Effects of Dendritic Cell-activated and Cytokine-induced Killer Cell Therapy on 22 Children with Acute Myeloid Leukemia after Chemotherapy

The efficiency of dendritic cell-activated and cytokine-induced killer cell（DC-CIK） therapy on children with acute myeloid leukemia（AML） after chemotherapy was investigated. Mononuclear cells were collected from children achieving complete remission after chemotherapy,cultured in vitro and transfused back into the same patient. Interleukin-2（IL-2） was injected subcutaneously every other day 10 times at the dose of 1×106 units. Peripheral blood lymphocyte subsets and minimal residual disease（MRD） were detected by flow cytometry. Function of bone marrow was monitored by methods of morphology,immunology,cytogenetics and molecular biology. The side effects were also observed during the treatment. The average follow-up period for all the 22 patients was 71 months and relapse occurred in two AML patients（9.1%）. The percentage of CD3＋/CD8＋ cells in peripheral blood of 15 patients at the 3rd month after DC-CIK treatment（36.73%±12.51%） was dramatically higher than that before treatment（29.20%±8.34%,P〈0.05）. The MRD rate was 〉0.1% in 5 patients before the treatment,and became lower than 0.1% 3 months after the treatment. During the transfusion of DC-CIK,side effects including fever,chills and hives appeared in 7 out of 22（31.82%） cases but disappeared quickly after symptomatic treatments. There were no changes in electrocardiography and liver-renal functions after the treatment. MRD in children with AML can be eliminated by DC-CIK therapy which is safe and has fewer side effects.

Detection and clinical significance of multidrug resistance-1 mRNA in bone marrow cells in children with acute lymphoblastic leukemia by real-time fluorescence quantitative RT-PCR

Objective： Multidrug resistance（MDR） is one of the most important reasons for treatment failure and recurrence of acute leukemia. Its manifestations are different in children with acute lymphoblastic leukemia（ALL） which may be due to different detection methods. This study was to detect the expression of MDR1 mRNA in bone marrow cells of children with ALL by real-time fluorescence- quantitative reverse transcription polymerase-chain reaction（FQ-RT-PCR）, and combine minimal residual desease（MRD） detection by flow cytometry（FCM） and to study their relationship with treatment response and prognosis of ALL. Methods：The MDR1 mRNA levels in bone marrow cells from 67 children with ALL[28 had newly diagnosed disease, 27 had achieved complete remission（CR）, 12 recurrent] and 22 children without leukemia were detected by FQ-RT-PCR. MRD was detected by FCM. The patients were observed for 9-101 months, with a median of 64 months. Results：Standard curves of human MDR1 and GAPDH genes were constructed successfully. MDR1 mRNA was detected in all children with a positive rate of 100%. The mRNA level of MDR1 was similar among the newly diagnosed ALL group, CR group, and control group（P 〉 0.05）, but significantly higher in the recurrence group than that in newly diagnosed disease group and control group（0.50 ± 0.55 vs. 0.09 ± 0.26 and 0.12 ± 0.23, P〈 0.05）. 54 ALL patients were followed up, and it was found that MDR1 mRNA level was significantly higher in ALL patients within 3 years duration than that of ALL patients with 3-6 years and over 6 years duration（0.63 ± 0.56 vs. 0.11 ± 0.12 and 0.04 ± 0.06, P〈 0.01）. For the 28 children with newly diagnosed disease, the MDR1 mRNA level was similar between WBC 〉 50 ~ 109 group and WBC〈50 × 10^9 group（P〉 0.05）. In the 33 CR patients, the MDR1 mRNA level was significantly higher in MRD〉10a group than that in MRD〈10a group（0.39 ± 0.47 vs. 0.03 ± 0.03, P 〈 0.05）. Conclusion：The sensitivity and specificity of FQ-RT-PCR in detecting MDR1 mRNA in bone marrowy cells of children with ALL patients are high. MDR1 mRNA is expressed in children with and without leukemia. MDR1 mRNA is highly expressed in the CR ALL patients with high MRD, recurrence and short duration（within 3 years）. Monitoring MRD and the MDR1 mRNA level might be helpful for individual treatment.

Parental Occupational Exposure and Risk of Acute Leukemia in Children: A Tunisian Population-Based Case-Control Study

Background: In recent decades, the incidence of children’s hematological malignancies has been increasing worldwide including Tunisia. Their severity is reflected in the importance of the medical, social and economic impact. This increase remains fully unexplained, and the involvement of genetic, environmental and occupational factors is strongly suspected. Materials and methods: Our study was a cross-sectional survey of the type case-control conducted in the University Hospital of Farhat Hached of Sousse during the period ranging between 1 July 2011 and 30 June 2012, and which included children with acute leukemia compared to children unharmed by neoplastic disease. Cases and controls were matched by age and gender. Our objective was to describe the socio-occupational characteristics of the parents of children with acute leukemia and to identify potential occupational factors implicated in the genesis of acute leukemia. Results: The number of acute leukemia cases in the Hematology Service and day hospital of the University Hospital of Farhat Hached during the study period was 66 cases divided into in 40 boys and 26 girls with a sex ratio of 1.53. Our cases and controls were matched by age and gender. The risk of incidence of leukemia in children from smoking fathers was higher (p = 0.02, OR = 2.24, IC = [1.11 - 4.52]). The risk of incidence of leukemia in children from alcoholic fathers was higher with p = 0.009, OR = 3.9;CI = [1.33 - 11.39]. After adjusting different variables, the difference persisted significantly with pa = 0.03 and ORa = 3.5, ICa = [1.09 - 11.6]. 25.7% of cases had a family history of blood disease and neoplasia, whereas no control presented that. The difference was statistically significant (p = 0.006, OR = 1.46, IC = [1.38 - 1.56]). The parental occupational exposures associated to the occurrence of acute leukemia in children were pesticides with a statistically significant difference (p = 0.03, OR = 2.94, IC = [1.06 - 8.13]). This difference persisted after adjustment with different variables pa = 0.01, ORa 3.75;ICa = [1.27 - 11.03]. This difference had become significant after adjustment with the different variables pa = 0.03, ORa = 2.67, ICa = [1.06 - 6.7]. Conclusion: Our results showed some support for a positive association between childhood acute leukemia risk and parental occupational exposure to pesticides and cement. Additionally, acute leukemia risk among children might be increased with parental alcohol consumption.

ADE as Induction Therapy Results in Treatment of Children with Non-M3 High-Risk Acute Myeloid Leukemia, an Extrapolable Achievement in Developing Countries

Background: In Mexico, AML survival is referred in 30%. Our aim was to evaluate results with ADE protocol as induction treatment in children with non-M3 AML in a public Mexican institution. Method: We included patients with AML in a single institution between 2005 and 2013. All non-M3-AML patients received ADE as induction therapy (cytarabine 100 mg/m2 in continuous infusion from day 1 to 7, daunorrubicin 30 mg/m2 days 1, 3, 5 and etoposide 100 mg/m2 over days 1 to 5). Patients received antibiotic prophylaxis and strict scheduled appointments to assure adherence and prevent avoidable emergencies. Main Results: Eighteen patients were included. Median age was 106 months. One patient died at diagnosis so 17 were eligible for induction results analysis;eleven needed two cycles and six patients three. Remission rate was 100%. Analyzing non-M3 patients overall survival was 80.2% at 100 months. No fatal complications were observed. Stratifying by number of cycles we observe that patients receiving one ADE cycle had a 0% overall survival at short follow up, with 2 ADE cycles 80% at 100 months and with 3 cycles 100% at 60 months. Conclusion: ADE induction therapy showed improved results in overall survival compared with other standard regimens. Following the protocol we obtained 100% remission. This is an important achievement in our population. Our focus must be to ameliorate maintenance final results. These results should be reproduced in other hospitals in Mexico and other countries.

左旋门冬酰胺酶、培门冬酶对急性淋巴细胞白血病患儿的治疗效果比较

目的 对比左旋门冬酰胺酶、培门冬酶对急性淋巴细胞白血病(ALL)患儿的治疗效果。方法 回顾性收集2016年6月至2022年9月无锡市儿童医院收治的所有ALL患儿临床资料,根据治疗方法不同随机选取左旋门冬酰胺酶组和培门冬酶组,例数各37例。两组均进行常规基础治疗,在此基础上,左旋门冬酰胺酶组采用左旋门冬酰胺酶进行治疗,培门冬酶组采用培门冬酶进行治疗,两组均治疗46天,并随访3个月。统计两组治疗46天的临床疗效及治疗期间不良反应发生情况,比较两组治疗前、治疗21天、46天后、随访3个月后糖脂代谢指标及治疗前、治疗21天、46天后细胞因子、凝血功能、肝功能。结果 治疗46天后,与左旋门冬酰胺酶组比较,培门冬酶组总缓解率差异无统计学意义(P>0.05),而完全缓解率更高(χ^(2)=4.874,P<0.05)。治疗前及治疗21天、46天后、随访3个月后,两组血清胰岛素、C肽水平呈降低趋势,不同时间点比较,差异具有统计学意义(P<0.05);治疗21天后,培门冬酶组高于左旋门冬酰胺酶组(t=3.372、3.704,P<0.05)。治疗46天后、随访3个月后,两组血清甘油三酯(TG)水平较治疗前、治疗21天后升高,培门冬酶组高于左旋门冬酰胺酶组(t=7.181、5.635,P<0.05)。治疗前、治疗21天、46天后,两组血清肿瘤坏死因子-α(TNF-α)、白介素-6(IL-6)、白介素-8(IL-8)、白介素-10(IL-10)、干扰素-γ(IFN-γ)、铁蛋白(SF)水平呈先升高后降低趋势,不同时间点比较,差异具有统计学意义(P<0.05);治疗21天后培门冬酶组高于左旋门冬酰胺酶组(t值介于3.785~7.921之间,均P<0.05);治疗46天后培门冬酶组低于左旋门冬酰胺酶组(t值介于2.983~7.000之间,均P<0.05)。两组凝血酶原时间(PT)、活化部分凝血活酶时间(APTT)时长呈先升高后降低趋势,培门冬酶组治疗21天后长于左旋门冬酰胺酶组(t=2.985,P<0.05);两组血浆纤维蛋白原(FIB)水平呈先降低后升高趋势,培门冬酶组治疗21天后低于左旋门冬酰胺酶组(t=5.711,P<0.05);两组血清D-二聚体(D-D)、纤维蛋白原降解产物(FDP)、丙氨酸氨基转移酶(ALT)、总胆汁酸(TBil)水平呈先升高后降低趋势,培门冬酶组治疗21天、46天后高于左旋门冬酰胺酶组(t值介于3.566~40.745之间,均P<0.05)。治疗期间,培门冬酶组总不良反应发生率高于左旋门冬酰胺酶组(χ^(2)=7.341,P<0.05)。结论 与左旋门冬酰胺酶相比,采用培门冬酶治疗ALL患儿对患儿胰岛功能和肝功能、凝血功能影响较大,安全性相对较差,但其在降低患者机体炎症反应方面应用效果更好,同时疗效更好,临床可根据患儿具体情况选取合适的药物进行治疗。

CCCG-ALL-2015方案治疗儿童急性淋巴细胞白血病复发的危险因素分析

目的分析儿童急性淋巴细胞白血病(acute lymphoblastic leukemia,ALL)经中国儿童肿瘤协作组急性淋巴细胞白血病2015方案(Chinese Children's Cancer Group ALL-2015 protocol,CCCG-ALL-2015)治疗后的累积复发率(cumulative incidence of relapse,CIR),并探讨影响复发的危险因素。方法回顾性分析2015年1月—2019年12月接受CCCG-ALL-2015方案治疗的852例患儿的临床资料,计算CIR并分析影响儿童急性B淋巴细胞白血病(B-ALL)复发的危险因素。结果852例ALL患儿中,146例(17.1%)发生复发,8年CIR为(19.8±1.6)%。B-ALL与急性T淋巴细胞白血病患儿的8年CIR比较差异无统计学意义(P>0.05)。146例复发患儿中,复发时间主要集中于极早期(62例,42.5%)和早期(46例,31.5%),极早期单纯骨髓复发42例(28.8%),早期单纯骨髓复发27例(18.5%)。Cox比例风险回归模型分析显示,融合基因MLLr阳性(HR=4.177,95%CI:2.086~8.364,P<0.001)和第46天微小残留病≥0.01%(HR=2.013,95%CI:1.163~3.483,P=0.012)是B-ALL患儿经CCCG-ALL-2015方案治疗后复发的危险因素。结论儿童ALL经CCCG-ALL-2015方案治疗后仍有较高的复发率,以极早期和早期单纯骨髓复发常见;第46天微小残留病≥0.01%、融合基因MLLr阳性与B-ALL复发密切相关。

基于Snyder希望理论的护理对急性白血病患儿及其照顾者的影响

目的探讨基于Snyder希望理论的沟通护理对急性白血病患儿治疗情绪及照顾者知识认知、心理状态的影响效果。方法选取2020年1月—2022年12月医院收治的符合纳入条件的150例急性白血病患儿作为研究对象,患儿均经免疫组化染色、骨髓形态细胞学等检查确诊。按照组间基线资料均衡可比的原则将其分对照组和观察组,每组75例,每例患儿纳入1名主要照顾者。对照组患儿及其照顾者接受常规护理,观察组患儿及其照顾者接受基于Snyder希望理论的健康教育,包括分级护理、家属赋权、家属正念减压三个方面,两组患儿及照顾者均持续护理干预1个月。比较两组患儿干预前后的治疗情绪[儿童抑郁障碍自评量表(DSRSC)、儿童焦虑性情绪障碍筛查量表(SCARED)]、患儿照顾者干预前后的知识认知评分及心理状态(Herth希望量表)。结果干预前,两组患儿DSRSC、SCARED评分比较差异无统计学意义(P>0.05),干预后观察组患儿DSRSC、SCARED评分均低于对照组,差异有统计学意义(P<0.05)。干预前,两组患儿照顾者认知评分比较差异无统计学意义(P>0.05)。干预后,观察组患儿照顾者认知评分高于对照组患儿照顾者,差异有统计学意义(P<0.05),干预前,两组患儿照顾者Herth评分比较差异无统计学意义(P>0.05)。干预后,观察组患儿照顾者Herth评分高于对照组患儿照顾者,差异有统计学意义(P<0.05)。结论基于Snyder希望理论的沟通护理应用于急性白血病患儿及照顾者中效果较好,不仅能够有效改善急性白血病患儿负性情绪,还可以丰富照顾者自身知识认知水平,提高其希望水平,使其积极辅助患儿配合医护人员,促进和谐医护患关系,确保治疗护理相关工作顺利实施。

259例急性淋巴细胞白血病患儿化疗致肝损伤相关因素分析

目的总结儿童急性淋巴细胞白血病(Acute lymphoblastic leukemia,ALL)患者化疗后发生肝损伤的情况,研究性分析ALL患儿发生肝损伤的危险因素。方法回顾性分析2019年1月-2022年4月新疆医科大学第一附属医院儿科259例ALL患儿化疗的临床资料,对年龄、体重指数(BMI)、性别、化疗阶段、白蛋白水平、血红蛋白水平、否使用大剂量甲氨蝶呤、感染、髓外预防相关因素进行数据搜集,先单因素分析,对显著性影响的因素再采用logistic回归进行多因素分析。结果单因素分析结果表明性别、各年龄段、不同BMI、各化疗阶段及是否使用大剂量甲氨蝶呤对化疗后肝损伤的发生均不具有统计学意义(P>0.05)。鞘内注射、贫血、低蛋白血症、感染更容易发生化疗后肝损伤,差异均具有统计学意义。Logistic回归结果表明低蛋白血症是化疗后肝损伤发生的独立危险因素。结论儿童ALL化疗肝损伤的发生率与贫血、低蛋白血症、感染、髓外预防有关。低蛋白血症是化疗后肝损伤的独立影响因素,化疗前需给予适当治疗,从而降低化疗后肝损伤的发生率。

急性髓系白血病患儿柔红霉素耐药与PD-L1蛋白表达相关

目的研究急性髓系白血病(AML)患儿柔红霉素(DNR)耐药与程序性死亡受体配体-1(PD-L1)蛋白表达的相关性。方法选取2016年1月至2022年12月郑州大学附属儿童医院收治的110例AML患儿骨髓样本作为研究组,以50名骨髓正常供体骨髓样本作为对照组。培养人AML细胞系HL60、THP-1、U-937、Molm-13,Western blot检测PD-L1蛋白表达量。构建LV-PD-L1-shRNA、LV-PD-L1-WT-OE慢病毒载体,分析PD-L1对Molm-13细胞DNR耐药的影响及机制。结果研究组PD-L1蛋白表达量高于对照组,AML细胞系中PD-L1蛋白表达量高于健康骨髓单个核细胞(BMMC)(P<0.05),PD-L1表达与AML患儿白细胞计数、骨髓原始细胞比率、预后危险分层、两个标准化学治疗方案后疾病缓解情况有关(P<0.05)。PD-L1高表达组总生存率低于PD-L1低表达组(P<0.05)。与LV-PD-L1-WT-OE组比较,LV-PD-L1-shRNA组PD-L1 mRNA表达量降低、细胞增殖活性降低、凋亡率升高(P<0.05),LV-PD-L1-shRNA可提高Molm-13细胞对DNR的敏感性。TCGA数据库分析显示,6-磷酸葡萄糖脱氢酶(G6PD)可能为PD-L1潜在的目标基因。结论PD-L1在儿童AML中高表达,与患儿化疗耐药有关,其可能通过调控G6PD引起DNR耐药。

贵州地区急性淋巴细胞白血病儿童TPMT、NUDT15基因多态性与6-MP耐受性分析

目的观察贵州地区ALL儿童TPMT、NUDT15基因多态性,探讨其与6-MP耐受性的关系。方法收集贵阳市儿童医院血液科住院的贵州地区ALL儿童。Sanger法检测患者NUDT15c.415C>T和TPMT*2、TPMT*3A、TPMT*3B、TPMT*3C基因型。所有ALL儿童均按CCLG-2008方案化疗,每周1次监测血常规及肝肾功能。根据2016新编WHO化疗药物毒性反应分度标准,出现Ⅲ~Ⅳ度与6-MP相关的毒性反应,称为6-MP不耐受(除外感染、其他药物影响)。分析TPMT、NUDT15基因多态性与6-MP不耐受的相关性。结果共纳入患者60例,检测到TPMT突变(中间代谢型)3例(5%),正常代谢型57例(95%)。NUDT15基因CT型12例(20%),TT型1例(1.7%),CC型(野生型)47例(78.3%)。NUDT15基因突变率21.7%(13/60)显著高于TPMT基因突变率5%(3/60),差异有统计学意义(P=0.007)。TPMT突变型3例均发生6-MP不耐受(100%),NUDT15突变型13例中11例发生6-MP不耐受(84.6%)。结论TPMT、NUDT15基因突变与6-MP不耐受相关(P<0.05),联合检测TPMT、NUDT15基因对调整6-MP使用,减少6-MP不良反应提供依据。

儿童急性淋巴细胞白血病直接医疗成本分析

目的分析急性淋巴细胞白血病(ALL)患儿直接医疗成本及构成比,为医疗制度的改革提供参考依据,为白血病患儿的规范治疗提供保障。方法收集2015年1月至2018年4月重庆医科大学附属儿童医院血液肿瘤科收治的ALL患儿110例,描述性分析ALL患儿的直接医疗成本,探讨其主要构成比。结果ALL患儿规范治疗期间,直接医疗成本主要由门诊费用(平均23597元)、一日化疗病房治疗费用(平均23216元)及普通病房住院费用(平均158152元)三部分构成,在这些费用中,其中药品费、治疗费及化验费所占比例较大。平均报销比例为59.1%(93415/158152),从住院时长上看,ALL患儿平均住院时间为131 d,日均住院费用为1207元(158152/131)。结论降低药品费用,规范的治疗和检查能降低医疗成本。全方位、多角度为白血病患儿家庭提供支持,为患儿的治疗提供有力保障。

ALL患儿诱导缓解期长春新碱联合应用三唑类抗真菌药物发生毒副作用单中心分析

目的研究急性淋巴细胞白血病(ALL)儿童诱导缓解期联合应用长春新碱与三唑类药物出现的毒副作用。方法回顾性分析2010年1月1日—2013年12月31日北京儿童医院诊断为ALL患儿在诱导缓解治疗过程中长春新碱和三唑类药物联合应用出现毒副作用。将患儿分为无联合用药组、长春新碱+伊曲康唑联合组,长春新碱+伏立康唑联合组,长春新碱+氟康唑联合组,分析4组患儿相关毒副作用的发生率及治疗预后。结果共纳入ALL患儿708例,发病中位年龄为8(1~16)岁。存在长春新碱与三唑类抗真菌药物联合应用组共215例,其中联合伊曲康唑组79例,联合伏立康唑组36例,联合氟康唑组100例。无联合用药组493例。联合用药组患儿相关并发症发生率:高血压37例(17.2%),趾端麻木39例(18.1%),腱反射迟钝4例(1.8%),腹痛腹胀42例(19.5%),肠梗阻5例(2.3%),低血钠43例(20%)。联合用药组相关并发症发生率均高于无联合用药物组(P<0.05)。联合用药组中,高血压发生率、腱反射迟钝发生率及低血钠发生率:伊曲康唑组与伏立康唑组无差别(P>0.05),但大于氟康唑组(P<0.05);趾端麻木、腹痛腹胀发生率:伊曲康唑组大于伏立康唑组大于氟康唑组(P<0.05);肠梗阻发生率:伏立康唑组大于伊曲康唑组大于氟康唑组(P<0.05)。对于发生的毒副作用,给予相关的对症处理及调整药物后,相关并发症均可以得到缓解及消失。结论在ALL患儿诱导缓解治疗过程中,三唑类药物联合长春新碱用药可能加重毒副作用发生,伊曲康唑和伏立康唑相比氟康唑可能更容易加重长春新碱毒性,故建议治疗过程中避免同时使用三唑类抗真菌药物及长春新碱。

程序性死亡配体1在儿童急性髓系白血病中的表达及对耐药的影响

目的研究程序性死亡配体1(PD-L1)在儿童初治急性髓系白血病(AML)中的表达及对白血病细胞耐药的影响。方法收集2020年1月至2021年1月郑州大学附属儿童医院血液肿瘤科收治的初诊40例AML病儿骨髓标本,收集同期进行骨髓检查正常病儿的骨髓标本18例作为正常对照组,比较两组骨髓中PD-L1的表达量,并分析初治AML病儿PD-L1的表达量与其临床特征之间的关系;慢病毒构建PD-L1过表达、干扰PD-L1表达的AML细胞,细胞活力检测试剂盒(CCK8)检测细胞增殖能力,并计算细胞对柔红霉素的药物敏感性;凋亡实验检测经柔红霉素诱导的细胞凋亡水平。结果与正常对照组0.887±0.064相比,初治儿童AML病儿骨髓单个核细胞PD-L1的表达量2.927±0.271显著增高(t=7.34,P<0.001);根据一个疗程诱导化疗是否达完全缓解(CR),将初治AML病儿一个疗程达CR者定义为CR组,将未达CR者定义为NR组,相较于CR组的2.346±0.190,NR组PD-L1基因的表达量5.249±0.662显著增高(t=4.22,P=0.003);病儿不同发病年龄,性别,法、美、英(FAB)分型,白细胞计数,预后分层间PD-L1基因相对表达量比较均差异无统计学意义(P>0.05),而1个疗程诱导化疗是否达CR与PD-L1基因相对表达量差异有统计学意义(P=0.018);过表达PD-L1的Molm-13细胞对柔红霉素具有更高的IC50值,更低的凋亡率;干扰PD-L1表达的THP1细胞对柔红霉素具有更低的IC50值,更高的凋亡率。结论PD-L1在初治AML病儿中表达增高,且PD-L1的高表达与1个疗程诱导治疗是否达CR显著相关;PD-L1可以促进AML细胞增殖、抑制凋亡,从而导致化疗耐药。

急性白血病患儿行为特征的潜在类别分析及影响因素

目的:利用潜在类别分析法探讨急性白血病患儿行为特征的潜在类别及影响因素,为制定白血病患儿行为问题精准干预策略提出循证依据。方法:便利抽样法选取重庆医科大学附属儿童医院血液科202例急性白血病患儿及其照顾者为研究对象,使用一般资料调查表、Rutter儿童行为问卷、一般家庭功能分量表、社会支持评定量表对其进行调查。利用潜在类别分析对急性白血病患儿行为特征进行分类,采用无序多分类logistic回归分析各因素对不同类别的影响。结果:急性白血病患儿行为特征可分为3种类型,其中冲动-不友善型占50%,情绪-躯体障碍型占33.66%,良好行为型占16.34%;无序多分类logistic回归结果显示,不健康的家庭功能、男性患儿易发展为冲动-不友善型,不健康的家庭功能、男性患儿、治疗期易发展为情绪-躯体障碍型,治疗期患儿易发展为情绪-躯体障碍型。结论:急性白血病患儿行为特征存在明显不同的分类特征,与家庭功能、性别、疾病阶段关系密切。因此应针对不同类别特征的急性白血病患儿制定个性化干预措施,预防或减少其行为问题的发生,进而提升其社会适应能力及生存质量。

EB病毒感染急性淋巴细胞白血病患儿临床特征分析

目的了解EB病毒感染急性淋巴细胞白血病(ALL)患儿的临床特征,为临床干预提供参考。方法选取2020年1月—2022年8月河北省儿童医院90例≤17岁ALL住院患儿,根据是否感染EB病毒分为感染组(78例)和未感染组(12例)。收集所有患儿临床资料,采用酶联免疫吸附试验检测患儿血清EB病毒抗体谱[抗EB病毒衣壳抗体IgM(EBV-CAIgM)、抗EB病毒早期抗体IgG(EBV-EAIgG)、抗EB病毒衣壳抗体IgG(EBV-CAIgG)、抗EB病毒核抗体IgG(EBV-NA1IgG)]。比较2组患儿临床特征和各项指标差异。结果感染组和未感染组性别、年龄差异均无统计学意义(P>0.05)。急性T淋巴细胞白血病(T-ALL)患儿中EB病毒感染占70.59%(12/17),急性B淋巴细胞白血病(B-ALL)患儿中,EB病毒感染占90.41%(66/73),不同免疫分型患儿EB病毒感染所占比例差异无统计学意义(P>0.05)。B-ALL患儿和T-ALL患儿既往感染所占比例均较高(>45%)。结论ALL患儿EB病毒既往感染比例较高,临床应加强对ALL患儿EB病毒的筛查和监测。

儿童非高危急性早幼粒细胞白血病诱导期加一剂蒽环类治疗的疗效和安全性SCCLG/SCCCG-APL协作组

目的成人非高危急性早幼粒细胞白血病(NHR-APL)的去化疗诱导治疗,其疗效和安全性在儿童患者中尚未得到验证,需开展儿童的研究。方法数据来自华南儿童APL协作组的前瞻性研究资料,≤16岁、完成诱导治疗的NHR-APL患儿纳入分析。在砷剂+全反式维甲酸诱导治疗的基础上,比较加或不加1剂量去甲氧柔红霉素/米托蒽醌10mg/m^(2)(化疗或无化疗组)的缓解情况和不良事件率。结果化疗组139例,无化疗组27例,两组的诱导治疗结果比较:达血液学完全缓解的中位天数分别为26.0(22.0,31.5)d和31.0(27.5,35.0)d(P=0.002);分子学完全缓解分别有29.5%和3.7%(P=0.005);外周血白细胞计数>10×10^(9)/L分别有43.2%和74.1%(P=0.003);最高白细胞中位数分别为8.6(IQR 4.9,18.4)×10^(9)/L和22.7(IQR 16.0,41.7)×10^(9)/L(P<0.001);确诊分化综合征分别有5.8%和33.3%(P<0.001);出凝血事件发生率分别为14.4%和51.9%(P<0.001)。感染、颅内高压、心和肝功能异常等不良事件的发生率两组相似(均P>0.1)。结论儿童NHR-APL可能有别于成人患者,与无化疗比较,诱导治疗加1剂量蒽环类疗效更好,并发症的风险更低。

初诊儿童急性髓系白血病合并中枢神经系统白血病的临床治疗及预后分析

目的 分析华南儿童急性髓系白血病(C-HUNAN-AML-15)方案应用于中枢神经系统白血病(CNSL)的临床特征及治疗预后,为AML CNSL的治疗提供参考依据。方法 回顾性分析2015年1月—2020年12月收治的CNSL患儿的ELN风险分层以及AML相关融合/突变基因发生率、比较化疗组与移植组生存的差异。结果 研究纳入584例AML,其中CNSL 18例,发病比例为3%。ELN风险分层低危组占50%,中危组占39%,高危组占11%。AML最常见的合并基因变异是AML1/ETO 39%(7/18)、WT1突变22%(4/18)、c-KIT突变22%(4/18)、MLL/AF9 17%(3/18)。18例中采用单纯化疗11例,造血干细胞移植7例,中位随访时间为16.5(1~62)个月。5年总体OS和EFS分别为(74.2±11.2)%、(75.2±10.9)%。其中化疗组的预计5年OS和EFS分别为(90.9±8.7)%、(90.9±8.7)%,均高于移植组的5年OS和EFS分别为(50.5±20.4)%、(51.4±20.4)%,但两组间OS和EFS尚未见统计学差异(P=0.114)。化疗组中FLAG-IDA组预计5年OS和EFS分别为(83.1±11.0%)、(81.8±11.6)%,较DAE组的5年OS和EFS(53.3±24.8)%、(53.3±24.8)%升高,但两组间OS和EFS亦尚未见统计学差异(P=0.263)。结论 华南地区儿童急性髓系白血病协作组中枢神经系统白血病(CNSL)在低中危组病例数高于高危组,通过大剂量阿糖胞苷联合鞘注治疗对低危合并CNSL的患儿预后较好。

1例急性淋巴细胞白血病患儿合并右手背坏死性筋膜炎的护理

总结1例急性淋巴细胞白血病患儿合并右手背坏死性筋膜炎的护理经验。护理要点包括感染防治、创面管理、疼痛控制、营养支持、康复指导与人文关怀。通过上述综合护理措施,患儿治疗78天后伤口愈合,继续按疗程化疗。

儿童急性髓系白血病早期流式微小残留病检测与预后相关性的临床研究

目的:探索应用多参数流式细胞术(MFC)监测儿童急性髓系白血病(AML)诱导化疗后骨髓微小残留病(MRD)对预测预后的价值。方法:回顾性分析2015年8月-2022年12月武汉儿童医院血液科97例初诊AML患儿接受诱导化疗第Ⅰ周期和第Ⅱ周期后采用MFC检测骨髓MRD的结果,并分析其与预后的相关性。结果:97例AML患儿诱导治疗Ⅰ后57名患儿MRD阳性(MRD1^(+),58.8%),诱导治疗Ⅱ后仍有19名患儿MRD阳性(MRD2^(+),19.6%)。Kaplan-Meier生存分析结果显示37例(64.9%)MRD1^(+)接受移植治疗患儿预计3年总生存(OS)率明显高于20例(35.1%)未接受移植治疗患儿(84.6%vs 40.0%,P=0.0001)。35例MRD1^(+)MRD2^(-)患儿中,接受移植的25例患儿3年OS率高于10例未移植患儿(87.2%vs 70.0%,P=0.3229)。19例MRD1^(+)MRD2^(+)患儿3年OS率低于35例MRD1^(+)MRD2^(-)患儿(57.4%vs 81.8%,P=0.059)。12例MRD2^(+)移植治疗患儿3年OS率高于MRD2+7例未移植患儿(80.8%vs 14.3%,P=0.0007)。12例MRD1^(+)MRD2^(+)移植患儿和25例MRD1^(+)MRD2-移植患儿3年OS差异无统计学意义(80.8%vs 87.2%,P=0.8868)。7例MRD1^(+)MRD2^(+)未移植患儿3年OS明显低于10例MRD1^(+)MRD2^(-)未移植患儿(14.3%vs 70.7%,P=0.0114)。进一步多因素分析结果显示MRD2^(+)和移植治疗是患儿预后的独立影响因素(P=0.031,0.000),MRD1^(+)对预测97例患儿总体生存无统计学差异(P=0.902)。结论:诱导化疗Ⅱ后MRD阳性是AML患儿预后不良的独立危险因素。MRD2^(+)预示着更差的预后,可筛选出需接受移植的患儿。MRD2^(+)不是患儿移植治疗禁忌症尽早移植明显改善高危患儿的预后。

口服营养补充对急性淋巴细胞白血病儿童诱导化疗期血液系统并发症等的影响——随机对照研究的中期结果

目的探讨口服营养补充(ONS)对急性淋巴细胞白血病(ALL)儿童诱导化疗期间血液系统并发症及感染的影响。方法2022年1月—2022年12月年龄<16岁ALL儿童36例符合入组条件且完成诱导治疗,按1∶1比例随机分为干预组和对照组各18例。对照组给予低脂饮食(膳食脂肪供能≤每日总能量的20%),干预组给予低脂饮食及高中链甘油三酯、高蛋白、高热卡的短肽型ONS 20mL/(kg·d),食用时间为诱导化疗VDLD阶段。比较两组诱导化疗期间血液系统并发症、输血制品和感染的发生情况。结果干预组与对照组比较,中性粒细胞缺乏持续时间更短(12.50±9.38d和19.11±10.06d,P=0.049)、恢复时间更早(25.39±4.5d和30.06±3.80d,P=0.002);血小板最低值水平较高(P=0.048),Ⅳ度血小板减少的出现时间更晚(P=0.009)、持续时间更短(P=0.024)和恢复时间更早(P=0.012),输血小板的例数和次数均低于对照组(P<0.05);发热天数、抗菌药的使用、总体感染均倾向于较少,但差异未显出统计学意义(P>0.05)。结论ALL儿童在诱导化疗期间使用短肽型ONS有助于提高血液系统对化疗的耐受性。终期研究结果将会得出更确切的结论。