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[大剂量化疗并随后进行造血细胞移植对在初次化疗中接受阿霉素治疗的恶性淋巴瘤患者左心室功能的影响]

[Effect of high-dose chemotherapy with subsequent transplantation of blood-forming cells on left ventricle function in patients with malignant lymphomas treated with doxorubicin in primary chemotherapy].

作者信息

Elbl L, Vásová I, Krejcí M, Navrátil M, Tomásková I, Jedlicka F, Chaloupka V, Mayer J, Vorlícek J

机构信息

Oddelení funkcního vysetrováni FN Brno, pracoviste Bohunice.

出版信息

Vnitr Lek. 2006 Mar;52(3):221-31.

Abstract

PURPOSE OF STUDY

The authors examined whether high-dose chemotherapy with hematogenic tissue transplantation might negatively affect function of left ventricle (LV) in oncology patients with malignant lymphomas initially treated with conventional chemotherapy consisting of doxorubicin (DOX) in contrast to patients treated without the transplantation in medium-term follow up.

PATIENTS AND METHODOLOGY

The follow up group included 77 patients (39 women/38 men) at the age of 36 +/- 15 (median 30, 16-67 years). All 77 patients were treated with initial chemotherapy with DOX, 22 out of that group later received high-dose chemotherapy with hematogenic tissue transplantation (HTT). 16 (73 %) patients of this subgroup underwent autologous transplantation and 5 (23 %) allogeneic transplantation. One female patient (4 %) underwent both autologous and allogeneic transplantation. The follow up period after completion of initial chemotherapy was 5-10 years (median 6 years). The patients were examined with rest echocardiography before start, after chemotherapy, and during follow-up examination. Spiroergometric test (SET) was only performed at the follow-up examination.

RESULTS

Both subgroups showed significant decrease of ejection fraction (EF) after chemotherapy, with further decrease in the control examination period, without mutual difference. While the HTT (HTT+) group showed no EF drop below 50 %, in the non-HTT (HTT-) group EF dropped in two (4 %) patients after chemotherapy and in four (8%) patients at the control examination. Progressing decrease of EF > 10 % was reported with 25 % of the HTT- patients (p < 0.05), but with just 13 % of the HTT+ patients (non-significant). The diastolic insufficiency (DF) was present identically in both groups with 36 % of the patients, which represents a statistically significant increase in comparison to the pre-chemotherapy condition. SET did not show any differences in burden toleration and circulation indicators between the two groups. The drop of pVO2 < 20 ml/kg/min occurred with 22 patients of both groups. Linear regression data analysis revealed existence of a significant relationship between EF change, some diastolic function indicators, pVO2 and cumulative dose of DOX (p < 0.05). The current age significantly and negatively correlated with pVO2 (p < 0.001) and DF indicators (p < 0.001). The follow up period inversely correlates with the changes of EF (p < 0.05) and pVO2 (p < 0.05), not correlating with diastolic function indicators. Multi-variant analysis did not confirm any higher risk of administration of high-dose chemotherapy with HTT for significant drop of EF or its drop down to the pathological zone below 50 % (OR = 0.46; non-significant), for discovery of reduced cardio-pulmonary performance (pVO2 < 20 ml/kg/min) (OR = 0.35; non-significant) or for development of diastolic dysfunction (OR = 1.0; non-significant).

CONCLUSIONS

Treatment with high-dose chemotherapy with HTT application within medium-term follow up does not result in any significant systolic or diastolic malfunction of myocardium and deterioration of cardiopulmonary performance in comparison to patients not undergoing this therapy. Treatment with cardiotoxic doxorubicin administered in the context of basic conventional chemotherapy is most likely to be responsible for occurrence of the pathological effects across the followed up group. Length of monitoring is a significant factor correlating with changed ejection fraction. This finding justifies the need for long-term prospective monitoring of ejection fraction of the left ventricle in adult patients treated with cardiotoxic chemotherapy.

摘要

研究目的

作者研究了接受造血组织移植的高剂量化疗是否会对最初接受含阿霉素(DOX)的常规化疗的恶性淋巴瘤肿瘤患者的左心室(LV)功能产生负面影响,对比中期随访中未接受移植治疗的患者。

患者与方法

随访组包括77例患者(39名女性/38名男性),年龄为36±15岁(中位数30岁,范围16 - 67岁)。所有77例患者均接受了含DOX的初始化疗,其中22例随后接受了造血组织移植(HTT)的高剂量化疗。该亚组中的16例(73%)患者接受了自体移植,5例(23%)接受了异体移植。1例女性患者(4%)接受了自体和异体移植。初始化疗完成后的随访期为5 - 10年(中位数6年)。在开始前、化疗后及随访检查时对患者进行静息超声心动图检查。仅在随访检查时进行运动心肺功能试验(SET)。

结果

两个亚组在化疗后射血分数(EF)均显著下降,在对照检查期进一步下降,两组间无差异。虽然HTT(HTT +)组的EF未降至50%以下,但在非HTT(HTT -)组中,2例(4%)患者化疗后EF下降,4例(8%)患者在对照检查时EF下降。HTT -组中有25%的患者EF下降>10%(p < 0.05),而HTT +组中只有13%的患者出现这种情况(无统计学意义)。两组中36%的患者存在相同程度的舒张功能不全(DF),与化疗前相比有统计学意义的增加。SET显示两组在负荷耐受和循环指标方面无差异。两组均有22例患者出现pVO2 < 20 ml/kg/min的下降。线性回归数据分析显示EF变化、一些舒张功能指标、pVO2与DOX累积剂量之间存在显著关系(p < 0.05)。当前年龄与pVO2(p < 0.001)和DF指标(p < 0.001)呈显著负相关。随访期与EF变化(p < 0.05)和pVO2变化(p < 0.05)呈负相关,与舒张功能指标无关。多变量分析未证实接受HTT的高剂量化疗会显著增加EF大幅下降或降至50%以下的病理区域的风险(OR = 0.46;无统计学意义),也未增加发现心肺功能降低(pVO2 < 20 ml/kg/min)的风险(OR = 0.35;无统计学意义)或舒张功能障碍的风险(OR = 1.0;无统计学意义)。

结论

与未接受该治疗的患者相比,中期随访中接受HTT的高剂量化疗不会导致心肌出现任何显著的收缩或舒张功能障碍以及心肺功能恶化。在基础常规化疗中使用具有心脏毒性的阿霉素治疗最有可能是整个随访组出现病理效应的原因。监测时长是与射血分数变化相关的一个重要因素。这一发现证明了对接受心脏毒性化疗的成年患者进行左心室射血分数长期前瞻性监测的必要性。

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