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    • 1. 发明专利
    • Protein modifier production inhibitor and evaluation method thereof
    • 蛋白质改性剂生产抑制剂及其评估方法
    • JP2004325444A
    • 2004-11-18
    • JP2004109556
    • 2004-04-02
    • Kiyoshi KurokawaToshio MiyataTokai Univ学校法人東海大学敏男 宮田清 黒川
    • MIYATA TOSHIOKUROKAWA KIYOSHI
    • G01N33/50A61K45/00A61P3/08A61P3/10A61P13/12G01N33/15G01N33/66
    • PROBLEM TO BE SOLVED: To actually alleviate type 2 diabetes-like symptoms, by administering a compound having AGEs inhibitory action on an SHR/NDmc-cp rat.
      SOLUTION: This evaluation method for a protein modifier production inhibitor has a process of administering a substance to be tested to the SHR/NDmc-cp rat, before and/or after type 2 diabetes-like simptoms are developed, a process for measuring the production level of a saccharified final product in the SHR/NDmc-cp rat and a process for evaluating that the substance to be tested has protein modifier production inhibitory action, when the substance to be tested has a saccharified final product producing level inhibitory action. By this method, a compound usable in the treatment and/or prevention of the disease caused by the production of AGEs can be screened.
      COPYRIGHT: (C)2005,JPO&NCIPI
    • 待解决的问题:通过向SHR / NDmc-cp大鼠施用具有AGEs抑制作用的化合物来实际减轻2型糖尿病样症状。 解决方案:蛋白质修饰剂生成抑制剂的评价方法在形成2型糖尿病模拟之前和/或之后具有向SHR / NDmc-cp大鼠施用待测物质的方法, 测定SHR / NDmc-cp大鼠中糖化最终产物的生产水平,以及待测试物质具有蛋白质调节剂产生抑制作用的评估方法,当待测物质具有糖化最终产物产生水平抑制作用 。 通过该方法,可以筛选可用于治疗和/或预防由AGE产生引起的疾病的化合物。 版权所有(C)2005,JPO&NCIPI
    • 2. 发明专利
    • Modified protein production inhibiter
    • 改良蛋白生产抑制剂
    • JP2007031359A
    • 2007-02-08
    • JP2005217668
    • 2005-07-27
    • Kiyoshi KurokawaToshio MiyataTokai Univ学校法人東海大学敏男 宮田清 黒川
    • MIYATA TOSHIOKUROKAWA KIYOSHI
    • A61K31/397A61K31/545A61M1/14A61M1/28A61P7/08A61P13/12A61P43/00
    • PROBLEM TO BE SOLVED: To provide a modified protein production inhibiter which does not have a hypotensive action and does not cause vitamin B6 deficiency.
      SOLUTION: This modified protein production inhibiter uses a compound having a free type or salt type β-lactam structure as an active ingredient. The compound having the free type or salt type β-lactam structure includes penicillin-based compounds (amoxicillin, ampicillin, oxacillin, or the like), cephem-based compounds (cefazolin, cefamandole, cefalexin, or the like), carbapenem-based compounds (thienamycin, imipenem, carpetimycin A or the like), monocyclic β-lactam-based compounds (nocardin, sulfazecin, azthreonam or the like), natural cephem-based compounds and other β-lactam-based compounds (cephalosporin C, deacetylcephalosporin C, cephamycin A, or the like).
      COPYRIGHT: (C)2007,JPO&INPIT
    • 待解决的问题:提供不具有降血压作用并且不引起维生素B6缺乏症的改良的蛋白质产生抑制剂。 解决方案:该修饰的蛋白质生产抑制剂使用具有游离型或盐型β-内酰胺结构的化合物作为活性成分。 具有游离型或盐型β-内酰胺结构的化合物包括青霉素类化合物(阿莫西林,氨苄青霉素,苯唑西林等),头孢类化合物(头孢唑啉,头孢氨噻肟,头孢氨苄等),碳青霉烯类化合物 (thienamycin,亚胺培南,地毯霉素A等),单环β-内酰胺类化合物(诺卡因,磺胺二甲腈,azthreonam等),天然头孢烯类化合物等β-内酰胺类化合物(头孢菌素C,脱乙酰头孢菌素C, 头孢霉素A等)。 版权所有(C)2007,JPO&INPIT
    • 7. 发明专利
    • Transcriptional regulatory sequence and use thereof
    • 转录调节序列及其用途
    • JP2003310268A
    • 2003-11-05
    • JP2002121315
    • 2002-04-23
    • Kiyoshi KurokawaToshio Miyata敏男 宮田清 黒川
    • KUROKAWA KIYOSHIMIYATA TOSHIO
    • G01N33/50A61K45/00A61K48/00A61P13/12A61P43/00C12N15/09C12Q1/68G01N33/15
    • PROBLEM TO BE SOLVED: To provide a transcriptional regulatory DNA. SOLUTION: A genom DNA region containing a sequence of about 4.0 kb on the upstream of a MEGSIN gene is separated and the base sequence is determined. A region positively regulating the transcription region is specified in the genom DNA region. An AP-1 bond motif in the region is found to exhibit an activity to positively regulate the transcription activity. The transcription activity is considerably lowered by deleting the sequence or transducing a variation from/into the sequence by a site-specific mutagenesis. The transcriptional regulatory DNA is useful as a transcriptional regulatory sequence specific to mesangium cell. The DNA is useful also as a transcriptional factor for controlling the expression of MEGSIS gene and the screening of medicines. COPYRIGHT: (C)2004,JPO
    • 要解决的问题:提供转录调控DNA。 解决方案:分离含有在MEGSIN基因上游的约4.0kb的序列的基因组DNA区域,并确定碱基序列。 在基因组DNA区域中规定了正调节转录区的区域。 发现该区域中的AP-1键基序表现出积极调节转录活性的活性。 通过位点特异性诱变缺失序列或转化序列中的变异,显着降低转录活性。 转录调控DNA可用作对肾小球系膜细胞特异性的转录调控序列。 该DNA也可用作控制MEGSIS基因表达和药物筛选的转录因子。 版权所有(C)2004,JPO