Gastrointestinal stromal tumor pathophysiology

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]

Pathophysiology

GISTs are thought to arise from interstitial cells of Cajal (ICC),[1] that are normally part of the autonomic nervous system of the intestine. They serve a pacemaker function in controlling motility.

Gross Pathology

Gastrointestinal stromal tumor of stomach. Courtesy of Ed Uthman, MD.


Endoscopic image of GIST in fundus of stomach, seen on retroflexion.


Same GIST seen on forward view of the endoscope showing overlying clot.


Genetics

Most (50-80%) GISTs arise because of a mutation in a gene called c-kit. This gene encodes a transmembrane receptor for a growth factor termed scf (stem cell factor). The c-kit/CD117 receptor is expressed on ICCs and a large number of other cells, mainly bone marrow cells, mast cells, melanocytes and several others. In the gut, however, a mass staining positive for CD117 is likely to be a GIST, arising from ICC cells.

The c-kit molecule comprises a long extracellular domain, a transmembrane segment, and an intracellular part. Mutations generally occur in the DNA encoding the intracellular part (exon 11), which acts as a tyrosine kinase to activate other enzymes. Mutations make c-kit function independent of activation by scf, leading to a high cell division rate and possibly genomic instability. It is likely that additional mutations are "required" for a cell with a c-kit mutation to develop into a GIST, but the c-kit mutation is probably the first step of this process.

The tyrosine kinase function of c-kit is vital in the therapy for GISTs.

References

  1. Miettinen M, Lasota J (2006). "Gastrointestinal stromal tumors: review on morphology, molecular pathology, prognosis, and differential diagnosis". Arch Pathol Lab Med. 130 (10): 1466–78. PMID 17090188.


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