Plasma-Derived Cell-Free DNA for the Diagnosis of Ocular-Involving Histiocytosis

IF 3.2 Q1 OPHTHALMOLOGY Ophthalmology science Pub Date : 2024-04-15 DOI:10.1016/j.xops.2024.100530

Jasmine H. Francis MD , Maria E. Arcila MD , Allison Sigler , Dana F. Bossert RN , David H. Abramson MD , Eli L. Diamond MD

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Abstract

Purpose

Circulating tumor DNA (ctDNA) is released into the plasma by many cancers and offers clinical applications including noninvasive diagnostics. Histiocytosis results from myelogenous clonal expansion of histiocytes, predominantly driven by mutations in the mitogen-activated protein kinase pathway that are potentially detectable by ctDNA-based sequencing assays. However, ocular-involving histiocytosis is often a diagnostic challenge leading to delayed diagnosis and the need for invasive biopsy of sensitive ocular structures. The purpose of this study is to determine whether sequencing of plasma-derived ctDNA can noninvasively diagnose ocular-involving histiocytosis.

Design

Single tertiary cancer referral center.

Participants

Twenty-four adult patients with ocular-involving histiocytosis and ctDNA sequencing.

Methods

Circulating tumor DNA was analyzed (via digital droplet polymerase chain reaction for BRAF V600E, and/or next-generation sequencing) and variant allele frequency was measured at initial presentation to our center. Patient demographics, clinical characteristics, and oncogenic mutations identified from tumor-based sequencing were recorded.

Main Outcome Measures

Plasma-derived ctDNA detectability of pertinent driver mutations of histiocytosis.

Results

At the initial presentation of 14 patients with ocular-involving histiocytosis, sequencing of plasma-derived ctDNA detected driver mutations for histiocytosis (BRAF V600E [10], KRAS [2], ARAF [1], and concurrent MAP2K1/KRAS [1]). Mutations found in circulating cell-free DNA were 100% concordant in 11 of 11 patients with mutations identified by solid tumor sequencing. Of 10 patients without driver mutation detected in ctDNA, 3 patients had alterations (CBL mutation or kinase fusion) not captured in the ctDNA sequencing assay, 3 were wildtype even by tumor sequencing; in 4 patients, tumor-based sequencing identified mutations (BRAF [2], MAP2K1 [2]) not detected in ctDNA. Detectable mutations in ctDNA were significantly more likely in patients with uveal infiltration (P = 0.036).

Conclusions

In this cohort, plasma-derived ctDNA was detectable and diagnostic in the majority of patients with ocular-involving histiocytosis. This suggests that if ocular histiocytosis is suspected (particularly if involving the uvea), noninvasive plasma-derived ctDNA analysis is a helpful diagnostic tool that may obviate the need to invasively biopsy sensitive ocular structures.

Financial Disclosure(s)

Proprietary or commercial disclosure may be found in the Footnotes and Disclosures at the end of this article.

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用于诊断眼组织细胞增生症的血浆衍生细胞游离 DNA

目的许多癌症都会向血浆中释放循环肿瘤 DNA（ctDNA），其临床应用包括无创诊断。组织细胞增生症是由组织细胞的骨髓性克隆扩增引起的，主要由丝裂原活化蛋白激酶通路中的突变驱动，可通过基于ctDNA的测序分析进行检测。然而，眼部侵袭性组织细胞增生症往往是诊断难题，导致诊断延迟，并需要对敏感的眼部结构进行侵入性活检。本研究的目的是确定血浆衍生的ctDNA测序是否能无创诊断眼球浸润性组织细胞增生症。方法分析循环肿瘤DNA（通过数字液滴聚合酶链反应检测BRAF V600E和/或下一代测序），并测量初次到本中心就诊时的变异等位基因频率。主要结果测量血浆来源的ctDNA对组织细胞增生症相关驱动基因突变的可检测性。结果14例眼部侵袭性组织细胞增生症患者初次发病时，血浆来源的ctDNA测序检测到组织细胞增生症的驱动基因突变（BRAF V600E [10]、KRAS [2]、ARAF [1]和并发的MAP2K1/KRAS [1]）。在循环无细胞DNA中发现的突变与实体瘤测序确定的突变100%一致。在ctDNA中未检测到驱动基因突变的10名患者中，3名患者的基因改变（CBL突变或激酶融合）未被ctDNA测序检测捕获，3名患者即使通过肿瘤测序也是野生型；在4名患者中，基于肿瘤的测序发现了ctDNA中未检测到的突变（BRAF [2]、MAP2K1 [2]）。结论在该队列中，大多数眼部侵袭性组织细胞增生症患者的血浆来源ctDNA均可检测并诊断出突变。这表明，如果怀疑患有眼组织细胞增生症（尤其是涉及葡萄膜的组织细胞增生症），无创的血浆衍生ctDNA分析是一种有用的诊断工具，可以避免对敏感的眼部结构进行有创活检。

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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