形态学在急性白血病诊断中的作用:系统综述

M. Sekar, Manasa Raj, P. Manivannan
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引用次数: 1

摘要

血液病理学家在急性白血病(AL)诊断中的作用始于外周血涂片或骨髓的形态学检查。成髓细胞的形态学特征包括“奥尔棒”和“Phi体”。在资源有限的情况下,细胞化学染色如髓过氧化物酶、苏丹黑B、周期性酸性希夫染色、非特异性酯酶和珀尔斯染色作为形态学分类的重要辅助手段。最近的世界卫生组织分类仍然支持形态学的应用,形态学要求存在≥20%的淋巴母细胞或髓母细胞/或其等效物(单核细胞、原细胞或巨核母细胞),并将其与临床特征、免疫表型(IP)和分子遗传学相结合,以诊断AL。形态学可以为t(8:21)、t(15:17)、t(16:16)的急性髓性白血病(AML)的特异性诊断提供线索。或者inv(16),如果分子检测证实了这种易位,则可以不考虑胚数而进行诊断。有一些有趣的发现,如具有“手镜”形态的母细胞,核分裂,突出的细胞质空泡,伪chediak - higashi颗粒,杯状核,以及其他有助于区分淋巴和髓性白血病的发育异常特征。唐氏综合征和AL发育不良患者可在形态学检查中发现短暂性骨髓增生异常。骨髓活检对抽吸涂片是非常有益和补充的,是诊断准确的细胞结构、细胞地形、发育不良、骨髓坏死、胶质骨髓转化、骨髓纤维化所必需的,并且可以使用免疫组织化学进行IP。AL的形态学检查不仅有助于诊断,而且有助于预测治疗后病例、伴有骨髓增生异常相关改变的AML、治疗相关的髓系肿瘤和混合表型AL的预后。造血细胞、囊胚样套细胞淋巴瘤、囊胚样形态的高级别B细胞淋巴、Burkitt白血病、原淋巴细胞白血病中的前淋巴细胞、毛细胞白血病变异、浆母细胞特别是浆母细胞白血病中的浆母细胞。或浆细胞白血病可以模拟AL, IP在这些情况下是有用的。因此,形态学应被视为AL病例分析的一种“金标准”起点。形态学检查不能代替,高级检查不能代替形态学检查。
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Role of Morphology in the Diagnosis of Acute Leukemias: Systematic Review
Abstract The role of hematopathologists in the diagnosis of acute leukemia (AL) starts with the morphological examination of either peripheral blood smear or bone marrow. The morphological hallmark for the myeloblast includes “Auer rods” and “Phi bodies.” The addition of cytochemical stains such as myeloperoxidase, Sudan Black B, periodic acid-Schiff stain, nonspecific esterase, and Perls' stain acts as an important adjunct to the morphological classification in the resource-constrained settings. The recent World Health Organization classification still endorses the utility of morphology which requires the presence of either ≥ 20% lymphoblasts or myeloblasts/or its equivalents (monoblasts, promonocytes, or megakaryoblasts) and integrates it with the clinical features, immunophenotyping (IP), and molecular genetics for making the diagnosis of AL. Morphology can give clue to the specific diagnosis of acute myeloid leukemia (AML) with t(8:21), t(15:17), t(16:16), or inv(16) and this diagnosis can be made irrespective of blasts count if such translocations are demonstrated by molecular tests. There are some interesting findings such as blasts with “hand-mirror” morphology, nuclear cleavage, prominent cytoplasmic vacuoles, pseudo-Chediak-Higashi granules, cup-like nucleus, and other dysplastic features helping in differentiating lymphoid and myeloid leukemias. Transient abnormal myelopoiesis in Down syndrome and hypoplastic AL can be picked up on morphological examination. Bone marrow biopsy would be greatly beneficial and complementary to aspirate smears and is required for diagnosing exact cellularity, topography of cells, dyspoiesis, myelonecrosis, gelatinous marrow transformation, myelofibrosis, and IP can be performed using immunohistochemistry. Morphological examination in AL is not only helpful for diagnosis but also useful for predicting the prognosis in posttherapy cases, AML with myelodysplasia-related changes, therapy-related myeloid neoplasms, and mixed phenotype AL. Hematogones, blastoid mantle cell lymphoma, high grade B cell lymphoid with blastoid morphology, Burkitt leukemia, prolymphocytes in prolymphocytic leukemia, hairy cell leukemia variant, plasmablasts especially in plasmablastic leukemia, or plasma cell leukemia can mimic AL and IP is useful in these situations. Hence, morphology should be considered as a kind of “gold-standard” starting point for the analysis of AL cases. Morphological examination cannot be replaced and advanced tests cannot be used as surrogate for morphology.
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期刊介绍: The journal will cover technical and clinical studies related to medical and pediatric oncology in human well being including ethical and social issues. Articles with clinical interest and implications will be given preference.
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