公开(公告)号：US20100297010A1

公开(公告)日：2010-11-25

申请号：US12600427

申请日：2008-05-16

申请人： Anka Bric ,  Lars Zender ,  Cornelius Miething ,  Uli Bialucha ,  Scott W. Lowe

发明人： Anka Bric ,  Lars Zender ,  Cornelius Miething ,  Uli Bialucha ,  Scott W. Lowe

IPC分类号： A61K49/00 ,  C12Q1/68 ,  A61K31/7088 ,  A61K31/711 ,  A61K38/00 ,  G01N33/574 ,  A61P35/00

CPC分类号： C12N15/1135 ,  A01K67/0271 ,  A01K67/0275 ,  A01K2207/05 ,  A01K2217/052 ,  A01K2227/105 ,  A01K2267/0331 ,  A01K2267/0393 ,  C07K14/82 ,  C12N15/1082 ,  C12N15/8509 ,  C12N2310/111 ,  C12N2310/14 ,  C12N2310/53 ,  C12N2320/12 ,  C12N2330/31 ,  C12N2799/027 ,  C12N2800/00

摘要： The present invention is directed to methods of identifying tumor suppressor genes in vivo, tumor suppressors thus found, methods of treatment taking advantage of the identified tumor suppressors, methods of and kits for diagnosis of cancer using the identified tumor suppressor, and pharmaceutical composition comprising an identified tumor suppressor or modulators thereof.

摘要翻译： 本发明涉及在体内鉴定肿瘤抑制基因的方法，所发现的肿瘤抑制因子，利用鉴定的肿瘤抑制基因的治疗方法，使用鉴定的肿瘤抑制基因的癌症诊断方法和药物组合物，以及包含 鉴定肿瘤抑制物或其调节剂。

公开(公告)号：US20100273660A1

公开(公告)日：2010-10-28

申请号：US12617624

申请日：2009-11-12

申请人： Lars Zender ,  Wen Xue ,  Scott Powers ,  Scott W. Lowe

发明人： Lars Zender ,  Wen Xue ,  Scott Powers ,  Scott W. Lowe

IPC分类号： C40B20/06 ,  C07K16/00 ,  C40B50/04 ,  C40B40/06 ,  C12N5/09 ,  C12Q1/68 ,  G01N33/574

CPC分类号： A01K67/0271 ,  A01K2217/058 ,  A01K2267/0331 ,  C07K14/4747 ,  C12N15/1079 ,  C12N15/8509 ,  C12N2510/04 ,  C12N2517/02 ,  C12N2799/027 ,  C12Q1/6886 ,  C12Q2600/154 ,  C12Q2600/178 ,  G01N33/5044 ,  G01N33/5067 ,  G01N33/5088 ,  G01N33/57415 ,  G01N33/57438 ,  G01N2500/00 ,  G01N2800/50 ,  G01N2800/52

摘要： In some aspects, the invention provides a genetically tractable in situ non-human animal model for hepatocellular carcinoma. The model is useful, inter alia, in understanding the molecular mechanisms of liver cancer, in understanding the genetic alterations that lead to chemoresistance or poor prognosis, and in identifying and evaluating new therapies against hepatocellular carcinomas. The liver cancer model of this invention is made by altering hepatocytes to increase oncogene expression, to reduce tumor suppressor gene expression or both and by transplanting the resulting hepatocytes into a recipient non-human animal.The present invention also provides methods for identifying and validating tumor suppressor genes by screening pools of shRNAs that target genomic regions deleted in human cancers, such as human hepatocellular carcinomas. The present invention also provides validated tumor suppressor genes, and methods of inhibiting cell proliferation and/or tumor growth, for example by expression of such tumor suppressor genes.

摘要翻译： 在一些方面，本发明提供了用于肝细胞癌的遗传易处的非人动物模型。 该模型除其他外，有助于理解肝癌的分子机制，了解导致化学耐药性或预后不良的遗传改变，以及鉴定和评估针对肝细胞癌的新疗法。 本发明的肝癌模型通过改变肝细胞以增加癌基因表达，减少肿瘤抑制基因表达或两者并通过将所得肝细胞移植到受体非人动物中来制备。 本发明还提供了通过筛选靶向人类癌症中缺失的基因组区域（例如人肝细胞癌）的shRNA的鉴定和验证肿瘤抑制基因的方法。 本发明还提供了经过验证的肿瘤抑制基因，以及例如通过表达这种肿瘤抑制基因来抑制细胞增殖和/或肿瘤生长的方法。

公开(公告)号：US08137907B2

公开(公告)日：2012-03-20

申请号：US12072115

申请日：2008-02-21

申请人： Lars Zender ,  Scott W. Lowe ,  Mona S. Spector

发明人： Lars Zender ,  Scott W. Lowe ,  Mona S. Spector

IPC分类号： C12Q1/68 ,  C07H21/04 ,  C07K16/00 ,  C12P19/34

CPC分类号： A01K67/0271 ,  A01K2217/058 ,  A01K2267/0331 ,  C07K14/4747 ,  C12N15/8509 ,  C12N2510/04 ,  C12N2517/02 ,  C12N2799/027 ,  G01N33/5067 ,  G01N33/57438 ,  G01N2500/00 ,  G01N2800/52

摘要： This invention provides a genetically tractable in situ non-human animal model for hepatocellular carcinoma. The model is useful, inter alia, in understanding the molecular mechanisms of liver cancer, in understanding the genetic alterations that lead to chemoresistance or poor prognosis, and in identifying and evaluating new therapies against hepatocellular carcinomas. The liver cancer model of this invention is made by altering hepatocytes to increase oncogene expression, to reduce tumor suppressor gene expression or both and by transplanting the resulting hepatocytes into a recipient non-human animal.This invention also relates to the use of RNA interference (RNAi) technology in vivo to efficiently identify genes associated with liver cancer, in particular those encoding tumor suppressors, by knocking out candidate genes using RNAi and observing whether tumors would develop.

摘要翻译： 本发明提供了用于肝细胞癌的遗传易处理的非人动物模型。 该模型除其他外，有助于理解肝癌的分子机制，了解导致化学耐药性或预后不良的遗传改变，以及鉴定和评估针对肝细胞癌的新疗法。 本发明的肝癌模型通过改变肝细胞以增加癌基因表达，减少肿瘤抑制基因表达或两者并通过将所得肝细胞移植到受体非人动物中来制备。 本发明还涉及RNA干扰（RNAi）技术在体内有效地鉴定与肝癌相关的基因，特别是编码肿瘤抑制因子的基因，通过使用RNAi敲除候选基因并观察肿瘤是否会发展。

公开(公告)号：US20100310504A1

公开(公告)日：2010-12-09

申请号：US12679835

申请日：2008-09-25

申请人： Scott W. Lowe ,  Valery Krizhanovsky ,  Lars Zender

发明人： Scott W. Lowe ,  Valery Krizhanovsky ,  Lars Zender

IPC分类号： A61K38/20 ,  A61K38/21 ,  A61K38/18 ,  A61K35/12 ,  A61K31/7052 ,  A61K39/395 ,  C12Q1/02 ,  A61P1/16

CPC分类号： A61K38/18 ,  A61K35/17 ,  A61K38/1774 ,  A61K38/19 ,  G01N33/5061 ,  G01N2510/00 ,  Y02A50/465

摘要： Fibrosis arises as part of a wound healing response that maintains organ integrity following catastrophic tissue damage, but can also contribute to a variety of human pathologies, including liver cirrhosis. The invention demonstrates that cellular senescence acts to limit the fibrogenic response to tissue damage, thereby establishing a role for the senescence program in pathophysiological settings beyond cancer. Accordingly, the methods of the invention relate to modulating cellular senescence in disease tissue that have elevated numbers of senescent cells, such as in fibrotic tissues.

摘要翻译： 纤维化是伤口愈合反应的一部分，其在灾难性组织损伤后维持器官完整性，但也可能导致多种人类病理，包括肝硬化。 本发明证明细胞衰老起限制对组织损伤的纤维形成反应，从而在衰老程序在癌症以外的病理生理环境中建立起一种作用。 因此，本发明的方法涉及调节具有升高的衰老细胞数量的疾病组织中的细胞衰老，例如在纤维组织中。

公开(公告)号：US07794941B2

公开(公告)日：2010-09-14

申请号：US11893086

申请日：2007-08-13

申请人： Scott Powers ,  Lars Zender ,  Rebecca A. Kohnz ,  Scott W. Lowe

发明人： Scott Powers ,  Lars Zender ,  Rebecca A. Kohnz ,  Scott W. Lowe

IPC分类号： C12Q1/68 ,  C12P19/34

CPC分类号： C12N5/0693 ,  A01K67/0271 ,  A01K2217/058 ,  A01K2227/105 ,  A01K2267/0331 ,  A61K38/1825 ,  C12N2501/119 ,  C12Q1/6886 ,  C12Q2600/106 ,  C12Q2600/112 ,  C12Q2600/136

摘要： The invention provides methods for diagnosing cancers in humans by detecting DNA amplifications in chromosomal region 8p22, which encompasses the FGF-20 gene and the EFHA2 gene. Also provided are cancer treatment methods using inhibitors of FGF-20 and EFHA2. The invention also provides methods for promoting successful regeneration of liver function. These methods can be used therapeutically to improve liver function following transplantation in both recipient and donor subjects.

摘要翻译： 本发明提供了通过检测包含FGF-20基因和EFHA2基因的染色体区域8p22中的DNA扩增来诊断人类癌症的方法。 还提供了使用FGF-20和EFHA2抑制剂的癌症治疗方法。 本发明还提供促进肝功能再生成功的方法。 这些方法可以治疗性地用于在接受者和供体受试者中移植后改善肝功能。

公开(公告)号：US20110035814A1

公开(公告)日：2011-02-10

申请号：US12301980

申请日：2007-05-23

申请人： Lars Zender ,  Scott W. Lowe ,  Mona S. Spector ,  Wen Xue

发明人： Lars Zender ,  Scott W. Lowe ,  Mona S. Spector ,  Wen Xue

IPC分类号： C12Q1/68 ,  C12N5/071 ,  A01K67/027 ,  C12Q1/02

CPC分类号： C12Q1/6886 ,  A01K2217/05 ,  A01K2267/0331 ,  C07K14/4747 ,  C07K14/82 ,  C12N2510/04 ,  C12Q2600/106 ,  C12Q2600/136 ,  C12Q2600/178

摘要： This invention provides methods of diagnosis, drug screening, and treatment based on the discovery that cIAP1 and Yap are co-amplified oncogenes that cooperate to contribute to oncogenesis and tumor maintenance.

摘要翻译： 本发明提供了诊断，药物筛选和治疗的方法，基于以下发现，cIAP1和Yap是共同扩增癌基因，其协作以有助于肿瘤发生和肿瘤维持。

公开(公告)号：US20090029872A1

公开(公告)日：2009-01-29

申请号：US12072115

申请日：2008-02-21

申请人： Lars Zender ,  Scott W. Lowe ,  Mona S. Spector

发明人： Lars Zender ,  Scott W. Lowe ,  Mona S. Spector

IPC分类号： C40B30/06 ,  C07H21/00 ,  C12Q1/68

CPC分类号： A01K67/0271 ,  A01K2217/058 ,  A01K2267/0331 ,  C07K14/4747 ,  C12N15/8509 ,  C12N2510/04 ,  C12N2517/02 ,  C12N2799/027 ,  G01N33/5067 ,  G01N33/57438 ,  G01N2500/00 ,  G01N2800/52

摘要： This invention provides a genetically tractable in situ non-human animal model for hepatocellular carcinoma. The model is useful, inter alia, in understanding the molecular mechanisms of liver cancer, in understanding the genetic alterations that lead to chemoresistance or poor prognosis, and in identifying and evaluating new therapies against hepatocellular carcinomas. The liver cancer model of this invention is made by altering hepatocytes to increase oncogene expression, to reduce tumor suppressor gene expression or both and by transplanting the resulting hepatocytes into a recipient non-human animal.This invention also relates to the use of RNA interference (RNAi) technology in vivo to efficiently identify genes associated with liver cancer, in particular those encoding tumor suppressors, by knocking out candidate genes using RNAi and observing whether tumors would develop.

摘要翻译： 本发明提供了用于肝细胞癌的遗传易处理的非人动物模型。 该模型除其他外，有助于理解肝癌的分子机制，了解导致化学耐药性或预后不良的遗传改变，以及鉴定和评估针对肝细胞癌的新疗法。 本发明的肝癌模型通过改变肝细胞以增加癌基因表达，减少肿瘤抑制基因表达或两者并通过将所得肝细胞移植到受体非人动物中来制备。 本发明还涉及RNA干扰（RNAi）技术在体内有效地鉴定与肝癌相关的基因，特别是编码肿瘤抑制因子的基因，通过使用RNAi敲除候选基因并观察肿瘤是否会发展。

公开(公告)号：US20090022685A1

公开(公告)日：2009-01-22

申请号：US11893611

申请日：2007-08-15

申请人： Scott W. Lowe ,  Gregory J. Hannon ,  Lars Zender ,  Wen Xue ,  Ross Dickins

发明人： Scott W. Lowe ,  Gregory J. Hannon ,  Lars Zender ,  Wen Xue ,  Ross Dickins

IPC分类号： A61K38/20 ,  A61K35/12 ,  A01K67/027 ,  G01N33/574 ,  A61P31/00 ,  C12Q1/02 ,  A61K31/7088 ,  A61K31/7105

CPC分类号： A01K67/0271 ,  A01K2267/0331 ,  C07K14/82 ,  C12N15/1135 ,  C12N2310/111 ,  C12N2310/14 ,  C12N2310/53 ,  C12N2320/50 ,  C12N2799/027 ,  C12N2830/006

摘要： This invention provides a genetically tractable in situ non-human animal model for hepatocellular carcinoma. The model is useful, inter alia, in understanding the molecular mechanisms of liver cancer, in understanding the genetic alterations (e.g., in oncogenes and tumor suppressor genes) that lead to chemoresistance or poor prognosis, and in identifying and evaluating new therapies against hepatocellular carcinomas. The liver cancer model of this invention is made by altering hepatocytes to increase oncogene expression, to reduce tumor suppressor gene expression or both, preferably by inducible, reversible, and/or tissue specific expression of double-stranded RNA molecules that interfere with the expression of a target gene, and by transplanting the resulting hepatocytes into a recipient non-human animal. The invention further provides a method to treat cancer involving cooperative interactions between a tumor cell senescence program and the innate immune system.

摘要翻译： 本发明提供了用于肝细胞癌的遗传易处理的非人动物模型。 该模型特别有助于了解肝癌的分子机制，了解导致化疗耐药性或预后不良的遗传改变（例如，致癌基因和肿瘤抑制基因），以及鉴定和评估针对肝细胞癌的新疗法 。 本发明的肝癌模型通过改变肝细胞以增加癌基因表达，减少肿瘤抑制基因表达或两者，优选通过诱导的，可逆的和/或组织特异性表达的双链RNA分子来制备，所述双链RNA分子干扰表达 靶基因，并将所得肝细胞移植到受体非人动物中。 本发明还提供了一种治疗涉及肿瘤细胞衰老程序与先天免疫系统之间协同作用的癌症的方法。

公开(公告)号：US20080188434A1

公开(公告)日：2008-08-07

申请号：US11893086

申请日：2007-08-13

申请人： Scott Powers ,  Lars Zender ,  Rebecca A. Kohnz ,  Scott W. Lowe

发明人： Scott Powers ,  Lars Zender ,  Rebecca A. Kohnz ,  Scott W. Lowe

IPC分类号： A61K31/70 ,  C12Q1/68 ,  C12N5/06 ,  A61P1/00 ,  A01K67/027

CPC分类号： C12N5/0693 ,  A01K67/0271 ,  A01K2217/058 ,  A01K2227/105 ,  A01K2267/0331 ,  A61K38/1825 ,  C12N2501/119 ,  C12Q1/6886 ,  C12Q2600/106 ,  C12Q2600/112 ,  C12Q2600/136

摘要： The invention provides methods for diagnosing cancers in humans by detecting DNA amplifications in chromosomal region 8p22, which encompasses the FGF-20 gene and the EFHA2 gene. Also provided are cancer treatment methods using inhibitors of FGF-20 and EFHA2. The invention also provides methods for promoting successful regeneration of liver function. These methods can be used therapeutically to improve liver function following transplantation in both recipient and donor subjects.

摘要翻译： 本发明提供了通过检测包含FGF-20基因和EFHA2基因的染色体区域8p22中的DNA扩增来诊断人类癌症的方法。 还提供了使用FGF-20和EFHA2抑制剂的癌症治疗方法。 本发明还提供促进肝功能再生成功的方法。 这些方法可以治疗性地用于在接受者和供体受试者中移植后改善肝功能。

公开(公告)号：US08895526B2

公开(公告)日：2014-11-25

申请号：US13260540

申请日：2010-03-29

申请人： Bruce Stillman ,  Scott W. Lowe ,  Anthony Mazurek ,  Johannes Ekkehart Zuber ,  Christopher Vakoc ,  Katherine McJunkin

发明人： Bruce Stillman ,  Scott W. Lowe ,  Anthony Mazurek ,  Johannes Ekkehart Zuber ,  Christopher Vakoc ,  Katherine McJunkin

IPC分类号： C12N15/11 ,  A01K67/027

CPC分类号： A61K31/185 ,  A01K67/0271 ,  A01K2207/05 ,  A01K2207/12 ,  A01K2227/105 ,  A01K2267/0331 ,  A01K2267/0393 ,  C12N15/111 ,  C12N2310/14 ,  C12N2310/531 ,  C12N2320/11 ,  C12N2330/51 ,  C12N2799/027 ,  C12N2830/003 ,  C12N2840/203

摘要： Provided is a mosaic mouse model for use in determining the potency of an shRNA in vivo for reducing survival of cancer cells of chemotherapy-resistant leukemia. The syngeneic mouse recipient is transplanted with tet-on competent leukemia cells carrying a bicistronic nucleic acid construct comprising a promoter operably linked to a fusion gene associated with chemotherapy-resistant leukemia, and a sequence encoding a reverse tet-transactivator protein, such that both coding sequences are co-expressed from the promoter. Also provided are methods of treating soft tissue cancers.

摘要翻译： 提供了一种用于确定shRNA在体内用于降低化疗耐药性白血病癌细胞存活的效力的镶嵌小鼠模型。 将携带双顺反子核酸构建体的tet-on感受态白血病细胞移植到同基因小鼠受体中，所述双顺反子核酸构建体包含可操作地连接于与耐化学药物性白血病相关的融合基因的启动子，以及编码反向tet-transactivator蛋白的序列， 序列由启动子共表达。 还提供了治疗软组织癌症的方法。