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AL淀粉样变性中肿瘤性浆细胞的免疫表型

Immunophenotype of neoplastic plasma cells in AL amyloidosis.

作者信息

Deshmukh M, Elderfield K, Rahemtulla A, Naresh K N

机构信息

Department of Histopathology, Hammersmith Hospital and Imperial College, London, UK.

出版信息

J Clin Pathol. 2009 Aug;62(8):724-30. doi: 10.1136/jcp.2009.065474.

Abstract

AIM

AL amyloidosis (ALA) is a form of plasma cell (PC) dyscrasia characterised by deposition of insoluble fibrillar deposits in various organs causing organ damage. This is believed to be the first study to evaluate the expression of CD79a, CD20, CD56, cyclin D1 and epithelial membrane antigen (EMA) in neoplastic PCs of ALA.

METHODS AND RESULTS

The study included 36 well-documented cases of ALA. In all cases presence of amyloid deposits had been documented by Congo Red stain in the bone marrow trephine biopsy (BMTB) and/or in other tissues. BMTBs showed varying degrees of PC infiltration (median 12%). In eight of the 36 cases with associated myeloma, the mean (2 x SE) percentage of PCs (PC%) was 34 (18)%, while in the remaining, PC% was 15 (4)%. Expression of CD20, CD79a, CD56, cyclin D1 and EMA was noted in 42%, 86%, 50%, 53% and 83% of cases, respectively. Aberrant antigen expression in the form of CD56 and/or cyclin D1 expression was seen in 79% of cases. Nine of 10 cases with small lymphoid-like PCs were positive for CD20 and all the 10 cases were positive for cyclin D1. On the other hand, among cases without small lymphoid-like morphology, CD20 and cyclin D1 expression was seen in only 6 of 26 and 8 of 26 cases respectively (p = 0.001 and 0.002 respectively). CD20 expression correlated with cyclin D1 expression (p = 0.045). Cytological atypia/pleomorphism was predictive of associated myeloma (p = <0.001).

CONCLUSION

Marrow involvement by neoplastic PCs in ALA can be identified by their aberrant antigen expression apart from light chain restriction, and rituximab as a possible treatment option may be explored in CD20-positive ALA.

摘要

目的

AL型淀粉样变性(ALA)是浆细胞(PC)发育异常的一种形式,其特征是不溶性纤维状沉积物在各器官沉积,导致器官损伤。据信,这是第一项评估CD79a、CD20、CD56、细胞周期蛋白D1和上皮膜抗原(EMA)在ALA肿瘤性PC中表达情况的研究。

方法与结果

该研究纳入36例记录完整的ALA病例。所有病例均通过刚果红染色在骨髓活检组织切片(BMTB)和/或其他组织中证实有淀粉样沉积物存在。BMTB显示不同程度的PC浸润(中位数为12%)。在36例合并骨髓瘤的病例中,8例PC的平均(2×标准误)百分比为34(18)%,其余病例中PC百分比为15(4)%。CD20、CD79a、CD56、细胞周期蛋白D1和EMA的表达分别见于42%、86%、50%、53%和83%的病例。79%的病例出现以CD56和/或细胞周期蛋白D1表达形式的异常抗原表达。10例小淋巴细胞样PC的病例中有9例CD20阳性,所有10例细胞周期蛋白D1均阳性。另一方面,在无小淋巴细胞样形态的病例中,CD20和细胞周期蛋白D1表达分别仅见于26例中的6例和8例(p值分别为0.001和0.002)。CD20表达与细胞周期蛋白D1表达相关(p = 0.045)。细胞异型性/多形性可预测合并骨髓瘤(p = <0.001)。

结论

除轻链限制外,肿瘤性PC对骨髓的累及可通过其异常抗原表达来识别,对于CD20阳性的ALA,可探索将利妥昔单抗作为一种可能的治疗选择。

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