4.4 Article

Intestinal hypomotility in systemic sclerosis: a histological study into the sequence of events

Journal

CLINICAL RHEUMATOLOGY
Volume 40, Issue 3, Pages 981-990

Publisher

SPRINGER LONDON LTD
DOI: 10.1007/s10067-020-05325-8

Keywords

Histology; Intestinal dysmotility; Pathogenesis; Systemic sclerosis

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The histological evaluation of intestinal involvement in systemic sclerosis (SSc) revealed differences in vascular changes, muscle layer fibrosis, and neuronal reduction between SSc patients and controls. The diversity among patients suggests parallel pathological processes, explaining the variety of histological features and clinical symptoms observed in SSc.
Objectives The pathogenesis of intestinal involvement in systemic sclerosis (SSc) is thought to be a sequential process (vascular, neuronal, and consecutive muscular impairment), but understanding of the underlying histological changes and how they translate to symptoms, is still lacking. Therefore, we systematically investigated histological characteristics of SSc in the intestines, compared to controls. Methods Autopsy material from the small bowel and colon was used for histological semiquantitative evaluation of the vasculature, enteric nervous system, interstitial cells of Cajal (ICC), and muscle layers, using a combination of histochemical and immunohistochemical stainings, according to guidelines of the Gastro 2009 International Working Group. Results Vascular changes were most frequently encountered, represented by intima fibrosis in both arteries and small vessels, and represented by venous dilatation. Second, generalized fibrosis of the circular muscle layer was significantly more found in SSc patients than in controls. Third, reduction of submucosal nerve fibers and myenteric neurons was shown in the colon of four SSc patients, which may explain severe symptoms of intestinal dysmotility. The density of myenteric ICC network was decreased in the small bowel of SSc patients. Conclusions The postulated sequential processes of intestinal involvement in SSc could not be supported by our histological evaluation. The interpatient diversity suggests that parallel processes occur, explaining the variety of histological features and clinical symptoms.

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