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Gut and Liver is an international journal of gastroenterology, focusing on the gastrointestinal tract, liver, biliary tree, pancreas, motility, and neurogastroenterology. Gut atnd Liver delivers up-to-date, authoritative papers on both clinical and research-based topics in gastroenterology. The Journal publishes original articles, case reports, brief communications, letters to the editor and invited review articles in the field of gastroenterology. The Journal is operated by internationally renowned editorial boards and designed to provide a global opportunity to promote academic developments in the field of gastroenterology and hepatology. +MORE
Yong Chan Lee |
Professor of Medicine Director, Gastrointestinal Research Laboratory Veterans Affairs Medical Center, Univ. California San Francisco San Francisco, USA |
Jong Pil Im | Seoul National University College of Medicine, Seoul, Korea |
Robert S. Bresalier | University of Texas M. D. Anderson Cancer Center, Houston, USA |
Steven H. Itzkowitz | Mount Sinai Medical Center, NY, USA |
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Hyun Gun Kim*, Kyu Chan Huh†, Hoon Sup Koo†, Seong-Eun Kim‡, Jin-Oh Kim*, Tae Il Kim§, Hyun-Soo Kim||, Seung-Jae Myung¶, Dong Il Park#, Jeong Eun Shin**, Dong-Hoon Yang¶, Suck-Ho Lee*, Ji Sung Lee††, Chang Kyun Lee‡‡, Dong Kyung Chang§§, Young-Eun Joo||||, Jae Myung Cha‡‡, Sung Pil Hong§, and Hyo Jong Kim‡‡
*Institute for Digestive Research, Department of Internal Medicine, Soonchunhyang University College of Medicine, Seoul, Korea
†Division of Gastroenterology, Department of Internal Medicine, Konyang University College of Medicine, Daejeon, Korea
‡Division of Gastroenterology, Department of Internal Medicine, Ewha Womans University School of Medicine, Seoul, Korea
§Division of Gastroenterology, Department of Internal Medicine, Yonsei University College of Medicine, Seoul, Korea
||Division of Gastroenterology, Department of Internal Medicine, Yonsei University Wonju College of Medicine, Wonju, Korea
¶Department of Gastroenterology, Asan Medical Center, University of Ulsan College of Medicine, Seoul, Korea
#Department of Internal Medicine, Kangbuk Samsung Hospital, Sungkyunkwan University School of Medicine, Seoul, Korea
**Division of Gastroenterology, Department of Internal Medicine, Dankook University College of Medicine, Cheonan, Korea
††Biostatistical Consulting Unit, Soonchunhynag University College of Medicine, Seoul, Korea
‡‡Division of Gastroenterology, Department of Internal Medicine, Kyung Hee University School of Medicine, Seoul, Korea
§§Division of Gastroenterology, Department of Internal Medicine, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul, Korea
||||Division of Gastroenterology, Department of Internal Medicine, Chonnam National University Medical School, Gwangju, Korea
Correspondence to: Kyu Chan Huh, Department of Internal Medicine, Konyang University College of Medicine, 158 Gwanjeodong-ro, Seo-gu, Daejeon 302-718, Korea, Tel: +82-42-600-9370, Fax: +82-42-600-9091, E-mail: kchuh2020@hanmail.net
This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
Gut Liver 2015;9(4):494-501. https://doi.org/10.5009/gnl14010
Published online October 7, 2014, Published date July 31, 2015
Copyright © Gut and Liver.
We investigated whether sodium picosulfate with magnesium citrate (SPMC) plus bisacodyl compares favorably with conventional polyethylene glycol (PEG) with respect to bowel cleansing adequacy, compliance, and safety.
We performed a multicenter, prospective, single-blinded study in outpatients undergoing daytime colonoscopies. Patients were randomized into a split preparation SPMC/bisacodyl group and a conventional split PEG group. We compared preparation adequacy using the Boston bowel preparation scale (BBPS), ease of use using a modified Likert scale (LS), compliance/satisfaction level using a visual analogue scale (VAS), and safety by monitoring adverse events during the colonoscopy between the two groups.
A total of 365 patients were evaluated by intention to treat (ITT) analysis, and 319 were evaluated by per protocol (PP) population analysis (153 for SPMC/bisacodyl, 166 for PEG). The mean total BBPS score was not different between the two groups in both the ITT and PP analyses (p>0.05). The mean VAS score for satisfaction and LS score for the ease of use were higher in the SPMC/bisacodyl group (p<0.001). The adverse event rate was lower in the SPMC/bisacodyl group than in the PEG group (p<0.05).
The SPMC/bisacodyl treatment was comparable to conventional PEG with respect to bowel preparation adequacy and superior with respect to compliance, satisfaction, and safety.
Keywords: Colonoscopy, Bowel preparation, Sodium picosulfate with magnesium citrate, Polyethylene glycols
Colonoscopy is considered the most effective colorectal cancer screening procedure.1 The maximal preventative effect of colonoscopy requires adequate visualization of the entire colon to facilitate detection and removal of all adenomas, which involves detailed observations associated with cecal intubation, longer withdrawal time, and adequate preparation. Bowel preparation is the most important colonoscopy quality indicator because it affects both the cecal intubation and adenoma detection rates.
The ideal preparation procedure should clean the colon without mucosal damage, electrolyte imbalance, or patient discomfort. The most commonly used preparation regimens are based on polyethylene glycol (PEG). PEG is a safe and highly effective colon cleansing agent that is widely accepted as a standard bowel preparation regimen.2,3 However, ingestion of a large volume of PEG, as well as its unpleasant taste, results in low compliance rates and unsatisfactory cleansing quality.4–6 The adequate cleansing rate by conventional PEG bowel preparation has been reported to be 70% to 77% by meta-analyses,2,5–7 which is similar to that in Korea (47% to 76%).8–11
Sodium picosulfate with magnesium citrate (SPMC) is a low-volume, dual-action bowel-cleansing agent used mostly in the United Kingdom and Canada as a tolerable preparation agent.12–15 Recently, SPMC was approved in the United States for bowel preparation before colonoscopy and it is also available in Korea as Picolight powder® (Phambio Korea Co., Ltd., Seoul, Korea).16,17 Each sachet of Picolight powder® contains 12-g citrate, 3.5-g magnesium oxide, an osmotic laxative, and 10-mg sodium picosulfate hydrate, a stimulant laxative. These ingredients are identical to those in Picolax® (Ferring, West Drayton, UK) and Pico-Salax® (Ferring, North York, Canada). SPMC acts locally in the colon as both a stimulant laxative by increasing the frequency and the force of peristalsis and promoting electrolyte and water retention in the colon, and an osmotic laxative by retaining fluids in the colon.18 In previous meta-analyses, SPMC was well tolerated by patients but may be less efficacious than other agents.14,19–21 Recently, several studies have investigated various methods of improving the cleansing efficacy of SPMC, including the addition of a laxative with SPMC, consuming fluids with SPMC, and the three-sachet-split method.22,23 However, these studies were conducted largely in Western populations12–15 and SPMC preparation has not been studied in an Asian population.
We conducted this study to investigate the cleansing efficacy, safety and tolerability of SPMC with bisacodyl as a substitute bowel preparation method to conventional large volume PEG in Koreans.
This was a multicenter, randomized, single blind, noninferiority trial conducted at 13 institutions belonging to the intestinal tumor research group of the Korean Association for the Study of Intestinal Disease (KASID) from June 2012 to January 2013. All participating endoscopists were faculty of a university hospital with colonoscopy expertise. Bias in endoscopist evaluation of colon cleansing was minimized by use of a single investigator blind design.
All subjects 20 to 75 years of age undergoing elective daytime outpatient colonoscopy at each institution were enrolled in this study. Exclusion criteria included previous colorectal surgery, ileus or bowel obstruction, significant constipation defined as <3 bowel movements per week with or without regular laxatives, ascites, heart failure, ischemic heart disease or coronary vessel disease within the last 6 month, inflammatory bowel disease, pregnancy, cognitive impairment, and renal impairment. This study was approved by the Institutional Review Board of each participating institution and registered with the open registry of the Clinical Research Information Service (http://cris.nih.go.kr) under the identifier KCT0000580. After informed consent, the patients were randomly assigned to one of two fixed-dose treatment arms, either split-dose SPMC with bisacodyl or splitdose PEG. Randomization was conducted using a computergenerated table prepared by an independent biostatistician.
All enrolled patients were instructed to consume a low-fiber diet 3 days before colonoscopy and fast in the evening of the day before colonoscopy. Participants in the SPMC group were given Picolight powder® (Phambio Korea Co., Ltd.) and instructed to ingest one sachet with 150-mL water followed by 2-L of water at 7 PM the day before the procedure and ingest another sachet with 150-mL water followed by 2-L water 4 hours before colonoscopy, based on previous reports.23 Participants in the SPMC group were further instructed to ingest two 5-mg bisacodyl tablets the night before colonoscopy. Those patients receiving standard PEG were instructed to use the split-dose method, whereby 2-L PEG for ingestion at 6 PM the day before colonoscopy and another 2-L PEG 4 hours before colonoscopy. All colonoscopies were scheduled to be performed before 13:00 hours.
The primary outcome was comparison of the colon-cleansing efficacy between the two preparation groups. Bowel cleansing was assessed by endoscopists who were blinded to the preparation method during the withdrawal phase of colonoscopy using the Boston bowel preparation scale (BBPS), a validated tool for assessment of the quality of colon cleansing.24 Each of the three segments of the colon (right, including the cecum and ascending colon; transverse, including the hepatic and splenic flexures; and left, including the descending colon, sigmoid, and rectum) was given a score from 0 to 3, defined as follows: 0=unprepared colon segment with mucosa not visible due to remnants of solid stool that cannot be cleared; 1=portion of mucosa of the colon segment seen, but other areas of the colon segment not as visible because of staining, residual stool, and/or opaque liquid; 2=minor amount of residual staining, small fragments of stool, and/or opaque liquid, but mucosa of colon segment visible; 3=entire mucosa of colon segment visible, with no residual staining, small fragments of stool, or opaque liquid.24 Adequate bowel preparation was defined a score ≥2 for all segments. Inadequate preparation was defined as a summed BBPS score <6 or a score in any segment <2.
Satisfaction with the preparation agent was assessed using a visual analogue scale (VAS) as 0 (worst) to 10 (best) on a questionnaire to patients. The tolerability of the bowel preparation was assessed via a standardized questionnaire administered to patients on the day of the colonoscopy, before receiving any preliminary sedation for the procedure. The questionnaires for the assessment of tolerability were composed of four sections describing the completeness of agent consumption, the ease, the taste and the intention to reuse the preparation. Patient could choose only one item for their responses.
The questionnaire for the completeness of agent consumption was as follows for the SPMC/bisacodyl group: (1) ‘2 sachets completely taken,’ or ‘not’; (2) additional water consumption completeness, ‘2-L for each sachet,’ ‘less than 2-L for each sachet,’ ‘1-L for each sachet,’ ‘less than 1-L for each sachet’; (3) overnight two tablets of bisacodyl, ‘completely taken,’ or ‘not.’
The questionnaire for the completeness of agent consumption was as follows for the conventional PEG group: ‘4-L completely taken,’ ‘over 75% taken,’ ‘over 50% taken,’ ‘less than 50% taken.’ The questionnaire regarding ease of use and taste of the bowel preparation was based on a modified five-point Likert scale (LS): ‘very easy (5 points),’ ‘easy (4 points),’ tolerable (3 points),’ ‘difficult (2 points),’ very difficult (1 point)’ and for taste as five points: ‘very good (5 points),’ ‘good (4 points),’ fair (3 points),’ ‘bad (2 points),’ ‘worst (1 point).’22 We determined ‘the tolerable group’ as those participants who selected three points or more in each of the assessments of ease of use and taste.
Safety was assessed by the incidence of adverse events reported as a ‘yes’ or ‘no’ response in a questionnaire and colonic mucosal change. Adverse events were defined as nausea, vomiting, abdominal pain, bloating, thirst, dizziness, or paresthesia during consumption of the preparation agents. The presence of mucosal changes including erythema or aphthous lesions, were recorded by endoscopists after colonoscopy. Blood chemistry and electrolyte level were not essential tests and were evaluated only when the patients had severe side effects, as determined by the endoscopist.
In calculating the sample size, we assumed a successful cleansing rate of 85% for the conventional PEG preparation based on previous data.5,13 We specified a noninferiority margin of −15% for the difference in adequate preparation rates defined as the rate in the SPMC/bisacodyl group minus the rate in the PEG group, and a one-sided significance level of 0.025. Assuming a 10% dropout rate, we calculated that we would need to enroll 186 patients in each group for an 80% statistical power to demonstrate noninferiority.
The intent to treat (ITT) population included all randomized participants and the patient who underwent colonoscopy. The per protocol (PP) population was determined as the enrolled patient who completed bowel preparation according to the preparation instructions for each and underwent colonoscopy. The outcome measurement and statistical analyses of cleansing efficacy, tolerability, satisfaction, and safety were performed for both the ITT and PP populations. The safety analysis was performed for the ITT population.
We assessed noninferiority by comparing the lower bound of the one-sided 97.5% confidence interval (CI) for the rate difference to −15% and testing the corresponding hypothesis that the difference would be >−15%.
Total BBPS, VAS, and the ease of use and taste scores were analyzed as a continuous variable, after confirmation of normal distribution, by Student t-test. We compared percentages of the BBPS score of each segment of colon, the completeness of preparation agents, the tolerability, ease of use, and taste based on a standardized patient questionnaire, and the incidence of both side effects and mucosal change between the groups using a Pearson chi-square test of Fisher exact test for pooled responses and records. All statistical analyses were performed using SAS version 9.3 (SAS Institute Inc., Cary, NC, USA). Statistical significance was defined as p<0.05.
Most of the participants that received SPMC/bisacodyl were able to consume the split dose of SPMC both on the day before (100%) and the day of (99.7%) the colonoscopy. The ratio of completeness of agent consumption was markedly higher in the SPMC/bisacodyl (99.4%) than conventional PEG (90.2%) groups (p<0.001). However, 28 patients in the SPMC/bisacodyl group and 18 in the PEG group did not complete the entire preparation process. Excluding these 46 patients, 319 patients (153 in the SPMC/bisacodyl, 166 in the PEG group) completed the entire preparation process and were analyzed as the PP population.
During the detailed preparation process for the SPMC/bisacodyl group, two tablets of 5-mg bisacodyl were consumed by 97.8% (n=179) of patients. However, 2-L of water was consumed after each sachet of SPMC by only 74% (n=134) of patients. Overall, 86% (n=156) of participants that received SPMC with bisacodyl consumed >75% of the total volume of water (3-L) after SPMC sachet consumption.
The SPMC/bisacodyl group achieved better overall colon cleansing than the PEG group, as measured by the ratio of adequate preparation based on BBPS. In the ITT analysis, the adequate preparation rate was 87.9% in the SPMC/bisacodyl group and 81.0% in the PEG group, similar to the results of the PP analysis (86.9% SPMC/bisacodyl vs 83.7% in the PEG group). The rate difference, defined as the rate of the SPMC/bisacodyl group—the rate in the PEG group, was 6.9% in the ITT analysis and 3.2% in the PP analysis. The lower bound of the one-sided 97.5% CI for rate difference rate was greater than the noninferiority margin of −15%, demonstrating noninferiority of the SPMC with bisacodyl group to the PEG group in both the ITT (one-sided 97.5% CI, −0.5% to 14.3%; p<0.001) and PP (one-sided 97.5% CI, −4.6% to 10.9%; p<0.001) analyses. However, there was no significant difference in mean BBPS when comparing the cleansing effect between the two preparation methods (Table 2). The mean BBPS of all colon segments for each group was higher than 2 points. The percentage of each BPSS score in all segments was also similar between the two preparation methods (Fig. 1).
The mean VAS scale of the SPMC/bisacodyl group was significantly superior to the PEG group, in both ITT (7.58±1.94 vs 5.79±2.43, p<0.001) and PP (7.62±1.95 vs 5.92±2.35, p<0.001) (Fig. 2). SPMC with bisacodyl was better tolerated than PEG with respect to ease of use and taste (Fig. 3). Using a modified five-point LS, the mean score for ease of use of SPMC/bisacodyl was higher than that of PEG (ITT, 3.57±0.82 vs 2.59±0.79, p<0.001; PP, 3.56±0.81 vs 2.63±0.78, p<0.001). The mean score for taste of SPMC/bisacodyl was also superior to that of PEG (ITT, 3.65±0.73 vs 2.60±0.79, p<0.001; PP, 3.69±0.71 vs 2.64±0.77, p<0.001). Furthermore, the ‘tolerable group’ ratio was a significantly higher proportion of the SPMC/bisacodyl than PEG with respect to ease of use (ITT, 94.5% vs 63.0%, p<0.001; PP, 94.8% vs 65.7%, p<0.001) and taste (ITT, 97.8% vs 60.3%, p<0.001; PP, 98.0% vs 61.4%, p<0.001). Finally, a positive response regarding the intention to reuse the received agent was higher in the SPMC/bisacodyl group than the PEG group (ITT, 83.2% vs 48.5%, p<0.001; PP, 80.5% vs 49.5%, p<0.001).
The overall prevalence of adverse effects related to preparation was lower in the SPMC/bisacodyl group than the PEG group (65.2% vs 77.7%, p=0.011). Symptoms of vomiting, abdominal pain, and paresthesia occurred at a similar rate in both groups, while nausea, bloating, thirst were more common in the conventional PEG group and dizziness was more common in the SPMC/bisacodyl group (Table 3). Mucosal changes including erythema (5.5% of the SPMC/bisacodyl group vs 4.9% of the PEG group by PP analysis, p=0.139) and aphthous lesion (2.2% in the SPMC/bisacodyl group only) were observed in only a small number of patients in each group.
Blood chemistry tests for serum electrolytes and renal function (blood urea nitrogen and creatinine) were performed in 58 participants. There was no difference in the blood examination rate between the groups (14.9% of SPMC/bisacodyl vs 16.8% of PEG group). While there were no abnormal blood chemistry findings in the SPMC/bisacodyl group, one hyponatremia and two hypochloridemia cases were identified in the patients who received conventional PEG preparation in the ITT population.
Although the small volume of SPMC is well tolerated and results in improved preparation compliance, its cleansing effect remains uncertain. Some studies in the United Kingdom reported that SPMC was less effective than conventional PEG in bowel preparation before colonoscopy.12–14 To improve the cleansing effect of SPMC, a split method using two sachets taken the evening the day before colonoscopy and 4 to 5 hours before colonoscopy, combined with a laxative, has been proposed.22,23,25 Additionally, sufficient fluid intake is critical to the quality of preparation with SPMC; 1.5- to 2-L are recommended for each sachet.23,26
In the current study, we based the SPMC and bisacodyl combination method used on previous comparisons of cleansing efficacy with that of conventional PEG.16,17,22 We designed the split SPMC method to comprise ingestion of two sachets of SPMC with 2-L of water per sachet, in combination with 10-mg bisacodyl. We also educated all participants to partake in a low-fiber diet 3 days before colonoscopy.27 With this preparation protocol, the adequate preparation rate of SPMC/bisacodyl was comparable to that of conventional PEG in both the ITT and PP analyses. In the noninferiority analysis, the lower bound of CI for the difference in the adequate preparation rate was greater than the noninferiority margin hypothesized in this study, and fulfilled the noninferiority condition. There were no differences in the mean BBPS scores and BBPS percentage scores in the right, transverse and left colon. Favorable comparisons between SPMC and PEG were likely due to the additional bisacodyl given to the SPMC group. Bisacodyl is a stimulant laxative that works directly on the colon to increase the frequency and force of peristalsis and enhance bowel movement. Therefore the use of a stimulant laxative in this study might have overcome the reported weaknesses of a SPMC-only preparation, especially in the right colon cleansing.12–14,22
In addition to addition of a stimulant laxative to the SPMC preparation regimen, sufficient fluid intake following each sachet of SPMC is also important. Good quality cleansing with at least 3-L of total fluid intake in SPMC preparations has been reported.16,17,22 Interestingly, SPMC/bisacodyl was significantly superior to conventional PEG with respect to satisfaction and tolerability, even though the patients were instructed to consume 2-L of water following ingestion of 150 mL with the SPMC sachet and only 74% of patients consumed the recommended fluid volume, lower than that for conventional PEG (90.2%) in the current study. Sufficient fluid intake is likely the most difficult obstacle to overcome in SPMC preparation. Although, we designed 2-L of fluid intake following ingestion of each SPMC sachet in this study, 1.5-L of fluid intake per sachet may be appropriate based on the excellent results reported previously.16,17,23
In our study, PEG produced more symptoms of nausea, bloating and thirst, which may be related to the taste and large volume. SPMC produced more dizziness, which may be a result of biochemical derangements and dehydration. Reports of the biochemical and hemodynamic effects of SPMC are limited. Given that SPMC acts in a similar fashion to sodium phosphate, SPMC is likely to cause similar fluid and electrolyte shifts. In one study, PEG was associated with a significant decrease in potassium, while SPMC was associated with significant decreases in chloride and significant increases in magnesium.14 In 2002, the Australian Adverse Drug Reactions Advisory Committee described 16 cases of serious adverse events with SPMC with no fatalities, eight reports of adverse events associated with hyponatremia, and four reports of syncope and dehydration without documented electrolyte abnormalities.28 Electrolyte abnormalities resulting in seizures were reported in a patient using SPMC.29 In the current study, blood chemistry and electrolyte tests were performed only when patients developed severe side effects, a total of 15.9% of the participants, with no abnormal findings. These safety results may be related to our exclusion of patients with serious comorbidities, such as renal impairment and cardiovascular concerns, and those older than 75 years. Although the normal blood test results in the SPMC/bisacodyl group may reflect the safety of SPMC to the healthy group, further evaluation regarding the safety of SPMC/bisacodyl is necessary.
Mucosal changes, including inflammation and ulceration, were reported in 3.5% of patients who received the SPMC preparation,30 which is similar to the SPMC/bisacodyl in the current study. Although a previous study reported that the rate of acute mucosal inflammation was 10-fold higher in patients receiving SPMC than PEG,30 our data suggest no difference in mucosal inflammation, such as erythematous changes or aphthous lesions.
Our study was limited in that we did not confirm interobserver agreement in the BBPS. However, we instructed the participating endoscopists in using the BBPS, a valid and reliable instrument for assessing bowel cleanliness, in detail in the study protocol. BBPS is easier to assess than the Ottawa scale, and no difficulties were encountered because all of the endoscopists were skilled in colonoscopy. Although the current study was designed to be single-blinded due to the differences in the administration of bowel preparations, and this represents a potential source of bias, precautions were taken to ensure the endoscopists remained blinded to the bowel preparation method. In particular, our findings suggest that SPMC/bisacodyl has advantages with respect to bowel cleansing, tolerability and safety compared to conventional PEG; however, our findings should not be generalized to a high-risk population because we excluded patients with renal insufficiency and cardiovascular concerns. The broad noninferiority margin (15%) is one of the weak points of the current study. Although its range estimated based on previous studies might be wide,5,13 the cleansing effect of SPMC with bisacodyl was comparable to that of conventional PEG not only in the noninferiority analysis but also in the simple comparison using the mean BBPS score and adequate preparation rate.
In conclusion, this is the first prospective randomized controlled study of SPMC conducted at multiple institutions in Korea and the first in an Asian population. The results indicate that split dosing of SPMC with bisacodyl was comparable to conventional PEG with respect to preparation adequacy and superior to conventional PEG with respect to tolerability, satisfaction and safety. Therefore, a split dosing of SPMC with bisacodyl is a good substitute for conventional PEG preparation before colonoscopy.
This study was conducted by the intestinal tumor research group of the Korean Association for the Study of Intestinal Disease (KASID).
CI, confidence interval.
Demographics and Baseline Characteristics of the Intention to Treat Population
Parameter | SPMC with bisacodyl (n=181) | Conventional 4-L PEG (n=184) | p-value* |
---|---|---|---|
Male sex | 94 (51.9) | 100 (54.4) | 0.644 |
Age, yr | 53.5±10.7 | 53.8±10.4 | 0.788 |
20–64 | 154 (85.1) | 154 (83.7) | 0.715 |
≥65 | 27 (14.9) | 30 (16.3) | |
Indication for colonoscopy | 0.195 | ||
Symptom evaluation | 38 (21) | 37 (20.1) | |
Screening | 68 (37.6) | 79 (42.9) | |
Surveillance | 50 (27.6) | 34 (18.5) | |
For endoscopic treatment | 25 (13.8) | 34 (18.5) |
Data are presented as mean±SD or number (%).
SPMC, sodium picosulfate with magnesium citrate; PEG, polyethylene glycol.
p-values were calculated using Student t-test or Pearson chi-square test, as appropriate.
Efficacy of Bowel Cleansing in Patients Undergoing Colonoscopy Using the Boston Bowel Preparation Scale
Colon segment | ITT population (n=365) | PP population (n=319) | ||||
---|---|---|---|---|---|---|
SPMC with bisacodyl (n=181) | Conventional 4-L PEG (n=184) | p-value* | SPMC with bisacodyl (n=153) | Conventional 4-L PEG (n=166) | p-value* | |
Right colon | 2.3±0.7 | 2.2±0.8 | 0.144 | 2.3±0.6 | 2.2±0.7 | 0.391 |
Transverse colon | 2.5±0.6 | 2.5±0.6 | 0.834 | 2.5±0.6 | 2.5±0.6 | 0.998 |
Left colon | 2.5±0.6 | 2.4±0.7 | 0.507 | 2.5±0.6 | 2.3±0.6 | 0.913 |
Total colon | 7.3±1.6 | 7.2±1.7 | 0.329 | 7.3±1.6 | 7.2±1.6 | 0.680 |
Data are presented as mean±SD.
ITT, intention to treat; PP, per protocol; SPMC, sodium picosulfate with magnesium citrate; PEG, polyethylene glycol.
p-values were calculated using Student t-test.
Comparison of Preparation-Related Adverse Events Using Intention to Treat Analysis
Adverse effect | SPMC with bisacodyl (n=181) | Conventional 4-L PEG (n=184) | p-value* |
---|---|---|---|
Nausea | 52 (28.7) | 78 (42.4) | 0.006 |
Vomiting | 23 (12.7) | 31 (16.9) | 0.265 |
Abdominal pain | 48 (26.5) | 44 (23.9) | 0.566 |
Bloating | 70 (38.7) | 103 (56.0) | 0.001 |
Thirst | 19 (10.5) | 39 (21.2) | 0.005 |
Dizziness | 44 (24.3) | 27 (14.7) | 0.020 |
Parasthesia | 3 (1.7) | 6 (3.3) | 0.503 |
Data are presented as number (%).
SPMC, sodium picosulfate with magnesium citrate; PEG, polyethylene glycol.
p-values were calculated using Student t-test or Pearson chi-square test, as appropriate.
Gut Liver 2015; 9(4): 494-501
Published online July 31, 2015 https://doi.org/10.5009/gnl14010
Copyright © Gut and Liver.
Hyun Gun Kim*, Kyu Chan Huh†, Hoon Sup Koo†, Seong-Eun Kim‡, Jin-Oh Kim*, Tae Il Kim§, Hyun-Soo Kim||, Seung-Jae Myung¶, Dong Il Park#, Jeong Eun Shin**, Dong-Hoon Yang¶, Suck-Ho Lee*, Ji Sung Lee††, Chang Kyun Lee‡‡, Dong Kyung Chang§§, Young-Eun Joo||||, Jae Myung Cha‡‡, Sung Pil Hong§, and Hyo Jong Kim‡‡
*Institute for Digestive Research, Department of Internal Medicine, Soonchunhyang University College of Medicine, Seoul, Korea
†Division of Gastroenterology, Department of Internal Medicine, Konyang University College of Medicine, Daejeon, Korea
‡Division of Gastroenterology, Department of Internal Medicine, Ewha Womans University School of Medicine, Seoul, Korea
§Division of Gastroenterology, Department of Internal Medicine, Yonsei University College of Medicine, Seoul, Korea
||Division of Gastroenterology, Department of Internal Medicine, Yonsei University Wonju College of Medicine, Wonju, Korea
¶Department of Gastroenterology, Asan Medical Center, University of Ulsan College of Medicine, Seoul, Korea
#Department of Internal Medicine, Kangbuk Samsung Hospital, Sungkyunkwan University School of Medicine, Seoul, Korea
**Division of Gastroenterology, Department of Internal Medicine, Dankook University College of Medicine, Cheonan, Korea
††Biostatistical Consulting Unit, Soonchunhynag University College of Medicine, Seoul, Korea
‡‡Division of Gastroenterology, Department of Internal Medicine, Kyung Hee University School of Medicine, Seoul, Korea
§§Division of Gastroenterology, Department of Internal Medicine, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul, Korea
||||Division of Gastroenterology, Department of Internal Medicine, Chonnam National University Medical School, Gwangju, Korea
Correspondence to: Kyu Chan Huh, Department of Internal Medicine, Konyang University College of Medicine, 158 Gwanjeodong-ro, Seo-gu, Daejeon 302-718, Korea, Tel: +82-42-600-9370, Fax: +82-42-600-9091, E-mail: kchuh2020@hanmail.net
This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
We investigated whether sodium picosulfate with magnesium citrate (SPMC) plus bisacodyl compares favorably with conventional polyethylene glycol (PEG) with respect to bowel cleansing adequacy, compliance, and safety.
We performed a multicenter, prospective, single-blinded study in outpatients undergoing daytime colonoscopies. Patients were randomized into a split preparation SPMC/bisacodyl group and a conventional split PEG group. We compared preparation adequacy using the Boston bowel preparation scale (BBPS), ease of use using a modified Likert scale (LS), compliance/satisfaction level using a visual analogue scale (VAS), and safety by monitoring adverse events during the colonoscopy between the two groups.
A total of 365 patients were evaluated by intention to treat (ITT) analysis, and 319 were evaluated by per protocol (PP) population analysis (153 for SPMC/bisacodyl, 166 for PEG). The mean total BBPS score was not different between the two groups in both the ITT and PP analyses (p>0.05). The mean VAS score for satisfaction and LS score for the ease of use were higher in the SPMC/bisacodyl group (p<0.001). The adverse event rate was lower in the SPMC/bisacodyl group than in the PEG group (p<0.05).
The SPMC/bisacodyl treatment was comparable to conventional PEG with respect to bowel preparation adequacy and superior with respect to compliance, satisfaction, and safety.
Keywords: Colonoscopy, Bowel preparation, Sodium picosulfate with magnesium citrate, Polyethylene glycols
Colonoscopy is considered the most effective colorectal cancer screening procedure.1 The maximal preventative effect of colonoscopy requires adequate visualization of the entire colon to facilitate detection and removal of all adenomas, which involves detailed observations associated with cecal intubation, longer withdrawal time, and adequate preparation. Bowel preparation is the most important colonoscopy quality indicator because it affects both the cecal intubation and adenoma detection rates.
The ideal preparation procedure should clean the colon without mucosal damage, electrolyte imbalance, or patient discomfort. The most commonly used preparation regimens are based on polyethylene glycol (PEG). PEG is a safe and highly effective colon cleansing agent that is widely accepted as a standard bowel preparation regimen.2,3 However, ingestion of a large volume of PEG, as well as its unpleasant taste, results in low compliance rates and unsatisfactory cleansing quality.4–6 The adequate cleansing rate by conventional PEG bowel preparation has been reported to be 70% to 77% by meta-analyses,2,5–7 which is similar to that in Korea (47% to 76%).8–11
Sodium picosulfate with magnesium citrate (SPMC) is a low-volume, dual-action bowel-cleansing agent used mostly in the United Kingdom and Canada as a tolerable preparation agent.12–15 Recently, SPMC was approved in the United States for bowel preparation before colonoscopy and it is also available in Korea as Picolight powder® (Phambio Korea Co., Ltd., Seoul, Korea).16,17 Each sachet of Picolight powder® contains 12-g citrate, 3.5-g magnesium oxide, an osmotic laxative, and 10-mg sodium picosulfate hydrate, a stimulant laxative. These ingredients are identical to those in Picolax® (Ferring, West Drayton, UK) and Pico-Salax® (Ferring, North York, Canada). SPMC acts locally in the colon as both a stimulant laxative by increasing the frequency and the force of peristalsis and promoting electrolyte and water retention in the colon, and an osmotic laxative by retaining fluids in the colon.18 In previous meta-analyses, SPMC was well tolerated by patients but may be less efficacious than other agents.14,19–21 Recently, several studies have investigated various methods of improving the cleansing efficacy of SPMC, including the addition of a laxative with SPMC, consuming fluids with SPMC, and the three-sachet-split method.22,23 However, these studies were conducted largely in Western populations12–15 and SPMC preparation has not been studied in an Asian population.
We conducted this study to investigate the cleansing efficacy, safety and tolerability of SPMC with bisacodyl as a substitute bowel preparation method to conventional large volume PEG in Koreans.
This was a multicenter, randomized, single blind, noninferiority trial conducted at 13 institutions belonging to the intestinal tumor research group of the Korean Association for the Study of Intestinal Disease (KASID) from June 2012 to January 2013. All participating endoscopists were faculty of a university hospital with colonoscopy expertise. Bias in endoscopist evaluation of colon cleansing was minimized by use of a single investigator blind design.
All subjects 20 to 75 years of age undergoing elective daytime outpatient colonoscopy at each institution were enrolled in this study. Exclusion criteria included previous colorectal surgery, ileus or bowel obstruction, significant constipation defined as <3 bowel movements per week with or without regular laxatives, ascites, heart failure, ischemic heart disease or coronary vessel disease within the last 6 month, inflammatory bowel disease, pregnancy, cognitive impairment, and renal impairment. This study was approved by the Institutional Review Board of each participating institution and registered with the open registry of the Clinical Research Information Service (http://cris.nih.go.kr) under the identifier KCT0000580. After informed consent, the patients were randomly assigned to one of two fixed-dose treatment arms, either split-dose SPMC with bisacodyl or splitdose PEG. Randomization was conducted using a computergenerated table prepared by an independent biostatistician.
All enrolled patients were instructed to consume a low-fiber diet 3 days before colonoscopy and fast in the evening of the day before colonoscopy. Participants in the SPMC group were given Picolight powder® (Phambio Korea Co., Ltd.) and instructed to ingest one sachet with 150-mL water followed by 2-L of water at 7 PM the day before the procedure and ingest another sachet with 150-mL water followed by 2-L water 4 hours before colonoscopy, based on previous reports.23 Participants in the SPMC group were further instructed to ingest two 5-mg bisacodyl tablets the night before colonoscopy. Those patients receiving standard PEG were instructed to use the split-dose method, whereby 2-L PEG for ingestion at 6 PM the day before colonoscopy and another 2-L PEG 4 hours before colonoscopy. All colonoscopies were scheduled to be performed before 13:00 hours.
The primary outcome was comparison of the colon-cleansing efficacy between the two preparation groups. Bowel cleansing was assessed by endoscopists who were blinded to the preparation method during the withdrawal phase of colonoscopy using the Boston bowel preparation scale (BBPS), a validated tool for assessment of the quality of colon cleansing.24 Each of the three segments of the colon (right, including the cecum and ascending colon; transverse, including the hepatic and splenic flexures; and left, including the descending colon, sigmoid, and rectum) was given a score from 0 to 3, defined as follows: 0=unprepared colon segment with mucosa not visible due to remnants of solid stool that cannot be cleared; 1=portion of mucosa of the colon segment seen, but other areas of the colon segment not as visible because of staining, residual stool, and/or opaque liquid; 2=minor amount of residual staining, small fragments of stool, and/or opaque liquid, but mucosa of colon segment visible; 3=entire mucosa of colon segment visible, with no residual staining, small fragments of stool, or opaque liquid.24 Adequate bowel preparation was defined a score ≥2 for all segments. Inadequate preparation was defined as a summed BBPS score <6 or a score in any segment <2.
Satisfaction with the preparation agent was assessed using a visual analogue scale (VAS) as 0 (worst) to 10 (best) on a questionnaire to patients. The tolerability of the bowel preparation was assessed via a standardized questionnaire administered to patients on the day of the colonoscopy, before receiving any preliminary sedation for the procedure. The questionnaires for the assessment of tolerability were composed of four sections describing the completeness of agent consumption, the ease, the taste and the intention to reuse the preparation. Patient could choose only one item for their responses.
The questionnaire for the completeness of agent consumption was as follows for the SPMC/bisacodyl group: (1) ‘2 sachets completely taken,’ or ‘not’; (2) additional water consumption completeness, ‘2-L for each sachet,’ ‘less than 2-L for each sachet,’ ‘1-L for each sachet,’ ‘less than 1-L for each sachet’; (3) overnight two tablets of bisacodyl, ‘completely taken,’ or ‘not.’
The questionnaire for the completeness of agent consumption was as follows for the conventional PEG group: ‘4-L completely taken,’ ‘over 75% taken,’ ‘over 50% taken,’ ‘less than 50% taken.’ The questionnaire regarding ease of use and taste of the bowel preparation was based on a modified five-point Likert scale (LS): ‘very easy (5 points),’ ‘easy (4 points),’ tolerable (3 points),’ ‘difficult (2 points),’ very difficult (1 point)’ and for taste as five points: ‘very good (5 points),’ ‘good (4 points),’ fair (3 points),’ ‘bad (2 points),’ ‘worst (1 point).’22 We determined ‘the tolerable group’ as those participants who selected three points or more in each of the assessments of ease of use and taste.
Safety was assessed by the incidence of adverse events reported as a ‘yes’ or ‘no’ response in a questionnaire and colonic mucosal change. Adverse events were defined as nausea, vomiting, abdominal pain, bloating, thirst, dizziness, or paresthesia during consumption of the preparation agents. The presence of mucosal changes including erythema or aphthous lesions, were recorded by endoscopists after colonoscopy. Blood chemistry and electrolyte level were not essential tests and were evaluated only when the patients had severe side effects, as determined by the endoscopist.
In calculating the sample size, we assumed a successful cleansing rate of 85% for the conventional PEG preparation based on previous data.5,13 We specified a noninferiority margin of −15% for the difference in adequate preparation rates defined as the rate in the SPMC/bisacodyl group minus the rate in the PEG group, and a one-sided significance level of 0.025. Assuming a 10% dropout rate, we calculated that we would need to enroll 186 patients in each group for an 80% statistical power to demonstrate noninferiority.
The intent to treat (ITT) population included all randomized participants and the patient who underwent colonoscopy. The per protocol (PP) population was determined as the enrolled patient who completed bowel preparation according to the preparation instructions for each and underwent colonoscopy. The outcome measurement and statistical analyses of cleansing efficacy, tolerability, satisfaction, and safety were performed for both the ITT and PP populations. The safety analysis was performed for the ITT population.
We assessed noninferiority by comparing the lower bound of the one-sided 97.5% confidence interval (CI) for the rate difference to −15% and testing the corresponding hypothesis that the difference would be >−15%.
Total BBPS, VAS, and the ease of use and taste scores were analyzed as a continuous variable, after confirmation of normal distribution, by Student t-test. We compared percentages of the BBPS score of each segment of colon, the completeness of preparation agents, the tolerability, ease of use, and taste based on a standardized patient questionnaire, and the incidence of both side effects and mucosal change between the groups using a Pearson chi-square test of Fisher exact test for pooled responses and records. All statistical analyses were performed using SAS version 9.3 (SAS Institute Inc., Cary, NC, USA). Statistical significance was defined as p<0.05.
Most of the participants that received SPMC/bisacodyl were able to consume the split dose of SPMC both on the day before (100%) and the day of (99.7%) the colonoscopy. The ratio of completeness of agent consumption was markedly higher in the SPMC/bisacodyl (99.4%) than conventional PEG (90.2%) groups (p<0.001). However, 28 patients in the SPMC/bisacodyl group and 18 in the PEG group did not complete the entire preparation process. Excluding these 46 patients, 319 patients (153 in the SPMC/bisacodyl, 166 in the PEG group) completed the entire preparation process and were analyzed as the PP population.
During the detailed preparation process for the SPMC/bisacodyl group, two tablets of 5-mg bisacodyl were consumed by 97.8% (n=179) of patients. However, 2-L of water was consumed after each sachet of SPMC by only 74% (n=134) of patients. Overall, 86% (n=156) of participants that received SPMC with bisacodyl consumed >75% of the total volume of water (3-L) after SPMC sachet consumption.
The SPMC/bisacodyl group achieved better overall colon cleansing than the PEG group, as measured by the ratio of adequate preparation based on BBPS. In the ITT analysis, the adequate preparation rate was 87.9% in the SPMC/bisacodyl group and 81.0% in the PEG group, similar to the results of the PP analysis (86.9% SPMC/bisacodyl vs 83.7% in the PEG group). The rate difference, defined as the rate of the SPMC/bisacodyl group—the rate in the PEG group, was 6.9% in the ITT analysis and 3.2% in the PP analysis. The lower bound of the one-sided 97.5% CI for rate difference rate was greater than the noninferiority margin of −15%, demonstrating noninferiority of the SPMC with bisacodyl group to the PEG group in both the ITT (one-sided 97.5% CI, −0.5% to 14.3%; p<0.001) and PP (one-sided 97.5% CI, −4.6% to 10.9%; p<0.001) analyses. However, there was no significant difference in mean BBPS when comparing the cleansing effect between the two preparation methods (Table 2). The mean BBPS of all colon segments for each group was higher than 2 points. The percentage of each BPSS score in all segments was also similar between the two preparation methods (Fig. 1).
The mean VAS scale of the SPMC/bisacodyl group was significantly superior to the PEG group, in both ITT (7.58±1.94 vs 5.79±2.43, p<0.001) and PP (7.62±1.95 vs 5.92±2.35, p<0.001) (Fig. 2). SPMC with bisacodyl was better tolerated than PEG with respect to ease of use and taste (Fig. 3). Using a modified five-point LS, the mean score for ease of use of SPMC/bisacodyl was higher than that of PEG (ITT, 3.57±0.82 vs 2.59±0.79, p<0.001; PP, 3.56±0.81 vs 2.63±0.78, p<0.001). The mean score for taste of SPMC/bisacodyl was also superior to that of PEG (ITT, 3.65±0.73 vs 2.60±0.79, p<0.001; PP, 3.69±0.71 vs 2.64±0.77, p<0.001). Furthermore, the ‘tolerable group’ ratio was a significantly higher proportion of the SPMC/bisacodyl than PEG with respect to ease of use (ITT, 94.5% vs 63.0%, p<0.001; PP, 94.8% vs 65.7%, p<0.001) and taste (ITT, 97.8% vs 60.3%, p<0.001; PP, 98.0% vs 61.4%, p<0.001). Finally, a positive response regarding the intention to reuse the received agent was higher in the SPMC/bisacodyl group than the PEG group (ITT, 83.2% vs 48.5%, p<0.001; PP, 80.5% vs 49.5%, p<0.001).
The overall prevalence of adverse effects related to preparation was lower in the SPMC/bisacodyl group than the PEG group (65.2% vs 77.7%, p=0.011). Symptoms of vomiting, abdominal pain, and paresthesia occurred at a similar rate in both groups, while nausea, bloating, thirst were more common in the conventional PEG group and dizziness was more common in the SPMC/bisacodyl group (Table 3). Mucosal changes including erythema (5.5% of the SPMC/bisacodyl group vs 4.9% of the PEG group by PP analysis, p=0.139) and aphthous lesion (2.2% in the SPMC/bisacodyl group only) were observed in only a small number of patients in each group.
Blood chemistry tests for serum electrolytes and renal function (blood urea nitrogen and creatinine) were performed in 58 participants. There was no difference in the blood examination rate between the groups (14.9% of SPMC/bisacodyl vs 16.8% of PEG group). While there were no abnormal blood chemistry findings in the SPMC/bisacodyl group, one hyponatremia and two hypochloridemia cases were identified in the patients who received conventional PEG preparation in the ITT population.
Although the small volume of SPMC is well tolerated and results in improved preparation compliance, its cleansing effect remains uncertain. Some studies in the United Kingdom reported that SPMC was less effective than conventional PEG in bowel preparation before colonoscopy.12–14 To improve the cleansing effect of SPMC, a split method using two sachets taken the evening the day before colonoscopy and 4 to 5 hours before colonoscopy, combined with a laxative, has been proposed.22,23,25 Additionally, sufficient fluid intake is critical to the quality of preparation with SPMC; 1.5- to 2-L are recommended for each sachet.23,26
In the current study, we based the SPMC and bisacodyl combination method used on previous comparisons of cleansing efficacy with that of conventional PEG.16,17,22 We designed the split SPMC method to comprise ingestion of two sachets of SPMC with 2-L of water per sachet, in combination with 10-mg bisacodyl. We also educated all participants to partake in a low-fiber diet 3 days before colonoscopy.27 With this preparation protocol, the adequate preparation rate of SPMC/bisacodyl was comparable to that of conventional PEG in both the ITT and PP analyses. In the noninferiority analysis, the lower bound of CI for the difference in the adequate preparation rate was greater than the noninferiority margin hypothesized in this study, and fulfilled the noninferiority condition. There were no differences in the mean BBPS scores and BBPS percentage scores in the right, transverse and left colon. Favorable comparisons between SPMC and PEG were likely due to the additional bisacodyl given to the SPMC group. Bisacodyl is a stimulant laxative that works directly on the colon to increase the frequency and force of peristalsis and enhance bowel movement. Therefore the use of a stimulant laxative in this study might have overcome the reported weaknesses of a SPMC-only preparation, especially in the right colon cleansing.12–14,22
In addition to addition of a stimulant laxative to the SPMC preparation regimen, sufficient fluid intake following each sachet of SPMC is also important. Good quality cleansing with at least 3-L of total fluid intake in SPMC preparations has been reported.16,17,22 Interestingly, SPMC/bisacodyl was significantly superior to conventional PEG with respect to satisfaction and tolerability, even though the patients were instructed to consume 2-L of water following ingestion of 150 mL with the SPMC sachet and only 74% of patients consumed the recommended fluid volume, lower than that for conventional PEG (90.2%) in the current study. Sufficient fluid intake is likely the most difficult obstacle to overcome in SPMC preparation. Although, we designed 2-L of fluid intake following ingestion of each SPMC sachet in this study, 1.5-L of fluid intake per sachet may be appropriate based on the excellent results reported previously.16,17,23
In our study, PEG produced more symptoms of nausea, bloating and thirst, which may be related to the taste and large volume. SPMC produced more dizziness, which may be a result of biochemical derangements and dehydration. Reports of the biochemical and hemodynamic effects of SPMC are limited. Given that SPMC acts in a similar fashion to sodium phosphate, SPMC is likely to cause similar fluid and electrolyte shifts. In one study, PEG was associated with a significant decrease in potassium, while SPMC was associated with significant decreases in chloride and significant increases in magnesium.14 In 2002, the Australian Adverse Drug Reactions Advisory Committee described 16 cases of serious adverse events with SPMC with no fatalities, eight reports of adverse events associated with hyponatremia, and four reports of syncope and dehydration without documented electrolyte abnormalities.28 Electrolyte abnormalities resulting in seizures were reported in a patient using SPMC.29 In the current study, blood chemistry and electrolyte tests were performed only when patients developed severe side effects, a total of 15.9% of the participants, with no abnormal findings. These safety results may be related to our exclusion of patients with serious comorbidities, such as renal impairment and cardiovascular concerns, and those older than 75 years. Although the normal blood test results in the SPMC/bisacodyl group may reflect the safety of SPMC to the healthy group, further evaluation regarding the safety of SPMC/bisacodyl is necessary.
Mucosal changes, including inflammation and ulceration, were reported in 3.5% of patients who received the SPMC preparation,30 which is similar to the SPMC/bisacodyl in the current study. Although a previous study reported that the rate of acute mucosal inflammation was 10-fold higher in patients receiving SPMC than PEG,30 our data suggest no difference in mucosal inflammation, such as erythematous changes or aphthous lesions.
Our study was limited in that we did not confirm interobserver agreement in the BBPS. However, we instructed the participating endoscopists in using the BBPS, a valid and reliable instrument for assessing bowel cleanliness, in detail in the study protocol. BBPS is easier to assess than the Ottawa scale, and no difficulties were encountered because all of the endoscopists were skilled in colonoscopy. Although the current study was designed to be single-blinded due to the differences in the administration of bowel preparations, and this represents a potential source of bias, precautions were taken to ensure the endoscopists remained blinded to the bowel preparation method. In particular, our findings suggest that SPMC/bisacodyl has advantages with respect to bowel cleansing, tolerability and safety compared to conventional PEG; however, our findings should not be generalized to a high-risk population because we excluded patients with renal insufficiency and cardiovascular concerns. The broad noninferiority margin (15%) is one of the weak points of the current study. Although its range estimated based on previous studies might be wide,5,13 the cleansing effect of SPMC with bisacodyl was comparable to that of conventional PEG not only in the noninferiority analysis but also in the simple comparison using the mean BBPS score and adequate preparation rate.
In conclusion, this is the first prospective randomized controlled study of SPMC conducted at multiple institutions in Korea and the first in an Asian population. The results indicate that split dosing of SPMC with bisacodyl was comparable to conventional PEG with respect to preparation adequacy and superior to conventional PEG with respect to tolerability, satisfaction and safety. Therefore, a split dosing of SPMC with bisacodyl is a good substitute for conventional PEG preparation before colonoscopy.
This study was conducted by the intestinal tumor research group of the Korean Association for the Study of Intestinal Disease (KASID).
CI, confidence interval.
Table 1 Demographics and Baseline Characteristics of the Intention to Treat Population
Parameter | SPMC with bisacodyl (n=181) | Conventional 4-L PEG (n=184) | p-value* |
---|---|---|---|
Male sex | 94 (51.9) | 100 (54.4) | 0.644 |
Age, yr | 53.5±10.7 | 53.8±10.4 | 0.788 |
20–64 | 154 (85.1) | 154 (83.7) | 0.715 |
≥65 | 27 (14.9) | 30 (16.3) | |
Indication for colonoscopy | 0.195 | ||
Symptom evaluation | 38 (21) | 37 (20.1) | |
Screening | 68 (37.6) | 79 (42.9) | |
Surveillance | 50 (27.6) | 34 (18.5) | |
For endoscopic treatment | 25 (13.8) | 34 (18.5) |
Data are presented as mean±SD or number (%).
SPMC, sodium picosulfate with magnesium citrate; PEG, polyethylene glycol.
Table 2 Efficacy of Bowel Cleansing in Patients Undergoing Colonoscopy Using the Boston Bowel Preparation Scale
Colon segment | ITT population (n=365) | PP population (n=319) | ||||
---|---|---|---|---|---|---|
SPMC with bisacodyl (n=181) | Conventional 4-L PEG (n=184) | p-value* | SPMC with bisacodyl (n=153) | Conventional 4-L PEG (n=166) | p-value* | |
Right colon | 2.3±0.7 | 2.2±0.8 | 0.144 | 2.3±0.6 | 2.2±0.7 | 0.391 |
Transverse colon | 2.5±0.6 | 2.5±0.6 | 0.834 | 2.5±0.6 | 2.5±0.6 | 0.998 |
Left colon | 2.5±0.6 | 2.4±0.7 | 0.507 | 2.5±0.6 | 2.3±0.6 | 0.913 |
Total colon | 7.3±1.6 | 7.2±1.7 | 0.329 | 7.3±1.6 | 7.2±1.6 | 0.680 |
Data are presented as mean±SD.
ITT, intention to treat; PP, per protocol; SPMC, sodium picosulfate with magnesium citrate; PEG, polyethylene glycol.
Table 3 Comparison of Preparation-Related Adverse Events Using Intention to Treat Analysis
Adverse effect | SPMC with bisacodyl (n=181) | Conventional 4-L PEG (n=184) | p-value* |
---|---|---|---|
Nausea | 52 (28.7) | 78 (42.4) | 0.006 |
Vomiting | 23 (12.7) | 31 (16.9) | 0.265 |
Abdominal pain | 48 (26.5) | 44 (23.9) | 0.566 |
Bloating | 70 (38.7) | 103 (56.0) | 0.001 |
Thirst | 19 (10.5) | 39 (21.2) | 0.005 |
Dizziness | 44 (24.3) | 27 (14.7) | 0.020 |
Parasthesia | 3 (1.7) | 6 (3.3) | 0.503 |
Data are presented as number (%).
SPMC, sodium picosulfate with magnesium citrate; PEG, polyethylene glycol.