公开(公告)号：US10407470B2

公开(公告)日：2019-09-10

申请号：US15908372

申请日：2018-02-28

Applicant: The Catholic University of America

Inventor： Venigalla B. Rao ,  Wadad Alsalmi

IPC: C07K14/16 ,  C07K14/005 ,  C12N7/00 ,  A61K9/70 ,  A61K39/21 ,  C07K1/22 ,  C07K1/36 ,  A61K39/12 ,  A61K39/00

Abstract: Provided herein are HIV vaccines that encompasses recombinant trimers that mimic native HIV-1 envelope trimers. Also provided are methods of administering to a subject in need thereof an HIV vaccine provided herein to elicit antibodies against a recombinant trimer in the subject. A recombinant trimer is formed by a recombinant protein comprising a recombinant HIV-1 gp140 fused to a tag through a linker at C-terminus of the recombinant HIV-1 gp140, wherein the linker is sufficiently long so that the tag is accessible for binding by a binding molecule bound on a solid matrix during purification of the recombinant trimer.

公开(公告)号：US09850288B2

公开(公告)日：2017-12-26

申请号：US14806735

申请日：2015-07-23

Applicant: THE CATHOLIC UNIVERSITY OF AMERICA

Inventor： Venigalla B. Rao ,  Wadad Alsalmi

IPC: A61K39/21 ,  C07K14/005 ,  C12N7/00 ,  A61K9/70 ,  C07K1/22 ,  C07K1/36 ,  A61K39/12 ,  C07K14/16 ,  A61K39/00

CPC classification number: C07K14/005 ,  A61K9/7023 ,  A61K39/00 ,  A61K39/12 ,  A61K39/21 ,  A61K2039/54 ,  A61K2039/627 ,  C07K1/22 ,  C07K1/36 ,  C07K14/162 ,  C07K2319/00 ,  C07K2319/20 ,  C07K2319/21 ,  C07K2319/22 ,  C07K2319/40 ,  C07K2319/50 ,  C12N7/00 ,  C12N2740/16022 ,  C12N2740/16043 ,  C12N2740/16051 ,  C12N2740/16111 ,  C12N2740/16122 ,  C12N2740/16134 ,  C12N2740/16234

Abstract: An approach of producing recombinant trimers that mimic native HIV-1 envelope trimers is developed. A recombinant protein forming the recombinant trimers encompasses a recombinant HIV-1 gp140 fused to a tag through a linker at C-terminus of the recombinant HIV-1 gp140. The linker is sufficiently long so that the tag is accessible for binding by a binding molecule bound on a solid matrix. After expressed in a cell, the recombinant protein is secreted into the culture medium and assembles into recombinant trimers therein. The recombinant trimers may be directly purified from the culture medium. Cleaved and uncleaved trimers from different clade viruses are produced.

公开(公告)号：US09523101B2

公开(公告)日：2016-12-20

申请号：US14322097

申请日：2014-07-02

Applicant: The Catholic University of America

Inventor： Venigalla B. Rao

IPC: C12N15/86 ,  C12N15/87 ,  C07K14/005 ,  C12N7/00 ,  C12N15/88 ,  A61K47/48 ,  A61K31/7088 ,  A61K31/711 ,  A61K48/00

CPC classification number: C12N15/86 ,  A61K31/7088 ,  A61K31/711 ,  A61K47/48776 ,  A61K47/6901 ,  A61K48/00 ,  C07K14/005 ,  C12N7/00 ,  C12N15/87 ,  C12N15/88 ,  C12N2795/10042 ,  C12N2795/10122 ,  C12N2795/10142 ,  C12N2795/10152

Abstract: Complex viruses are assembled from simple protein subunits by sequential and irreversible assembly. During genome packaging in bacteriophages, a powerful molecular motor assembles at the special portal vertex of an empty prohead to initiate packaging. An aspect of the invention relates to the phage T4 packaging machine being highly promiscuous, translocating DNA into finished phage heads as well as into proheads. Single motors can force exogenous DNA into phage heads at the same rate as into proheads and phage heads undergo repeated initiations, packaging multiple DNA molecules into the same head. This shows that the phage DNA packaging machine has unusual conformational plasticity, powering DNA into an apparently passive capsid receptacle, including the highly stable virus shell, until it is full. These features allow for the design of a novel class of nanocapsid delivery vehicles.

公开(公告)号：US20150017198A1

公开(公告)日：2015-01-15

申请号：US14320731

申请日：2014-07-01

Applicant: The Catholic University of America

Inventor： Venigalla B. RAO ,  Pan Tao

IPC: C07K14/24

CPC classification number: C07K14/24 ,  A61K39/0291 ,  A61K2039/5256 ,  C07K14/005 ,  C07K2319/21 ,  C07K2319/40 ,  C07K2319/735 ,  C12N2795/10123 ,  Y02A50/407

Abstract: Techniques from two basic approaches, structure-based immunogen design and phage T4 nanoparticle delivery, are developed to construct new plague vaccines. The NH2-terminal β-strand of F1 of Yersinia pestis is transplanted to the COOH-terminus of F1 of Yersinia pestis and the NH2-terminus sequence flanking the β-strand of F1 of Yersinia pestis is duplicated to eliminate polymerization but to retain the T cell epitopes. The mutated F1 is fused to the V antigen of Yersinia pestis to thereby form a fusion protein F1mut-V mutant, which produces a completely soluble monomer. The fusion protein F1mut-V is then arrayed on phage T4 nanoparticles via a small outer capsid protein, Soc, from a T4 phage or a T4-related phage. Both the soluble and T4 decorated F1mut-V provided approximately 100% protection to mice and rats against pneumonic plague evoked by high doses of Yersinia pestis CO92.

Abstract translation: 开发了两种基本方法，基于结构的免疫原设计和噬菌体T4纳米颗粒递送的技术来构建新的疫苗疫苗。 将鼠疫耶尔森氏菌的F1的NH2-末端和一串被移植到鼠疫耶尔森氏菌的F1的COOH-末端，并且重复鼠疫耶尔森氏菌的F1侧链的NH2-末端序列，以消除聚合，但保留 T细胞表位。 突变的F1融合到鼠疫耶尔森氏菌的V抗原，从而形成融合蛋白F1mut-V突变体，其产生完全可溶的单体。 然后通过T4噬菌体或与T4相关的噬菌体的小外壳衣壳蛋白Soc，将融合蛋白F1mut-V排列在噬菌体T4纳米颗粒上。 可溶性和T4装饰的F1mut-V都能够对小鼠和大鼠提供大约100％的抗高剂量鼠疫耶尔森氏菌CO92诱发的肺炎瘟疫。

公开(公告)号：US20140335158A1

公开(公告)日：2014-11-13

申请号：US14322097

申请日：2014-07-02

Applicant: The Catholic University of America

Inventor： Venigalla B. Rao

IPC: C12N15/86 ,  A61K47/48 ,  C12N7/00

CPC classification number: C12N15/86 ,  A61K31/7088 ,  A61K31/711 ,  A61K47/48776 ,  A61K47/6901 ,  A61K48/00 ,  C07K14/005 ,  C12N7/00 ,  C12N15/87 ,  C12N15/88 ,  C12N2795/10042 ,  C12N2795/10122 ,  C12N2795/10142 ,  C12N2795/10152

Abstract: Complex viruses are assembled from simple protein subunits by sequential and irreversible assembly. During genome packaging in bacteriophages, a powerful molecular motor assembles at the special portal vertex of an empty prohead to initiate packaging. An aspect of the invention relates to the phage T4 packaging machine being highly promiscuous, translocating DNA into finished phage heads as well as into proheads. Single motors can force exogenous DNA into phage heads at the same rate as into proheads and phage heads undergo repeated initiations, packaging multiple DNA molecules into the same head. This shows that the phage DNA packaging machine has unusual conformational plasticity, powering DNA into an apparently passive capsid receptacle, including the highly stable virus shell, until it is full. These features allow for the design of a novel class of nanocapsid delivery vehicles.

Abstract translation: 复杂病毒通过顺序和不可逆组装由简单蛋白质亚基组装。 在噬菌体的基因组包装过程中，一个强大的分子马达组装在一个空头颅的特殊门户顶点，开始包装。 本发明的一个方面涉及高度混杂的噬菌体T4包装机，将DNA转运到成品噬菌体头以及pro头中。 单个电机可以将外源DNA以与头孢子相同的速率强制进入噬菌体头，并且噬菌体头经历反复引发，将多个DNA分子包装在相同的头中。 这表明噬菌体DNA包装机具有不寻常的构象可塑性，将DNA提供到明显被动的衣壳容器中，包括高度稳定的病毒壳，直至其充满。 这些特征允许设计一种新型的纳米框输送车辆。

公开(公告)号：US12241080B2

公开(公告)日：2025-03-04

申请号：US17546183

申请日：2021-12-09

Applicant: The Catholic University of America

Inventor： Venigalla B. Rao ,  Jingen Zhu

IPC: C12N15/86 ,  C12N7/00

Abstract: Described is an “artificial virus” (AV) programmed with biomolecules that can enter human cells and carry out precise human genome modification. The AVs comprise: at least one viral vector, such as bacteriophage T4; at least one therapeutic molecule, such as DNA, RNA, protein and their complex; and a lipid coating. Also described is a method of human genome modification, using such an AV, and a method of program such an AV.

公开(公告)号：US20240207101A1

公开(公告)日：2024-06-27

申请号：US18544787

申请日：2023-12-19

Applicant: The Catholic University of America

Inventor： Christopher Brian RAUB ,  George NEHMETALLAH ,  Santiago O. CORREA

IPC: A61F13/02 ,  A61L15/18 ,  A61L15/32 ,  A61L15/60 ,  C12M1/12 ,  C12M1/34 ,  C12M3/00 ,  C12N5/077

CPC classification number: A61F13/0289 ,  A61L15/18 ,  A61L15/325 ,  A61L15/60 ,  C12M21/08 ,  C12M25/14 ,  C12M41/36 ,  C12N5/0656 ,  C12N2513/00 ,  C12N2533/30 ,  C12N2533/54 ,  C12N2537/10

Abstract: A method and apparatus including an inverted microscope sample stage, a photomask, a light diffuser, a light pipe, and a light source. The light source is confocal with an inverted microscope, and the apparatus is configured to produce a ruthenium-mediated photocrosslink pattern into a subject. The photomask may be disposed between the inverted microscope sample stage and the light diffuser. The light diffuser may be disposed between the photomask and the light pipe. The light pipe may be disposed between the light diffuser and the light source. The light source may be disposed above the light pipe,

公开(公告)号：US11821097B2

公开(公告)日：2023-11-21

申请号：US17470105

申请日：2021-09-09

Applicant: The Catholic University of America

Inventor： Xiaolong Luo ,  Piao Hu

IPC: C25D17/00 ,  C25D17/10 ,  C25D1/00

CPC classification number: C25D17/002 ,  C25D1/00 ,  C25D17/10

Abstract: The present disclosure relates to a device for and a method of interfacial electrofabrication of freestanding biopolymer membranes comprising at least one anode; at least one cathode; at least one anode electrolyte; and at least one cathode electrolyte, wherein at least a portion of the at least one anode electrolyte and the at least one cathode electrolyte form an interface, wherein at least one polyelectrolyte complex membrane (PECM) forms at the interface of the at least one anode electrolyte and the at least one cathode electrolyte, wherein the at least one anode electrolyte and the at least one cathode electrolyte are separated by the PECM, wherein the at least one anode is disposed in the at least one anode electrolyte, wherein the at least one cathode is disposed in the at least one cathode electrolyte, and wherein the at least one anode and the at least one cathode are distal from the interface of the at least one anode electrolyte and the at least one cathode electrolyte.

公开(公告)号：US20230026666A1

公开(公告)日：2023-01-26

申请号：US17736181

申请日：2022-05-04

Applicant: The Catholic University of America

Inventor： Venigalla B. RAO ,  Himanshu BATRA

IPC: C12N15/86 ,  C12N5/0783 ,  C12N7/00

Abstract: Described is an engineered viral particle programmed with T cell targeting specificity. The viral particles comprise: at least one viral vector, such as bacteriophage T4; and at least one CD4-binding protein displayed on the surface of the viral vector. Also described is a method of reactivate latent HIV-1 and cure patient with HIV-1 infection, using such an engineered viral particle.

公开(公告)号：US20220010335A1

公开(公告)日：2022-01-13

申请号：US17488542

申请日：2021-09-29

Applicant: The Catholic University of America

Inventor： Venigalla B. RAO ,  Jingen ZHU

IPC: C12N15/86

Abstract: Described is hybrid viral vector comprising: a first virus such as bacteriophage T4; one or more second virus such as adeno-associated virus (AAV) attached to the first virus through cross-bridges, such as avidin-biotin cross-bridges; one or more DNA molecules packaged in the first virus; one or more nucleic acid molecules packaged in the second virus; and one or more proteins displayed on the surface of the first virus. Also described are methods of making and using such a hybrid viral vector.