Barrett's oesophagus

"Endoscopically-visible segment of metaplastic columnar mucosa in the oesophagus, with intestinal metaplasia proven histologically."

• Note differing definitions between UK and USA - requirement of intestinal metaplasia (as indicated by goblet cells) is uncertain. USA says goblet cells required, UK says not required.

• Complication of GORD - GORD is the ONLY cause of BO

• Not currently recommended in Australia, but can be done overseas as per below
• Indications for screening to look for Barrett's: (if multiple risk factors and have had GORD for >5 years)
  • Age >50
  • Male
  • White
  • Hiatal hernia
  • Obesity
  • Nocturnal reflux
  • Smoker
  • First-degree relative with Barrett's and/or adenocarcinoma
• Only need to screen each patient once.
• If they have oesophagitis, give PPI for 3/12 and screen again

• Dysplasia in Barrett's is characterised by cytologic malignant changes including atypical nuclei, increased mitoses, and lack of surface maturation
• Dysplasia is most common closer to GOJ in a long segment of Barrett's
• HGD is distinguished from LGD by more prominent cytologic or architectural derangements
• Remains dysplasia as long as it is confined to the epithelium without invasion of the basement membrane, regardless of the degree of abnormality
• Histological grading is based on the Vienna classification system - non-dysplastic, indeterminate, LGD, HGD, intra-mucosal carcinoma
  • Lots of intra-observer variation. In particular, LGD from general pathologists is downgraded to non-dysplastic by specialist pathologists in 73% of cases
  • Indefinite for dysplasia means equivocal for inflammation or dysplasia - 11.4% pooled annual risk for progressing to LGD and 0.6% for progression to carcinoma
• Precursor for oesophageal adenocarcinoma
  • Non-dysplastic - 0.3 per 100 person-years
  • LGD - 0.5
  • HGD - 6.6
  • Overall incidence of oesophageal adenocarcinoma in BE patients is about 40x the general population
• Long segment is >=3cm - significantly higher risk of progression to carcinoma
• Short tongues <1cm/'variable Z-line' were previously called ultra-short segment Barrett's, but do not constitute increased malignancy risk and no need to biopsy if no concerns for dysplasia

• Careful endoscopy - white light and NBI are both useful
  • Suspect when GOJ (proximal extent of rugae) is >=1cm distal to the z-line
  • Barrett's has a characteristic salmon pink colour and velvety texture
  • Firstly identify the segment of columnar epithelium, and also look for areas of irregularity within it
  • Use Prague classification system (see 'endoscopy' topic)
  • Note hiatal hernias
  • Seattle protocol for biopsies
• Oesophagitis + Barrett's
  • If LA C or D oesophagitis is found, the pathologist will have trouble identifying dysplasia and a diagnosis of 'indeterminate' is likely
  • If no concerns for cancer, put them on high-dose PPI and re-scope in 6-8 weeks
• Irregular z-line:
  • Found in 10-15% of patients
  • When the SCJ lies above the GOJ, but without any confluence, forming tongues shorter than 1cm, and thus does not fulfil criteria for BO
  • It can harbour histological intestinal metaplasia, but the progression rate to BO is low, let alone to malignancy, so no further evaluation or screening is recommended

1. Therapy for GORD
2. Prevention of progression/treatment of BE

• • Refer to centre with EMR/ESD for resection

• • No increased risk of malignancy
  • No clear guidelines, but probably don't need to do another scope

• • Symptom relief
  • Continue PPI indefinitely
  • Don't recommend anti-reflux surgery just because of theoretical risk of progression - incidence of cancer appears to be low
  • If can't control symptoms with lifestyle and medication, then they need anti-reflux surgery (exactly same as uncomplicated GORD)
  • Radiofrequency ablation is unproven in this population
  • Surveillance:
    • Non-dysplastic BE - 3-5 yearly - but could do much more frequently to limit progression to that which can be treated endoscopically - some UGI surgeons do yearly scopes
      • If short segment (<3cm), thoroughly biopsied, and no dysplasia, surveillance every five years (10% risk of dysplasia)
      • Long segment every three years (31% risk of dysplasia)
    • Consider stopping surveillance in elderly or unfit patients, similar to NBCSP

• • BD PPI
  • Re-scope Seattle protocol 3-6/12
  • If still indefinite, review with experienced pathologist and either surveillance every 12 months or referral to Barrett's centre
  • Most will regress to non-dysplastic

• • Repeat endoscopy ASAP with Seattle protocol if you didn't do it initially - need to exclude more advanced disease
  • Need to review slides with experienced pathologist
  • Either start on PPI or increase existing dose
  • American College of Gastroenterology suggests either endoscopic eradication (then follow-up endoscopy in 6 months) or surveillance every six months for one year and then annually until reversion
    • Most sensible way is probably to check persistence, and refer for ablation if persistent
  • Can be offered anti-reflux surgery - given that most patients with LGD regress after surgery
  • If persistent, may need mucosal ablation

• • Review slides with experienced pathologist
  • Indication for intervention - ideally RFA
  • Most get endoscopic therapy, followed by surveillance gastroscopy three months later
  • Careful repeat biopsy - look out for focus of invasive carcinoma - use every imaging modality available - white light, NBI, acetic acid
  • Small lesions - endoscopic resection - ideally take full thickness of mucosa and submucosa
  • Can evaluate lesions larger than 1-2cm for invasion using EUS - key point would be whether it is T1a or T1b
  • If HGD or T1a (without LVI), options are oesophageal preservation therapy vs oesophagectomy
    • Oncologically equivalent, but long-term surveillance and multiple initial scopes required, and recurrence is a risk
    • Oesophagectomy historically gets good results in this group, with mortality under 1%
    • However, endoscopic treatment and surveillance is much better now

• Goals are removal of BE epithelium, while preserving overall integrity of the oesophagus and accurately staging dysplasia or invasive disease
• Should have close surveillance and PPI afterwards
• Beware the risk of 'buried glands' - areas of Barrett's epithelium hidden beneath areas of new squamous epithelium, even if the risk of malignancy in those glands appears to be low
• Radiofrequency ablation
  • Most commonly used endoscopic therapy
  • This is the HALO device, although I think it has been renamed now to 'Barrx'
  • Much more effective than photodynamic therapy with a lower stricture and overall complication rate
  • Delivered with either a circumferential balloon or an electrical plate. The treated mucosa is replaced by neosquamous mucosa. The standard ablation program uses two double pulses of 12 J/sq cm.
  • AIM-II trial - 81% of patients with HGD and 90% of patients with LGD had eradication of dysplasia. 4% had their dysplasia progress to a higher grade.
• Argon plasma coagulation
• Cryotherapy
  • Generally well tolerated with little pain and low stricture rates
  • Does not require the probe to be in contact with tissue
  • Use either a balloon or endoscopic spray catheter to deliver liquid nitrogen
  • Eradicated LGD and HGD at 91% and 81% respectively in one study
  • Can be used as salvage therapy after failed RFA
• Photodynamic therapy
• Endoscopic mucosal resection
  • Best for visible segments
  • Commonly use 'Duette' system (Cook)
• Endoscopic submucosal dissection
  • Better with >2cm
  • Best option for cancer
• Surveillance after eradication
  • Previous HGD: 1, 2, 3, 4, 5, 7, 10 years after treatment
  • Previous LGD: 1, 3, and 5 years after treatment