中华老年多器官疾病杂志
中華老年多器官疾病雜誌
중화노년다기관질병잡지
CHINESE JOURNAL OF MULTIPLE ORGAN DISEASES IN THE ELDERLY
2013年
8期
570-574
,共5页
路瑾%鲍立%卢锡京%刘艳荣%赖悦云%黄晓军
路瑾%鮑立%盧錫京%劉豔榮%賴悅雲%黃曉軍
로근%포립%로석경%류염영%뢰열운%황효군
Waldenstrom巨球蛋白血症%免疫表型分型%细胞遗传学%治疗
Waldenstrom巨毬蛋白血癥%免疫錶型分型%細胞遺傳學%治療
Waldenstrom거구단백혈증%면역표형분형%세포유전학%치료
Waldenstrom macroglobulinemia%immunophenotyping%cytogenetics%therapy
目的分析Waldenstrom巨球蛋白血症(WM)形态学、细胞免疫表型、细胞遗传学以及分子生物学(MICM)异常的特点。方法收集1999至2010年MICM资料完整的初治WM患者41例,男27例、女14例。回顾性分析其临床表现、骨髓形态、细胞免疫表型、细胞遗传学、免疫球蛋白重链基因重排、黑色素瘤优先表达抗原(PRAME)的表达及其与临床预后之间的关系。结果本组中高危患者占58.5%。细胞免疫表型分析:CD19阳性100.0%,CD20阳性97.6%,CD38阳性74.1%,FMC7阳性36.9%,CD5阳性10.0%,CD23阳性31.6%,HLA-DR阳性83.3%,CXCR4阳性85.7%。常规细胞遗传学以及荧光原位杂交发现特异性细胞遗传学异常。PRAME在WM中表达增加,且与骨髓中淋巴细胞数相关, MAGEC1/CT7在WM中不表达。WM使用含利妥昔单抗联合化疗较环磷酰胺+长春地辛+醋酸泼尼松(COP)方案治疗未见生存优势。结论 WM具有独特的MICM特征,通过MICM的综合检测有助于早期诊断WM并对疾病进行监测,利妥昔单抗治疗未见明显优势。
目的分析Waldenstrom巨毬蛋白血癥(WM)形態學、細胞免疫錶型、細胞遺傳學以及分子生物學(MICM)異常的特點。方法收集1999至2010年MICM資料完整的初治WM患者41例,男27例、女14例。迴顧性分析其臨床錶現、骨髓形態、細胞免疫錶型、細胞遺傳學、免疫毬蛋白重鏈基因重排、黑色素瘤優先錶達抗原(PRAME)的錶達及其與臨床預後之間的關繫。結果本組中高危患者佔58.5%。細胞免疫錶型分析:CD19暘性100.0%,CD20暘性97.6%,CD38暘性74.1%,FMC7暘性36.9%,CD5暘性10.0%,CD23暘性31.6%,HLA-DR暘性83.3%,CXCR4暘性85.7%。常規細胞遺傳學以及熒光原位雜交髮現特異性細胞遺傳學異常。PRAME在WM中錶達增加,且與骨髓中淋巴細胞數相關, MAGEC1/CT7在WM中不錶達。WM使用含利妥昔單抗聯閤化療較環燐酰胺+長春地辛+醋痠潑尼鬆(COP)方案治療未見生存優勢。結論 WM具有獨特的MICM特徵,通過MICM的綜閤檢測有助于早期診斷WM併對疾病進行鑑測,利妥昔單抗治療未見明顯優勢。
목적분석Waldenstrom거구단백혈증(WM)형태학、세포면역표형、세포유전학이급분자생물학(MICM)이상적특점。방법수집1999지2010년MICM자료완정적초치WM환자41례,남27례、녀14례。회고성분석기림상표현、골수형태、세포면역표형、세포유전학、면역구단백중련기인중배、흑색소류우선표체항원(PRAME)적표체급기여림상예후지간적관계。결과본조중고위환자점58.5%。세포면역표형분석:CD19양성100.0%,CD20양성97.6%,CD38양성74.1%,FMC7양성36.9%,CD5양성10.0%,CD23양성31.6%,HLA-DR양성83.3%,CXCR4양성85.7%。상규세포유전학이급형광원위잡교발현특이성세포유전학이상。PRAME재WM중표체증가,차여골수중림파세포수상관, MAGEC1/CT7재WM중불표체。WM사용함리타석단항연합화료교배린선알+장춘지신+작산발니송(COP)방안치료미견생존우세。결론 WM구유독특적MICM특정,통과MICM적종합검측유조우조기진단WM병대질병진행감측,리타석단항치료미견명현우세。
Objective To analyze the morphology, immunophenotypes, cytogenetics and molecular biology (MICM) abnomaities of Waldenstrom macroglobulinemia (WM). Methods Clinical data of 41 patients with newly diagnosed WM from 1999 to 2010 were collected and studied retrospectively (including 27 males and 14 females). Their clinical manifestations, cell morphology in bone marrow, immunophenotypes, and cytogenetics, immunoglobulin heavy chain gene rearrangement, and expression of preferentially expressed antigen of melanoma (PRAME) were examined by G-banding and FISH, PCR-IgH and RQ-PCR-PRAME and MAGE C1/CT7, and the results were analyzed with clinical prognosis. Results The incidence of high risk patients accounted for 58.5%. Their imunnophenotypes was 100.0%positive to CD19, 97.6%positive to CD20, 74.1%positive to CD38, 36.9%positive to FMC7, 10.0% positive to CD5, 31.6%positive to CD23, 83.3%positive to HLA-DR, and 85.7%positive to CXCR4. There were specific cytogenetic abnormalities found by G-Banding and FISH. RQ-PCR-PRAME had high quantities in WM, which was related to the number of lymphocyte in bone marrow. The MAGE C1/CT7 was negatively expressed in WM. There was no significant survival difference between the Rituximab containing regimen and COP (cyclophosphamide combined with vindisine and prednisone) in treatment of WM. Conclusion WM has specific MICM characteristics. Integrating those measures is helpful to diagnose WM as early as possible, and to monitor the disease during the treatment. Rituximab has no survival benefit in this cohort of patients.
