Angiotensin-converting enzyme 2 alleviates liver fibrosis through the renin-angiotensin system

The present letter to the editor is related to the study titled‘Angiotensin-converting enzyme 2 improves liver fibrosis in mice by regulating autophagy of hepatic stellate cells’.Angiotensin-converting enzyme 2 can alleviate liver fibrosis by regulating autophagy of hepatic stellate cells and affecting the renin-angiotensin system.

血清胰岛素样生长因子-2、甲胎蛋白、γ-谷氨酰转肽酶同工酶II及异常凝血酶原联合检测在肝癌诊断中的价值

目的探讨血清胰岛素样生长因子-2(IGF-2)及甲胎蛋白(AFP)、γ-谷氨酰转肽酶同工酶II(GGT-II)和异常凝血酶原(APT)联合检测在肝癌诊断中的临床价值,筛选理想的血清肿瘤标志物组合。方法应用放射免疫法检测114例肝癌患者、47例健康体检者和28例肝部良性疾病患者血清IGF-2,同时应用电化学发光免疫分析法测定同一批研究对象的血清AFP、GGT-II、APT的水平,用ROC曲线对各项指标的诊断效能进行分析和评价。结果肝癌患者的血清IGF-2水平及三种血清肿瘤标志物水平均明显高于健康体检组和肝良性疾病组,差异有统计学意义(均P<0.05)。IGF-2和AFP、GGT-II、APT在特异性为95.6%(43/45)时,灵敏度分别为76.0%(57/75)、53.3%(40/75)、66.7%(50/75)和42.7%(32/75),以IGF-2最高,在受试者工作特征曲线(ROC曲线)下面积(AUC)分别为0.88、0.836、0.891和0.697,以IGF-2与GGT-II较高;联合检测显著提高诊断灵敏度和诊断效能,联合检测以(IGF-2)+(GGT-II)与(IGF-2)+(AFP)+(GGT-II)较好,灵敏度分别达到了94.7%(71/75)和97.3%(73/75),AUC分别为0.969和0.984。结论血清中IGF-2、AFP、GGT-II和APT对于肝癌的诊断均有一定的临床价值,IGF-2与AFP、GGT-II、APT联合检测可显著提高肝癌诊断的灵敏度和效能。

Co(II)和Ni(II)2-乙酰吡啶乙醇胺配合物合成与结构

目的以Co(II),Ni(II)的氯化物和2-乙酰吡啶、乙醇胺为原料合成新型Schiff碱配合物,并对其结构进行测定。方法采用"一锅煮"法合成得到了两个新的配合物[C23H22N4OCoCl2].(CH3CH2OH)(1)和[C23H22N4ONiCl2].(CH3CH2OH)(2)。结果根据结构分析推测,2-乙酰吡啶、乙醇胺在金属离子模板作用下,发生复杂的反应,形成了新的Schiff碱配体。结论配合物的结构测定表明,新的N4配体与中心金属离子形成1:1的配合物,其中有3个N原子与金属配位,另有2个抗衡阴离子Cl-参与配位,配位单元呈畸变的三角双锥构型[MN3Cl2]。

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 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 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.

Synthesis and Crystal Structure of Tri(4-(3-hydroxy2-ethyl-4-pyridinone-1-yl)-aniline Condensation Salicylaldehydato) Monohydratotricopper(II)Dimethylformamide Monohydrate Solvate

The title complex [Cu3L3(H2O)]DMFH2O (H2L = 4-(3-hydroxy-2-ethyl-4- pyridinone-1-yl)-aniline condensation salicylaldehyde) was obtained. The single-crystal X-ray study shows that it is a trinuclear compound [Cu3(C20H15N2O3)3(H2O)]DMFH2O. The coordi- nation sphere about each copper ion in the complex consists of two oxygen atoms from hydroxylpyridinone moiety of one ligand and one oxygen and one nitrogen atoms from salicyladehyde Schiff-base moiety of another ligand arranged in a slightly distorted square planar geometry. Among the three copper ions, one (Cu(2)) is coordinated by the other oxygen atom of water molecule on the fifth coordinate position to form a distorted square pyramid geometry. The crystal is of monoclinic, space group P21/c with a = 12.9202(5), b = 27.197(1), c = 17.0116(7) ? b = 100.588(1), V = 5875.9(4) 3, Z = 4, C63H57N7O12Cu3, Mr = 1294.78, Dc = 1.464 g/cm3, m = 1.146 mm-1, F(000) = 2668, R = 0.0784 and wR = 0.1546 for 6926 observed reflections with I > 2s(I). The differences of coordinate bond lengths are observed between anhydrous and hydrous units: in the former unit, the average bond lengths are 1.978 ?for CuN (azomethine), 1.883 ?for CuO (phenolic) in Schiff-base moiety, 1.959 ?for CuO (keto), and 1.919 ?for CuO (hydroxy) in hydroxypyridinone moiety; while those in the latter are longer with the following corresponding values: 1.985(5), 1.908(5), 1.993(5) and 1.919(4) ? respectively. The Cu(2)O (water) bond length is 2.375(6) ?

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.

Synthesis and Crystal Structure of Dichlorobis-(1-methylimidazoline-2(3H)-thione-S) Cobalt(II)

The reaction of anhydrous cobalt(II) dichloride with 1-methylimidazoline-2(3H)- thione in dichloromethane solution gave the title complex, [Co(C4H6N2S)2Cl2]. X-ray single-crystal analysis revealed that the complex crystallizes in a monoclinic system, space group P21/c, a = 13.9707(10), b = 10.0435(7), c = 10.3910(6) ?, β = 91.181(3)o, V = 1457.70(17) ?3, Z = 4, C8H12Cl2N4S2Co, Mr = 358.17, Dc = 1.632 g/cm3, μ = 1.813 mm–1, F(000) = 724, the final R = 0.0710 and wR = 0.1224 for 1549 observed reflections with I > 2σ(I). The Co atom is coordinated by two S atoms from two 1-methylimidazoline-2(3H)-thione ligands and two chloride ions in a slightly distorted tetrahedral geometry. The intramolecular classical hydrogen-bonding interactions involving chloride ions and N–H groups of the heterocyclic thione ligands are observed. The offset π-π stacking interactions between the imidazole rings of adjacent molecules with a face-to-face dis- tance of 3.604 ? are found in the packing diagram.

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.

吡啶-2,6-二羧酸镉(II)配合物的合成及晶体结构研究

以吡啶-2,6-二羧酸为配体,CdCl2·2.5H2O为金属源,采用溶剂热法单晶培养技术,合成了一种新型羧酸镉配合物 (C14H12Cd2N2O11)n,并利用X射线单晶衍射仪测定了配合物的结构。(C14H12Cd2N2O11)n属于orthorhombic晶系,P b c n空间群,晶胞参数为a= 12.223(6)?,b=17.233(9)?,c= 13.439(7)?,α=90.00°,β=90.00°,γ=90.00°,Volume = 2831(3)?3,Z = 4。CCDC number:1563525。

VPA联合HA14-1对Bcl-2高表达的BALL-1细胞作用的实验研究

目的:观察体内外丙戊酸(VPA)和HA14-1联合应用对Bc l-2高表达的白血病细胞的杀伤效能。方法:(1)将BALL-1分为对照组、VPA组、HA14-1组、VPA+HA14-1组,作用后流式细胞法检测各组凋亡率、Bc l-2的平均荧光指数(MFI)以及胱冬肽酶(caspase)3、8和9的含量;(2)NOD/SC ID鼠在接种BALL-1后24 h按(1)分组进行实验。记录各组小鼠的存活时间;流式细胞仪检测各组小鼠外周血、骨髓、肝、肺、脾组织中CD19的表达。结果:(1)HA14-1+VPA组凋亡率高达(76.5±6.9)%,与另3组比较P<0.01。HA14-1组和联合作用组中Bc l-2低于其它两组,caspase 9和3的含量则较高,差异显著;联合作用组上述3种指标与其它组的差异更显著(P<0.01)。Caspase 8在各组间无显著差异。(2)HA14-1+VPA组小鼠生存(87.5±4.5)d,显著长于其它3组,而其它3组之间无明显差异。HA14-1+VPA组CD19在外周血、骨髓、肝、脾中的表达显著低于另3组。结论:HA14-1与VPA联合用药,可克服Bc l-2高表达造成的对VPA的抗性。

1,25-(OH)_2D_3对肺纤维化大鼠肺泡Ⅱ型上皮细胞中Ca^(2+)浓度和PI3K/AKT/mTOR通路的影响

目的特发性肺纤维化(idiopathic pulmonary fibrosis,IPF)是一种慢性炎症性疾病,病因不明,缺乏有效的治疗方法。文中旨在探讨肺泡Ⅱ型上皮细胞中Ca^(2+)和PI3K/AKT/mTOR通路在大鼠IPF中的作用,以及1,25-(OH)_2D_3对Ca^(2+)浓度和PI3K/AKT/mTOR通路的影响。方法 150只雄性SD大鼠随机分为:预防组(对照组Ⅰ、模型组Ⅰ、给药组Ⅰ,每组20只)和治疗组(对照组Ⅱ、模型组Ⅱ、给药组Ⅱ,每组30只)。对照组Ⅰ/Ⅱ行气管暴露手术,气管内给以200μL/只的无菌等渗盐水,并分别于第2和14天开始腹腔注射等渗盐水(200μL/只);模型组Ⅰ/Ⅱ气管内灌注博来霉素(5 mg/kg),并分别于手术后第2和14天开始腹腔注射维生素D3的溶剂(0.1%乙醇和99.9%的丙二醇,1μL/g体重);给药组Ⅰ/Ⅱ气管内灌注博来霉素(5 mg/kg),并分别于手术后第2和14天开始腹腔注射1,25-(OH)_2D_3(2μg/kg体重)。大鼠气管内注射博来霉素建立IPF模型,给药组腹腔注射1,25-(OH)_2D_3进行预防和治疗。检测各组大鼠肺组织中羟脯氨酸的含量,分离肺泡Ⅱ型上皮细胞并用Fluo-3AM荧光负载,激光共聚焦显微镜检测细胞内Ca^(2+)浓度。RT-PCR方法检测PI3K、AKT、mTOR mRNA的表达水平。结果模型组Ⅰ/Ⅱ和给药组Ⅰ/Ⅱ中大鼠肺组织中羟脯氨酸的含量、肺泡Ⅱ型上皮细胞内Ca^(2+)浓度以及PI3K、AKT、mTOR mRNA表达,在各时间点与相应对照组Ⅰ/Ⅱ相比均明显升高(P<0.05或P<0.01);给药组Ⅰ/Ⅱ与模型组Ⅰ/Ⅱ相比,上述指标均有显著降低(P<0.05或P<0.01)。模型组Ⅰ/Ⅱ和给药组Ⅰ/Ⅱ中Ca^(2+)浓度与PI3K、AKT、mTOR mRNA表达之间具有显著正相关(r=0.598 8、r=0.623 0、r=0.6603,P<0.01;r=0.7012、r=0.6323、r=0.7403,P<0.01)。结论 PI3K-AKT-mTOR通路在大鼠IPF的发生发展中起重要作用,1,25-(OH)_2D_3可以降低肺泡Ⅱ型上皮细胞内Ca^(2+)的浓度,抑制PI3K-AKT-mTOR通路,进而抑制IPF的发生发展。

偶联法合成2,4-二氟联苯

目的合成2,4-二氟联苯。方法用P,O双齿螯合钯配合物催化偶联反应合成目标化合物。结果所合成的目标化合物的熔点、红外光谱、核磁谱与有关文献报道一致。结论所用工艺具有原料易得、收率高的特点,反应条件温和,适用于2,4-二氟联苯原料的生产。

2-吡啶甲醛缩对氨基苯甲酸席夫碱Co(Ⅱ)、Cd(Ⅱ)配合物的合成及晶体结构

为了探究席夫碱及其配合物的空间结构,利用常温静置法合成了2-吡啶甲醛缩对氨基苯甲酸席夫碱的配合物1([Co L2(H2O)2]·5H2O)和配合物2({[Cd(L)(HL)(H2O)]·Cl O4·H2O}n(HL=2-吡啶甲醛缩对氨基苯甲酸;L=2-吡啶甲醛缩对氨基苯甲酸根)),并用X射线单晶衍射方法测得了二者的晶体结构.结果显示:配合物1为单斜晶系,空间群为P21/c;配合物2为正交晶系,空间群是Pbca.结构分析表明:配合物1中的Co2+离子采用六配位模式,分别与2个配体分子中的4个N原子和2个水分子中的2个O原子配位形成单核分子;配合物2为一维链状结构,每个Cd2+离子采用七配位模式,分别与HL中的2个N原子,L中的2个N原子、2个O原子以及水中的O原子进行配位.

8-羟基喹啉-2-醛-芳香酰腙Cu(Ⅱ)配合物的合成及其与DNA相互作用

合成并表征8-羟基喹啉-2-醛-苯甲酰腙Cu(II)配合物(2 a)和8-羟基喹啉-2-醛-对羟基苯甲酰腙Cu(II)配合物(2b),利用黏度滴定、紫外光谱和荧光光谱法研究它们与CT-DNA相互作用情况.实验结果表明,配合物2 a和2b均为良好的DNA插入试剂,它们与DNA的结合常数分别为1.162×106L.mol-1和6.934×106L.mol-1,均为潜在的抗肿瘤药物.

丙戊酸联合HA14-1诱导Bcl-2高表达的白血病细胞株BALL-1凋亡

目的观察体内外丙戊酸(VPA)和HA14-1联合应用对Bcl-2高表达的白血病细胞的杀伤效能及对外周血象的影响。方法(1)将BALL-1分为空白对照组1、mmol/L VPA组5、mmol/L VPA组、15 mmol/L VPA组,作用72 h,流式细胞仪检测各组细胞凋亡结果;(2)将BALL-1分为对照组、VPA组、HA14-1组、VPA+HA14-1组,作用后流式细胞法检测各组凋亡率;(3)每组6只NOD/SCID鼠在每只鼠接种1×107/0.2 ml BALL-1后24 h按如下分组进行实验:①对照组;②HA14-1组,经尾静脉注射灭菌HA14-1 25 mg.kg-1.d-1,共7天;③VPA组,注射灭菌VPA 250 mg.kg-1.d-1,共7天;④HA14-1+VPA组,注射灭菌HA14-1 25 mg.kg-1.d-1,4小时后再注射灭菌VPA 250 mg.kg-1.d-1,共7天。记录各组小鼠的存活时间。(4)将普通小白鼠共24只按(3)方法进行分组,比较几组普通小鼠的生存率、存活时间,及外周血细胞计数。结果(1)VPA15 mmol/L作用72 h BALL-1凋亡率为(24.8±2.8)%,与其它3组比较P<0.01;另3组之间比较P>0.05。(2)HA14-1组、VPA组凋亡率分别为(4.6±0.1)%(、4.8±0.5)%,与对照组比较,P>0.05。HA14-1+VPA组凋亡率高达(76.5±6.9)%,与另3组比较P<0.01。(3)HA14-1+VPA组小鼠生存天数为(87.5±4.5)天,显著长于其他3组,而其他3组之间无差异。(4)HA14-1单独作用组和HA14-1与VPA联合作用组表现为白细胞与血小板轻微而短期下降,而小鼠的生存率、存活时间无显著性差异。结论HA14-1与VPA联合用药,可克服Bcl-2高表达造成的对VPA的抗性。

PTK787对VEGF及VEGFR-2在急性髓系白血病中表达的影响

目的检测酪氨酸激酶抑制剂PTK787对急性髓系白血病小鼠血清VEGF浓度及其受体VEGFR-2 mRNA表达水平的影响,进一步探讨PTK787抗急性髓性白血病的作用机制。方法建立急性髓系白血病(AML)SCID小鼠模型,采用酶联免疫吸附试验(ELISA)和反转录PCR(RT-PCR)分别动态检测不同时间点正常小鼠、白血病小鼠及PTK787治疗组小鼠外周血清VEGF浓度及其受体VEGFR-2 mRNA表达的水平变化。结果 (1)正常小鼠和患病小鼠均表达VEGF及VEGFR-2 mRNA;(2)患病组外周血清VEGF浓度和VEGFR-2 mRNA的表达均显著高于正常组小鼠(P<0.05),而且随着病程的进展逐渐升高;(3)PTK787治疗组小鼠外周血清VEGF浓度及其受体VEGFR-2 mRNA表达的水平均较患病组明显降低(P<0.05)。结论 PTK78抗急性髓性白血病的作用与降低血清VEGF及其受体VEGFR-2 mRNA表达的水平密切相关。

新型2-取代苯基-1H-咪唑[4,5-f][1,10]邻菲啰啉基Ru(Ⅱ)配合物的光电性质

为获取具有活性官能团的接枝型、高性能荧光传感配合物,合成了2-(4-氨基苯基)-1H-咪唑[4,5-f][1,10]邻菲啰啉(CImPB-NH2)、2-(4-羟基苯基)-1H-咪唑[4,5-f][1,10]邻菲啰啉(CImPB-OH)、2-(4-羧基苯基)-1H-咪唑[4,5-f][1,10]邻菲啰啉(CImPB-COOH)和2-(4-硝基苯基)-1H-咪唑[4,5-f][1,10]邻菲啰啉(CImPB-NO2)四种配体,借助紫外-可见(UV-Vis)吸收光谱、荧光(PL)光谱、循环伏安法(CV)和含时密度泛函理论(TD-DFT)对上述四种配体与过渡金属元素钌(Ru)所形成的配合物的光电性能进行研究.结果表明:四种配合物均在可见光区域有较强吸收,发光范围覆盖绿色到红色光波段.在极性溶剂N,N-二甲基甲酰胺(DMF)中,以2-(4-氨基苯基)-1H-咪唑[4,5-f][1,10]邻菲啰啉为配体所构建的钌配合物([Ru(CImPB-NH2)(bpy)2]2+的荧光量子产率(Φ)较不含咪唑环的5-氨基邻菲啰啉合钌([Ru(phen-NH2)(bpy)2]2+)的提高了67%,以2-(4-羧基苯基)-1H-咪唑[4,5-f][1,10]邻菲啰啉所构建的钌配合物([Ru(CImPB-COOH)(bpy)2]2+)的Φ可达29.8%,是[Ru(phen-NH2)(bpy)2]2+的18倍.理论计算表明:配体中取代苯环、咪唑环和邻菲啰啉的稠环共平面,形成共价大π体系,其有效共轭长度较邻菲啰啉母体有显著增加,配合物是以Ru为中心的近似八面体构型,理论计算的电子吸收光谱和跃迁性质与实验结果相一致.上述研究有可能为接枝型、高性能荧光传感配合物的设计和筛选提供实验依据.

氯球CPS表面固载2,6-双(2-苯并咪唑)吡啶金属Cu(Ⅱ)配合物的催化氧化反应研究

利用2,6-双(2-苯并咪唑)吡啶(bbp)在氯甲基化交联聚苯乙烯(CPS)微球上进行烷基化反应,形成改性微球CPS-bbp,然后与Cu^(2+)盐配位,制得固体配合物CPS-Cu(Ⅱ)-bbp,分别采用核磁、红外、紫外-可见吸收光谱、扫描电子显微镜(SEM)/X线能谱(EDS)、热重分析对配合物的结构与形貌进行表征和观察.最后,将配合物作为催化剂,分别研究其在氧化苯甲醇、苯乙烯和环己烯氧化反应中的催化性能.结果表明,在以叔丁基过氧化氢为氧化剂,CPS-Cu(Ⅱ)-bbp为催化剂条件下,苯甲醇氧化产物只有苯甲醛,其转化率可达93.7%;苯乙烯的主要氧化产物为氧化苯乙烯,其转化率为89.1%,产物选择性为60.7%;氧化环己烯的主要氧化产物为α-环己烯酮,转化率为67.9%,选择性达96.7%.