丝裂原活化通路激酶抑制剂相关视网膜病变：上游抑制与下游抑制的特征是否不同？

IF 0.9 Q4 OPHTHALMOLOGY

Ocular Oncology and Pathology Pub Date : 2023-08-01 Epub Date: 2023-02-08 DOI:10.1159/000529127

Jasmine H Francis, William Foulsham, Julia Canestraro, James J Harding, Eli L Diamond, Alexander Drilon, David H Abramson

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引用次数: 0

摘要

导言：许多癌症都存在丝裂原活化通路激酶（MAPK）失调的问题，因此阻断这一通路成为治疗目标。然而，MAPK抑制剂可能导致包括视网膜病变在内的不良反应。本研究比较了服用对MAPK有不同抑制作用的药物（直接干扰丝裂原活化蛋白激酶激酶（MEK）或细胞外信号调节激酶（ERK）抑制剂，或通过干扰表皮生长因子受体（FGFR）信号转导间接抑制）的患者浆液性视网膜病变的临床和形态学特征：这项回顾性观察研究是对一家三级肿瘤转诊中心前瞻性收集的汇总数据进行的研究。在接受 MAPK 抑制剂（FGFR、MEK 和 ERK 抑制剂分别为 171、107 和 61 例）治疗转移性癌症的 339 例患者中，本研究纳入了 65 例经光学相干断层扫描（OCT）证实有视网膜病变证据的患者的 128 只眼睛。主要结果是与基线 OCT 相比，治疗引起的脉络膜/视网膜 OCT 异常的特征：所有接受三类药物（FGFRi、MEKi、ERKi）治疗的患者，视网膜病变均表现为双侧视网膜下积液灶，累及眼窝，无需干预即可逆转。三类药物之间存在显著差异：上游靶点（表皮生长因子受体抑制剂）的视网膜病变患者比例、每只眼睛的积液灶数量、视网膜内水肿的眼睛比例以及有症状患者的比例最小，而下游靶点（MEK或ERK抑制剂）的比例最大：本研究表明，MAPK通路抑制剂可能会导致视网膜下积液灶，并根据所涉及的靶点（表皮生长因子受体、MEK或ERK）而具有独特的临床和形态特征。MAPK通路越往下游，视网膜病变越常见、症状越严重（积液灶越多、积液形态越复杂）。

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Mitogen-Activated Pathway Kinase Inhibitor-Associated Retinopathy: Do Features Differ with Upstream versus Downstream Inhibition?

Introduction: Many cancers have derangement of the mitogen-activated pathway kinase (MAPK), making this pathway blockade a therapeutic target. However, inhibitors of MAPK can result in adverse effects including retinopathy. This study compares clinical and morphological characteristics of serous retinal disturbances in patients taking agents with variable inhibition of MAPK: either direct interference of mitogen-activated protein kinase kinase (MEK) or extracellular signal-regulated kinase (ERK) inhibitors or with indirect inhibition via interference with FGFR signaling.

Methods: This retrospective observational study of prospectively collected pooled data is from a single tertiary oncology referral center. Of 339 patients receiving MAPK inhibitors (171, 107, and 61 on FGFR, MEK, and ERK inhibitors, respectively) for treatment of metastatic cancer, this study included 128 eyes of 65 patients with evidence of retinopathy confirmed by optical coherence tomography (OCT). The main outcome was characteristics of treatment-emergent choroid/retinal OCT abnormalities as compared to baseline OCT.

Results: In all patients on one of three drug classes (FGFRi, MEKi, ERKi), the retinopathy manifested as subretinal fluid foci that were bilateral, fovea involving, and reversible without intervention. There were notable differences between the three classes of drugs: the proportion of patients with retinopathy, number of fluid foci per eye, proportion of eyes with intraretinal edema, and the proportion of symptomatic patients was least for the upstream target (FGFR inhibitors) and greatest for the downstream targets (MEK or ERK inhibitors).

Conclusion: This study shows MAPK pathway inhibitors may cause subretinal fluid foci with unique clinical and morphological characteristics depending on the target (FGFR, MEK, or ERK) implicated. Retinopathy is more common, more symptomatic, and more severe (more fluid foci, more expansive fluid configurations) the further downstream the MAPK pathway is inhibited.

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来源期刊

Ocular Oncology and Pathology OPHTHALMOLOGY-

CiteScore

2.40

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0.00%

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