Orphan Gpr182 suppresses ERK-mediated intestinal proliferation during regeneration and adenoma formation

<p class="first" id="d6614614e242">Orphan GPCRs provide an opportunity to identify potential pharmacological targets, yet their expression patterns and physiological functions remain challenging to elucidate. Here, we have used a genetically engineered knockin reporter mouse to map the expression pattern of the <i>Gpr182</i> during development and adulthood. We observed that <i>Gpr182</i> is expressed at the crypt base throughout the small intestine, where it is enriched in crypt base columnar stem cells, one of the most active stem cell populations in the body. <i>Gpr182</i> knockdown had no effect on homeostatic intestinal proliferation in vivo, but led to marked increases in proliferation during intestinal regeneration following irradiation-induced injury. In the <i>Apc ^Min </i> mouse model, which forms spontaneous intestinal adenomas, reductions in <i>Gpr182</i> led to more adenomas and decreased survival. Loss of <i>Gpr182</i> enhanced organoid growth efficiency ex vivo in an EGF-dependent manner. <i>Gpr182</i> reduction led to increased activation of ERK1/2 in basal and challenge models, demonstrating a potential role for this orphan GPCR in regulating the proliferative capacity of the intestine. Importantly, <i>GPR182</i> expression was profoundly reduced in numerous human carcinomas, including colon adenocarcinoma. Together, these results implicate <i>Gpr182</i> as a negative regulator of intestinal MAPK signaling–induced proliferation, particularly during regeneration and adenoma formation. </p>