RET signalling in the pituitary: a double-edged sword for differentiation, apoptosis and therapeutic strategies in acromegaly.

Endocrine-related cancer Pub Date : 2025-01-23 Print Date: 2025-03-01 DOI:10.1530/ERC-24-0156

Miguel Chenlo, Ignacio Bernabeu, Márta Korbonits, Clara V Alvarez

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Abstract

The discovery of RET mutations in multiple endocrine neoplasia type 2A (MEN2A) in 1993 ignited a revolution in our understanding of this versatile receptor. Since then, the influence of RET has expanded to encompass diverse organs, including the pituitary gland. This review explores the multifaceted role of RET in somatotrophs, focusing on two opposing pathways: proliferation versus differentiation and apoptosis. The binding of glial-derived neurotrophic factor (GDNF) to RET promotes pituitary cell survival and inhibits PIT1-dependent differentiation, while low levels of GDNF trigger differentiation via PIT1. Excessive PIT1, on the other hand, will lead to apoptosis through caspase-3 activation involving the adaptor protein AIP and CDKN2A-ARF/p53. Pathogenic mutations in AIP can disrupt this apoptotic pathway, contributing to somatotrophinoma or prolactinoma development. In this concise review, we highlight the potential of CDKN2A-ARF expression as a prognostic marker for therapy response and discuss the promise of novel RET tyrosine kinase inhibitors for aggressive somatotrophinomas.

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垂体RET信号：端肢肥大症的分化、凋亡和治疗策略的双刃剑。

1993年，多发性内分泌瘤2A （MEN2A）中RET突变的发现点燃了我们对这种多功能受体的理解的革命。从那时起，RET的影响已经扩大到包括脑垂体在内的各种器官。这篇综述探讨了RET在生长激素中的多方面作用，重点关注两种相反的途径：增殖对抗分化和凋亡。胶质源性神经营养因子（GDNF）与RET的结合促进垂体细胞存活并抑制PIT1依赖性分化，而低水平的GDNF通过PIT1触发分化。另一方面，过多的PIT1会通过涉及接头蛋白AIP和CDKN2A-ARF的caspase-3激活导致细胞凋亡。AIP的致病性突变可以破坏这种凋亡途径，促进生长激素瘤或催乳素瘤的发展。在这篇简明的综述中，我们强调了CDKN2A-ARF表达作为治疗反应的预后标志物的潜力，并讨论了新型RET酪氨酸激酶抑制剂治疗侵袭性生长激素瘤的前景。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Endocrine-related cancer

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