评估激活哺乳动物雷帕霉素靶点通路在基底细胞癌中的作用,将其作为一种新的治疗方法。

Anne Lynn S Chang, Ryanne Brown, Shufeng Li, Nicolas Betancourt, Joyce Teng
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引用次数: 0

摘要

靶向哺乳动物雷帕霉素靶标(mTOR)通路是治疗基底细胞癌(BCC)的一种潜在新方法,但该通路的激活在人类 BCC 中尚未得到很好的描述。本研究的目的是评估 BCC(散发性和综合征)中是否存在 mTOR 通路激活,并报告一例戈林综合征(GS)患者,其临床可疑 BCC 对通过局部西罗莫司治疗抑制 mTOR 有反应。经斯坦福大学机构审查委员会批准后,对来自戈林综合征患者(n = 25)、散发性 BCC(n = 35)和对照组织的存档 BCC 进行免疫组化分析,以检测 mTOR 通路的激活情况,并由皮肤病理学家评估免疫组化染色强度。与正常皮肤相比,BCC 的 eIF4EBP1 水平升高(Padjusted = 0.0336),而 eIF4EBP1 是 mTOR 的下游;与 mTOR 相互作用的丝氨酸/苏氨酸激酶 Phospho-(AKT) 也显著升高(核周:Padjusted < 0.0001;胞浆:Padjusted = 0.0021)。在对一名患有 GS 的儿童患者进行标签外局部使用 1%西罗莫司治疗时,我们注意到新的 BCC 增生有所减少,临床上怀疑为 BCC 的现有肿瘤也缩小了。这种治疗方法在连续使用两年后耐受性良好,在此期间无需其他治疗。外用西罗莫司是一种治疗散发性和GS相关性BCC的有效候选药物。我们需要开展多中心、前瞻性研究,以了解外用 mTOR 抑制剂在 BCC 治疗中的疗效和安全性,并确定 mTOR 下游的免疫组化标记物是否具有预测价值,以识别最有可能对外用 mTOR 抑制剂(如西罗莫司)产生反应的 BCC。
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Assessment of Mammalian Target of Rapamycin Pathway Activation in Basal Cell Carcinoma as a New Therapeutic Approach.
Targeting the mammalian target of rapamycin (mTOR) pathway represents a potentially novel approach to treat basal cell carcinoma (BCC), but activation of this pathway has not been well described in human BCCs. The purpose of this study was to assess whether mTOR pathway activation occurs in BCCs (both sporadic and syndromic) and report a case of a patient with Gorlin syndrome (GS) whose clinically suspicious BCCs responded to mTOR inhibition through topical sirolimus treatment. After Stanford Institutional Review Board Approval, archived BCCs from patients with GS (n = 25), sporadic BCCs (n = 35), and control tissues were subjected to immunohistochemical analysis for the activation of mTOR pathway, and immunohistochemical staining intensity was evaluated by a dermatopathologist. BCCs (compared with normal skin) had elevated levels of eIF4EBP1 (Padjusted = 0.0336), which is downstream of mTOR. a serine/threonine kinase Phospho-(AKT), which interacts with mTOR, was also significantly elevated (perinuclear: Padjusted < 0.0001; cytoplasmic: Padjusted = 0.0021). When off-label topical 1% sirolimus was used on a pediatric patient with GS, we noted reduction of new BCC development and decreased size of existing neoplasms clinically suspicious for BCCs. This treatment was well tolerated after 2 years of continuous use, with no other treatments needed during this period. Topical sirolimus is a promising therapeutic candidate against both sporadic and GS-associated BCC. Multicenter, prospective studies are needed to understand the efficacy and safety of topical mTOR inhibitors in BCC treatment, and ascertain whether the immunohistochemical markers downstream of mTOR could have predictive value in identifying BCCs most likely to respond to topical mTOR inhibitors, such as sirolimus.
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