J F W M Bartelsman scite author profile

Scleroderma is a multisystem disorder frequently resulting in disturbed GI motility. Although, especially early in the disease, symptomatic improvement is achieved with prokinetic agents, more severe GI manifestations of scleroderma may be difficult to treat, leading to parenteral feeding and hospitalization. Recently, a new serotonin (5-HT4) receptor agonist prucalopride was shown to have remarkable prokinetic properties, resulting in symptomatic improvement and increased frequency of defecation in patients with chronic functional constipation. Here we report two cases of scleroderma with GI manifestation in which previous prokinetic treatment failed, but where the patients were successfully treated with prucalopride. Our data suggest that prucalopride may be a promising and effective drug to treat GI motility disorders in scleroderma. However, further placebo-controlled double blind studies are needed for full documentation of the usefulness of prucalopride in patients with scleroderma.

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Barrettʼs oesophagus

Bartelsman

Hameeteman

Tytgat

1992

European Journal of Cancer Prevention

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Surveillance of Barrett esophagus in the Netherlands: A postal questionnaire

Sandick¹,

Bartelsman²,

Lanschot³

et al. 1998

Gastroenterology

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J F W M Bartelsman

Laparoscopic or conventional Nissen fundoplication for gastrooesophageal reflux disease: randomised clinical trial

Treatment of Gi dysmotility in scleroderma with the new enterokinetic agent prucalopride

Barrettʼs oesophagus

Surveillance of Barrett esophagus in the Netherlands: A postal questionnaire

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