A Phase II Study of Antineoplastons A10 and AS2-1 in Children with Low-Grade Astrocytomas—Final Report (Protocol BT-13)

Nonresectable Low-Grade Astrocytomas (LGA) can compromise function and threaten life. For the majority of patients, the most appropriate strategy is initial chemotherapy followed by Radiation Therapy (RT). Since curative treatment is not available for most of these patients, it is reasonable to conduct clinical studies to evaluate new agents. This Phase II study evaluates efficacy and safety of Antineoplastons A10 and AS2-1 (ANP) in LGA. Sixteen children diagnosed with LGA were treated. They included 12 males and 4 females, ages 1.6 - 17.4 years (median 10.6). Efficacy was evaluated in 16 patients. The majority of patients were previously treated, but 1 patient had stereotactic biopsy only. Out of the remaining 15 patients, 6 patients received chemotherapy, and 7 patients had surgery, and 2 patients received RT and chemotherapy after surgery. The patients received treatment with ANP administered daily every 4 hours (median dose of A10 was 7.71 g/kg/d and AS2-1 was 0.26 g/kg/d) until objective response or stable disease was documented and for 8 months thereafter. The duration of ANP IV ranged from 1.4 to 286 weeks with a median of 83 weeks. A complete response was documented in 25.0%, partial response in 12.5%, and stable disease in 37.5%. Overall survival was 67.7% at 5 years, and 54.2% at 10 and 15 years. Progression-free survival was 48.1%, 34.4% and 34.4% at 5, 10, and 15 years respectively. The treatment was associated with grade 3 or grade 4 Adverse Drug Experiences (ADE) in 6 patients. There were two hypernatremias of grade 4 (12%). Grade 3 ADE included urinary frequency (6%), fatigue (6%) and hypernatremia (6%). There were no chronic toxicities, and there was a high quality of survival. ANP shows efficacy with a very good toxicity profile in this cohort of children with low-grade astrocytoma.

A Phase II Study of Antineoplastons A10 and AS2-1 in Adult Patients with Recurrent Glioblastoma Multiforme: Final Report (Protocol BT-21)

Treatment of recurrent glioblastoma multiforme (RGBM) creates one of the most difficult challenges to neuro-oncology. The purpose of this study is to evaluate the outcome of adults with high-grade glioma with special attention to RGBM patients treated with Antineoplastons (ANP) A10 and AS2-1 injections. The study was conducted according to Protocol BT-21, which accrued patients who failed standard radiation therapy (RT) and chemotherapy. There were 40 candidates registered in the study. Among the intent-to-treat (ITT) population, there were 30 cases of RGBM that progressed during and after prior treatment, 4 patients with anaplastic astrocytoma (AA), 1 with anaplastic mixed glioma (AMG), and 5 with persistent GBM. The aim of this paper is to evaluate the responses, survival and toxicity of all 40 patients, the efficacy in 30 patients with RGBM, and in 24 patients with RGBM who received at least 28 days of ANP (ERGBM). All RGBM patients were treated before with RT and chemotherapy, except one patient who only had surgery (patient refused radiation). In this group, 63% had one recurrence, 30% had two recurrences, and 7% had three recurrences. The median duration of ANP and ITT was 12 weeks and the median dosage of ANP A10 was 6.52 g/kg/d and ANP AS2-1 was 0.23 g/kg/d. Responses were assessed by gadolinium-enhanced magnetic resonance imaging (MRI) repeated every eight weeks. In the ITT population, objective responses (ORs) were determined in 10% of cases (complete response—CR, and partial response—PR in 5% each). Progression-free survival (PFS) in ITT at six months was 17.5%. Overall survival (OS) was 28.3% at one year, 2.6% at two years, five and ten years. In the RGBM population, objective responses (ORs) were determined in 13.3% of cases (CR and PR in 6.7% each). PFS in RGBM at six months was 16.7%. OS was 34.7% at one year, 3.47% at two years, five?and ten years. In the ERGBM population, ORs were determined in 16.7% of cases (CR and PR in?8.3% each). PFS in ERGBM at six months was 20.8%, OS was 39.3% at one year, 4.4% at two years, five and ten years. The treatment was well-tolerated with reversible Grades 3 and 4 toxicity in 17.5% of patients (7 patients who experienced multiple toxicities) and no chronic toxicity. In conclusion, the study reached efficacy endpoint. ANP is well-tolerated and compares favorably to the current treatment for RGBM.

A Phase II Study of Antineoplastons A10 and AS2-1 in Children with High-Grade Glioma. Final Report (Protocol BT-06), and Review of Recent Trials

Standard treatment for high-grade glioma involves surgical resection followed by radiation therapy and temozolomide. Unfortunately, there are no standard treatment recommendations after recurrence and new therapies are needed for patients whose tumor recurs after first-line treatment. This single-arm, two-stage, interventional Phase II study evaluated the efficacy and safety of a combination of antineoplastons A10 and AS2-1. Nineteen patients were enrolled in the study (safety population), but fifteen patients with a median age of 9.4 years who met eligibility criteria were evaluated. The majority of subjects (12/15) were Caucasian and 8/15 (53%) were female. More than half (53%) of patients were diagnosed with glioblastoma and 33% with anaplastic astrocytoma. All patients had failed standard therapy including surgery, radiation, and chemotherapy. Antineoplastons were administered intravenously every four hours (median dose of A10 6.9 g/kg/d and AS2-1 0.30 g/kg/d) until objective response was documented and thereafter for a further 8 months. Clinical evaluations were performed every 8 weeks. All patients enrolled in the study were included in the safety analysis but only patients fulfilling the inclusion criteria were included in the efficacy evaluation. The duration of treatment with antineoplastons ranged from 2 weeks to 120 weeks. A complete response was documented in 2/15 (13%), partial response in 2/15 (13%), stable disease in 3/15 (20%). Progression-free survival at six months was 47% and overall survival (OS) at one year was 33.3%. One patient (6.7%) survived 10 years from treatment start. A small group of patients suffered reversible Grade 3 and 4 toxicities including hypernatremia 2/19 (11%) and decrease of neutrophils 1/19 (5%). There were no chronic toxicities. There was improvement of quality of life in patients who had objective response. It is concluded that antineoplastons show efficacy with an acceptable profile in this cohort of patients with recurrent high-grade glioma.

A Phase II Study of Antineoplastons A10 and AS2-1 in Children with Recurrent, Refractory or Progressive Primary Brain Tumors—Final Report (Protocol BT-22)

Primary malignant brain tumors are a leading cause of cancer-related death in children. This Phase II study evaluated the efficacy and safety of Antineoplastons A10 and AS2-1 (ANP) in children who developed progression during standard treatment. A total of 43 children were recruited to the study, but only 41 met eligibility criteria. There were twelve cases of glioblastoma multiforme (GBM), eight anaplastic astrocytomas (AA), twelve diffuse intrinsic pontine gliomas (DIPG), three supertentorial primitive neuroectodermal tumors (sPNET), three cases of medulloblastoma and one case each of anaplastic ependymoma (AE), atypical teratoid rhabdoid tumor (AT/RT), and disseminated pilocytic astrocytoma (PAD). ANP was administered intravenously daily every four hours (median dose of A10 8.74 g/kg/d and AS2-1 0.35 g/kg/d), until objective response (OR) was documented, and then a further eight months. All enrolled patients were included in safety, but only eligible patients in the efficacy evaluation. A total of 12.2% of patients obtained OR;2.4% complete response (CR) and 9.8% partial response (PR). Stable disease (SD) was determined in 17.1% and progressive disease (PD) in 43.9% of cases. There were 26.8% of nonevaluable (NE) cases due to premature discontinuation. Out of five OR cases, four patients were diagnosed with recurrent DIPG and one with recurrent AA. Median progression-free survival (PFS) was 2.5 months. Median overall survival was 4.8 months. OS at 6 months was 46.3%, one year was 12.2%, and 4.8% at two, five, and ten years. The longest survivor is a patient diagnosed with DIPG and gliosarcoma who remains alive more than 15 years. A group of eleven patients reported grade 3 and 4 toxicity including hypernatremia in eight cases, somnolence in two cases, and hypokalemia in one case. There were no chronic toxicities, and the quality of life was very good. The largest group of patients were represented by DIPG, GBM, and AA. The best results were obtained in the DIPG and AA groups. In the DIPG group, CR was in 8.3%, PR was 25%, median PFS was 4.8 months, median OS was 6.1 months, and OS at 6 months was 58.3%, at one year 25%, and 8.3% at two, five, and ten years. In the AA group, PR was 12.5%, median PFS was 3.7 months, median OS was 4.7 months, and OS at 6 months was 37.5%, and 12.5%, at one, two, five, and ten years. In conclusion, antineoplastons showed efficacy and acceptable toxicity in patients with recurrent, refractory or progressive primary brain tumors.

A Phase II Study of Antineoplastons A10 and AS2-1 in Patients with Brainstem Gliomas. The Report on Non-Diffuse Intrinsic Pontine Glioma (Protocol BT-11)

Inoperable brainstem gliomas (BSG) are among the most difficult to treat malignancies. In the intent-to-treat (ITT) population of the BT-11 study for BSG, forty patients (median age 11.2 years old) were enrolled. Antineoplastons A10 and AS2-1 (ANP) were administered intravenously daily. The median daily dose of A10 was 8.70 g/kg/day and AS2-1 was 0.32 g/kg/day. Efficacy analyses were conducted in two subgroups: recurrent pediatric diffuse intrinsic pontine glioma (RPDIPG, N?= 17) and non-diffuse intrinsic pontine glioma (NDIPG, N?= 11). This paper reports the results of the study of the efficacy and safety of ANP in patients with NDIPG. The results in the RPDIPG group were reported before;complete response (CR) was 6%, partial response (PR) 23.5%, and stable disease (SD) 17.6%. One year overall survival (OS) was 29.4%, 2 years 11.8%, and 5, 10, and 15 years 6%. In the NDIPG group, there were 36% CR and 27.5% SD. OS at 1, 5, 10, and 15 years was 82%, 73%, 62%, and 50% correspondingly. There was only one serious adverse event (9%) reported in NDIPG represented by hypokalemia, Grade 4. The results suggest that ANP shows efficacy and an acceptable tolerability profile in patients with RPDIPG and NDIPG.

A Phase II Study of Antineoplastons A10 and AS2-1 in Children with Brain Tumors. Final Report (Protocol BT-10)

Despite dramatic progress over the last 50 years in the treatment of many childhood cancers, primary brain tumors remain the leading cause of death in pediatric oncology. This phase II study evaluated the efficacy and safety of Antineoplastons A10 and AS2-1 given in combination (ANP). Thirty-four patients, with a median age of 10.4 years, were enrolled in the study. Thirty-two patients (94.1%), were Caucasians while 21 (61.8%) were female and 13 were male (38.2%). Twenty-four patients (70.6%) suffered from a brainstem glioma (BSG) or high-grade tumor. Ten patients (29.4%) suffered from a low-grade tumor. A distinct sub-group of three patients with low grade tumors had a ganglioglioma (GG). Eighty-two percent of patients had failed standard treatment. Daily ANP was administered by IV infusion, every four hours, until an objective response (OR) was documented, and then for an additional eight months. The median doses of A10 and AS2-1 were 11.64 g/kg/d and 0.45 g/kg/d, respectively. A complete response (CR) was documented in two patients (5.9%), a partial response (PR) in four patients (11.8%), and stable disease (SD) in six patients (17.6%). Objective responses were observed in diffuse intrinsic pontine glioma (DIPG), thalamic pilocytic astrocytoma with brainstem involvement, ganglioglioma and pilocytic astrocytoma. Six-month progression-free survival (PFS) was 35.3%. Overall survival (OS) at two and five years was 37.6% and 34.5%, respectively. Two patients experienced grade 4 hypernatremia while three experienced grade 3 hypokalemia. In this group of patients, ANP showed good efficacy and an acceptable toxicity profile.

A Phase II Study of Antineoplastons A10 and AS2-1 in Adult Patients with Primary Brain Tumors—Final Report (Protocol BT-09)

Antineoplastons A10 and AS2-1 (ANP) are synthetic derivatives of glutamine, isoglutamine, and phenylacetic acid. In 1993, a phase II clinical trial program began according to protocols based on the initial protocol, BT-06, which was transferred from the National Institutes of Health (NIH). Protocol BT-09 was designed for different types of primary brain tumors in adults that were not curable by standard treatment. The study was designed as a single arm, two-stage, phase II trial of ANP as a monotherapy in a high-risk, poor-prognosis population. The total number of registered subjects was 40. The majority of patients were diagnosed with high-grade tumors (N = 33). In this group, 12 patients carried diagnosis of anaplastic astrocytoma (AA) and 11 patients of glioblastoma. In the group of low-grade tumors (N = 7), there were 6 cases of low-grade glioma, and 1 neurocytoma grade 2. A group of 12 patients did not receive any prior treatment, 12 patients had surgical resection only, 5 patients received radiation therapy (RT) only, and 11 patients received both RT and chemotherapy. The median duration of ANP was 16.6 weeks. The median dosage of A10 was 7.16 g/kg/d and AS2-1 was 0.27 g/kg/d. Responses were accessed by gadolinium-enhanced magnetic resonance imaging (MRI). Objective responses (OR) in all patients were 22.5% and in the AA group were 41.7% of patients. The median progression-free survival (PFS) in the AA group was 5.4 months. The median overall survival (OS) was 12.7 months and OS at 1 and 2 years was 54.5% and 45.5% correspondingly. The treatment was well-tolerated with reversible grade 3 and 4 toxicities in 35% of all patients (N = 40). In conclusion, the study reached efficacy endpoint and ANP was well-tolerated and compared favorably to the current treatment of AA.

PCI术后AMI患者血清CXCL10、sST2、sTLT-1水平变化

目的 探讨急性心肌梗死(acute myocardial infarction,AMI)患者经皮冠状动脉介入治疗(percutaneous coronary intervention,PCI)前后血清CXC趋化因子配体10(CXCL10)、可溶性生长刺激表达基因2蛋白(sST2)、可溶性髓样细胞触发受体样转录因子-1(sTLT-1)水平变化,并分析其对预后的预测价值。方法 选取110例AMI患者为研究对象,依据PCI术后1年预后情况分为预后不良组(n=29)、预后良好组(n=81)。比较2组患者临床资料及血清CXCL10、sST2、sTLT-1水平。多因素logistic回归分析预后不良影响因素。分别构建含与不含血清CXCL10、sST2、sTLT-1的预测模型,采用受试者操作特征(ROC)曲线分析不同预测模型对预后的预测价值。结果 预后不良组术后1个月、术后3个月血清CXCL10、sST2、sTLT-1水平高于预后良好组,差异有统计学意义(P<0.05);多支病变、Killip心功能分级增加、支架置入数增多、血清cTnI、D-D水平及术后3个月血清CXCL10、sST2、sTLT-1水平升高为预后不良的独立危险因素(P<0.05);术后3个月血清CXCL10、sST2、sTLT-1水平联合预测预后不良的曲线下面积(AUC)大于单独指标预测,且含血清CXCL10、sST2、sTLT-1预测方案预测预后不良的AUC大于不含血清CXCL10、sST2、sTLT-1预测方案(P<0.05)。结论 AMI患者PCI治疗后血清CXCL10、sST2、sTLT-1水平变化与预后密切相关,联合检测其水平对预后具有一定预测价值。

带状疱疹患者外周血IL-2与IL-10水平及临床意义

目的 研究带状疱疹 (HZ)患者Th1/Th2型细胞因子水平及临床意义。方法 采用双抗体夹心ELISA法测定HZ患者急性期及恢复期血清白细胞介素 2 (IL 2 )和白细胞介素 10 (IL 10 )水平。结果 HZ患者急性期血清IL 2水平较正常对照组明显下降 ,IL 10水平明显升高 (P <0 .0 1) ;恢复期血清IL 2水平较急性期明显升高 ,而血清IL 10则明显下降 (P <0 .0 1) ;且HZ患者急性期和恢复期IL 2与IL 10呈负相关性 (P <0 .0 1)。结论 HZ患者外周血Th1/Th2型细胞因子失调 ,在HZ的发生发展中可能起作用。

IL-10抑制人肾系膜细胞环氧化酶-2及其介导的前列腺素E_2的释放

目的观察白细胞介素 - 10 (IL - 10 )对 IL - 1β诱导的人系膜细胞 (HMC)前列腺素 E2 (PGE2 )释放及环氧化酶 - 2(COX- 2 )基因和蛋白表达的影响。方法应用放射免疫测定法检测 HMC培养上清中 PGE2 ,应用 RT- PCR和 western blot检测 COX- 2 m RNA和蛋白水平。结果 1IL - 1β显著上调 PGE2 释放及 COX- 2基因和蛋白的表达 (P均 <0 .0 1) ;2 IL - 10对基础状态下 PGE2 释放及 COX- 2基因和蛋白表达无明显影响 (P>0 .0 5 ) ;3 IL - 10可呈剂量依赖性地下调 IL - 1β诱导的 PGE2 释放及 COX- 2 m RNA和蛋白表达 (P<0 .0 1)。结论 IL - 10抑制 IL - 1β诱导的 HMC PGE2 释放及 COX- 2表达 ,提示 :IL -

2，3-二氯-5，6-二氰基-1，4-苯醌／NaNO2催化9，10-二氢蒽氧化脱氢

设计了一种由2,3-二氯-5,6-二氰基-1,4-苯醌(DDQ)和NaNO2组成的复合催化剂,该催化剂在9,10-二氢蒽氧化脱氢生成蒽的反应中表现出很高的催化活性和选择性.在120℃和1.3MPaO2下反应8h,9,10-二氢蒽转化率达到99%以上,蒽的选择性为99%.采用红外光谱和核磁共振方法对催化氧化脱氢的反应历程进行了研究.结果表明,9,10-二氢蒽氧气氧化脱氢生成蒽的反应是通过DDQ/DDQH2和NO2/NO两个氧化还原对的电子传递来推动的,以DDQ/NaNO2为催化剂可以有效催化9,10-二氢蒽氧化脱氢生成蒽.

RMPP患儿血清IL-2、IL-6、IL-10和TGF-β_1检测及分析

目的探讨IL-2、IL-6、IL-10和转化生长因子(TGF)-β1在儿童难治性肺炎支原体肺炎(RMPP)发病中的作用,为临床提供依据。方法选择25例RMPP患儿(RMPP组),分别于急性期和恢复期采用ELISA法测定血清IL-2、IL-6、IL-10和TGF-β1,并与25例肺炎支原体肺炎(MPP)患儿(MPP组)和15例健康儿童(对照组)对照。结果 RMPP组急性期及恢复期血清IL-2、IL-10水平均显著低于MPP组和对照组,IL-6、TGF-β1水平均显著高于MPP组和对照组(P均<0.05);RMPP组和MPP组组内上述各项指标在急性期及恢复期均有显著差异(P均<0.05),恢复期MPP组IL-2、IL-6与对照组无显著差异。结论 IL-2、IL-6、IL-10和TGF-β1可能参与了RMPP的发病机制,检测其血清水平可为临床判断MPP病情及预后提供依据。

弥散性毒性甲状腺肿患儿血清白细胞介素-10、12水平变化的意义

目的观察弥散性毒性甲状腺肿(GD)儿童在疾病不同阶段血清IL-10、12水平变化的临床意义。方法采用酶联免疫吸附法(ELISA)测定GD患儿疾病不同阶段(新发病、治疗未缓解、治疗缓解3个阶段)血清IL-10、12水平。检测游离T3、T4(FT3、FT4),敏感TSH(sTSH),甲状腺微粒体抗体(TMAb)、甲状腺球蛋白抗体(TGAb)、甲状腺受体抗体(TRAb)、甲状腺刺激抗体(TSI)水平并分析其间的关系。结果IL-10、12在GD新发病组均显著高于未缓解组、缓解组和健康对照组(Pa<0.05)。IL-12与sTSH呈显著负相关(r=-0.309 P<0.05),IL-10与FT4、FT3呈显著正相关(r=0.350,0.334 Pa<0.05)。结论IL-10、12均参与GD的发病,可作为病情监测的指标。

成纤维细胞在博来霉素致肺纤维化中高表达IL-2、β-catenin、TGF-β_1和IL-10

目的检测肺纤维化形成过程中肺组织和肺成纤维细胞是否表达IL-2、β-连环蛋白(β-catenin)、TGF-β1和IL-10并探讨其意义。方法 SD大鼠48只,随机分为博来霉素(实验组)24只和生理盐水组24只(对照组),博来霉素组气管内给药复制大鼠肺纤维化动物模型(博来霉素3 mg/kg),生理盐水组气管内注射等量生理盐水。在第7天及第28天分别处死动物,取肺组织并分离培养原代肺成纤维细胞。用免疫组织化学和免疫细胞化学方法检测肺组织和肺成纤维细胞中的IL-2、β-catenin、TGF-β1和IL-10的表达。结果与对照组大鼠肺组织和原代成纤维细胞相比,在第7天及28天,实验组的IL-2、β-catenin、TGF-β1和IL-10的表达水平都有显著的升高,随着时间的延长和肺纤维化的加重而更为明显,差异具有统计学意义。结论肺组织中的成纤维细胞,具有分泌IL-2,β-catenin,TGF-β1和IL-10等多种细胞因子的能力,通过分泌这些细胞因子,影响肺纤维化病理进程。

白细胞介素-10抑制人肾系膜细胞环氧化酶-2及磷脂酶A_2基因及蛋白表达的实验研究

目的 :观察白细胞介素 10 (IL 10 )对IL 1β诱导的人系膜细胞 (HMC)前列腺素E2 (PGE2 )释放和胞浆型磷脂酶A2 (cPLA2 )及环氧化酶 2 (COX 2 )基因和蛋白表达的影响。 方法 :利用体外培养的人系膜细胞 (HMC) ,设立对照组、IL 10 (2 5ng/L)处理组、IL 1β(10ng/L)处理组及IL 10 +IL 1β处理组 ;采用放射免疫测定法检测各组HMC培养上清中PGE2 ,应用RT PCR和WesternBlot检测各组cPLA2 、COX 2mRNA和蛋白水平。 结果 :正常情况下 ,HMC低水平表达cPLA2 、COX 2mRNA和蛋白并释放少量的PGE2 ;IL 1β能显著上调HMCPGE2 释放及cPLA2 、COX 2mRNA和蛋白的表达 (P均 <0 0 1) ;IL 10对基础状态下的HMCPGE2 释放及cPLA2 、COX 2mRNA和蛋白表达无明显影响 (P均 >0 0 5 ) ,但可显著下调IL 1β诱导的PGE2 释放及cPLA2 、COX 2mRNA和蛋白表达 (P均 <0 0 1)。 结论 :IL 10抑制IL 1β诱导的HMCPGE2 释放及cPLA2 和COX 2表达 ,提示IL

小鼠VCAM-1表达载体的构建及稳定高表达间充质干细胞系C3H10T 1/2的建立

本研究旨在构建小鼠血管细胞粘附分子-1(vascular cell adhesion molecule-1,VCAM-1)的逆转录病毒载体,通过转染建立稳定高表达VCAM-1的间充质干细胞(mesenchymal stem cells,MSC),并初步探讨VCAM-1基因过表达对MSC免疫学特性的影响。以小鼠脾脏组织总RNA为模板,通过RT-PCR扩增小鼠VCAM-1基因cDNA,应用基因工程技术将扩增的cDNA片段插入PMSCVmigr-1逆转录病毒载体,构建重组逆转录病毒表达质粒PMSCVmigr-1-mVCAM-1,经限制性内切酶酶切分析及测序鉴定后,用脂质体转染技术转染293细胞,收获含有病毒颗粒的上清;用病毒上清感染间充质干细胞系(C3H10T 1/2)并检测其表达。采用3H-TdR掺入法测定高表达VCAM-1的MSC在淋巴母细胞转化实验中对淋巴细胞增殖的抑制作用。结果表明:酶切和测序鉴定证实,正确构建了小鼠VCAM-1的重组逆转录病毒表达质粒。逆转录病毒上清感染MSC后流式细胞术检测到目的基因VCAM-1在MSC表面高表达。高表达VCAM-1的MSC对刀豆素A诱导的淋巴细胞增殖具有显著抑制作用,且呈剂量效应关系。结论:成功构建了小鼠VCAM-1基因的重组逆转录病毒质粒并使其在MSC中稳定高表达。高表达VCAM-1的MSC对体外淋巴细胞增殖具有很强的抑制效果。本课题为进一步研究VCAM-1基因调控MSC干预免疫相关性疾病奠定了实验基础。

前列腺素E_2对急性坏死性胰腺炎大鼠IL-10、TNF-α及IL-1β的调控和对肺组织损伤的影响

目的 :探讨前列腺素E2 (PGE2 )对大鼠急性坏死性胰腺炎 (ANP)中血清白介素 10 (IL 10 )、肿瘤坏死因子 (TNF α)以及白介素 1β(IL 1β)的含量及肺组织损伤的影响。 方法 :将SD大鼠 91只随机分 4组 :假手术对照组 (n =7) ,ANP组 (n =2 8) ,PGE2 前处理组 (n =2 8) ,PGE2 后处理组 (n =2 8) ;观察同组不同时间 ,不同组同时间的IL 1β、TNF α和IL 10的动态变化 ,并观察各组肺组织的病理切片。 结果 :各指标在 1h、3h、6h和 12hPGE2 前处理组和PGE2 后处理组与ANP组相比较差异有显著性 (P <0 .0 1) ,在PGE2 前处理组 ,TNF α、IL 1β下降更加明显 ,IL 10升高两组都很明显 ,而且有PGE2 保护的两组 ,其肺组织损伤出现较迟、较轻。结论 :IL 1β和TNF α在大鼠ANP的全身性反应过程中起重要的递质作用 ,IL 10能抵抗它们的作用。PGE2 能降低ANP大鼠血清中IL 1β、TNF α含量 ,提高IL 10含量 。

鼻咽癌患者HIF-1α、VEGF-C、COX-2和IL-10表达研究

目的探讨鼻咽癌患者缺氧诱导因子-1α(HIF-1α)、血管内皮生长因子-C(VEGF-C)、环氧合酶-2(COX-2)和白细胞介素-10(IL-10)的表达、相互关系及临床意义。方法选取鼻咽癌病变组织72例,鼻咽炎对照组25例,健康对照组25例。采用免疫组化法检测组织中HIF-1α、VEGF-C和COX-2;用酶联免疫吸附试验(ELISA)检测血清中IL-10的表达。结果鼻咽癌组织内存在HIF-1α、VEGF-C、COX-2和IL-10的表达,差异有统计学意义(P<0.05);与预后呈负相关;而与年龄、性别、肿块类型无关。HIF-1α、VEGF-C、COX-2和IL-10与临床分期有关,随着临床分期的增高表达增强(P<0.05)。HIF-1α、VEGF-C和COX-2的表达与淋巴结转移有关,有淋巴结转移组阳性率明显高于无淋巴结转移组(P<0.05)。肿瘤中央区HIF-1α、VEGF的表达水平较周边区高,肿瘤表达水平与微血管密度(MVD)密切相关(P<0.05)。IL-10与淋巴转移无关。HIF-1α与VEGF、COX-2与VEGF呈正相关,其余无直接相关性。结论 HIF-1α、VEGF-C、COX-2和IL-10的异常表达参与了鼻咽癌的发生发展,联合检测上述指标可能为鼻咽癌的早期诊断、治疗、预后的判断提供有力的临床指导。

纯铁及40Cr钢在熔融LiCl-10%Li_2O中的腐蚀行为

采用浸没法腐蚀实验研究了纯铁及40Cr在750℃下,熔融LiCl10Li2O(%,质量分数)中的腐蚀行为。实验结果表明,纯铁和40Cr在750℃熔融LiCl10%Li2O中的腐蚀产物均为LiFeO2,腐蚀减重均随时间的延长而增大,并且40Cr的腐蚀减重略低于纯铁。在本实验条件下,奥氏体的耐蚀性能优于铁素体。

TLR2、IL-10 mRNA的表达及树突状细胞分布在外阴硬化性苔藓中的临床意义

目的:探讨与免疫相关的TLR2、IL-10 mRNA及树突状细胞与外阴硬化性苔藓(VLS)发生和发展的关系。方法:选取VLS石蜡标本50例(早期和进展期各25例),外阴正常皮肤15例。采用免疫组化S-P法检测CD1α在组织中的分布,RT-PCR法检测TLR2和IL-10 mRNA在组织中的表达。结果:CD1α阳性细胞在VLS进展期中明显高于正常外阴皮肤(P<0.05)。TLR2、IL-10的mRNA表达在VLS进展期中明显高于正常外阴皮肤(P<0.05);TLR2、IL-10 mRNA和CD1α表达在早期VLS中略增加,与正常外阴皮肤相比无统计学差异(P>0.05)。结论:VLS的进展期TLR2、IL-10 mRNA及树突状细胞增多,预示局部组织内免疫抑制作用增强。