Sistrunk J Woody, Shifrin Alexander, Frager Marc, Bardales Ricardo H, Thomas Johnson, Fishman Norman, Goldberg Philip, Guttler Richard, Grant Edward
Jackson Thyroid & Endocrine Clinic, Jackson, Mississippi.
Department of Surgery, Hackensack Meridian Health Jersey Shore University Medical Center, Neptune, New Jersey.
J Am Soc Cytopathol. 2020 Jul-Aug;9(4):232-241. doi: 10.1016/j.jasc.2020.02.002. Epub 2020 Mar 10.
We evaluated the clinical performance of an expanded mutation panel in combination with microRNA classification (MPTX) for the management of indeterminate thyroid nodules.
MPTX included testing of fine-needle aspirates from multiple centers with a combination of ThyGeNEXT mutation panel for strong and weak driver oncogenic changes and ThyraMIR microRNA risk classifier (both from Interpace Diagnostics; Pittsburgh, PA). MPTX test status (positive or negative) and MPTX clinical risk classifications (low, moderate, or high risk) were determined blind to patient outcomes. Surgical pathology and clinical follow-up records of patients from multiple centers were used to determine patient outcomes. MPTX performance was assessed by Kaplan Meier analysis for cancer-free survival of patients, with risk of malignancy determined by hazard ratio (HR).
Our study included 140 patients with AUS/FLUS or FN/SFN nodules, of which 13% had malignancy. MPTX negative test status and MPTX low risk results conferred a high probability (94%) that patients would remain cancer-free. MPTX positive test status (HR 11.2, P < 0.001) and MPTX moderate-risk results (HR 8.5, P = 0.001) were significant risk factors for malignancy, each conferring a 53% probability of malignancy. MPTX high-risk results elevated risk of malignancy even more so, conferring a 70% probability of malignancy (HR 38.5, P < 0.001).
MPTX test status accurately stratifies patients for risk of malignancy. Further classification using MPTX clinical risk categories enhances utility by accurately identifying patients at low, moderate, or high risk of malignancy at the low rate of malignancy encountered when clinically managing patients with indeterminate thyroid nodules.
我们评估了一种扩展突变检测组合联合微小RNA分类(MPTX)在不确定甲状腺结节管理中的临床性能。
MPTX包括对来自多个中心的细针穿刺抽吸物进行检测,采用ThyGeNEXT突变检测组合检测强和弱驱动致癌变化,以及ThyraMIR微小RNA风险分类器(均来自Interpace诊断公司;宾夕法尼亚州匹兹堡)。MPTX检测状态(阳性或阴性)和MPTX临床风险分类(低、中或高风险)在不了解患者结局的情况下确定。使用多个中心患者的手术病理和临床随访记录来确定患者结局。通过Kaplan Meier分析评估MPTX对患者无癌生存的性能,恶性风险由风险比(HR)确定。
我们的研究纳入了140例具有不典型细胞/滤泡性病变不明意义(AUS/FLUS)或滤泡性新生物/可疑滤泡性新生物(FN/SFN)结节的患者,其中13%患有恶性肿瘤。MPTX检测阴性状态和MPTX低风险结果使患者无癌的概率很高(94%)。MPTX检测阳性状态(HR 11.2,P < 0.001)和MPTX中度风险结果(HR 8.5,P = 0.001)是恶性肿瘤的显著风险因素,每种情况的恶性概率均为53%。MPTX高风险结果使恶性风险更高,恶性概率为70%(HR 38.5,P < 0.001)。
MPTX检测状态可准确对患者的恶性风险进行分层。使用MPTX临床风险类别进行进一步分类可提高实用性,通过在临床管理不确定甲状腺结节患者时以低恶性率准确识别低、中或高恶性风险的患者。
