Interventions to reduce acute and late adverse gastrointestinal effects of pelvic radiotherapy for primary pelvic cancers

Abstract

Background

An increasing number of people survive cancer but a significant proportion have gastrointestinal side effects as a result of radiotherapy (RT), which impairs their quality of life (QoL).

Objectives

To determine which prophylactic interventions reduce the incidence, severity or both of adverse gastrointestinal effects among adults receiving radiotherapy to treat primary pelvic cancers.

Search methods

We conducted searches of CENTRAL, MEDLINE, and Embase in September 2016 and updated them on 2 November 2017. We also searched clinical trial registries.

Selection criteria

We included randomised controlled trials (RCTs) of interventions to prevent adverse gastrointestinal effects of pelvic radiotherapy among adults receiving radiotherapy to treat primary pelvic cancers, including radiotherapy techniques, other aspects of radiotherapy delivery, pharmacological interventions and non‐pharmacological interventions. Studies needed a sample size of 20 or more participants and needed to evaluate gastrointestinal toxicity outcomes. We excluded studies that evaluated dosimetric parameters only. We also excluded trials of interventions to treat acute gastrointestinal symptoms, trials of altered fractionation and dose escalation schedules, and trials of pre‐ versus postoperative radiotherapy regimens, to restrict the vast scope of the review.

Data collection and analysis

We used standard Cochrane methodology. We used the random‐effects statistical model for all meta‐analyses, and the GRADE system to rate the certainty of the evidence.

Main results

We included 92 RCTs involving more than 10,000 men and women undergoing pelvic radiotherapy. Trials involved 44 different interventions, including radiotherapy techniques (11 trials, 4 interventions/comparisons), other aspects of radiotherapy delivery (14 trials, 10 interventions), pharmacological interventions (38 trials, 16 interventions), and non‐pharmacological interventions (29 trials, 13 interventions). Most studies (79/92) had design limitations. Thirteen studies had a low risk of bias, 50 studies had an unclear risk of bias and 29 studies had a high risk of bias. Main findings include the following:

Radiotherapy techniques: Intensity‐modulated radiotherapy (IMRT) versus 3D conformal RT (3DCRT) may reduce acute (risk ratio (RR) 0.48, 95% confidence interval (CI) 0.26 to 0.88; participants = 444; studies = 4; I2 = 77%; low‐certainty evidence) and late gastrointestinal (GI) toxicity grade 2+ (RR 0.37, 95% CI 0.21 to 0.65; participants = 332; studies = 2; I2 = 0%; low‐certainty evidence). Conformal RT (3DCRT or IMRT) versus conventional RT reduces acute GI toxicity grade 2+ (RR 0.57, 95% CI 0.40 to 0.82; participants = 307; studies = 2; I2 = 0%; high‐certainty evidence) and probably leads to less late GI toxicity grade 2+ (RR 0.49, 95% CI 0.22 to 1.09; participants = 517; studies = 3; I2 = 44%; moderate‐certainty evidence). When brachytherapy (BT) is used instead of external beam radiotherapy (EBRT) in early endometrial cancer, evidence indicates that it reduces acute GI toxicity (grade 2+) (RR 0.02, 95% CI 0.00 to 0.18; participants = 423; studies = 1; high‐certainty evidence).

Other aspects of radiotherapy delivery: There is probably little or no difference in acute GI toxicity grade 2+ with reduced radiation dose volume (RR 1.21, 95% CI 0.81 to 1.81; participants = 211; studies = 1; moderate‐certainty evidence) and maybe no difference in late GI toxicity grade 2+ (RR 1.02, 95% CI 0.15 to 6.97; participants = 107; studies = 1; low‐certainty evidence). Evening delivery of RT may reduce acute GI toxicity (diarrhoea) grade 2+ during RT compared with morning delivery of RT (RR 0.51, 95% CI 0.34 to 0.76; participants = 294; studies = 2; I2 = 0%; low‐certainty evidence). There may be no difference in acute (RR 2.22, 95% CI 0.62 to 7.93, participants = 110; studies = 1) and late GI toxicity grade 2+ (RR 0.44, 95% CI 0.12 to 1.65; participants = 81; studies = 1) between a bladder volume preparation of 1080 mls and that of 540 mls (low‐certainty evidence). Low‐certainty evidence on balloon and hydrogel spacers suggests that these interventions for prostate cancer RT may make little or no difference to GI outcomes.

Pharmacological interventions: Evidence for any beneficial effects of aminosalicylates, sucralfate, amifostine, corticosteroid enemas, bile acid sequestrants, famotidine and selenium is of a low or very low certainty. However, evidence on certain aminosalicylates (mesalazine, olsalazine), misoprostol suppositories, oral magnesium oxide and octreotide injections suggests that these agents may worsen GI symptoms, such as diarrhoea or rectal bleeding.

Non‐pharmacological interventions: Low‐certainty evidence suggests that protein supplements (RR 0.23, 95% CI 0.07 to 0.74; participants = 74; studies = 1), dietary counselling (RR 0.04, 95% CI 0.00 to 0.60; participants = 74; studies = 1) and probiotics (RR 0.43, 95% CI 0.22 to 0.82; participants = 923; studies = 5; I2 = 91%) may reduce acute RT‐related diarrhoea (grade 2+). Dietary counselling may also reduce diarrhoeal symptoms in the long term (at five years, RR 0.05, 95% CI 0.00 to 0.78; participants = 61; studies = 1). Low‐certainty evidence from one study (108 participants) suggests that a high‐fibre diet may have a beneficial effect on GI symptoms (mean difference (MD) 6.10, 95% CI 1.71 to 10.49) and quality of life (MD 20.50, 95% CI 9.97 to 31.03) at one year. High‐certainty evidence indicates that glutamine supplements do not prevent RT‐induced diarrhoea. Evidence on various other non‐pharmacological interventions, such as green tea tablets, is lacking.

Quality of life was rarely and inconsistently reported across included studies, and the available data were seldom adequate for meta‐analysis.

Authors' conclusions

Conformal radiotherapy techniques are an improvement on older radiotherapy techniques. IMRT may be better than 3DCRT in terms of GI toxicity, but the evidence to support this is uncertain. There is no high‐quality evidence to support the use of any other prophylactic intervention evaluated. However, evidence on some potential interventions shows that they probably have no role to play in reducing RT‐related GI toxicity. More RCTs are needed for interventions with limited evidence suggesting potential benefits.

Author(s)

Theresa A Lawrie, John T Green, Mark Beresford, Linda Wedlake, Sorrel Burden, Susan E Davidson, Simon Lal, Caroline C Henson, H. Jervoise N Andreyev

Abstract

Plain language summary

Interventions to reduce digestive side effects of pelvic x‐ray treatment

Background-Radiotherapy (RT: x‐ray treatment) is a common anti‐cancer treatment that often cures people of their cancer, but can damage the gastrointestinal (digestive) tract and lead to distressing short‐term (acute) and long‐term (late) gastrointestinal side effects, which can start many months or years after the radiotherapy has finished. These side effects, such as diarrhoea, faecal urgency (a sudden need to pass stool), and faecal incontinence (leakage of stool from the rectum) can damage a person's quality of life (QoL). We conducted this review to establish whether there are any treatments that can be given to people undergoing pelvic radiotherapy (RT) to reduce gastrointestinal side effects.

Methods-We searched the medical literature up to 2 November 2017 and selected randomised controlled trials (RCTs) of any preventive treatment (intervention) given to people undergoing RT for pelvic cancer (such as bladder, endometrial, cervix, rectum and prostate cancers). We combined data from similar RCTs to provide a summary estimate of the effect of an intervention and made a judgement about how confident (certain) we are of the findings, using established methods (GRADE).

Results-We identified 92 RCTs involving 44 different interventions to reduce RT‐related gastrointestinal side effects. These included new methods (RT techniques) and other aspects of delivering RT (lower RT dosages, different bladder volumes, morning or evening RT delivery, injected gels or rectally‐inserted balloons (spacers] to protect the rectum, and other options), drugs (aminosalicylates, amifostine, corticosteroids, famotidine, octreotide, magnesium oxide, misoprostol, selenium, sodium butyrate, smectite, sucralfate, superoxide dismutase), and non‐drug treatments (different types of diets, glutamine, counselling, green tea, and other options). We found some evidence to show that certain interventions have no role to play in reducing gastrointestinal side effects (particularly glutamine supplements, misoprostol suppositories, oral magnesium oxide and octreotide injections). However, we found little good evidence (moderate or high certainty) to show that any of the options is helpful. The exceptions to this are the evidence on RT techniques, which shows that conformal (modern) RT techniques are better than older RT techniques, and evidence that vaginal brachytherapy (small radioactive balls placed in the vagina) for early endometrial cancer reduces acute gastrointestinal side effects compared with external‐beam radiotherapy.

Conclusions-Modern (conformal) RT methods are helpful in reducing RT‐related side effects. There is insufficient evidence to robustly support the use of any single drug or non‐drug option or other RT delivery device/option to reduce RT‐related gastrointestinal effects. More high‐quality research is needed.

Author(s)

Theresa A Lawrie, John T Green, Mark Beresford, Linda Wedlake, Sorrel Burden, Susan E Davidson, Simon Lal, Caroline C Henson, H. Jervoise N Andreyev

Reviewer's Conclusions

Authors' conclusions 

Implications for practice 

Conformal radiotherapy techniques are an improvement on older radiotherapy techniques. IMRT may be better than 3DCRT in terms of GI toxicity but the evidence to support this is uncertain. There is insufficient high‐quality evidence to support the use of any other prophylactic intervention evaluated, and evidence on several of the potential interventions shows that they have no role to play in reducing RT‐related GI toxicity. In the absence of better evidence on preventive interventions to reduce GI side effects, an individualised, person‐centred approach with ongoing monitoring of nutrition and GI symptomatology, during and after RT, seems prudent, to ensure timely management of symptoms as they arise. This approach is likely to require a multidisciplinary team of oncologists, dietitians, gastroenterologists and other support staff, which might require organisational changes in some settings.

Implications for research 

There are 12 ongoing trials registered with clinical trials registries that are relevant to this review: these included two trials of brachytherapy (NCT00807768; NCT01839994), one trial of a diet intervention (NCT02516501), three trials of probiotics (NCT01706393; NCT01790035; NCT02351089), five trials of IMRT (NCT01164150; NCT01641497; NCT01672892; NCT02151019; NCT00326638) and one trial of acupuncture Asadpour 2017.

Long‐term follow‐up data are awaited on a trial of sulfasalazine compared with placebo (Miller 2016).

Evidence on the following interventions is incomplete or lacking and the evidence base could benefit from further research:

  • Endorectal balloons and prerectal spacers
  • Evening delivery of RT, reduced dose volume interventions, hypoxic RT
  • Pharmacological agents with free radical scavenging properties, including amifostine and famotidine
  • Non‐pharmacological interventions, including single nutrient and other diets, probiotics and green tea
  • Enemas, including sucralfate enemas and corticosteroid enemas
  • Statins and ACE inhibitors

Adherence to certain interventions, particularly dietary ones, can be challenging for study participants; measuring and assessing compliance should therefore be integral to these types of studies, to provide the high‐certainty evidence needed in this field.

Much research to date has been investigator‐led and might have lacked the resources (including a multidisciplinary team and sufficient funding) necessary to conduct high‐quality studies, particularly ensuring adequate sample size, compliance and long‐term follow‐up. This may partly be due to the fact that preventing and managing radiation‐induced toxicity is not the responsibility of a single type of clinician. Investigators considering conducting research in this field should ensure that their studies are well‐designed, with multidisciplinary collaboration, and adequately powered to answer their research question, with adherence to CONSORT guidelines (CONSORT 2012) for reporting of findings.

A similar Cochrane Review of treatment interventions for acute radiation‐induced GI toxicity might be of value, as treatment of acute GI toxicity might impact the development of late GI toxicity.

Get full text at The Cochrane Library