The roles of AIP and GPR101 in familial isolated pituitary adenomas (FIPA).

The roles of AIP and GPR101 in familial isolated pituitary adenomas (FIPA).

Vasilev, Vladimir;Daly, Adrian F;Trivellin, Giampaolo;Stratakis, Constantine A;Zacharieva, Sabina;Beckers, Albert;
endocrine-related cancer 2020
204
vasilev2020theendocrinerelated

Abstract

Familial isolated pituitary adenomas (FIPA) is one of the most frequent conditions associated with an inherited presentation of pituitary tumors. FIPA can present with pituitary adenomas of any secretory/non-secretory type. Mutations in the gene for the aryl-hydrocarbon receptor interacting protein (AIP) have been identified in approximately 20% of FIPA families and are the most frequent cause (29%) of pituitary gigantism. Pituitary tumors in FIPA are larger, occur at a younger age and display more aggressive characteristics and evolution than sporadic adenomas. This aggressiveness is especially marked in FIPA kindreds with AIP mutations. Special attention should be paid to young patients with pituitary gigantism and/or macroadenomas as AIP mutations are prevalent in these groups. Duplications on chromosome Xq26.3 involving the gene GPR101 lead to X-linked acrogigantism (X-LAG), a syndrome of pituitary gigantism beginning in early childhood; three kindreds with X-LAG have presented in the setting of FIPA. Management of pituitary adenomas in the setting of FIPA, AIP mutations and GPR101 duplications is often more complex than in sporadic disease due to early onset disease, aggressive tumor growth and resistance to medical therapy.

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