ANDREW SCHARENBERG
Medical Practice at Sand Point Way, Seattle, WA

2013031, Nov 28, 2013

May 13, 2013

13/892805

Roman Galetto - Paris, FR
Agnès Gouble - Paris, FR
Stéphanie Grosse - Saint-Cyr sur Morin, FR
Cécile Mannioui - Villiers sur Marne, FR
Laurent Poirot - Paris, FR
Andrew Scharenberg - Seattle WA, US
Julianne Smith - Le Plessis Robinson, FR

A61K 35/14

424 9371, 435375

Methods for developing engineered T-cells for immunotherapy that are both non-alloreactive and resistant to immunosuppressive drugs. The present invention relates to methods for modifying T-cells by inactivating both genes encoding target for an immunosuppressive agent and T-cell receptor, in particular genes encoding CD52 and TCR. This method involves the use of specific rare cutting endonucleases, in particular TALE-nucleases (TAL effector endonuclease) and polynucleotides encoding such polypeptides, to precisely target a selection of key genes in T-cells, which are available from donors or from culture of primary cells. The invention opens the way to standard and affordable adoptive immunotherapy strategies for treating cancer and viral infections.

2009016, Jun 25, 2009

Mar 27, 2007

12/295201

Andrew M. Scharenberg - Seattle WA, US

CHILDREN'S HOSPITAL & REGIONAL MEDICAL CENTER - Seattle WA

C12N 15/87, C12N 9/24, C40B 30/04, C40B 40/02

435456, 435455, 435200, 506 9, 506 14

According to particular exemplary aspects, DNA target site binding and cleavage properties of native, variant or modified homing endonucleases (HE) (e.g., LAGLIDAG (LHE), HNH, His-Cys Box, GIY-YIG, I-SspI-type, and fusions, muteins or variants thereof) in solution are recapitulated on the cell surface (e.g., as assessed by flow cytometric analysis) to provide for novel cells expressing one or more cell surface HEs (e.g., expressing one or more HE binding and/or cleavage specificities), novel cell libraries, and high-throughput methods for assessing target site binding, target site cleavage. The rapid analysis of HE and LHE-DNA interactions on the cell surface with concurrent sorting options provides for high-throughput library screening affording rapid identification, analysis and isolation of novel HEs or LHEs having novel sequence specificities. Such novel sequence specificities, obtained by said methods provide novel methods for introducing targeted DNA-strand cleavage events, and novel chromatin immunoprecipitation methods (CHIP methods).

7063959, Jun 20, 2006

Dec 20, 1999

09/869486

Andrew Scharenberg - Seattle WA, US

Beth Israel Deaconess Medical Center, Inc. - Boston MA

C12P 21/06, A61K 38/17, C07K 1/00, C07H 21/04, C07H 21/02

435 691, 530350, 536 231, 536 235, 514 12, 514 2

Nucleic acids encoding SOC/CRAC calcium channel polypeptides, including fragments and biologically functional variants thereof and encoded polypeptides are provided. The nucleic acids and polypeptides disclosed herein are useful as therapeutic and diagnostic agents. Agents that selectively bind to the foregoing polypeptides and genes also are provided.

2012027, Nov 1, 2012

Feb 24, 2012

13/405183

Andrew M. Scharenberg - Seattle WA, US
Michael T. Certo - Seattle WA, US
Kamila S. Gwiazda - Seattle WA, US

SEATTLE CHILDREN'S RESEARCH INSTITUTE - Seattle WA

C12N 9/96, A61P 37/02, A61P 31/18, C12N 15/90, A61K 38/46

424 942, 435188, 435462, 424 946

The present disclosure relates to the co-expression of an endonuclease with an end-processing enzyme for the purpose of enhanced processing of the polynucleotide ends generated by endonuclease cleavage.

8614300, Dec 24, 2013

Mar 9, 2012

13/416854

Andrew M. Scharenberg - Seattle WA, US

Beth Israel Deconess Medical Center, Inc. - Boston MA

C07K 16/40, C07K 16/46, C07K 16/00, G01N 33/53

53038826, 53038815, 5303881, 5303879, 5303873, 5303871, 435 71

The invention pertains to nucleic acids encoding a mutT domain-containing polypeptide, including fragments and biologically functional variants thereof. The invention also pertains to therapeutics and diagnostics involving the foregoing polypeptide and nucleic acids and agents that bind the foregoing polypeptide and nucleic acids. The invention also pertains to the identification of a novel mutT domain in human TrpC7, a polypeptide previously described as a putative calcium ion channel. Accordingly, the invention also pertains to methods and compositions for identifying agents useful in modulating mutT domain-mediated calcium or other ion transport in cells expressing a polypeptide comprising a mutT domain and a calcium or other ion channel.

8440638, May 14, 2013

Jul 20, 2005

11/658069

John M. Denu - McFarland WI, US
Andrew M. Scharenberg - Seattle WA, US

Wisconsin Alumni Research Foundation - Madison WI
University of Washington - Seattle WA

A61K 31/7076, A61K 31/7052, A61K 31/455, C07H 19/167, C07H 19/20, C07H 19/173

514 45, 514 46, 514 47, 514 42, 514356, 536 221, 536 276, 435375

Compositions and methods are disclosed which are effective for modulating glucose homeostasis, calcium ion flux and cell death in target cells.

2007003, Feb 8, 2007

Jun 16, 2006

11/454636

Andrew Scharenberg - Seattle WA, US

Beth Israel Deaconess Medical Center, Inc. - Boston MA

A61K 39/395, C07K 16/44

424141100, 530388150

Nucleic acids encoding SOC/CRAC calcium channel polypeptides, including fragments and biologically functional variants thereof and encoded polypeptides are provided. The nucleic acids and polypeptides disclosed herein are useful as therapeutic and diagnostic agents. Agents that selectively bind to the foregoing polypeptides and genes also are provided.