专利检索 ap:("University of Notre Dame du Lac") AND inv:"ALVES, Nathan" 第 1 页

1.

发明授权
SELECTIVE UV CROSSLINKING OF PEPTIDES AND FUNCTIONAL MOIETIES TO IMMUNOGLOBULINS 有权

公开(公告)号：EP2970440B1

公开(公告)日：2019-11-20

申请号：EP14768752.9

申请日：2014-03-14

申请人： University of Notre Dame du Lac

发明人： BILGICER, Zihni, Basar , ALVES, Nathan

IPC分类号： C07K16/00 , C07K16/46 , A61K41/00 , G01N33/531

2.

发明公开
SELECTIVE UV CROSSLINKING OF PEPTIDES AND FUNCTIONAL MOIETIES TO IMMUNOGLOBULINS 有权
标题翻译： FUNKTIONELLEN EINHEITEN MIT IMMUNGLOBULINEN的UV-VERNETZUNG VON PEPTIDEN

公开(公告)号：EP2970440A1

公开(公告)日：2016-01-20

申请号：EP14768752.9

申请日：2014-03-14

申请人： University Of Notre Dame Du Lac

发明人： BILGICER, Zihni, Basar , ALVES, Nathan

IPC分类号： C07K16/00 , C07K16/46 , A61K41/00

摘要： A method of crosslinking a hetero-bifunctional photo crosslinking compound to an immunoglobulin having at least one heterocyclic photo reactive group and at least one non-photo reactive group where the non-photo reactive group is coupled to an effector molecule and the photo reactive group is coupled to the nucleotide binding site of an immunoglobulin. Alternatively, the photo crosslinker contains an orthogonal reactive group such as a thiol, which can be coupled to an effector molecule or functionalized ligand.

摘要翻译： 本发明提供了将异双官能光交联化合物交联至具有至少一个杂环光反应性基团和至少一种非光反应性基团的免疫球蛋白的方法，其中非光反应性基团与效应分子偶联，光反应性基团与免疫球蛋白的核苷酸结合位点偶联。或者，光交联剂包含正交反应性基团，例如硫醇，其可与效应子分子或官能化配体偶联。

3.

发明公开
NANOPARTICLE DRUG DELIVERY SYSTEMS 审中-公开
标题翻译：纳米粒子给药系统

公开(公告)号：EP2950785A2

公开(公告)日：2015-12-09

申请号：EP14746863.1

申请日：2014-02-04

申请人： University Of Notre Dame Du Lac

发明人： BILGICER, Zihni Basar , ASHLEY, Jonathan , KIZILTEPE-BILGICER, Tanyel , STEFANICK, Jared , ALVES, Nathan

IPC分类号： A61K9/127 , A61K38/00 , A61K47/48 , A61P35/00

CPC分类号： A61K47/48815 , A61K9/0014 , A61K9/0019 , A61K9/008 , A61K9/1271 , A61K9/2054 , A61K9/4858 , A61K38/05 , A61K38/07 , A61K47/542 , A61K47/62 , A61K47/6911

摘要： The invention provides pharmaceutical compositions and method of using the compositions, wherein the compositions comprise liposomes or micelles that contain one or more targeting peptides and/or anticancer drugs. In various embodiments, the components of the liposomes can include a) a phospholipid and optionally a lipid that is not a phospholipid; b) a pegylated lipid; c) a peptide-ethylene glycol (EG)-lipid conjugate wherein the peptide is a targeting ligand, and d) one or more drug-conjugated lipid, encapsulated drugs, or a combination thereof. The peptide- EG-lipid conjugate can be, for example, a compound of Formula (I) or Formula (II). The ethylene glycol (EG) segments of the peptide-EG-lipid conjugate can be, for example, EG6 to about EG36; and the EG segment can be conjugated to one or more lysine moieties.