公开(公告)号：US20100062976A1

公开(公告)日：2010-03-11

申请号：US12555787

申请日：2009-09-08

申请人： Selvaraj A. Naicker ,  Randall W. Yatscoff ,  Robert T. Foster ,  Mark Abel ,  Seetharaman Jayaraman ,  Hans-Jurgen Mair ,  Jean-Michel Adam ,  Bruno Lohri

发明人： Selvaraj A. Naicker ,  Randall W. Yatscoff ,  Robert T. Foster ,  Mark Abel ,  Seetharaman Jayaraman ,  Hans-Jurgen Mair ,  Jean-Michel Adam ,  Bruno Lohri

IPC分类号： A61K38/13

CPC分类号： C07K7/645 ,  A61K9/0095 ,  A61K9/1075 ,  A61K9/4858 ,  A61K38/00 ,  A61K38/13 ,  B82Y5/00 ,  C07K7/64 ,  Y10S530/806

摘要： The invention is directed to isomeric mixtures of cyclosporine analogues that are structurally similar to cyclosporine A. The mixtures possess enhanced efficacy and reduced toxicity over the individual isomers and over naturally occurring and other presently known cyclosporines and cyclosporine derivatives. Embodiments of the present invention are directed toward cis and trans-isomers of cyclosporin A analogs referred to as ISATX247, and derivatives thereof. ISATX247 isomers and alkylated, arylated, and deuterated derivatives are synthesized by stereoselective pathways where the particular conditions of a reaction determine the degree of stereoselectivity. Stereoselective pathways may utilize a Wittig reaction, or an organometallic reagent comprising inorganic elements such as boron, silicon, titanium, and lithium. The ratio of isomers in a mixture may range from about 10 to 90 percent by weight of the (E)-isomer to about 90 to 10 percent by weight of the (Z)-isomer, based on the total weight of the mixture.

摘要翻译： 本发明涉及结构类似于环孢霉素A的环孢菌素类似物的异构体混合物。该混合物具有比单个异构体和天然存在的和其它目前已知的环孢菌素和环孢菌素衍生物更强的功效和降低的毒性。 本发明的实施方案涉及称为ISATX247的环孢菌素A类似物的顺式和反式异构体及其衍生物。 ISATX247异构体和烷基化，芳基化和氘代衍生物通过立体选择性途径合成，其中反应的特定条件决定了立体选择性的程度。 立体选择性途径可以利用维蒂希反应或包含无机元素如硼，硅，钛和锂的有机金属试剂。 基于混合物的总重量，混合物中异构体的比例可以为（E） - 异构体的约10至90重量％至（Z） - 异构体的约90至10重量％。

公开(公告)号：US07521421B2

公开(公告)日：2009-04-21

申请号：US11280666

申请日：2005-11-15

申请人： Selvaraj Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

发明人： Selvaraj Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

IPC分类号： A61K38/00

CPC分类号： C07K7/645 ,  A61K38/00 ,  C07B59/008 ,  C07K1/13 ,  C07K7/64 ,  Y10S530/806 ,  Y10S530/807

摘要： Cyclosporine derivatives are disclosed which possess enhanced efficacy and reduced toxicity over naturally occurring and other presently known cyclosporins and cyclosporine derivatives. The cyclosporine derivatives of the present invention are produced by chemical and isotopic substitution of the cyclosporine A (CsA) molecule by: (1) Chemical substitution and optionally deuterium substitution of amino acid 1; and (2) deuterium substitution at key sites of metabolism of the cyclosporine A molecule such as amino acids 1, 4, 9. Also disclosed are methods of producing the cyclosporine derivatives and method of producing immunosuppression with reduced toxicity with the disclosed cyclosporine derivatives.

摘要翻译： 公开了与天然存在的和其他目前已知的环孢菌素和环孢菌素衍生物相比具有增强的功效和降低的毒性的环孢菌素衍生物。 本发明的环孢菌素衍生物通过以下方式通过环孢菌素A（CsA）分子的化学和同位素取代产生：（1）氨基酸1的化学取代和任选的氘取代; 和（2）在环孢菌素A分子的代谢关键位置的氘代替，例如氨基酸1,4,9。还公开了产生环孢菌素衍生物的方法和与所公开的环孢菌素衍生物一起产生具有降低的毒性的免疫抑制的方法。

公开(公告)号：US07060672B2

公开(公告)日：2006-06-13

申请号：US10274419

申请日：2002-10-17

申请人： Selvaraj A. Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

发明人： Selvaraj A. Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

IPC分类号： A61K38/13

CPC分类号： A61K9/1075 ,  A61K9/0095 ,  A61K9/4858 ,  A61K38/13 ,  A61K47/10

摘要： The present invention relates to formulations containing cyclosporin analogs that are structurally similar to cyclosporin A, in particular isomeric mixtures of cyclosporin analogs that are structurally similar to cyclosporin A. The formulations form stable microemulsion preconcentrates and may provide superior drug bioavailability and/or may reduce one or more adverse effects associated with the administration of cyclosporin. Also disclosed are methods for using and preparing the formulations.

摘要翻译： 本发明涉及结构上类似于环孢菌素A的环孢菌素类似物的制剂，特别是在结构上类似于环孢菌素A的环孢菌素类似物的异构体混合物中。制剂形成稳定的微乳液预浓缩物，并可提供优异的药物生物利用度和/或减少一种 或更多与施用环孢菌素相关的不良反应。 还公开了使用和制备制剂的方法。

公开(公告)号：US06939878B2

公开(公告)日：2005-09-06

申请号：US10754488

申请日：2004-01-09

申请人： Selvaraj Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

发明人： Selvaraj Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

IPC分类号： A61L31/16 ,  C07D498/18 ,  A61P35/02 ,  A61P37/06

CPC分类号： C07D498/18 ,  A61L31/16 ,  A61L2300/416

摘要： The synthesis of deuterated analogues of rapamycin is disclosed together with a method for use for inducing immunosupression and in the treatment of transplantation rejection, graft vs host disease, autoimmune diseases, diseases of inflammation leukemia/lymphoma, solid tumors, fungal infections, hyperproliferative vascular disorders. Also described is a method for the synthesis of water soluble deuteratred rapamycin compounds and their use as described above.

摘要翻译： 公开雷帕霉素的氘代类似物的合成以及用于诱导免疫抑制的方法和用于治疗移植排斥反应，移植物抗宿主病，自身免疫性疾病，炎症性白血病/淋巴瘤疾病，实体瘤，真菌感染，过度增殖性血管疾病 。 还描述了合成水溶性氘化雷帕霉素化合物的方法及其用途如上所述。

公开(公告)号：US06710053B2

公开(公告)日：2004-03-23

申请号：US10300015

申请日：2002-11-20

申请人： Selvaraj Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

发明人： Selvaraj Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

IPC分类号： A61K31445

CPC分类号： C07D498/18 ,  A61L31/16 ,  A61L2300/416

摘要： The synthesis of deuterated analogues of rapamycin is disclosed together with a method for use for inducing immunosupression and in the treatment of transplantation rejection, graft vs host disease, autoimmune diseases, diseases of inflammation leukemia/lymphoma, solid tumors, fungal infections, hyperproliferative vascular disorders. Also described is a method for the synthesis of water soluble deuteratred rapamycin compounds and their use as described above.

摘要翻译： 公开雷帕霉素的氘代类似物的合成以及用于诱导免疫抑制的方法和用于治疗移植排斥反应，移植物抗宿主病，自身免疫性疾病，炎症性白血病/淋巴瘤疾病，实体瘤，真菌感染，过度增殖性血管疾病 。 还描述了合成水溶性氘化雷帕霉素化合物的方法及其用途如上所述。

公开(公告)号：US06225323B1

公开(公告)日：2001-05-01

申请号：US09125173

申请日：1998-08-11

申请人： Randall W. Yatscoff ,  Robert T. Foster ,  Selvaraj Naicker

发明人： Randall W. Yatscoff ,  Robert T. Foster ,  Selvaraj Naicker

IPC分类号： A61K31437

CPC分类号： C07D213/86 ,  C07C233/65 ,  C07C233/78 ,  C07D213/87 ,  C07D277/46 ,  C07D285/135 ,  C07D311/16

摘要： A series of activated iodo-benzamide derivatives are described as antineoplastic and antiviral drug compounds. The compounds generally possess a chelating group, a thiol trapping group and an activating group. The presumptive mechanism of action in preventing cancer cell and virus replication is through inhibition of the binding of transcription factors to zinc finger binding domains. The compounds are effective in inhibiting growth of a variety of human and animal tumor and leukemia cell lines at low concentrations.

公开(公告)号：US20130078280A1

公开(公告)日：2013-03-28

申请号：US13684574

申请日：2012-11-26

申请人： Selvaraj A. Naicker ,  Randall W. Yatscoff ,  Robert T Foster

发明人： Selvaraj A. Naicker ,  Randall W. Yatscoff ,  Robert T Foster

IPC分类号： A61K38/13

CPC分类号： C07K7/645 ,  A61K9/0095 ,  A61K9/1075 ,  A61K9/4858 ,  A61K38/00 ,  A61K38/13 ,  B82Y5/00 ,  C07K7/64 ,  Y10S530/806

摘要： The invention is directed to isomeric mixtures of cyclosporine analogues that are structurally similar to cyclosporine A. The mixtures possess enhanced efficacy and reduced toxicity over the individual isomers and over naturally occurring and other presently known cyclosporines and cyclosporine derivatives. Embodiments of the present invention are directed toward cis and trans-isomers of cyclosporin A analogs referred to as ISATX247, and derivatives thereof. Mixtures of ISATX247 isomers exhibit a combination of enhanced potency and reduced toxicity over the naturally occurring and presently known cyclosporins. ISATX247 isomers and alkylated, arylated, and deuterated derivatives are synthesized by stereoselective pathways where the particular conditions of a reaction determine the degree of stereoselectivity. The ratio of isomers in a mixture may range from about 10 to 90 percent by weight of the (E)-isomer to about 90 to 10 percent by weight of the (Z)-isomer, based on the total weight of the mixture.

摘要翻译： 本发明涉及结构类似于环孢霉素A的环孢菌素类似物的异构体混合物。该混合物具有比单个异构体和天然存在的和其它目前已知的环孢菌素和环孢菌素衍生物更强的功效和降低的毒性。 本发明的实施方案涉及称为ISATX247的环孢菌素A类似物的顺式和反式异构体及其衍生物。 ISATX247异构体的混合物显示与天然存在的和目前已知的环孢菌素相比，其效力和毒性降低的组合。 ISATX247异构体和烷基化，芳基化和氘代衍生物通过立体选择性途径合成，其中反应的特定条件决定了立体选择性的程度。 基于混合物的总重量，混合物中异构体的比例可以为（E） - 异构体的约10至90重量％至（Z） - 异构体的约90至10重量％。

公开(公告)号：US07829533B2

公开(公告)日：2010-11-09

申请号：US12197199

申请日：2008-08-22

申请人： Selvaraj A. Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

发明人： Selvaraj A. Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

IPC分类号： A61K38/13

CPC分类号： A61K9/1075 ,  A61K9/0095 ,  A61K9/4858 ,  A61K38/13 ,  A61K47/10

摘要： The present invention relates to formulations containing cyclosporin analogs that are structurally similar to cyclosporin A, in particular isomeric mixtures of cyclosporin analogs that are structurally similar to cyclosporin A. The formulations form stable microemulsion preconcentrates and may provide superior drug bioavailability and/or may reduce one or more adverse effects associated with the administration of cyclosporin. Also disclosed are methods for using and preparing the formulations.

摘要翻译： 本发明涉及结构上类似于环孢菌素A的环孢菌素类似物的制剂，特别是在结构上类似于环孢菌素A的环孢菌素类似物的异构体混合物中。制剂形成稳定的微乳液预浓缩物，并可提供优异的药物生物利用度和/或减少一种 或更多与施用环孢菌素相关的不良反应。 还公开了使用和制备制剂的方法。

公开(公告)号：US20090054311A1

公开(公告)日：2009-02-26

申请号：US12197199

申请日：2008-08-22

申请人： Selvaraj A. Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

发明人： Selvaraj A. Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

IPC分类号： A61K38/13 ,  A61P37/06

CPC分类号： A61K9/1075 ,  A61K9/0095 ,  A61K9/4858 ,  A61K38/13 ,  A61K47/10

摘要： The present invention relates to formulations containing cyclosporin analogs that are structurally similar to cyclosporin A, in particular isomeric mixtures of cyclosporin analogs that are structurally similar to cyclosporin A. The formulations form stable microemulsion preconcentrates and may provide superior drug bioavailability and/or may reduce one or more adverse effects associated with the administration of cyclosporin. Also disclosed are methods for using and preparing the formulations.

摘要翻译： 本发明涉及结构上类似于环孢菌素A的环孢菌素类似物的制剂，特别是在结构上类似于环孢菌素A的环孢菌素类似物的异构体混合物中。制剂形成稳定的微乳液预浓缩物，并可提供优异的药物生物利用度和/或减少一种 或更多与施用环孢菌素相关的不良反应。 还公开了使用和制备制剂的方法。

公开(公告)号：US20080171850A1

公开(公告)日：2008-07-17

申请号：US11969174

申请日：2008-01-03

申请人： Selvaraj Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

发明人： Selvaraj Naicker ,  Randall W. Yatscoff ,  Robert T. Foster

IPC分类号： C07K7/64

CPC分类号： C07K7/645 ,  A61K9/0095 ,  A61K9/1075 ,  A61K9/4858 ,  A61K38/00 ,  A61K38/13 ,  B82Y5/00 ,  C07K7/64 ,  Y10S530/806

摘要： The invention is directed to isomeric mixtures of cyclosporine analogues that are structurally similar to cyclosporine A. The mixtures possess enhanced efficacy and reduced toxicity over the individual isomers and over naturally occurring and other presently known cyclosporines and cyclosporine derivatives. Embodiments of the present invention are directed toward cis and trans-isomers of cyclosporin A analogs referred to as ISATX247, and derivatives thereof. Mixtures of ISATX247 isomers exhibit a combination of enhanced potency and reduced toxicity over the naturally occurring and presently known cyclosporins. ISATX247 isomers and alkylated, arylated, and deuterated derivatives are synthesized by stereoselective pathways where the particular conditions of a reaction determine the degree of stereoselectivity. The ratio of isomers in a mixture may range from about 10 to 90 percent by weight of the (E)-isomer to about 90 to 10 percent by weight of the (Z)-isomer, based on the total weight of the mixture.

摘要翻译： 本发明涉及结构类似于环孢霉素A的环孢菌素类似物的异构体混合物。该混合物具有比单个异构体和天然存在的和其它目前已知的环孢菌素和环孢菌素衍生物更强的功效和降低的毒性。 本发明的实施方案涉及被称为ISA 247的环孢菌素A类似物及其衍生物的顺式和反式异构体。 ISA 247异构体的混合物显示了与天然存在的和目前已知的环孢菌素相比增强的效力和降低的毒性的组合。 通过立体选择性途径合成烷基化，芳基化和氘代衍生物，其中反应的特定条件决定了立体选择性的程度。 基于混合物的总重量，混合物中异构体的比例可以为（E） - 异构体的约10至90重量％至（Z） - 异构体的约90至10重量％。