中国肿瘤临床
中國腫瘤臨床
중국종류림상
CHINESE JOURNAL OF CLINICAL ONCOLOGY
2015年
7期
373-377
,共5页
李婵娟%赵海丰%赵伟鹏%李倩%赵智刚%王晓芳%于泳%王亚非%张翼鷟
李嬋娟%趙海豐%趙偉鵬%李倩%趙智剛%王曉芳%于泳%王亞非%張翼鷟
리선연%조해봉%조위붕%리천%조지강%왕효방%우영%왕아비%장익작
骨髓增生异常综合征%急性髓系白血病%临床特征%病因%治疗
骨髓增生異常綜閤徵%急性髓繫白血病%臨床特徵%病因%治療
골수증생이상종합정%급성수계백혈병%림상특정%병인%치료
myelodysplastic syndrome%acute myeloid leukemia%clinicopathological features%etiology%treatment
目的:探讨恶性肿瘤继发骨髓增生异常综合征/急性髓系白血病(t-MDS/AML)的病因、临床特点及治疗策略。方法:对2008年1月至2014年7月在天津医科大学肿瘤医院就诊的11例t-MDS/AML患者的临床资料进行回顾性分析。结果:11例恶性肿瘤患者前期均有不同程度的细胞毒药物、抗代谢药物、含紫杉类药物(和)或放射线治疗史,与t-MDS/AML确诊中位间隔时间为36个月;患者主要表现为乏力、呼吸困难、发热、出血等血细胞减少相关症状;以对症支持治疗,免疫调节治疗及化疗为主,中位OS为28个月,中位DFS为19个月,3年总生存率44.4%。结论:t-MDS/AML继发于肿瘤性疾病或非肿瘤性疾病行细胞毒药物化疗或放疗后,总体疗效欠佳,预后不良;在制定放、化疗方案前,应充分考虑可能导致t-MDS/AML的危险因素,认真评估治疗受益及风险。
目的:探討噁性腫瘤繼髮骨髓增生異常綜閤徵/急性髓繫白血病(t-MDS/AML)的病因、臨床特點及治療策略。方法:對2008年1月至2014年7月在天津醫科大學腫瘤醫院就診的11例t-MDS/AML患者的臨床資料進行迴顧性分析。結果:11例噁性腫瘤患者前期均有不同程度的細胞毒藥物、抗代謝藥物、含紫杉類藥物(和)或放射線治療史,與t-MDS/AML確診中位間隔時間為36箇月;患者主要錶現為乏力、呼吸睏難、髮熱、齣血等血細胞減少相關癥狀;以對癥支持治療,免疫調節治療及化療為主,中位OS為28箇月,中位DFS為19箇月,3年總生存率44.4%。結論:t-MDS/AML繼髮于腫瘤性疾病或非腫瘤性疾病行細胞毒藥物化療或放療後,總體療效欠佳,預後不良;在製定放、化療方案前,應充分攷慮可能導緻t-MDS/AML的危險因素,認真評估治療受益及風險。
목적:탐토악성종류계발골수증생이상종합정/급성수계백혈병(t-MDS/AML)적병인、림상특점급치료책략。방법:대2008년1월지2014년7월재천진의과대학종류의원취진적11례t-MDS/AML환자적림상자료진행회고성분석。결과:11례악성종류환자전기균유불동정도적세포독약물、항대사약물、함자삼류약물(화)혹방사선치료사,여t-MDS/AML학진중위간격시간위36개월;환자주요표현위핍력、호흡곤난、발열、출혈등혈세포감소상관증상;이대증지지치료,면역조절치료급화료위주,중위OS위28개월,중위DFS위19개월,3년총생존솔44.4%。결론:t-MDS/AML계발우종류성질병혹비종류성질병행세포독약물화료혹방료후,총체료효흠가,예후불량;재제정방、화료방안전,응충분고필가능도치t-MDS/AML적위험인소,인진평고치료수익급풍험。
Objective:To investigate the etiology, clinical characteristics, and treatment of myelodysplastic syndrome/acute my-eloid leukemia (t-MDS/AML) secondary to malignant tumors. Methods: We retrospectively analyzed 11 patients with t-MDS/AML and investigated the treatment of primary tumors, clinical manifestations, treatment, and survival of t-MDS/AML patients. Results:A total of 11 patients were exposed to cytotoxic chemotherapeutic agents or radiation therapy for their primary tumors. The median laten-cy was 36 months. Common symptoms were fatigue, dyspnea, bleeding, and infection, all of which were related to deficits in hemato-poiesis. Therapeutic regimen included support therapy, immunomodulatory therapy, and chemotherapy. The median overall survival and disease-free survival periods were 28 months and 19 months, respectively, and the overall survival rate for 3 years was 44.4%. Conclu-sion:t-MDS/AML is a serious complication of chemotherapy or radiotherapy for a malignant or nonmalignant condition. The curative effect is limited, and prognosis is poor. Therefore, we should take t-MDS/AML into consideration when making treatment plans for can-cer patients to evaluate treatment benefits and to avoid treatment-related complications.
