Colin A. Walsh,1 Wendy Allen,1 Katrina Parkin,1 Chinmoy Mukerjee2 Kate H. Moore1
1Department of Urogynaecology St George Hospital, University of New South Wales, Sydney, 2Department of Microbiology, St George Hospital, University of New South Wales, Sydney, Australia
Correspondence: Professor Kate Moore, Pitney Clinical Sciences Building, St George Hospital, Kogarah, NSW 2217 Australia. Tel: +61.2.9113 2054. E-mail: k.moore@unsw.edu.au
Key words: bacteriuria, detrusor overactivity, overactive bladder, refractory, urinary tract infection.
Contributions: CW, data collection, data analysis, manuscript preparation; WA, data collection; KP, data collection; CM, Microbiological analysis; KM, study design, manuscript editing.
Conflict of interest: the authors report no conflicts of interest.
Funding: Colin Walsh is partially funded by a University of New South Wales International Research Scholarship.
Received for publication: 25 April 2011.
Accepted for publication: 30 June 2011.
This work is licensed under a Creative Commons Attribution NonCommercial 3.0 License (CC BY-NC 3.0).
©Copyright C.A. Walsh et al., 2011
Licensee PAGEPress, Italy
Urogynaecologia 2011; 25:e4
doi:10.4081/uij.2011.e4
AbstractBackground. Previous studies suggest an association between idiopathic detrusor overactivity (IDO) and high-count bacteriuria (>105 CFU/mL). Recently, the importance of low-count bacteriuria (103-105 CFU/mL) in dysuric women with has been recognised. However, the optimal microbiological threshold for women with overactive bladder (OAB) symptoms remains unclear. |
Since the diagnosis of the unstable bladder was introduced in the 1970s by Bates and others,1,2 continence clinicians have been puzzled by the etiology of this condition. Over the decades, theories on the underlying cause for idiopathic detrusor overactivity (IDO) have ranged from a psychosomatic disorder3 to alterations in neuropeptide distribution4,5 and urothelial dysfunction.6 Most studies on the etiology of IDO have been conducted in patients with refractory IDO (RIDO), that is, those women who do not respond to conventional anti-cholinergic therapy.7 Although there is little consensus on the precise definition of refractory, longitudinal studies provide evidence that a substantial proportion of patients with IDO do not respond to standard management.8,9
With the introduction of the broader term overactive bladder (OAB), the exclusion of significant bacteriuria became an essential diagnostic criterion for this syndrome. However, there has been considerable evolution in the diagnostic criteria for significant bacteriuria in recent years, with increasing recognition of the importance of low-count bacteriuria (103-105 CFU/mL.10 Indeed, both the Infectious Diseases Society of America and the European Association of Urology have stipulated that the quantitative threshold for significant bacteriuria in acutely dysuric women should include low bacterial counts.11,12
However, the appropriate microbiological threshold in excluding significant bacteriuria in women the OAB syndrome without dysuria remains unclear. Two recent studies have demonstrated a substantial 25-30% incidence of bacteriuria ≥103 CFU/mL in women with OAB.13,14 The background comparative incidence of low-count bacteriuria in control women without OAB symptoms was not reported by these authors. The present study was carried out in a tertiary urogynecology center, in which IDO has been the major focus of research for almost two decades. This study was precipitated by the anecdotal finding that many women with RIDO who presented with an acute exacerbation of their urge incontinence symptoms, but no dysuria, were found to have bacterial cystitis. In view of the recent shift in focus towards low-count bacteriuria, we undertook a prospective comparative analysis of low-count and high-count bacteriuria in women with RIDO vs a control group of women without OAB symptoms.
A 2-year prospective cohort study of women aged 18-80 years with refractory IDO. RIDO was defined as failure to respond to ≥2 anti-cholinergic agents coupled with out-patient bladder training for ≥1 year, with persistent disabling symptoms on frequency-volume char.15 All study participants had urodynamically-proven DO without neurological disease. Eligible women were recruited and asked to submit a standard mid-stream urine (MSU) specimen for culture and sensitivity whenever their OAB symptoms (frequency, urgency, nocturia, urge incontinence) were acutely exacerbated. Women with co-existent stress incontinence were not excluded, provided the patient reported OAB symptoms to be the most bothersome. Full inclusion and exclusion criteria are detailed in Table 1. Women attending our unit with pure stress incontinence or mild pelvic organ prolapse, who denied all OAB symptoms on direct questioning, were asked to supply control MSU specimens for comparative analysis. All women with IDO in our unit are initially managed with lifestyle advice and bladder training, with anti-cholinergic medication added in as required. Peri- and post-menopausal women are treated with regular topical vaginal estrogen. All study patients were instructed on clean-catch MSU collection according to a standard regime to minimise contamination. Briefly, the urethral meatus is cleansed, the labia parted, voiding commenced and a sterile container is inserted into the urinary stream and removed, without interruption to the stream. Each MSU specimen was refrigerated at 4°C immediately after collection and transported to the laboratory in a refrigerated container within 2 hours. The study was performed in collaboration with our Microbiology department and MSU specimens from study participants were cultured at the 103 CFU/mL threshold (to include low-count bacteriuria) rather than the usual 105 CFU/mL. Specimens were cultured using Horse Blood Agar incubated at 35°C in 7% CO2 and McConkey's agar incubated at 35°C in air. These culture media grow all known pathogens and contaminants. Pyuria was determined using haemocytometer counts on uncentrifuged urine specimens, with counts of >10 white blood cells (WBC)/μL considered significant. Any bacteriuria ≥103 CFU/mL was considered a positive urine culture, in accordance with recent guidelines.12 Specimens with bacteriuria <103 CFU/mL were considered sterile. Women with positive cultures received 5 days of appropriate oral antibiotic therapy, according to sensitivity testing.
Categorical data were analysed using Fisher’s exact test. Data collated for age showed evidence of non-normality using the Shapiro-Wilk’s test. As such, median age was compared using the Mann-Whitney test for non-parametric data. Two-tailed P values were used throughout and the 5% level was considered significant. Statistical analysis was performed using Statsdirect statistical package 2.7.2 (Statsdirect Ltd, Cheshire, UK).
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Table 1. Study inclusion and exclusion criteria. |
Between November 2007 and November 2009, 50 women with urodynamically-proven non-neurogenic DO, who met our strict criterion for refractory, were recruited into the study. Fifty control women, who denied all OAB symptoms, were also recruited. There were no differences in age (P=0.15), menopausal status (P=0.50) or history of prior continence surgery (P=0.17) between the RIDO and control groups (Table 2). The median duration of OAB symptoms for the RIDO women was 10 years and they had trialled a median of 3 anti-cholinergic medications. Over the 2-year study period, 168 MSU specimens were provided by the RIDO group and 50 MSU specimens from the control group, for a total 218 study urine specimens. Women with RIDO provided a median of 3 urine samples during the study period and control women provided one MSU per patient.
The incidence of any bacteriuria ≥103 CFU/mL was significantly higher in the MSU specimens obtained from women with RIDO compared to those without OAB symptoms (P<0.0001, Table 3). Analysis of low-count (103-105 CFU/mL) bacteriuria only also demonstrated a significant difference between groups (P=0.0091, Table 3). Overall, at least one positive culture was obtained from 56% (28/50) of women with RIDO. E. coli was the predominant microbiological organism cultured from women with RIDO, accounting for 58% (38/65) of total positive cultures (Table 4). Subset analysis by bacteria showed that the only significant difference was with streptococci; the proportion of specimens positive for streptococci was higher in the low-count specimens (6/21) vs the high-count specimens (2/44; P=0.01; Table 4). In the RIDO group, specimens positive for high-count bacteriuria were more likely to be associated with significant pyuria (84%; 37/44) than those positive for low-count bacteriuria (23%; 5/21) only (P<0.0001; Table 4).
The median age of women with RIDO in this study was 62.5 (Inter-quartile range 53-70) years. Overall, among the women with RIDO, bacteriuric urine specimens were collected from older women when compared to specimens which were sterile (67 years vs 63 years respectively; P=0.04). However, within the positive specimens, those which grew low-count bacteriuria were collected from significantly younger women than those which grew high-count bacteriuria (58 years vs 67 years respectively; P=0.0009).
Among women with RIDO, 32% (16/50) had a history of previous continence surgery, who supplied 63 study urine specimens. MSU specimens obtained from women with previous continence surgery were significantly more likely to grow bacteriuria ≥103 CFU/mL (35/63) compared to those from women with RIDO and no history of continence surgery (30/105; P=0.0006), despite no difference in PVR between the sub-groups (P=0.24) and PVR<100 mL in all women with RIDO.
All women with cultures positive for low-count or high-count bacteriuria received a course of antibiotic therapy. Although the severity of urgency was generally reduced on frequency-volume chart in the RIDO group following antibiotics, formal assessment of urgency symptoms was not undertaken in this study.
 |
Table 2. Baseline demographic data. |
 |
Table 3. Results of formal culture at 103 CFU/mL threshold. |
 |
Table 4. Bacterial etiology by quantity of bacteriuria in women with refractory idiopathic destrusor overactivity. |
Extensive research into the etiology of IDO has been undertaken in recent decades but the underlying cause remains elusive. An association between OAB symptoms and bacterial cystitis has been postulated.16,17,18 The concept of refractory IDO is frequently mentioned in the literature but poorly defined.7 A longitudinal study of Australian women found a 65% rate of non-responders to treatment at a median follow-up of 8 years.8 A recent long-term study of UK women reported an 88% rate of persistent IDO on urodynamics at ≥10 years following instigation of treatment.9 Clinical management of this refractory group is moving towards sacral neuromodulation and intravesical neurotoxin.19 These interventions are invasive, expensive and not without risk to the patient, making the identification of potentially-treatable exacerbating factors, such as bacteriuria, imperative.
In parallel with the work on the etiology of IDO, our understanding of what constitutes significant bacteriuria in the diagnosis of urunary tract infection (UTI) has developed considerably. The traditional definition of significant bacteriuria [>105 colony-forming units (CFU) per milliliter) was described in 1957 by Edward Kass, a Harvard nephrologist.20 However, Kass was mainly interested in a practical threshold which could be used to distinguish probable infected specimens from those likely to be simply contaminated, at a time when pyelonephritis was a major source of mortality.20,21 He did acknowledge that lesser degrees of bacteriuria may be associated with infection. Since then, the focus has shifted towards women with lower urinary tract symptoms; numerous studies have found that 30-50% of urine cultures from acutely dysuric women fail to meet Kass’ microbiological standard.10 Expert guidelines now support the inclusion of low-count bacteriuria in women with acute dysuria.11,12 In contrast, there is a paucity of data on the incidence of bacteriuria 103-105 CFU/mL in women with IDO without dysuria. Previous studies linking female urinary incontinence and bacterial cystitis were performed using Kass’ older, less sensitive microbiological definition. Moore et al. reported bacterial cystitis in 6% of women with DO undergoing urodynamics, compared to 1% in stress incontinent controls.16 A study of 913 post-menopausal women found the basal rate of incontinence to be higher for women who experienced UTIs, even after controlling for the acute incontinence surrounding an infective episode.17 Neither of these studies considered low-count bacteriuria. The presence of bacteriuria also impacts on the accuracy of urodynamic testing. Bhatia et al. performed repeat urodynamic studies on 15 women who had significant bacteriuria (≥105 CFU/mL) during initial cystometric testing. They found that the incidence of DO fell by 50% after eradication of the UTI, although urodynamic parameters such as first desire to void and maximum cystometric capacity were unchanged.18
Currently, there is a dearth of evidence on the significance of bacteriuria, particularly low-count bacteriuria in women with frequency/urgency/nocturia. Khasriya et al. reported on 470 women with lower urinary tract symptoms (LUTS) without dysuria.13 By incorporating low-count bacteriuria, the incidence of positive specimens increased from 15% (using the traditional culture threshold of 105 CFU/mL) to 29%. However, this study was primarily examining the role of dipstick urinalysis and the specimens were obtained from a wide range of women without urodynamic diagnoses. A similar German study reported an almost identical 28% incidence of bacteriuria ≥103 CFU/mL in women with OAB without symptoms of acute UTI (dysuria, fever or haematuria).14 However, neither study presented a suitable control group to allow comparative analysis (although the former paper does include a small, mixed-gender control group). Thus, while an incidence of 28-29% appears high (and likely is), background data regarding the incidence in the general female population is not, to our knowledge, available.
The aim of the present study was to examine the incidence of bacteriuria and low-count bacteriuria among a severely affected group of women with RIDO, compared to the incidence in women without OAB symptoms. Only women with IDO were recruited as, compared to women with OAB syndrome without DO, women with urodynamically-proven DO have more incontinent episodes and earlier abnormal sensory symptoms.22 Furthermore, this group would generally be considered candidates for sacral neuromodulation or intravesical neurotoxin, which may be inappropriate if bacteriuria has not been excluded. The present study finds that, in women with RIDO, the incidence of bacteriuria during an episode of symptomatic exacerbation, using a sensitive microbiological threshold, is 39%. This is considerable and is higher than similar incidences quoted for women with OAB symptoms only.14 Furthermore, our data show that the comparative incidence amongst similarly aged women without OAB symptoms is significantly lower (6%, Table 3), which has not previously been reported.
The European Association of Urology has recently published guidelines which support the treatment of low bacterial counts in acute UTI.12 These echo guidelines published in 1992 by the Infectious Diseases Society of America (IDSA).11 However, it was also noted that a marginally higher threshold (≥103 CFU/mL) improved specificity (90% vs 85%) with little loss of sensitivity (80% vs 95%) compared to ≥102 and, in addition, could be more easily identified by routine microbiological techniques.12 Despite these expert guidelines, many laboratories continue to use the traditional threshold of ≥105 CFU/ml when determining bacteriuria that requires treatment.23 Indeed, the recent joint consensus document on the terminology of pelvic floor dysfunction by the International Continence Society/ International Urogynaecological Association, endorses a threshold of >105 CFU/ml for voided specimens in the diagnosis of UTI.24 The present study shows that, among women with RIDO, one-third of bacteriuric specimens grow low-count bacteriuria only, which would be missed if a >105 CFU/mL threshold is maintained.
The impact of age on rates of bacteriuria in this study is notable. In general, positive urine cultures were obtained from older women, which is consistent with previous reports.25 However, amongst the positive cultures, those positive for low-count bacteriuria only were obtained from significantly younger women than those with high-count bacteriuria. Several theories have been proposed to explain the phenomenon of low-count bacteriuria, including urinary dilution, an early phase of infection, the presence of an inhibitor or following antibiotic therapy.26 An interesting Israeli study examined the natural history of low-count and high-count UTI over 2 days without antibiotic treatment. Among women with a baseline low-count UTI, 50% had progressed to a high-count infection after 48 hours, which substantiates the theory that low-count bacteriuria simply represents an earlier stage in the infective process.27 To our knowledge, a possible association between low bacterial counts younger aged women has not previously been suggested.
Pyuria has traditionally been used to distinguish true infection from colonisation. Most women with bacteriuria >105 CFU/mL will have pyuria. Recent expert guidelines include pyruia as part of the diagnostic algorithm for UTI.12 However the relationship between bacteriuria 103-105 CFU/mL and pyuria is less clear. The previous study of 470 women with OAB by Khasriya et al. noted a trend towards reduced pyuria in low-count compared to high-count bacteriuria (P=0.078).13 Another study, on bladder biopsies from patients with the OAB syndrome, found that the presence of significant pyuria in urine did not predict the histological finding of chronic cystitis.28 Furthermore, the high rate of natural progression of low-count to high-count bacteriuria suggests that low bacterial counts, even in the absence of pyuria, cannot be dismissed as clinically insignificant.27
In the present study, bacteriuria 103-105 CFU/mL was significantly less likely to be associated with pyuria (P<0.0001). It is notable that destruction of urinary leukocytes begins almost immediately after specimen collection. We refrigerated our specimens immediately at 4°C and transported them to the laboratory within 2 hours in all cases. However, refrigeration slows but does not eliminate WBC lysis. White cell destruction in refrigerated specimens is approximately 20% in the first 2 hours after collection,29 which may have impacted on the rates of pyuria reported here although one would expect all specimens to be equally vulnerable to this effect.
We acknowledge a number of limitations with the present study. Firstly, microbiological analysis was performed on MSU specimens rather than CSU, which may overestimate the incidence of bacteriuria. However, most women with IDO will continue to provide mid-stream, rather than catheter, specimens at times of worsening OAB symptoms, thus enhancing the clinical applicability of our findings. Secondly, although anecdotal evidence suggested an improvement in IDO symptoms following antibiotic treatment of bacteriuria, formal assessment of patients’ symptoms pre- and post-treatment was not undertaken. Statistical evidence of symptomatic improvement following antimicrobial therapy of women with IDO and bacteriuria will likely require a randomized placebo controlled trial. Finally, the debate regarding the clinical importance of low-count bacteriuria without pyuria will continue. Although several studies have consistently demonstrated reduced rates of pyuria in lower bacterial counts, objective evidence of symptomatic improvement will be needed to substantiate the notion that, among women with IDO, bacteriuria without pyuria is clinically meaningful.
A substantial proportion of women with IDO are refractory to standard treatment and contemporary management of these cases may include invasive neuromodulation and intravesical neurotoxin. Recent expert guidelines endorse the inclusion of low bacterial counts (103-105 CFU/mL) in the diagnosis of acute UTI but the incidence of this low-count bacteriuria in women with refractory IDO is poorly studied.
In the present study, we were quite surprised to find that almost 40% of women with RIDO and an acute exacerbation of symptoms had significant bacteriuria on MSU. For the first time, we can report that this incidence is significantly higher than among a control group of similarly-aged women without OAB symptoms. One-third of positive cultures grew low-count bacteriuria only. Low-count bacteriuria was seen in younger women and was more likely to resolve following appropriate antibiotic therapy. The management of women with RIDO experiencing an acute worsening of symptoms should include a search for bacteriuria and a low-count microbiological threshold should be considered.
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