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    COMBINATION BACTERIOLYTIC THERAPY FOR THE TREATMENT OF TUMORS
    31.
    发明公开
    COMBINATION BACTERIOLYTIC THERAPY FOR THE TREATMENT OF TUMORS 有权
    溶菌联合治疗肿瘤的治疗

    公开(公告)号:EP1446012A1

    公开(公告)日:2004-08-18

    申请号:EP02786766.2

    申请日:2002-11-21

    申请人: The Johns Hopkins University School of Medicine

    发明人: DANG, Long KINZLER, Kenneth, W. VOGELSTEIN, BERT

    IPC分类号: A01N63/00 A01N65/00 A61K48/00 C12N1/12 C12N1/20 G01N33/53

    CPC分类号: C12R1/145 A61K31/475 A61K35/742 A61K38/193 A61K41/00 A61K45/06 C12N1/36 A61K2300/00

    摘要: Current chemotherapeutic approaches for cancer are in part limited by the inability of drugs to destroy neoplastic cells within poorly vascularized compartments of tumors. We have here systematically assessed anaerobic bacteria for their capacity to grow expansively within avascutar compartments of transplanted tumors. Among 26 different strains tested, one (Clostridium novyi) appeared particularly promising. We created a strain of C. novyi devoid of its lethal toxin (C. novyi-NT) and showed that intravenously injected C. novyi-NT spores germinated within the avascular regions of tumors in mice and destroyed surrounding viable tumor cells. When C. novyi-NT spores were administered together with conventional chemotherapeutic drugs, extensive hemorrhagic necrosis of tumors often developed within 24 hours, resulting in significant and prolonged anti-tumor effects. This strategy, called combination bacteriolytic therapy (COBALT), has the potential to add a valuablle dimension to the treatment of cancer.

    C-MYC IS ACTIVATED BY BETA-CATENIN AND TCF-4
    32.
    发明授权
    C-MYC IS ACTIVATED BY BETA-CATENIN AND TCF-4 有权
    C-MYC被激活通过β-catenin和TCF-4

    公开(公告)号:EP1104475B1

    公开(公告)日:2004-05-26

    申请号:EP99943741.1

    申请日:1999-08-20

    申请人: The Johns Hopkins University School of Medicine

    发明人: HE, Tong-Chuan VOGELSTEIN, Bert KINZLER, Kenneth, W.

    IPC分类号: C12N15/63 C12Q1/68 C07K14/27

    CPC分类号: C07K14/47 A61K38/00 A61K48/00 C07K14/4705 C12Q1/6897

    摘要: The APC tumor suppressor protein binds to β-catenin, a protein recently shown to interact with Tcf/Lef transcription factors. Here, the gene encoding a Tcf family member that is expressed in colonic epithelium (hTcf-4) was cloned and characterized. hTcf-4 transactivates transcription only when associated with β-catenin. Nuclei of APC-/- colon carcinoma cells were found to contain a stable β-catenin-hTCF-4 complex that was constitutively active, as measured by transcription of a Tcf reporter gene. Reintroduction of APC removed β-catenin from hTcf4 and abrogated the transcriptional transactivation. Constitutive transcription of TCF target genes, caused by loss of APC function, may be a crucial event in the early transformation of colonic epithelium. It is also shown here that the products of mutant APC genes found in colorectal tumors are defective in regulating β-catenin/Tcf-4 transcriptional activation. Furthermore, colorectal tumors with intact APC genes were shown to contain subtle activating mutations of β-catenin that altered functionally significant phosphorylation sites. These results indicate that regulation of β-catenin is critical to APC"s tumor suppressive effect and that this regulation can be circumvented by mutations in either APC or β-catenin.

    MITOCHONDRIAL DOSIMETER
    35.
    发明公开
    MITOCHONDRIAL DOSIMETER 审中-公开
    MITOCHONDRIALER DOSIMETER

    公开(公告)号:EP1320627A2

    公开(公告)日:2003-06-25

    申请号:EP01918690.7

    申请日:2001-03-15

    申请人: The Johns Hopkins University

    发明人: FLISS, Makiko SIDRANSKY, David JEN, Jin POLYAK, Komelia VOGELSTEIN, Bert KINZLER, Kenneth, W.

    IPC分类号: C12Q1/68

    CPC分类号: C12Q1/6809 C12Q1/6883 C12Q1/6886 C12Q2600/156 C12Q2600/158

    摘要: Mitochondrial mutations occur as a product of contact of a person with an environmental pollutant. Mitochondrial mutations are readily detectable in body fluids. Measurement of mitochondrial mutations in body fluids can be used as a dosimeter to monitor exposure to the environmental pollutant. Mitochondrial mutations can also be detected in cancer patients. Probes and primers containing mutant mitochondrial sequences can be used to monitor patient condition.

    摘要翻译: 线粒体突变作为人与环境污染物接触的产物发生。 线粒体突变在体液中容易检测。 体液中线粒体突变的测量可用作剂量计来监测对环境污染物的暴露。 线粒体突变也可以在癌症患者中检测到。 含有突变线粒体序列的探针和引物可用于监测患者状况。

    ENDOTHELIAL CELL EXPRESSION PATTERNS
    36.
    发明公开
    ENDOTHELIAL CELL EXPRESSION PATTERNS 审中-公开
    表达者肛门内皮细胞

    公开(公告)号:EP1307557A2

    公开(公告)日:2003-05-07

    申请号:EP01961827.1

    申请日:2001-08-01

    申请人: The Johns Hopkins University

    发明人: ST. CROIX, Brad KINZLER, Kenneth, W. VOGELSTEIN, Bert

    IPC分类号: C12N15/12 C07K16/28 C07K19/00 A61K39/395 A61P35/00 C07K14/705 C12N5/10 A61K39/00 G01N33/50 G01N33/574 A61K38/17 A61K51/10 A61P9/00 C12Q1/68 A61K48/00

    CPC分类号: C07K16/30 A61K2039/505

    摘要: To gain a better understanding of tumor angiogenesis, new techniques for isolating endothelial cells (ECs) and evaluating gene expression patterns were developed. When transcripts from ECs derived from normal and malignant colorectal tissues were compared with transcripts from non-endothelial cells, over 170 genes predominantly expressed in the endothelium were identified. Comparison between normal- and tumor-derived endothelium revealed 79 differentially expressed genes, including 46 that were specifically elevated in tumor-associated endothelium. Experiments with representative genes from this group demonstrated that most were similarly expressed in the endothelium of primary lung, breast, brain, and pancreatic cancers as well as in metastatic lesions of the liver. These results demonstrate that neoplastic and normal endothelium in humans are distinct at the molecular level, and have significant implications for the development of anti-angiogenic therapies in the future.

    摘要翻译: 为了更好地了解肿瘤血管生成,开发了分离内皮细胞(ECs)和评估基因表达模式的新技术。 将来自正常和恶性结肠直肠组织的ECs的转录物与来自非内皮细胞的转录物进行比较,鉴定出主要在内皮中表达的170多个基因。 正常和肿瘤衍生的内皮的比较显示79个差异表达的基因,其中46个在肿瘤相关内皮特异性升高。 来自该组的代表性基因的实验表明,大多数类似物在原发性肺癌,乳腺癌,脑癌和胰腺癌以及肝转移性损伤的内皮中均表达。 这些结果表明,人类的肿瘤和正常内皮在分子水平上是不同的,并且对未来抗血管生成疗法的发展具有重要意义。

    CONVERTING DIPLOIDY TO HAPLOIDY FOR GENETIC DIAGNOSIS
    38.
    发明公开
    CONVERTING DIPLOIDY TO HAPLOIDY FOR GENETIC DIAGNOSIS 有权
    Diploidie的折算HAPLODIE的遗传诊断

    公开(公告)号:EP1220952A2

    公开(公告)日:2002-07-10

    申请号:EP00968746.8

    申请日:2000-10-06

    申请人: The Johns Hopkins University

    发明人: VOGELSTEIN, Bert KINZLER, Kenneth, W. YAN, Hai PAPADOPOULOS, Nicholas

    IPC分类号: C12Q1/68 C12N15/06 C12N5/26

    CPC分类号: C12N5/166 C12Q1/6886 C12Q2600/156

    摘要: Detection of mutations associated with hereditary diseases is complicated by the diploid nature of mammalian cells. Mutations present in one allele are often masked by the wild-type sequence of the other allele. Individual alleles can be isolated from every chromosome within somatic cell hybrids generated from a single fusion. Nucleic acids from the hybrids can be analyzed for mutations in an unambiguous manner. This approach was used to detect two cancer-causing mutations that had previously defied genetic diagnosis. One of the families studied, Warthin Family G, was the first kindred with a hereditary colon cancer syndrome described in the biomedical literature.