NATIONAL INSTITUTE FOR HEALTH AND CLINICAL EXCELLENCE

Interventional procedure consultation document

Photodynamic therapy for Barrett's oesophagus

 

1       Provisional recommendations

1.1  Current evidence on the efficacy of photodynamic therapy (PDT) in patients with Barrett’s oesophagus with high-grade dysplasia (HGD) is adequate, provided that patients are followed up in the long term thereafter. There are no major safety concerns, although there is a risk of oesophageal stricture, and photosensitivity reactions are common. This procedure may be used in patients with Barrett’s oesophagus with HGD provided that normal arrangements are in place for clinical governance, consent and audit.

1.2  Current evidence on the efficacy and safety of PDT in patients with Barrett’s oesophagus with either low-grade dysplasia (LGD) or no dysplasia is inadequate in quality and quantity, and the balance of risks and benefits is not clear. Therefore, in these patients, the procedure should be used only with special arrangements for clinical governance, consent and audit or research.

1.3  Clinicians wishing to undertake PDT in patients with Barrett’s oesophagus with either LGD or no dysplasia should take the following actions.

·     Inform the clinical governance leads in their Trusts.

·     Ensure that patients and their carers understand the uncertainty about the procedure’s safety and efficacy and provide them with clear written information. In addition, the use of NICE’s information for patients (‘Understanding NICE guidance’) is recommended (available from www.nice.org.uk/guidance/IPGXXX/publicinfo). [[details to be completed at publication]]

·     Audit and review clinical outcomes of patients with Barrett’s oesophagus other than HGD having PDT (see section 3.1).

1.4  Patient selection for PDT in patients with Barrett’s oesophagus should be done by a multidisciplinary team experienced in the management of the condition.

1.5  PDT for Barrett’s oesophagus should only be carried out by endoscopists with specific training in this procedure.

2       The procedure

2.1    Indications and current treatments

2.1.1  Barrett’s oesophagus is a condition characterised by abnormal epithelium of the oesophagus and is associated with gastro-oesophageal reflux disease. In some patients, Barrett’s oesophagus may progress, through metaplasia and dysplasia, to neoplasia (oesophageal adenocarcinoma).

2.1.2  Cancer risk is higher for Barrett’s oesophagus patients with HGD (some of whom may already have developed early-stage cancer) than for those with LGD or no dysplasia. Patients with HGD are usually offered oesophagectomy, or frequent endoscopic surveillance and re-biopsy (with the aim of detecting neoplastic changes early) followed by oesophagectomy. Endoscopic treatments aiming to remove or ablate abnormal epithelium include endoscopic mucosal resection, argon plasma coagulation (APC), radiofrequency ablation, laser ablation, cryotherapy and multipolar electrocoagulation.

2.1.3  Patients with LGD or no dysplasia are usually offered regular endoscopic surveillance.

2.2    Outline of the procedure

2.2.1  PDT is usually carried out in an outpatient setting with the patient under intravenous sedation. A photosensitising agent is injected intravenously and is activated by illuminating the selected area with a laser inserted into the oesophagus. The photosensitising agent absorbs the light and forms high-energy oxygen molecules that cause necrosis of the Barrett’s epithelium through a photochemical effect. 

2.2.2  For extensive Barrett’s oesophagus, more than one treatment session may be required.

2.2.3  Patients are advised to avoid exposure to bright light and direct sunlight for several weeks after the procedure to minimise risk of photosensitivity reactions.

Sections 2.3 and 2.4 describe efficacy and safety outcomes from the published literature that the Committee considered as part of the evidence about this procedure. For more detailed information on the evidence, see the overview, available at www.nice.org.uk/IP232aoverview.

 

2.3    Efficacy

2.3.1  A randomised controlled trial (RCT) of 208 patients with HGD treated by PDT and omeprazole or omeprazole alone reported absence of HGD in 75% (104/138) and 36% (25/70) of patients respectively at 18-month follow-up (p < 0.0001). At 5-year follow-up, 48% and 4% of patients respectively still had no HGD (p < 0.0001).

2.3.2  An RCT of 72 patients without dysplasia treated by PDT or APC reported complete response (defined as reversal of columnar to squamous epithelium) in 50% (17/34) and 97% (33/34) of patients respectively at 12-month follow-up (p < 0.0001).

2.3.3  An RCT of 36 patients with LGD treated by PDT or a placebo reported biopsy-confirmed regression at 59–61 month follow-up in 89% (16/18) and 11% (2/18) of patients respectively (p < 0.001).

2.3.4  The RCT of 208 patients treated by PDT and omeprazole or omeprazole alone reported adenocarcinoma development in 15% (21/138) and 29% (20/70) of patients respectively during 5-year follow-up.

2.3.5  The Specialist Advisers listed key efficacy outcomes as reversal of dysplasia, prevention of dysplasia progression to adenocarcinoma and reversal of metaplasia.

2.4    Safety

2.4.1  One patient died 3 days after PDT treatment, with transmural oesophageal necrosis without perforation, in an RCT of 40 patients (13 with single-dose PDT vs 13 with two-dose PDT vs 14 with APC). 

2.4.2  Oesophageal stricture was reported in 36% (49/138), 3% (1/34), 33% (20/60), 15% (2/13), and 27% (35/131) of patients treated by PDT in the RCTs of 208, 72, 60, 26 and a non-randomised controlled trial of 199 patients respectively. Most were treated successfully with dilatation but 2 patients suffered perforation, requiring oesophagectomy.

2.4.3  Dysphagia was reported in 19% (absolute figure not stated) of patients treated by PDT in the RCT of 208 patients (timing of events not stated).

2.4.4  Photosensitivity reactions within 90 days of treatment were reported in 69% of patients in the PDT arm of the RCT of 208 patients (absolute figures not stated). Photosensitivity reactions occurred in 15% (5/34) and 15% (2/13) of patients in RCTs of 72 and 26 patients respectively, and in 60% (77/129) of patients in the non-randomised controlled trial of 199 patients. 

2.4.5  In the RCT of 72 patients treated by PDT or APC, buried glands were reported in 24% (4/17) and 21% (7/33) of patients respectively (difference reported as ‘non-significant’).

2.4.6  The Specialist Advisers listed anecdotal adverse events as pain and inflammation, ulceration and severe hypotension after the use of PDT with 5-aminolevulinic acid. They considered theoretical adverse events to include decompensation in patients with cirrhosis of the liver, and skin and retinal damage due to photosensitisation.

3     Further information

3.1  This guidance requires that clinicians undertaking the procedure make special arrangements for audit. NICE has identified relevant audit criteria and is developing an audit tool (which is for use at local discretion), which will be available when the guidance is published.

3.2  This procedure is a review of IPG82 published in 2004.

3.3  For related NICE guidance see www.nice.org.uk

Bruce Campbell
Chairman, Interventional Procedures Advisory Committee
February 2010

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 It is the responsibility of consultees to accurately cite academic work in order that they can be validated.