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1.发明授权公开(公告)号:US07175828B2
公开(公告)日:2007-02-13
申请号:US10677076
申请日:2003-09-30
申请人: Mark A. Findeis , Malcolm L. Gefter , Gary F. Musso , Ethan R. Signer , James Wakefield , Susan Molineaux , Joseph Chin , Jung-Ja Lee , Michael Kelley , Sonja Komar , Christopher C. Arico-Muendel , Kathryn Phillips , Neil J. Hayward
发明人: Mark A. Findeis , Malcolm L. Gefter , Gary F. Musso , Ethan R. Signer , James Wakefield , Susan Molineaux , Joseph Chin , Jung-Ja Lee , Michael Kelley , Sonja Komar , Christopher C. Arico-Muendel , Kathryn Phillips , Neil J. Hayward
CPC分类号: C07K5/101 , A61K38/00 , C07K5/1027 , C07K7/06 , C07K14/4711 , G01N33/6896 , G01N2333/4709 , G01N2800/2821
摘要: Compounds that modulate natural β amyloid peptide aggregation are provided. The modulators of the invention comprise a peptide, preferably based on a β amyloid peptide, that is comprised entirely of D-amino acids. Preferably, the peptide comprises 3–5 D-amino acid residues and includes at least two D-amino acid residues independently selected from the group consisting of D-leucine, D-phenylalanine and D-valine. In a particularly preferred embodiment, the peptide is a retro-inverso isomer of a β amyloid peptide, preferably a retro-inverso isomer of Aβ17-21. In certain embodiments, the peptide is modified at the amino-terminus, the carboxy-terminus, or both. Preferred amino-terminal modifying groups include cyclic, heterocyclic, polycyclic and branched alkyl groups. Preferred carboxy-terminal modifying groups include an amide group, an alkyl amide group, an aryl amide group or a hydroxy group. Pharmaceutical compositions comprising the compounds of the invention, and diagnostic and treatment methods for amyloidogenic diseases using the compounds of the invention, are also disclosed.
摘要翻译: 提供调节天然β淀粉样肽聚集的化合物。 本发明的调节剂包含优选基于β-淀粉样肽的肽,其完全由D-氨基酸组成。 优选地,肽包含3-5个D-氨基酸残基,并且包括独立地选自D-亮氨酸,D-苯丙氨酸和D-缬氨酸的至少两个D-氨基酸残基。 在特别优选的实施方案中,肽是β淀粉样肽的逆反异构体,优选Abeta 17-21的逆反异构体。 在某些实施方案中,肽在氨基末端,羧基末端或两者都被修饰。 优选的氨基末端修饰基团包括环状,杂环,多环和支链烷基。 优选的羧基末端修饰基团包括酰胺基,烷基酰胺基,芳基酰胺基或羟基。 还公开了包含本发明化合物的药物组合物,以及使用本发明化合物的淀粉样变性疾病的诊断和治疗方法。
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公开(公告)号:US5817626A
公开(公告)日:1998-10-06
申请号:US404831
申请日:1995-03-14
申请人: Mark A. Findeis , Howard Benjamin , Marc B. Garnick , Malcolm L. Gefter , Arvind Hundal , Laura Kasman , Gary Musso , Ethan R. Signer , James Wakefield , Michael J. Reed
发明人: Mark A. Findeis , Howard Benjamin , Marc B. Garnick , Malcolm L. Gefter , Arvind Hundal , Laura Kasman , Gary Musso , Ethan R. Signer , James Wakefield , Michael J. Reed
CPC分类号: C07K14/4711 , A61K38/00
摘要: Compounds that act to modulate the aggregation of natural .beta. amyloid peptides (.beta.-AP) are disclosed. The .beta. amyloid modulators of the invention can promote .beta.-AP aggregation or, more preferably, can inhibit natural .beta.-AP aggregation. Furthermore, the modulators are capable of altering natural .beta.-AP aggregation when the natural .beta.-APs are in a molar excess amount relative to the modulators. Preferred .beta. amyloid modulators comprise amino-terminally biotinylated .beta. amyloid peptide compounds. Pharmaceutical compositions comprising the compounds of the invention, and methods of altering natural .beta.-AP aggregation using the compounds of the invention, are also disclosed.
摘要翻译: 公开了用于调节天然β淀粉样肽(β-AP)聚集的化合物。 本发明的β淀粉样蛋白调节剂可以促进β-AP聚集,更优选可以抑制天然β-AP聚集。 此外,当天然β-APs相对于调节剂摩尔过量时,调节剂能够改变天然的β-AP聚集。 优选的β淀粉样蛋白调节剂包含氨基末端生物素化的β淀粉样蛋白肽化合物。 还公开了包含本发明化合物的药物组合物和使用本发明化合物改变天然β-AP聚集的方法。
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3.发明授权公开(公告)号:US06689752B2
公开(公告)日:2004-02-10
申请号:US09895443
申请日:2001-06-29
申请人: Mark A. Findeis , Malcolm L. Gefter , Gary Musso , Ethan R. Signer , James Wakefield , Susan Molineaux , Joseph Chin , Jung-Ja Lee , Michael Kelley , Sonja Komar-Panicucci , Christopher C. Arico-Muendel , Kathryn Phillips , Neil J. Hayward
发明人: Mark A. Findeis , Malcolm L. Gefter , Gary Musso , Ethan R. Signer , James Wakefield , Susan Molineaux , Joseph Chin , Jung-Ja Lee , Michael Kelley , Sonja Komar-Panicucci , Christopher C. Arico-Muendel , Kathryn Phillips , Neil J. Hayward
IPC分类号: A61K3807
CPC分类号: C07K5/101 , A61K38/00 , C07K5/1027 , C07K7/06 , C07K14/4711 , G01N33/6896 , G01N2333/4709 , G01N2800/2821
摘要: Compounds that modulate natural &bgr; amyloid peptide aggregation are provided. The modulators of the invention comprise a peptide, preferably based on a &bgr; amyloid peptide, that is comprised entirely of D-amino acids. Preferably, the peptide comprises 3-5 D-amino acid residues and includes at least two D-amino acid residues independently selected from the group consisting of D-leucine, D-phenylalanine and D-valine. In a particularly preferred embodiment, the peptide is a retro-inverso isomer of a &bgr; amyloid peptide, preferably a retro-inverso isomer of A&bgr;17-21. In certain embodiments, the peptide is modified at the amino-terminus, the carboxy-terminus, or both. Preferred amino-terminal modifying groups include cyclic, heterocyclic, polycyclic and branched alkyl groups. Preferred carboxy-terminal modifying groups include an amide group, an alkyl amide group, an aryl amide group or a hydroxy group. Pharmaceutical compositions comprising the compounds of the invention, and diagnostic and treatment methods for amyloidogenic diseases using the compounds of the invention, are also disclosed.
摘要翻译: 提供调节天然β淀粉样肽聚集的化合物。 本发明的调节剂包含优选基于β-淀粉样肽的肽,其完全由D-氨基酸组成。 优选地,肽包含3-5个D-氨基酸残基,并且包括独立地选自D-亮氨酸,D-苯丙氨酸和D-缬氨酸的至少两个D-氨基酸残基。 在特别优选的实施方案中,肽是β淀粉样肽的逆反异构体,优选Abeta17-21的逆反异构体。 在某些实施方案中,肽在氨基末端,羧基末端或两者都被修饰。 优选的氨基末端修饰基团包括环状,杂环,多环和支链烷基。 优选的羧基末端修饰基团包括酰胺基,烷基酰胺基,芳基酰胺基或羟基。 还公开了包含本发明化合物的药物组合物,以及使用本发明化合物的淀粉样变性疾病的诊断和治疗方法。
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4.发明授权公开(公告)号:US06277826B1
公开(公告)日:2001-08-21
申请号:US09356931
申请日:1999-07-19
申请人: Mark A. Findeis , Malcolm L. Gefter , Gary Musso , Ethan R. Signer , James Wakefield , Susan Molineaux , Joseph Chin , Jung-Ja Lee , Michael Kelley , Sonja Komar-Panicucci , Christopher C. Arico-Muendel , Kathryn Phillips , Neil J. Hayward
发明人: Mark A. Findeis , Malcolm L. Gefter , Gary Musso , Ethan R. Signer , James Wakefield , Susan Molineaux , Joseph Chin , Jung-Ja Lee , Michael Kelley , Sonja Komar-Panicucci , Christopher C. Arico-Muendel , Kathryn Phillips , Neil J. Hayward
IPC分类号: A61K3806
CPC分类号: C07K5/101 , A61K38/00 , C07K5/1027 , C07K7/06 , C07K14/4711 , G01N33/6896 , G01N2333/4709 , G01N2800/2821
摘要: Compounds that modulate natural &bgr; amyloid peptide aggregation are provided. The modulators of the invention comprise a peptide, preferably based on a &bgr; amyloid peptide, that is comprised entirely of D-amino acids. Preferably, the peptide comprises 3-5 D-amino acid residues and includes at least two D-amino acid residues independently selected from the group consisting of D-leucine, D-phenylalanine and D-valine. In a particularly preferred embodiment, the peptide is a retro-inverso isomer of a &bgr; amyloid peptide, preferably a retro-inverso isomer of A&bgr;17-21. In certain embodiments, the peptide is modified at the amino-terminus, the carboxy-terminus, or both. Preferred amino-terminal modifying groups include cyclic, heterocyclic, polycyclic and branched alkyl groups. Preferred carboxy-terminal modifying groups include an amide group, an alkyl amide group, an aryl amide group or a hydroxy group. Pharmaceutical compositions comprising the compounds of the invention, and diagnostic and treatment methods for amyloidogenic diseases using the compounds of the invention, are also disclosed.
摘要翻译: 提供调节天然β淀粉样肽聚集的化合物。 本发明的调节剂包含优选基于β-淀粉样肽的肽,其完全由D-氨基酸组成。 优选地,肽包含3-5个D-氨基酸残基,并且包括独立地选自D-亮氨酸,D-苯丙氨酸和D-缬氨酸的至少两个D-氨基酸残基。 在特别优选的实施方案中,肽是β淀粉样肽的逆反异构体,优选Abeta17-21的逆反异构体。 在某些实施方案中,肽在氨基末端,羧基末端或两者都被修饰。 优选的氨基末端修饰基团包括环状,杂环,多环和支链烷基。 优选的羧基末端修饰基团包括酰胺基,烷基酰胺基,芳基酰胺基或羟基。 还公开了包含本发明化合物的药物组合物,以及使用本发明化合物的淀粉样变性疾病的诊断和治疗方法。
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公开(公告)号:US5854204A
公开(公告)日:1998-12-29
申请号:US612785
申请日:1996-03-14
申请人: Mark A. Findeis , Howard Benjamin , Marc B. Garnick , Malcolm L. Gefter , Arvind Hundal , Laura Kasman , Gary Musso , Ethan R. Signer , James Wakefield , Michael Reed , Susan Molineaux , William Kubasek , Joseph Chin , Jung-Ja Lee , Michael Kelley
发明人: Mark A. Findeis , Howard Benjamin , Marc B. Garnick , Malcolm L. Gefter , Arvind Hundal , Laura Kasman , Gary Musso , Ethan R. Signer , James Wakefield , Michael Reed , Susan Molineaux , William Kubasek , Joseph Chin , Jung-Ja Lee , Michael Kelley
IPC分类号: A61K39/02 , A61K31/00 , A61K38/00 , A61K51/00 , A61P25/00 , C07K7/06 , C07K14/47 , C07K14/435 , C07K7/08
CPC分类号: C07K14/4711 , A61K38/00
摘要: Compounds that modulate the aggregation of amyloidogenic proteins or peptides are disclosed. The modulators of the invention can promote amyloid aggregation or, more preferably, can inhibit natural amyloid aggregation. In a preferred embodiment, the compounds modulate the aggregation of natural .beta. amyloid peptides (.beta.-AP). In a preferred embodiment, the .beta. amyloid modulator compounds of the invention are comprised of an A.beta. aggregation core domain and a modifying group coupled thereto such that the compound alters the aggregation or inhibits the neurotoxicity of natural .beta. amyloid peptides when contacted with the peptides. Furthermore, the modulators are capable of altering natural .beta.-AP aggregation when the natural .beta.-APs are in a molar excess amount relative to the modulators. Pharmaceutical compositions comprising the compounds of the invention, and diagnostic and treatment methods for amyloidogenic diseases using the compounds of the invention, are also disclosed.
摘要翻译: 公开了调节淀粉样蛋白形成蛋白或肽聚集的化合物。 本发明的调节剂可以促进淀粉样蛋白聚集,更优选可以抑制天然淀粉样蛋白聚集。 在优选的实施方案中,化合物调节天然β淀粉样蛋白肽(β-AP)的聚集。 在优选的实施方案中,本发明的β淀粉样蛋白调节剂化合物由Aβ聚集核心结构域和与其偶联的修饰基团组成,使得当与肽接触时,该化合物改变聚集或抑制天然β淀粉样肽的神经毒性。 此外,当天然β-APs相对于调节剂摩尔过量时,调节剂能够改变天然的β-AP聚集。 还公开了包含本发明化合物的药物组合物,以及使用本发明化合物的淀粉样变性疾病的诊断和治疗方法。
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公开(公告)号:US06214795B1
公开(公告)日:2001-04-10
申请号:US08747599
申请日:1996-11-12
申请人: Howard Benjamin , Ling Chai , Mark A. Findeis , William Goodwin , Arvind Hundal , David I. Israel , Michael Kelley , Martin P. Keough , Kuanghui Lu , Farah Natoli , Alicia Peticolas , Ethan R. Signer , Malcolm L. Gefter
发明人: Howard Benjamin , Ling Chai , Mark A. Findeis , William Goodwin , Arvind Hundal , David I. Israel , Michael Kelley , Martin P. Keough , Kuanghui Lu , Farah Natoli , Alicia Peticolas , Ethan R. Signer , Malcolm L. Gefter
IPC分类号: C07K700
摘要: This invention provides peptide compounds that bind to either a fibroblast growth factor (FGF) or a fibroblast growth factor receptor (FGFR) and, accordingly, are useful for modulating FGFR activity. Preferably, the FGFR is FGFR2-IIIC. Preferably, the FGF is basic FGF. Preferably the peptide compound comprises an amino acid sequence: (Y/F)-(L/F/I)-(R/D/E/S/Y/G)-(Q/L/Y)-Y-(M/L/K/R)-(L/M/D/E/N/S)-(R/L/S/T)-(L/F/M/V) (SEQ ID NO: 1). The invention further comprises pharmaceutical compositions comprising the peptide compounds of the invention and a pharmaceutically acceptable carrier. The invention still further provides methods of modulating FGFR activity using the peptide compounds of the invention.
摘要翻译: 本发明提供了与成纤维细胞生长因子(FGF)或成纤维细胞生长因子受体(FGFR)结合的肽化合物,因此可用于调节FGFR活性。 优选地,FGFR是FGFR2-IIIC。 优选地,FGF是碱性FGF。 优选地,肽化合物包含氨基酸序列:(Y / F) - (L / F / I) - (R / D / E / S / Y / G) - (Q / L / Y)-Y-(M / L / K / R) - (L / M / D / E / N / S) - (R / L / S / T) - (L / F / M / V)(SEQ ID NO:1)。 本发明还包括包含本发明的肽化合物和药学上可接受的载体的药物组合物。 本发明还提供使用本发明的肽化合物调节FGFR活性的方法。
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7.发明授权
公开(公告)号:US5985242A
公开(公告)日:1999-11-16
申请号:US920162
申请日:1997-08-27
申请人: Mark A. Findeis , Malcolm L. Gefter , Gary Musso , Ethan R. Signer , James Wakefield , Susan Molineaux , Joseph Chin , Jung-Ja Lee , Michael Kelley , Sonja Komar-Panicucci , Christopher C. Arico-Muendel , Kathryn Phillips , Neil J. Hayward
发明人: Mark A. Findeis , Malcolm L. Gefter , Gary Musso , Ethan R. Signer , James Wakefield , Susan Molineaux , Joseph Chin , Jung-Ja Lee , Michael Kelley , Sonja Komar-Panicucci , Christopher C. Arico-Muendel , Kathryn Phillips , Neil J. Hayward
CPC分类号: C07K14/4711 , A61K38/00
摘要: Compounds that modulate natural .beta. amyloid peptide aggregation are provided. The modulators of the invention comprise a peptide, preferably based on a .beta. amyloid peptide, that is comprised entirely of D-amino acids. Preferably, the peptide comprises 3-5 D-amino acid residues and includes at least two D-amino acid residues independently selected from the group consisting of D-leucine, D-phenylalanine and D-valine. In a particularly preferred embodiment, the peptide is a retro-inverso isomer of a .beta. amyloid peptide, preferably a retro-inverso isomer of A.beta..sub.17-21. In certain embodiments, the peptide is modified at the amino-terminus, the carboxy-terminus, or both. Preferred amino-terminal modifying groups include cyclic, heterocyclic, polycyclic and branched alkyl groups. Preferred carboxy-terminal modifying groups include an amide group, an alkyl amide group, an aryl amide group or a hydroxy group. Pharmaceutical compositions comprising the compounds of the invention, and diagnostic and treatment methods for amyloidogenic diseases using the compounds of the invention, are also disclosed.
摘要翻译: 提供调节天然β淀粉样肽聚集的化合物。 本发明的调节剂包含优选基于β-淀粉样肽的肽,其完全由D-氨基酸组成。 优选地,肽包含3-5个D-氨基酸残基,并且包括独立地选自D-亮氨酸,D-苯丙氨酸和D-缬氨酸的至少两个D-氨基酸残基。 在特别优选的实施方案中,肽是β淀粉样蛋白肽的逆反异构体,优选Aβ17-21的逆反式异构体。 在某些实施方案中,肽在氨基末端,羧基末端或两者都被修饰。 优选的氨基末端修饰基团包括环状,杂环,多环和支链烷基。 优选的羧基末端修饰基团包括酰胺基,烷基酰胺基,芳基酰胺基或羟基。 还公开了包含本发明化合物的药物组合物,以及使用本发明化合物的淀粉样变性疾病的诊断和治疗方法。
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公开(公告)号:US5854215A
公开(公告)日:1998-12-29
申请号:US475579
申请日:1995-06-07
申请人: Mark A. Findeis , Howard Benjamin , Marc B. Garnick , Malcolm L. Gefter , Arvind Hundal , Laura Kasman , Gary Musso , Ethan R. Signer , James Wakefield , Michael J. Reed
发明人: Mark A. Findeis , Howard Benjamin , Marc B. Garnick , Malcolm L. Gefter , Arvind Hundal , Laura Kasman , Gary Musso , Ethan R. Signer , James Wakefield , Michael J. Reed
CPC分类号: C07K14/4711 , A61K38/00
摘要: Compounds that act to modulate the aggregation of natural .beta. amyloid peptides (.beta.-AP) are disclosed. The .beta. amyloid modulators of the invention can promote .beta.-AP aggregation or, more preferably, can inhibit natural .beta.-AP aggregation. Furthermore, the modulators are capable of altering natural .beta.-AP aggregation when the natural .beta.-APs are in a molar excess amount relative to the modulators. Pharmaceutical compositions comprising the compounds of the invention, and methods of altering natural .beta.-AP aggregation using the compounds of the invention, are also disclosed.
摘要翻译: 公开了用于调节天然β淀粉样肽(β-AP)聚集的化合物。 本发明的β淀粉样蛋白调节剂可以促进β-AP聚集,更优选可以抑制天然β-AP聚集。 此外,当天然β-APs相对于调节剂摩尔过量时,调节剂能够改变天然的β-AP聚集。 还公开了包含本发明化合物的药物组合物和使用本发明化合物改变天然β-AP聚集的方法。
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公开(公告)号:US20110009343A1
公开(公告)日:2011-01-13
申请号:US12643258
申请日:2009-12-21
申请人: Mark A. Findeis , Howard Benjamin , Marc B. Garnick , Malcolm L. Gefter , Arvind Hundal , Laura Kasman , Gary Musso , Ethan R. Signer , James Wakefield , Michael J. Reed
发明人: Mark A. Findeis , Howard Benjamin , Marc B. Garnick , Malcolm L. Gefter , Arvind Hundal , Laura Kasman , Gary Musso , Ethan R. Signer , James Wakefield , Michael J. Reed
CPC分类号: C07K14/4711 , A61K38/00
摘要: Compounds that modulate the aggregation of amyloidogenic proteins or peptides are disclosed. The modulators of the invention can promote amyloid aggregation or, more preferably, can inhibit natural amyloid aggregation. In a preferred embodiment, the compounds modulate the aggregation of natural β amyloid peptides (β-AP). In a preferred embodiment, the β amyloid modulator compounds of the invention are comprised of an Aβ aggregation core domain and a modifying group coupled thereto such that the compound alters the aggregation or inhibits the neurotoxicity of natural β amyloid peptides when contacted with the peptides. Furthermore, the modulators are capable of altering natural β-AP aggregation when the natural β-APs are in a molar excess amount relative to the modulators. Pharmaceutical compositions comprising the compounds of the invention, and diagnostic and treatment methods for amyloidogenic diseases using the compounds of the invention, are also disclosed.
摘要翻译: 公开了调节淀粉样蛋白形成蛋白或肽聚集的化合物。 本发明的调节剂可以促进淀粉样蛋白聚集,更优选可以抑制天然淀粉样蛋白聚集。 在优选的实施方案中,所述化合物调节天然物质的聚集。 淀粉样蛋白肽(&bgr; -AP)。 在优选实施例中, 本发明的淀粉样蛋白调节剂化合物由A&Bgr; 聚集核心结构域和与其偶联的修饰基团,使得所述化合物改变聚集或抑制天然蛋白的神经毒性; 当与肽接触时,淀粉样蛋白肽。 此外,当天然和重组相对于调节剂摩尔量过多时,调节剂能够改变天然和重组蛋白的聚集。 还公开了包含本发明化合物的药物组合物,以及使用本发明化合物的淀粉样变性疾病的诊断和治疗方法。
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公开(公告)号:US07658917B2
公开(公告)日:2010-02-09
申请号:US10463729
申请日:2003-06-17
申请人: Mark A. Findeis , Howard Benjamin , Marc B. Garnick , Malcolm L. Gefter , Arvind Hundal , Ethan R. Signer , James Wakefield , Laura Kasman , Gary Musso , Michael J. Reed
发明人: Mark A. Findeis , Howard Benjamin , Marc B. Garnick , Malcolm L. Gefter , Arvind Hundal , Ethan R. Signer , James Wakefield , Laura Kasman , Gary Musso , Michael J. Reed
CPC分类号: C07K14/4711 , A61K38/00
摘要: Compounds that modulate the aggregation of amyloidogenic proteins or peptides are disclosed. The modulators of the invention can promote amyloid aggregation or, more preferably, can inhibit natural amyloid aggregation. In a preferred embodiment, the compounds modulate the aggregation of natural β amyloid peptides (β-AP). In a preferred embodiment, the β amyloid modulator compounds of the invention are comprised of an Aβ aggregation core domain and a modifying group coupled thereto such that the compound alters the aggregation or inhibits the neurotoxicity of natural β amyloid peptides when contacted with the peptides. Furthermore, the modulators are capable of altering natural β-AP aggregation when the natural β-APs are in a molar excess amount relative to the modulators. Pharmaceutical compositions comprising the compounds of the invention, and diagnostic and treatment methods for amyloidogenic diseases using the compounds of the invention, are also disclosed.
摘要翻译: 公开了调节淀粉样蛋白形成蛋白或肽聚集的化合物。 本发明的调节剂可以促进淀粉样蛋白聚集,更优选可以抑制天然淀粉样蛋白聚集。 在优选的实施方案中,化合物调节天然β淀粉样肽(β-AP)的聚集。 在优选的实施方案中,本发明的β淀粉样蛋白调节剂化合物由Abeta聚集核心结构域和与其偶联的修饰基团组成,使得当与肽接触时该化合物改变聚集或抑制天然β淀粉样肽的神经毒性。 此外,当天然β-AP相对于调节剂为摩尔过量时,调节剂能够改变天然β-AP聚集。 还公开了包含本发明化合物的药物组合物,以及使用本发明化合物的淀粉样变性疾病的诊断和治疗方法。
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