Female Sexual Dysfunction and Diabetes: A Systematic Review and Meta‐Analysis

Sexual dysfunction is reported in diabetic women (female sexual dysfunction [FSD]). To examine the frequency of FSD in diabetic women, and its clinical or metabolic correlates, through meta‐analysis of available studies. We searched in MEDLINE, EMBASE, Cochrane Library, and in reference lists of art...

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Bibliographic Details
Published in:Journal of sexual medicine 2013-04, Vol.10 (4), p.1044-1051
Main Authors: Pontiroli, Antonio E., Cortelazzi, Donatella, Morabito, Alberto
Format: Article
Language:English
Subjects:
Age Factors
Body Mass Index
Depression - complications
Diabetes Complications
Diabetes Mellitus
Female
Humans
Meta‐Analysis
Sexual Dysfunction
Sexual Dysfunction, Physiological - etiology
Sexual Dysfunctions, Psychological - etiology
Women
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Summary:Sexual dysfunction is reported in diabetic women (female sexual dysfunction [FSD]). To examine the frequency of FSD in diabetic women, and its clinical or metabolic correlates, through meta‐analysis of available studies. We searched in MEDLINE, EMBASE, Cochrane Library, and in reference lists of articles and systematic reviews; we considered human clinical studies published as full articles reporting on FSD in diabetic and control women. In total, we considered 26 studies, including 3,168 diabetic and 2,823 control women. Frequency of FSD and score of Female Sexual Function Index (FSFI) as a function of study size, patient details (age, body mass index [BMI], duration of diabetes, metabolic control [HbA1c], chronic complications, Beck Depression Inventory [BDI] score). Frequency of FSD was higher in type 1 (OR [95%CI] 2.27 [1.23, 4.16]), in type 2 diabetes (2.49 [1.55, 3.99]), and in “any diabetes” (type 1 and 2) women (2.02 [1.49, 2.72]) than in controls for any duration of diabetes. FSFI was lower in type 1 (−0.27 [−0.41, −0.12]), in type 2 diabetes (−0.65 [−0.75, −0.54]), and in “any diabetes” women (−0.80 [−0.88, −0.71]) than in controls. Depression was significantly more frequent in diabetic than in control women. At meta‐regression only BMI was significantly associated with effect size (P = 0.005). At weighed regression, the only significant association was found between age and FSFI (P = 0.059). The limitations were as follows: only studies of observational nature were available, and heterogeneity was seen among studies. FSD is more frequent in diabetic than in control women, but it is still poorly understood; low FSFI is associated with high BMI. Further studies are necessary to better understand risk factors for FSD in diabetic women.
ISSN:1743-6095
1743-6109
DOI:10.1111/jsm.12065