference in relation to BMD for femoral SD, although we found no association between BMD and 25 (OH) D levels in women; this association only occurred in BPPV in the total population. The exact pathophysiology of diabetic damage to the peripheral vestibular organ is not yet fully understood. However, a loss of sacculate type I hair cells has been described in human subjects with DM.²⁶26 Kocdor P, Kaya S, Erdil M, Cureoglu S, Paparella MM, Adams ME. Vascular and neuroepithelial histopathology of the saccule in humans with diabetes mellitus. Otol Neurotol 2016;37(05):553-557^,²⁷27 Degerman E, Rauch U, Lindberg S, Caye-Thomasen P, Hultgårdh A, Magnusson M. Expression of insulin signalling components in the sensory epithelium of the human saccule. Cell Tissue Res 2013;352(03):469-478 Glucose uptake is regulated in most tissues by the expression of glucose transporters on cell surfaces.²⁸28 Thorens B, Mueckler M. Glucose transporters in the 21st Century. Am J Physiol Endocrinol Metab 2010;298(02):E141-E145 In DM, the saccule represents the main structure of the maze affected by pathological damage due to endolymphatic hydrops. Cohen et al²⁹29 Cohen HS, Kimball KT, Stewart MG. Benign paroxysmal positional vertigo and comorbid conditions. ORL J Otorhinolaryngol Relat Spec 2004;66(01):11-15 analyzed a cohort of 112 patients with BPPV, of whom 24 (14%) had DM. The authors pointed out that this prevalence is higher than the 4% rate of diabetics in the United States population. A recent literature review suggests that a large number of peripheral vestibular changes such as BPPV and DM may be strongly influenced by blood insulin and blood glucose levels.³⁰30 Gioacchini FM, Albera R, Re M, Scarpa A, Cassandro C, Cassandro E. Hyperglycemia and diabetes mellitus are related to vestibular organs dysfunction: truth or suggestion? A literature review. Acta Diabetol 2018;55(12):1201-1207

Recently a meta-analysis did not support the lower vitamin D level relationship with BPPV occurrence. However, it supports, with normal heterogeneity, the fact that recurrent episodes of BPPV are associated with low vitamin D.³⁰30 Gioacchini FM, Albera R, Re M, Scarpa A, Cassandro C, Cassandro E. Hyperglycemia and diabetes mellitus are related to vestibular organs dysfunction: truth or suggestion? A literature review. Acta Diabetol 2018;55(12):1201-1207

Although in our study we found a significant difference within the subgroup, in the BPPV-adjusted analysis with a higher amount of vitamin D in its group, we did not find this difference in the general study population, constituting serum 25 (OH) D levels in the BPPV group (27.8 ng/ml) and in the control group decreased serum levels (23.8 ng/ml). One explanation for the non-association found between low BMD levels, hypovitaminosis D, 25 (OH) D levels, and DM in relation to BPPV in the general population may be related to the fact that the serum 25 (OH) D level in the population was not sufficiently low in our study as compared with the study by Talaat et al,¹⁰10 Talaat HS, Abuhadied G, Talaat AS, Abdelaal MS. Lowbone mineral density and vitamin D deficiency in patients with benign positional paroxysmal vertigo. Eur Arch Otorhinolaryngol 2015;272(09):2249-2253 which indicates that the vitamin D concentration in the control group (19.5 ng/ml) is higher than in the BPPV group (16.0 ng/ml). Another explanation concerns latitude differences involving hours of sun exposure. This could explain the variation in serum levels in different studies,²⁰20 Holick MF, Binkley NC, Bischoff-Ferrari HA, et al; Endocrine Society. Evaluation, treatment, and prevention of vitamin D deficiency: an Endocrine Society clinical practice guideline. J Clin Endocrinol Metab 2011;96(07):1911-1930^,²¹21 Souberbielle JC, Body JJ, Lappe JM, et al. Vitamin D and musculoskeletal health, cardiovascular disease, autoimmunity and cancer: Recommendations for clinical practice. Autoimmun Rev 2010;9(11):709-715^,³¹31 Holick MF. Vitamin D deficiency. N Engl J Med 2007;357(03):266-281^,³²32 McGrath JJ, Féron FP, Burne TH, Mackay-Sim A, Eyles DW. Vitamin D3-implications for brain development. J Steroid Biochem Mol Biol 200489-90(1-5):557-560 since vitamin D is acquired in humans through the production of 7 dehydrocholesterol, provitamin D3 in the skin, absorption of UVB radiation and ingestion.³¹31 Holick MF. Vitamin D deficiency. N Engl J Med 2007;357(03):266-281

32 McGrath JJ, Féron FP, Burne TH, Mackay-Sim A, Eyles DW. Vitamin D3-implications for brain development. J Steroid Biochem Mol Biol 200489-90(1-5):557-560

33 Lanteri P, Lombardi G, Colombini A, Banfi G. Vitamin D in exercise: physiologic and analytical concerns. Clin Chim Acta 2013;415:45-53

34 Grant WB. Benefits of ultraviolet-B irradiance and vitamin D in youth. J Steroid Biochem Mol Biol 2013;136:221-223

35 Scott D, Ebeling PR, Sanders KM, Aitken D, Winzenberg T, Jones G. Vitamin d and physical activity status: associations with five-year changes in body composition and muscle function in communitydwelling older adults. J Clin Endocrinol Metab 2015;100(02):670-678

36 Bell NH, Godsen RN, Henry DP, Shary J, Epstein S. The effects of muscle-building exercise on vitamin D and mineral metabolism. J Bone Miner Res 1988;3(04):369-373^-³⁷37 Karatas A, Acar Yüceant G, Yüce T, Haci C, Cebi IT, Salviz M. Association of benign paroxysmal positional vertigo with osteoporosis and vitamin D deficiency: a case-controlled study. J Int Adv Otol 2017;13(02):259-265

Mean serum vitamin D concentrations may differ between institutions in the study country.⁸8 Jeong SH, Kim JS, Shin JW, et al. Decreased serum vitamin D in idiopathic benign paroxysmal positional vertigo. J Neurol 2013;260(03):832-838^,¹⁰10 Talaat HS, Abuhadied G, Talaat AS, Abdelaal MS. Lowbone mineral density and vitamin D deficiency in patients with benign positional paroxysmal vertigo. Eur Arch Otorhinolaryngol 2015;272(09):2249-2253^,³⁸38 AlGarni MA, Mirza AA, Althobaiti AA, Al-Nemari HH, Bakhsh LS. Association of benign paroxysmal positional vertigowith vitamin D deficiency: a systematic review and meta-analysis. Eur Arch Otorhinolaryngol 2018;275(11):2705-2711^,³⁹39 Buki B, Ecker M, Junger H, Lundberg YW. Deficiência de vitamina D e vertigem posicional paroxística benigna. Eur Arch Otorhinolaryngol 2013;80:201-204 Therefore, direct comparison of values in the study results requires close attention. These differences in serum levels may be one of the factors for the divergence of research findings regarding the relationship between vitamin D and BPPV.

The strengths of the present study include the bone densitometry test, the application of Dix-Hallpike diagnostic maneuver, and the 25 (OH) D dosages. The limitations include the of self-reported vertigo complaint. However, the use of self-reported measures of vertigo complaint is habitual in prospective studies due to its simplicity and low-costs.⁴⁰40 Bazoni JA, Mendes WS, Moreira MD, et al. Queixa de vertigem e prática de atividade física regular em idosos. Rev CEFAC 2013;15:1447-1452 In addition, the vertigo complaint was supported by the application of Dix-Hallpike maneuver.

From the specific literature and the results of the present research, it is shown the need to verify the comorbidities involved in the BPPV for good targeting of the better treatment selection.

Conclusion

Although there was no association between low levels of BMD, hypovitaminosis D, and levels of vitamin D (25 (OH) D with BPPV in the general population of this study, in the elderly group with DM and BPPV, it was found significant difference for SD of the femur, and, in the group with BPPV, there was a statistically significant difference for the amount of vitamin D found and for the age.

Financial Assistance

Fundação Nacional de Desenvolvimento de Ensino Superior Particular (FUNADESP).

References

¹
von Brevern M, Bertholon P, Brandt T, et al. Benign paroxysmal positional vertigo: Diagnostic criteria. J Vestib Res 2015;25(3-4):105-117
²
Burlamaqui JC, Campos CAH, Mesquita Neto O. Manobra de Epley para Vertigem Postural Paroxistica Benigna: revisão sistemática. Acta Otorrinolaringol. 2006;24:38-45
³
Dix MR, Hallpike CS. The pathology, symptomatology and diagnosis of certain common disorders of the vestibular system. Ann Otol Rhinol Laryngol 1952;61(04):987-1016
⁴
von Brevern M, Radtke A, Lezius F, et al. Epidemiology of benign paroxysmal positional vertigo: a population based study. J Neurol Neurosurg Psychiatry 2007;78(07):710-715
⁵
Silva C, Amorim AM, Paiva A. Benign paroxysmal positional vertigo-a review of 101 cases. Acta Otorrinolaringol Esp 2015;66(04):205-209
⁶
Cho EI, White JA. Positional vertigo: as occurs across all age groups. Otolaryngol Clin North Am 2011;44(02):347-360, viii
⁷
Marom T, Oron Y, Watad W, Levy D, Roth Y. Revisiting benign paroxysmal positional vertigo pathophysiology. Am J Otolaryngol 2009;30(04):250-255
⁸
Jeong SH, Kim JS, Shin JW, et al. Decreased serum vitamin D in idiopathic benign paroxysmal positional vertigo. J Neurol 2013;260(03):832-838
⁹
Gans R. Benign paroxysmal positional vertigo: a common dizziness sensation. Audiology online serial on the internet. 2002. Disponivel em: URL: http://www.audiologyonline.com/articles/article_detail.asp?article_id1/486 Acesso em 14 junho 2018.
» http://www.audiologyonline.com/articles/article_detail.asp?article_id1/486
¹⁰
Talaat HS, Abuhadied G, Talaat AS, Abdelaal MS. Lowbone mineral density and vitamin D deficiency in patients with benign positional paroxysmal vertigo. Eur Arch Otorhinolaryngol 2015;272(09):2249-2253
¹¹
Mikulec AA, Kowalczyk KA, Pfitzinger ME, Harris DA, Jackson LE. Negative association between treated osteoporosis and benign paroxysmal positional vertigo in women. J Laryngol Otol 2010;124(04):374-376
¹²
Yu S, Liu F, Cheng Z, Wang Q; K Yu S. Association between osteoporosis and benign paroxysmal positional vertigo: a systematic review. BMC Neurol 2014;14:110
¹³
Parham K, Leonard G, Feinn RS, Lafreniere D, Kenny AM. Prospective clinical investigation of the relationship between idiopathic benign paroxysmal positional vertigo and bone turnover: a pilot study. Laryngoscope 2013;123(11):2834-2839
¹⁴
Tuzun S, Eskiyurt N, Akarirmak U, et al; Turkish Osteoporosis Society. The impact of a FRAX-based intervention threshold in Turkey: the FRAX-TURK study. Arch Osteoporos 2012;7:229-235
¹⁵
Lee JH, O'Keefe JH, Bell D, Hensrud DD, Holick MF. Vitamin D deficiency an important, common, and easily treatable cardiovascular risk factor? J Am Coll Cardiol 2008;52(24):1949-1956
¹⁶
Spirdurso WW. Dimensoes Fisicas do Envelhecimento. Barueri, Manole2005
¹⁷
Brasil (2012). Resolução 466, de 12 de dezembro de 2012. In Uniao DOd (ed).
¹⁸
Miller MH. A integração dos achados audiológicos. In: Katz J (Org). Tratado de audiologia clínica. São Paulo: Manole; 1999; 3:268-70
¹⁹
Bhattacharyya N, Baugh RF, Orvidas L, et al; American Academy of Otolaryngology-Head and Neck Surgery Foundation. Clinical practice guideline: benign paroxysmal positional vertigo. Otolaryngol Head Neck Surg 2008;139(05, Suppl 4):S47-S81
²⁰
Holick MF, Binkley NC, Bischoff-Ferrari HA, et al; Endocrine Society. Evaluation, treatment, and prevention of vitamin D deficiency: an Endocrine Society clinical practice guideline. J Clin Endocrinol Metab 2011;96(07):1911-1930
²¹
Souberbielle JC, Body JJ, Lappe JM, et al. Vitamin D and musculoskeletal health, cardiovascular disease, autoimmunity and cancer: Recommendations for clinical practice. Autoimmun Rev 2010;9(11):709-715
²²
OMS. World Health Report. Suica: WHO; 2010
²³
Lapenna R, Faralli M, Del Zompo MR, Cipriani L, Mobaraki PD, Ricci G. Reliability of an anamnestic questionnaire for the diagnosis of benign paroxysmal positional vertigo in the elderly. Aging Clin Exp Res 2016;28(05):881-888
²⁴
Ding J, Liu L, Kong WK, Chen XB, Liu X. Serum levels of 25-hydroxy vitamin D correlate with idiopathic benign paroxysmal positional vertigo. Biosci Rep 2019;39(04):BSR20190142
²⁵
Yang CJ, Kim Y, Lee HS, Park HJ. Bone mineral density and serum 25-hydroxyvitamin D in patients with idiopathic benign paroxysmal positional vertigo. J Vestib Res 2018;27(5-6):287-294
²⁶
Kocdor P, Kaya S, Erdil M, Cureoglu S, Paparella MM, Adams ME. Vascular and neuroepithelial histopathology of the saccule in humans with diabetes mellitus. Otol Neurotol 2016;37(05):553-557
²⁷
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Publication Dates

Publication in this collection
28 Aug 2020
Date of issue
Jul-Sep 2020

History

Received
04 May 2019
Accepted
12 Sept 2019

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[1] Financial Assistance

Fundação Nacional de Desenvolvimento de Ensino Superior Particular (FUNADESP).

GENERAL CHARACTERISTICS	N (%)
GROUPS
With BPPV	N = 17 (15.6%)
Without BPPV	N = 92 (84.4%)
GENDER
Female	N = 69 (63.3%)
Male	N = 40 (36.7%)
AGE RANGE
60-64 years	N = 32 (29.4%)
65-74 years	N = 58 (53.2%)
75 years and over	N = 19 (17.4%)
Mean ± standard deviation	68.7 ± 6.1^a a (mean and standard deviation).
VITAMIN D	25.5 ± 8.7^a a (mean and standard deviation).
Normal (≥ 30 ng/ml)	N = 26 (23.9%)
Insufficiency (21-29 ng/ml)	N = 49 (45.0%)
Deficiency (≤ 29 ng/ml)	N = 34 (31.2%)
HYPOVITAMINOSIS D
Normal (≥ 30 ng/ml)	N = 26 (23.9%)
Hypovitaminosis D (≤ 29 ng/ml)	N = 83 (71.6%)
BMD
Normal	N = 21 (19.3%)
Osteopenia	N = 56 (51.4%)
Osteoporosis	N = 32 (29.4%)

		BPPV	Controls (without BPPV)	P (Mann-Whitney test)
Quantitative Variables
Age (years)		67 [10]^b b Median and interquartile range	68 [7.75]	p = 0.728 U = 823.500
Vitamin D (ng/ml)		27.8 [10.10]	23.8 [11.28]	p = 0.260 U = 917.000
Categorical variables				P (Chi-square test)
Sex	Female	15 (88.2%)	54 (58.7%)	p = 0.020^* * Statistically significant difference. X² = 5.390
Sex	Male	2 (11.8%)	38 (41.3%)
Physical activity	No-active	10 (17.9%)	46 (82.1%)	p = 0.504 X² = 0.447
Physical activity	Active	7 (13.2%)	46 (86.8%)	p = 0.504 X² = 0.447
Vitamin D classification	Normal	6 (35.3%)	20 (21.7%)	p = 0.304 X² = 2.317
	Insufficiency	8 (47.1%)	41 (44.6%)
	Deficiency	3 (17.6%)	31 (33.7%)
D hypovitaminosis	Normal	6 (35.3%)	20 (21.7%)	p = 0.371 X² = 0.801
D hypovitaminosis	Hypovitaminosis	11 (64.7%)	72 (78.3%)	p = 0.371 X² = 0.801
Spine BMD	Normal	4 (23.5%)	45 (48.9%)	p = 0.125 X² = 4.019
	Insufficiency	8 (47.1%)	30 (32.6%)
	Deficiency	5 (29.4%)	17 (18.5%)
Tinnitus	Yes	9 (52.9%)	35 (38%)	p = 0.250 X² = 1.323
Tinnitus	No	8 (47.1%)	57 (62%)	p = 0.250 X² = 1.323
Hypertension	Yes	12 (70.6%)	52 (56.5%)	p = 0.279 X² = 1.171
Hypertension	No	5 (29.4%)	40 (43.5%)	p = 0.279 X² = 1.171
DM	Yes	5 (29.4%)	20 (21.7%)	p = 0.706 X² = 0.142
DM	No	12 (70.6%)	72 (78.3%)	p = 0.706 X² = 0.142
Headache	Yes	9 (52.9%)	28 (30.4%)	p = 0.072 X² = 3.241
Headache	No	8 (47.1%)	64 (69.6%)	p = 0.072 X² = 3.241

	BPPV (cases) N = 17	P (BPPV group)	Without BPPV (controls) N = 92	P (control group)
Variables
Vitamin D (ng/ml)	27.8 [10.1]	p = 0.001^* * Statistically significant difference.	23.8 [11.28]	p = 0.704
Age (years)	67.0 [10.0]	p = 0.001^* * Statistically significant difference.	68 [7.75]	p = 0.273