公开(公告)号：US20120196894A1

公开(公告)日：2012-08-02

申请号：US13499844

申请日：2010-09-28

申请人： Mark T. Bilodeau ,  Melissa Egbertson ,  Ahren Green ,  John C. Hartnett ,  Yiwei Li

发明人： Mark T. Bilodeau ,  Melissa Egbertson ,  Ahren Green ,  John C. Hartnett ,  Yiwei Li

IPC分类号： A61K31/136 ,  C07D215/38 ,  A61K31/47 ,  C07C255/59 ,  A61K31/4706 ,  C07D311/74 ,  A61K31/352 ,  A61P29/00 ,  C07D215/44 ,  C07C211/48 ,  A61K31/277

CPC分类号： C07C215/20 ,  A61K31/133 ,  C07C25/02 ,  C07C211/34 ,  C07C215/44 ,  C07C255/58 ,  C07C2602/10 ,  C07D215/38 ,  C07D215/44 ,  C07D311/74 ,  C07D311/76 ,  C07D405/04 ,  C07D405/06

摘要： The present invention relates to compositions and methods that modulate at least one TRP family member. Specifically, the present invention relates to novel TRPA1 antagonists and their use in the treatment of pain such as chronic inflammatory and neuropathic pain. Compounds that can modulate one or more TRPA1 functions are useful in many aspects including, but not limited to, maintaining calcium homeostasis; maintaining sodium homeostasis; modulating intracellular calcium levels; modulating membrane polarization (membrane potential); modulating cation levels; and/or treating or preventing diseases, disorders, or conditions associated with calcium homeostasis, sodium homeostasis, calcium or sodium dyshomeostasis, or membrane polarization/hyperpolarization (including hypo and hyperexcitability), and/or treating or preventing diseases, disorders, or conditions associated with regulation or misregulation of TRPA1 expression or function. The present invention further relates to methods and compositions that antagonize both a function of TRPA1 and a function of one or more additional TRP channels.

摘要翻译： 本发明涉及调节至少一种TRP家族成员的组合物和方法。 具体地说，本发明涉及新型TRPA1拮抗剂及其用于治疗慢性炎性和神经性疼痛等疼痛的用途。 可以调节一种或多种TRPA1功能的化合物在许多方面是有用的，包括但不限于维持钙稳态; 维持钠稳态; 调节细胞内钙含量; 调节膜极化（膜电位）; 调节阳离子水平; 和/或治疗或预防与钙稳态相关的疾病，病症或病症，钠稳态，钙或钠血管平衡，或膜极化/超极化（包括低钠和过度兴奋性）和/或治疗或预防与疾病，病症或病症相关 与TRPA1表达或功能调节或失调。 本发明还涉及拮抗TRPA1的功能和一种或多种另外的TRP通道的功能的方法和组合物。

公开(公告)号：US08829196B2

公开(公告)日：2014-09-09

申请号：US13499844

申请日：2010-09-28

申请人： Mark T. Bilodeau ,  Melissa Egbertson ,  Ahren Green ,  John C. Hartnett ,  Yiwei Li

发明人： Mark T. Bilodeau ,  Melissa Egbertson ,  Ahren Green ,  John C. Hartnett ,  Yiwei Li

IPC分类号： C07D215/38 ,  C07C215/20 ,  C07C211/34 ,  C07C25/02 ,  A61K31/133

CPC分类号： C07C215/20 ,  A61K31/133 ,  C07C25/02 ,  C07C211/34 ,  C07C215/44 ,  C07C255/58 ,  C07C2602/10 ,  C07D215/38 ,  C07D215/44 ,  C07D311/74 ,  C07D311/76 ,  C07D405/04 ,  C07D405/06

摘要： The present invention relates to compositions and methods that modulate at least one TRP family member. Specifically, the present invention relates to novel TRPA1 antagonists and their use in the treatment of pain such as chronic inflammatory and neuropathic pain. Compounds that can modulate one or more TRPA1 functions are useful in many aspects including, but not limited to, maintaining calcium homeostasis; maintaining sodium homeostasis; modulating intracellular calcium levels; modulating membrane polarization (membrane potential); modulating cation levels; and/or treating or preventing diseases, disorders, or conditions associated with calcium homeostasis, sodium homeostasis, calcium or sodium dyshomeostasis, or membrane polarization/hyperpolarization (including hypo and hyperexcitability), and/or treating or preventing diseases, disorders, or conditions associated with regulation or misregulation of TRPA1 expression or function. The present invention further relates to methods and compositions that antagonize both a function of TRPA1 and a function of one or more additional TRP channels.

摘要翻译： 本发明涉及调节至少一种TRP家族成员的组合物和方法。 具体地说，本发明涉及新型TRPA1拮抗剂及其用于治疗慢性炎性和神经性疼痛等疼痛的用途。 可以调节一种或多种TRPA1功能的化合物在许多方面是有用的，包括但不限于维持钙稳态; 维持钠稳态; 调节细胞内钙含量; 调节膜极化（膜电位）; 调节阳离子水平; 和/或治疗或预防与钙稳态相关的疾病，病症或病症，钠稳态，钙或钠血管平衡，或膜极化/超极化（包括低钠和过度兴奋性）和/或治疗或预防与疾病，病症或病症相关 与TRPA1表达或功能调节或失调。 本发明还涉及拮抗TRPA1的功能和一种或多种另外的TRP通道的功能的方法和组合物。

公开(公告)号：US07544677B2

公开(公告)日：2009-06-09

申请号：US11659606

申请日：2005-08-19

申请人： Mark T. Bilodeau ,  Nicholas D. P. Cosford ,  John C. Hartnett ,  Yiwei Li ,  Jun Liang ,  Peter J. Manley ,  Lou Anne Neilson ,  Tony Siu ,  Zhicai Wu

发明人： Mark T. Bilodeau ,  Nicholas D. P. Cosford ,  John C. Hartnett ,  Yiwei Li ,  Jun Liang ,  Peter J. Manley ,  Lou Anne Neilson ,  Tony Siu ,  Zhicai Wu

IPC分类号： A61K31/541 ,  A61K31/5355 ,  A61K31/519 ,  C07D471/04 ,  C07D519/00 ,  A61P35/00

CPC分类号： C07D471/04

摘要： The present invention is directed to compounds which contain substituted 5-deazapteridine moieties which inhibit the activity of Akt, a serine/threonine protein kinase. The invention is further directed to chemotherapeutic compositions containing the compounds of this invention and methods for treating cancer comprising administration of the compounds of the invention.

摘要翻译： 本发明涉及含有抑制Akt（丝氨酸/苏氨酸蛋白激酶）活性的取代的5-取代哌啶部分的化合物。 本发明还涉及含有本发明化合物的治疗组合物和治疗癌症的方法，包括施用本发明化合物。

公开(公告)号：US08389720B2

公开(公告)日：2013-03-05

申请号：US13127898

申请日：2009-11-03

申请人： James C. Barrow ,  Mark T. Bilodeau ,  Christopher D. Cox ,  John C. Hartnett ,  Nathan R. Kett ,  Yiwei Li ,  Peter J. Manley ,  Jeffrey Melamed ,  William D. Shipe ,  B. Wesley Trotter ,  Amy Zartman

发明人： James C. Barrow ,  Mark T. Bilodeau ,  Christopher D. Cox ,  John C. Hartnett ,  Nathan R. Kett ,  Yiwei Li ,  Peter J. Manley ,  Jeffrey Melamed ,  William D. Shipe ,  B. Wesley Trotter ,  Amy Zartman

IPC分类号： A61K31/551 ,  A61K31/5355 ,  A61K31/497 ,  A61K31/519 ,  A61K31/4412 ,  A61K31/4704 ,  C07D243/08 ,  C07D413/14 ,  C07D471/04 ,  C07D401/14 ,  C07D401/12 ,  C07D405/14

CPC分类号： A61K31/47 ,  C07D401/12 ,  C07D405/12

摘要： The present invention is directed to quinolone compounds which are antagonists of neuropeptide S receptors, and which are useful in the treatment or prevention of neurological and psychiatric disorders and diseases in which the neuropeptide S receptor is involved. The invention is also directed to pharmaceutical compositions comprising these compounds and the use of these compounds and compositions in the prevention or treatment of such diseases in which the neuropeptide S receptor is involved.

摘要翻译： 本发明涉及作为神经肽S受体的拮抗剂的喹诺酮化合物，其可用于治疗或预防神经和精神疾病以及涉及神经肽S受体的疾病。 本发明还涉及包含这些化合物的药物组合物以及这些化合物和组合物在预防或治疗涉及神经肽S受体的疾病中的用途。

公开(公告)号：US20110212946A1

公开(公告)日：2011-09-01

申请号：US13127898

申请日：2009-11-03

申请人： James C. Barrow ,  Mark T. Bilodeau ,  Christopher D. Cox ,  John C. Hartnett ,  Nathan R. Kett ,  Yiwei Li ,  Peter J. Manley ,  Jeffrey Melamed ,  William D. Shipe ,  B. Wesley Trotter ,  Amy Zartman

发明人： James C. Barrow ,  Mark T. Bilodeau ,  Christopher D. Cox ,  John C. Hartnett ,  Nathan R. Kett ,  Yiwei Li ,  Peter J. Manley ,  Jeffrey Melamed ,  William D. Shipe ,  B. Wesley Trotter ,  Amy Zartman

IPC分类号： A61K31/4704 ,  C07D405/14 ,  A61K31/496 ,  A61K31/55 ,  C07D401/12 ,  A61K31/4709 ,  C07D413/12 ,  A61K31/5377 ,  C07D215/227 ,  A61P25/00

CPC分类号： A61K31/47 ,  C07D401/12 ,  C07D405/12

摘要： The present invention is directed to quinolone compounds which are antagonists of neuropeptide S receptors, and which are useful in the treatment or prevention of neurological and psychiatric disorders and diseases in which the neuropeptide S receptor is involved. The invention is also directed to pharmaceutical compositions comprising these compounds and the use of these compounds and compositions in the prevention or treatment of such diseases in which the neuropeptide S receptor is involved.

摘要翻译： 本发明涉及作为神经肽S受体的拮抗剂的喹诺酮化合物，其可用于治疗或预防神经和精神疾病以及涉及神经肽S受体的疾病。 本发明还涉及包含这些化合物的药物组合物以及这些化合物和组合物在预防或治疗涉及神经肽S受体的疾病中的用途。

公开(公告)号：US07910561B2

公开(公告)日：2011-03-22

申请号：US11792121

申请日：2005-12-09

申请人： Jeannie M. Arruda ,  Brian T. Campbell ,  Nicholas D. P. Cosford ,  Jacob M. Hoffman ,  Essa H. Hu ,  Mark E. Layton ,  Yiwei Li ,  Jun Liang ,  Kevin J. Rodzinak ,  Tony Siu ,  Brian A. Stearns ,  Lida R. Tehrani ,  Mark T. Bilodeau ,  Peter J. Manley

发明人： Jeannie M. Arruda ,  Brian T. Campbell ,  Nicholas D. P. Cosford ,  Jacob M. Hoffman ,  Essa H. Hu ,  Mark E. Layton ,  Yiwei Li ,  Jun Liang ,  Kevin J. Rodzinak ,  Tony Siu ,  Brian A. Stearns ,  Lida R. Tehrani ,  Mark T. Bilodeau ,  Peter J. Manley

IPC分类号： A01N43/04 ,  A01N43/58 ,  A01N43/42 ,  A61K31/541 ,  A61K31/70 ,  A61K31/50 ,  A61K31/495 ,  A61K31/52 ,  C09B25/00 ,  C07D487/00 ,  C07D491/00 ,  C07H15/00

CPC分类号： C07D471/04

摘要： The present invention is directed to compounds which contain substituted naphthyridines which inhibit the activity of Akt, a serine/threonine protein kinase. The invention is further directed to chemotherapeutic compositions containing the compounds of this invention and methods for treating cancer comprising administration of the compounds of the invention. These substituted naphthyridines have unexpected advantageous properties when compared to other naphthyridines reported in PCT publication WO2003/086394, such unexpected advantageous properties may include increased cellular potency/solubility, greater selectivity, enhanced pharmacokinetic properties, lack of off target activity and so on.

摘要翻译： 本发明涉及含有抑制Akt（丝氨酸/苏氨酸蛋白激酶）活性的取代萘啶的化合物。 本发明还涉及含有本发明化合物的治疗组合物和治疗癌症的方法，包括施用本发明化合物。 与PCT公开WO2003 / 086394中报道的其它萘啶类相比，这些取代的萘啶具有意想不到的有利性质，这种意想不到的有利性质可包括增加的细胞效力/溶解度，更大的选择性，增强的药物动力学性质，缺乏目标活性等。

公开(公告)号：US20080287457A1

公开(公告)日：2008-11-20

申请号：US11792121

申请日：2005-12-09

申请人： Jeannie M. Arruda ,  Brian T. Campbell ,  Nicholas D.P. Cosford ,  Jacob M. Hoffman ,  Essa H. Hu ,  Mark E. Layton ,  Yiwei Li ,  Jun Liang ,  Kevin J. Rodzinak ,  Tony Siu ,  Brian A. Stearns ,  Lida R. Tehrani ,  Mark T. Bilodeau ,  Peter J. Manley

发明人： Jeannie M. Arruda ,  Brian T. Campbell ,  Nicholas D.P. Cosford ,  Jacob M. Hoffman ,  Essa H. Hu ,  Mark E. Layton ,  Yiwei Li ,  Jun Liang ,  Kevin J. Rodzinak ,  Tony Siu ,  Brian A. Stearns ,  Lida R. Tehrani ,  Mark T. Bilodeau ,  Peter J. Manley

IPC分类号： A61K31/496 ,  C07D487/04 ,  A61P35/04 ,  A61K31/4375

CPC分类号： C07D471/04

摘要： The present invention is directed to compounds which contain substituted naphthyridines which inhibit the activity of Akt, a serine/threonine protein kinase. The invention is further directed to chemotherapeutic compositions containing the compounds of this invention and methods for treating cancer comprising administration of the compounds of the invention. These substituted naphthyridines have unexpected advantageous properties when compared to other naphthyridines reported in PCT publication WO2003/086394, such unexpected advantageous properties may include increased cellular potency/solubility, greater selectivity, enhanced pharmacokinetic properties, lack of off target activity and so on.

摘要翻译： 本发明涉及含有抑制Akt（丝氨酸/苏氨酸蛋白激酶）活性的取代萘啶的化合物。 本发明还涉及含有本发明化合物的治疗组合物和治疗癌症的方法，包括施用本发明化合物。 与PCT公开WO2003 / 086394中报道的其它萘啶类相比，这些取代的萘啶具有意想不到的有利性质，这种意想不到的有利性质可包括增加的细胞效力/溶解度，更大的选择性，增强的药物动力学性质，缺乏目标活性等。

公开(公告)号：US08260925B2

公开(公告)日：2012-09-04

申请号：US12266916

申请日：2008-11-07

申请人： Ping Chen ,  Robert K. Foster ,  Yiwei Li ,  Elizabeth A. Ruth

发明人： Ping Chen ,  Robert K. Foster ,  Yiwei Li ,  Elizabeth A. Ruth

IPC分类号： G06F15/173 ,  G06F13/00 ,  G06F9/46

CPC分类号： G06F9/45558 ,  G06F2009/4557 ,  G06F2009/45579

摘要： In one embodiment, a data structure stores information about the number of client virtual I/O adapters, the number of possible destination VIOS hosts and the number of available slots on those hosts. The information is used to iteratively assign adapters to available slots of the VIOS hosts of the destination server to which a client partition is to be migrated. A method comprises testing the data structure to determine whether conditions exist that make allocation of the adapter to a VIOS host unquestionable.

摘要翻译： 在一个实施例中，数据结构存储关于客户端虚拟I / O适配器的数量，可能的目的地VIOS主机的数量和这些主机上的可用时隙数量的信息。 该信息用于迭代地将适配器分配给要迁移客户端分区的目标服务器的VIOS主机的可用插槽。 一种方法包括测试数据结构以确定是否存在将适配器分配给VIOS主机的条件是不容置疑的。

公开(公告)号：US20110118315A1

公开(公告)日：2011-05-19

申请号：US13012045

申请日：2011-01-24

申请人： John H. Hutchinson ,  Petpiboon Peppi Prasit ,  Mark Moran ,  Jillian F. Evans ,  Yiwei Li ,  Jasmine Eleanor Zunic ,  Jeannie M. Arruda ,  Nicholas Simon Stock ,  Brian Andrew Stearns ,  Mustapha Haddach ,  Jeffrey Roger Roppe

发明人： John H. Hutchinson ,  Petpiboon Peppi Prasit ,  Mark Moran ,  Jillian F. Evans ,  Yiwei Li ,  Jasmine Eleanor Zunic ,  Jeannie M. Arruda ,  Nicholas Simon Stock ,  Brian Andrew Stearns ,  Mustapha Haddach ,  Jeffrey Roger Roppe

IPC分类号： A61K31/444 ,  A61P11/00 ,  A61P29/00 ,  A61P11/06 ,  A61P9/00

CPC分类号： C07D401/14 ,  C07D401/12 ,  C07D403/10 ,  C07D413/14 ,  C07D417/12 ,  C07D417/14 ,  C07D471/04

摘要： Described herein are compounds and pharmaceutical compositions containing such compounds, which modulate the activity of 5-lipoxygenase-activating protein (FLAP). Also described herein are methods of using such FLAP modulators, alone and in combination with other compounds, for treating respiratory, cardiovascular, and other leukotriene-dependent or leukotriene mediated conditions or diseases.

摘要翻译： 本文描述了含有调节5-脂氧合酶活化蛋白（FLAP）的活性的化合物的化合物和药物组合物。 本文还描述了使用这样的FLAP调节剂单独和与其它化合物组合用于治疗呼吸，心血管和其它白三烯依赖性或白细胞三烯介导的病症或疾病的方法。

公开(公告)号：US20100122124A1

公开(公告)日：2010-05-13

申请号：US12266916

申请日：2008-11-07

申请人： Ping Chen ,  Robert K. Foster ,  Yiwei Li ,  Elizabeth A. Ruth

发明人： Ping Chen ,  Robert K. Foster ,  Yiwei Li ,  Elizabeth A. Ruth

IPC分类号： G06F9/455 ,  G06F11/07

CPC分类号： G06F9/45558 ,  G06F2009/4557 ,  G06F2009/45579

摘要： In one embodiment, a data structure stores information about the number of client virtual I/O adapters, the number of possible destination VIOS hosts and the number of available slots on those hosts. The information is used to iteratively assign adapters to available slots of the VIOS hosts of the destination server to which a client partition is to be migrated. A method comprises testing the data structure to determine whether conditions exist that make allocation of the adapter to a VIOS host unquestionable.

摘要翻译： 在一个实施例中，数据结构存储关于客户端虚拟I / O适配器的数量，可能的目的地VIOS主机的数量和这些主机上的可用时隙数量的信息。 该信息用于迭代地将适配器分配给要迁移客户端分区的目标服务器的VIOS主机的可用插槽。 一种方法包括测试数据结构以确定是否存在将适配器分配给VIOS主机的条件是不容置疑的。