Mehdi Ouaïssi 1, 2, 3 and Stephanie Tran 1, 2, 3 and Diane Mege 1, 2, 3 and Vivien Latrasse 1, 2, 3 and Alain Barthelemy 4 and Nicolas Pirro 1 and Philippe Grandval 5 and James Lassey 2 and Igor Sielezneff 1, 2 and Bernard Sastre 1, 2, 3 and Mathieu Coulange 1, 4
Academic Editor:Lorenzo Fuccio
1, Aix-Marseille University, UMR 911, Campus Sante Timone, 13005 Marseille, France
2, Department of Digestive Surgery, AP-HM Timone Hospital, Pôle DACCORD, 13385 Marseille, France
3, Atelier Provençal d'ecriture Medicale, France
4, Hyperbaric Medicine, Sainte Marguerite Hospital, Aix-Marseille University, UMR MD2, 13385 Marseille, France
5, Department of Gastroenterology, AP-HM Timone Hospital, Pôle DACCORD, 13385 Marseille, France
Received 22 June 2013; Revised 8 October 2013; Accepted 4 November 2013; 27 January 2014
This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
1. Introduction
Pelvic radiation disease (PRD) induced by radiation occurs in 2-11% of patients undergoing pelvic radiation for urologic and gynecologic malignancies [1-4]. PRD occurs 3 months after radiotherapy and is characterized by the painless passage of blood per rectum (clots or streaking of the stool), mucous rectal discharge, frequent bowel movements, and rectal pain. Less commonly, bowel obstruction, fistulae, bowel perforation, and severe rectal bleeding requiring blood transfusions are observed. Treatments for PRD are not universally successful. Current modalities include pharmacological agents such as oral and rectal steroids, 5-amino salicylates, sucralfate, short chain fatty acid enemas, oral metronidazole, and oral vitamins E and C [5, 6]. Acute hemorrhage could imply local haemostatic treatments including topical formalin, yttrium-aluminum-garnet (YAG), laser and/or surgical intervention consisting of defunctioning colostomy in severe cases [5]. Hyperbaric oxygen therapy (HBOT) has previously been described as a noninvasive therapeutic option for the treatment of radiation PRD [7]. HBOT is thought to promote neovascularization by improving oxygenation thus increasing the p02 and promoting wound healing in the damaged rectal mucosa, thereby reducing bleeding [8]. Cochrane's review concludes that HBOT in late tissue radiation injury is associated with improved outcome though the review was based on small trial series. In the present study, we are assessing the efficacy of HBOT in 44 consecutive patients with PRD who were resistant to conventional oral or topical treatments [6].
2. Materials and Methods
2.1. Type of Study
Between January 2001 and December 2009, forty-four patients with PRD, from the department of digestive surgery and hyperbaric Medicine unit prospectively included in this study and treated with HBOT. Before treatment, PRD was confirmed by sigmoidoscopy and biopsy in all patients.
2.2. Types of Participants
We included all patients with PRD following radiation therapy for pelvic cancer. The patient characteristics are listed in Table 1. There were anal cancer ( [figure omitted; refer to PDF] %), prostate cancer ( [figure omitted; refer to PDF] %), uterine cancer ( [figure omitted; refer to PDF] %), and other types of cancer ( [figure omitted; refer to PDF] %) (Table 1). Diagnosis of PRD was established by endoscopy showing edematous and inflamed mucosa. PRD symptoms are tenesmus, rectal bleeding, stenosis, occlusion/constipation, fistulas, and incontinence. All patients were free of oncological disease.
Table 1: Demographical data of population.
| [figure omitted; refer to PDF] (%) |
Age (years) |
|
Median | 65.7 (39-85) |
Gender |
|
Female | 18 (41) |
Male | 26 (59) |
Comorbidities |
|
Diabetes | 2 (4.5) |
Hypertension | 16 (36.4) |
Arteriopathy | 9 (20.4) |
Tabaco | 16 (36.4) |
Coronary disease | 7 (15.9) |
Corticotherapy | 5 (11.3) |
Immunosuppressive treatment | 15 (34) |
| |
Type of cancer treated by radiation |
|
Prostate | 18 (40.9) |
Anal | 8 (18.2) |
Gynecologic cancer |
|
Uterus | 8 (18.2) |
Endometrial | 5 (11.3) |
Another | 5 (11.3) |
2.3. Types of Outcome Measures
The Undersea and Hyperbaric Medical Society defines HBOT as a treatment where a patient intermittently breathes 100% oxygen while the treatment chamber is pressurized to greater than sea level (1 absolute atm ATA). HBOT is thought to promote neovascularization by improving oxygenation thus increasing the pO2 to the damaged tissue, normalizing the tissue, and promoting wound healing to the damaged rectal mucosae, thereby reducing bleeding.
All patients received HBOT as a treatment of their PRD. The chamber was pressurized to 2.5 absolute atm and patients were treated for 60 minutes with 100% oxygen. Before HBOT, a history and physical investigation was performed by HBOT-trained specialists to validate the indication and eliminate the contraindications to HBO. Standard administration of HBOT was 20 sessions and was continued until a decrease in symptoms was observed. Treatment was given on a once-a-day basis, 5 to 7 days a week.
The pretreatment characteristics of the patients, the type of radiation received, SOMA-LENT score [9], the number of HBOT, the timing of the onset and reduction of symptoms, endoscopic injuries, the severity of the CRP, and the toxicity of treatment were collected prospectively.
The SOMA-LENT Scale (Table 2) [9] evaluates three different fields. First, subjective symptoms including tenesmus, mucus loss, defecation frequency, and pain and then objective symptoms including bleeding, ulceration, and stenosis are assessed. The third part details the medical management of all the symptoms (tenesmus and defecation frequency, pain, bleeding, ulceration, stenosis, and incontinence). The SOMA-LENT Scale defines 4 grades of increasing severity, of each criterion. The score can range from 0 to 56.
Table 2: SOMA-LENT Scale [9-22].
| Grade 1 | Grade 2 | Grade 3 | Grade 4 | Score |
Subjective |
|
|
|
|
|
Tenesmus | Occasional urgency | Frequent urgency | Constant urgency | Nonresponder |
|
Mucus lost | Occasional | Frequent | Constant | Nonresponder |
|
Incontinence | Occasional | Frequent | Constant | Nonresponder |
|
Defecation frequency | 2-4 times/day | 4-8 times/day | >8 times/day | Incontrol diarrhea |
|
Pain | Occasional and minimal | Frequent and tolerable | Constant and intense | Nonresponder and atrocious |
|
Objective |
|
|
|
|
|
Bleeding | Hide | Occasional >2/week | Constant/daily | Brutal bleeding |
|
Ulceration | Superficial <=1 cm² | Superficial >1 cm² | Deep ulcer | Perforation. Fistula |
|
Stenosis | >2/3 normal diameter without dilation | 1/3 a 2/3 normal diameter with dilation | <1/3 normal diameter | Complete stenosis |
|
Management |
|
|
|
|
|
Tenesmus and defecation frequency | Occasional <=2 antidiarrhea medication/week | Usually >2 antidiarrhea medication/week | Several >2 antidiarrhea medication/day | Surgery/colostomy |
|
Pain | Occasional, nonopiate treatment | Usually nonopiate treatment | Usually with opiate treatment | Surgery |
|
Bleeding | Laxatives, for treatment | Occasional blood transfusion | Frequent blood transfusion | Surgery/colostomy |
|
Ulceration | Dietary management, laxatives | Occasional corticosteroids | Steroids rectal injection, HBOT | Surgery/colostomy |
|
Stenosis | Dietary management | Occasional dilation | Usually dilation | Surgery |
|
Incontinence | Occasional use of protective pads | Frequent use of protective pads | Constant use of protective pads | Surgery/colostomy |
|
2.4. Statistical Analysis
Values are expressed as mean, median, and range. Statistical analysis was performed using GraphPad Software. Data are expressed as mean ± standard deviation or median with interquartile range. The differences between the two groups were analyzed using the Mann-Whitney [figure omitted; refer to PDF] test or Student's [figure omitted; refer to PDF] -test. One-way analysis of variance or Kruskal-Wallis test was performed to compare more than two groups. Multivariate survival analysis using Cox's regression model was conducted. To compare categorical variables, the chi-square or Fisher exact test was used. Kaplan-Meier method was used to estimate overall and relapse-free survival. For all tests, a [figure omitted; refer to PDF] value of less than 0.05 was considered significant.
3. Results
The median age of the cohort was 65.7 years (39-85). There were 18 females and 26 males. Median of delay between radiotherapy and the beginning of PRD symptoms was 16 months and the median of delay between radiotherapy and HBOT was 26 months (3-175). The median of followup was 8 months (3-17). PRD was associated chronic phase of radiation-induced damage in bladder for 17 patients (38%), in ileum for 2 patients (4%), and in sigmoid for 4 patients (9%).
Before HBOT, all patients had oral or topical treatments. Twenty-seven percent of patients required blood transfusion ( [figure omitted; refer to PDF] ). Electrocautery or argon plasma was performed on 13.6% ( [figure omitted; refer to PDF] ) of patients. Corticosteroids enema was used on 29.6% ( [figure omitted; refer to PDF] ) of patients; 6 of these patients also received formol enema. Twenty-seven percent ( [figure omitted; refer to PDF] ) of patients required colostomy due to anal incontinence ( [figure omitted; refer to PDF] ), stenosis ( [figure omitted; refer to PDF] ), and fistula or sepsis ( [figure omitted; refer to PDF] ). No medical treatment was performed during HBOT.
The median number of sessions was 35, ranging from 6 to 90. Only one patient stopped precociously the HBOT (after 6 sessions) due to transient myopia.
At the end of followup twenty-six patients (59%) had a decreased SOMA-LENT score after HBOT, ten patients (22.8%) had a SOMA-LENT score unmodified, and eight patients (18.3%) showed an increase of the SOMA-LENT score. The median of SOMA-LENT score before HBOT was significantly greater, 14 (0-36), than after HBOT with the SOMA-LENT score of 12 (0-38) ( [figure omitted; refer to PDF] ) (Figure 1).
Figure 1: Median score for SOMA-LENT before HBOT versus SOMA-LENT after HBOT per patient and per symptom. * [figure omitted; refer to PDF] . HBOT: hyperbaric oxygen therapy. Managing bleeding: patient required instrumental and/or blood transfusion Bleeding: patients with acute rectorrhagia.
[figure omitted; refer to PDF]
HBOT decreased many symptoms: tenesmus, mucus loss, defecation frequency, bleeding, ulceration, and stenosis, with significant difference in tenesmus ( [figure omitted; refer to PDF] ), bleeding ( [figure omitted; refer to PDF] ), ulceration ( [figure omitted; refer to PDF] ), and management of ulceration ( [figure omitted; refer to PDF] ) after HBOT (Figure 1). Concerning patients with colostomy, 33% ( [figure omitted; refer to PDF] ) benefited from colostomies closure.
HBOT was generally well tolerated. Four patients had transient hearing problems. No cancer recurrence was found.
4. Discussion
PRD is seen after radiotherapy for any pelvic malignancy, including that of the bladder, the prostate, and the uterus. Although the complex pathological process of radiation-induced injury to the rectum begins immediately following exposure, it may require weeks to months to become clinically apparent [3, 4]. Late effects of radiation are seen from damaged to slowly replicating cells and by the induction of proinflammatory and procoagulation cytokine signaling pathways, leading to edema, fibrosis, and ultimately ischemia in the muscularis [10]. It is estimated that up to 30% of patients undergoing pelvic radiotherapy have acute rectal toxicities with 15% of patients experiencing chronic symptoms [11].
There are no standard therapies for radiation-induced proctopathy and a number of treatments have been described with varying efficacy, including pharmacotherapy, sclerotherapy, and HBOT [5].
By increasing systemic oxygen partial pressure, HBOT increases the delivery of oxygen to ischemic tissues [12], thereby promoting angiogenesis, nutrient influx, and fibroblast proliferation [12]. Several small retrospective series suggest that hyperbaric oxygen can successfully treat radiation-induced proctopathy with response rates between 40% and 60% [13]. A recent randomized, placebo controlled trial showed statistically significant improvement in wound healing with hyperbaric oxygen in patients with late radiation tissue necrosis compared to patients receiving normal air at 2 atmospheres [14]. In our study we demonstrate that HBOT had a significant impact on decreasing tenesmus and hemorrhage. Many patients had a failed medical treatment before HBOT as reported in a randomized control trial [14].
Our study population consisted of patients with severe radiation proctopathy after radiotherapy for pelvic cancer in whom multiple attempts at management including steroid injection, anti-inflammatory suppositories, and argon plasma laser coagulation failed. Due to our relatively small sample size, no inferences can be made on the outcomes in relation to prior treatments received. However, rectal bleeding was significantly reduced with an improvement in more than half of the patients. Rectal ulcers showed favorable responses to HBOT with partial or complete resolution in 20% of patients.
We used a standard scoring system to directly compare our outcomes to those from other series. Fewer than 20% of patients with this degree of injury heal spontaneously. Our series showed a favorable response (60% improved) with HBOT in patients with severe radiation proctitis refractory to treatment. Improvements were seen in mucus lost, defecation frequency, pain, stenosis, bleeding, and ulceration, and especially in tenesmus, bleeding, and ulceration which seemed to be most improved.
The optimal dose of oxygen is not known. In our study, we used an average of 35 treatments. Using an average of 24 treatments (two atmospheres for 105 min per session), Woo et al. reported improvement in 10 of 18 study patients with radiation proctitis [15]. Furthermore, Feldmeier et al. have reported their experience in using HBOT in eight patients with large or small bowel injuries who were given a median number of 20 treatments, whereby 75% of those who had at least 22 treatments had complete resolution of their symptoms [16]. Shorter durations (60 min) to enhance patient compliance and 26 treatment sessions have been used by Mayer and colleagues [17]. This prospective study, although nonrandomized with a small sample size, suggests a significant and prolonged response with HBOT in a challenging patient population. Overall the prognosis is favorable and further studies will require long-term followup to determine the durability of response to HBOT [18].
The most common complications experienced with HBOT delivery are mild and transient, including barotraumatic otitis, confinement anxiety, temporary myopia, and euphoria. More severe effects include rare seizures from central nervous system oxygen toxicity and pulmonary oxygen toxicity. In a series of 782 patients undergoing HBOT, 17% experienced ear pain with 3.4% having visually confirmed barotraumatic otitis [19]. In our series of 44 patients, HBOT was extremely well tolerated with only one patient who stopped HBOT for reversible myopia. Otherwise, our study as in the literature [16] is not in favor of increased risk of cancer recurrence.
This study confirms the interest of HBOT in chronic radiation proctitis resistant to conventional treatments [20, 21]. A multicenter study comparing HBOT with conventional treatments would clarify the role of this indication.
Conflict of Interests
The authors declare that there is no conflict of interests regarding the publication of this paper.
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Copyright © 2014 Mehdi Ouaïssi et al. This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
Abstract
Pelvic radiation disease (PRD) occurs in 2-11% of patients undergoing pelvic radiation for urologic and gynecologic malignancies. Hyperbaric oxygen therapy (HBOT) has previously been described as a noninvasive therapeutic option for the treatment of PRD. the purpose of study was to analyze prospectively the results of HBOT in 44 consecutive patients with PRD who were resistant to conventional oral or topical treatments. Material and Methods. The median age of the cohort was 65.7 years (39-85). Twenty-seven percent of patients required blood transfusion ( n = 12 ). The median of delay between radiotherapy and HBOT was 26 months (3-175). We evaluated the results of HBOT, using SOMA-LENT Scale. Results. SOMA-LENT score was decreased in 59% of patient. The median of SOMA-LENT score before HBOT was significantly higher, being equal to 14 (0-36), than after HBOT with the SOMA-LENT score of 12 (0-38) ( P = 0.003 ). Tenesmus ( P = 0.02 ), bleeding ( P = 0.0001 ), and ulceration ( P = 0.001 ) significantly decreased after HBOT. Regarding patients with colostomy, 33% ( n = 4 ) benefited from colostomies closure. HBOT was generally well tolerated. Only one patient stopped precociously due to transient myopia. Conclusion. This study is in favor of the interest of HBOT in pelvic radiation disease treatment (PRD).
You have requested "on-the-fly" machine translation of selected content from our databases. This functionality is provided solely for your convenience and is in no way intended to replace human translation. Show full disclaimer
Neither ProQuest nor its licensors make any representations or warranties with respect to the translations. The translations are automatically generated "AS IS" and "AS AVAILABLE" and are not retained in our systems. PROQUEST AND ITS LICENSORS SPECIFICALLY DISCLAIM ANY AND ALL EXPRESS OR IMPLIED WARRANTIES, INCLUDING WITHOUT LIMITATION, ANY WARRANTIES FOR AVAILABILITY, ACCURACY, TIMELINESS, COMPLETENESS, NON-INFRINGMENT, MERCHANTABILITY OR FITNESS FOR A PARTICULAR PURPOSE. Your use of the translations is subject to all use restrictions contained in your Electronic Products License Agreement and by using the translation functionality you agree to forgo any and all claims against ProQuest or its licensors for your use of the translation functionality and any output derived there from. Hide full disclaimer