Akgul Mahmut, Al-Obaidy Khaleel I, Cheng Liang, Idrees Muhammad T
Pathology, Albany Medical Center, Albany, New York, USA.
Department of Pathology and Laboratory Medicine, Indiana University School of Medicine, Indianapolis, Indiana, USA.
J Clin Pathol. 2022 Nov;75(11):772-775. doi: 10.1136/jclinpath-2021-207478. Epub 2021 Jun 24.
Low-grade oncocytic tumour (LOT) has recently been introduced as a potential distinct entity.
At the Indiana University department of pathology, primary renal epithelial neoplasms between 2005 and 2020 were searched after appropriate institutional review board permissions.
Twenty-three cases (male/female ratio 14/9) with a median age of 66 (23-84 years) were identified. The majority of patients underwent partial nephrectomy (15/23, 65%), with a median tumour size of 4.0 cm (2.2-10.5 cm). Only one case had infiltration beyond the kidney (perinephric fat). Solid/diffuse proliferation of tightly packed oncocytic tumour cells and occasional tubule formations, with an abrupt edematous change in the stroma with loosely connected small clusters of tumour cells. Along with diffuse CK7 expression with lack of CD117 in all cases, vimentin was positive in 8/23 cases (35%, 5 focal). CD10 was expressed in 6/13 (46%, 4 focal). Alpha-Methylacyl-CoA Racemase (AMACR) was positive in 5/8 (63%) cases. Focal but intense cytoplasmic colloidal iron stain was present in 3/20 (15%) cases. Luminal or cytoplasmic/perinuclear precipitation was observed in 8/20 (40%) cases. Succinate Dehydrogenase B (SDHB) was performed in 6 cases, with all retained expression.
LOT is a clinically indolent and potentially benign entity with distinguishable morphology and immunohistochemical profile that can be performed and be easily interpreted in most of surgical pathology settings. Additional studies with larger cohorts, comprehensive molecular evaluation and longer follow-up are needed to definitively recognise these tumours as a separate entity and to further address the possibility of active surveillance options in eligible patients.
低度恶性嗜酸细胞瘤(LOT)最近被认为是一种潜在的独特实体。
在获得印第安纳大学病理学系机构审查委员会的适当许可后,检索了2005年至2020年期间的原发性肾上皮性肿瘤。
共鉴定出23例患者(男/女比例为14/9),中位年龄为66岁(23 - 84岁)。大多数患者接受了部分肾切除术(15/23,65%),肿瘤中位大小为4.0 cm(2.2 - 10.5 cm)。仅1例肿瘤侵犯至肾外(肾周脂肪)。紧密排列的嗜酸细胞瘤细胞呈实性/弥漫性增生,偶见小管形成,间质突然出现水肿改变,伴有松散连接的小簇肿瘤细胞。所有病例均弥漫性表达CK7且不表达CD117,23例中有8例(35%,5个灶性)波形蛋白呈阳性。13例中有6例(46%,4个灶性)表达CD10。5/8(63%)例α-甲基酰基辅酶A消旋酶(AMACR)呈阳性。3/20(15%)例可见局灶性但强烈的细胞质胶体铁染色。8/20(40%)例观察到管腔或细胞质/核周沉淀。对6例进行了琥珀酸脱氢酶B(SDHB)检测,所有病例均保留表达。
LOT是一种临床惰性且可能为良性的实体,具有可区分的形态学和免疫组化特征,在大多数外科病理环境中均可进行且易于解读。需要进行更大样本量的队列研究、全面的分子评估以及更长时间的随访,以明确将这些肿瘤认定为一个独立实体,并进一步探讨符合条件的患者进行主动监测的可能性。
