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Rescooped by Gilbert C FAURE from Cancer Immunotherapy Review and Collection
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Engineered T Cells for Leukemia: A Review of Current Approaches and Applications - Targeted Oncology

Engineered T Cells for Leukemia: A Review of Current Approaches and Applications - Targeted Oncology | Hematology | Scoop.it
This review addresses the basics of CAR T-cell design and reviews data from published clinical studies in leukemia.

 

Abstract

Chimeric antigen receptor T cells (CAR T cells), engineered from individual patients to specifically target tumor-associated antigens, have shown extraordinary promise in the management of B-cell malignancies. Moreover, CAR T cells are being developed for a myriad of other hematologic malignancies. First-generation CAR T cells demonstrated only modest efficacy because of inadequate activation, persistence, and proliferation, but the addition of one (second-generation) or more (third-generation) costimulatory molecules has produced a marked improvement in efficacy. Clinical trials are recruiting patients with leukemia, and CARs are being tested for patients with a large variety of both solid and liquid tumors. It seems likely that CAR T-cell therapy will become an established option in the near future for patients with B-cell malignancies. Significant questions remain about optimal timing for administration, product preparation, and CAR design to optimize response across malignancy types. This review addresses the basics of CAR T-cell design and reviews data from published clinical studies in leukemia. It also contains commentary on the prospects of this promising new therapeutic strategy.

 


Via Krishan Maggon
Gilbert C FAURE's insight:

Targeted Oncology

 

Engineered T Cells for Leukemia: A Review of Current Approaches and Applications

 

Pallawi Torka, MD, and Elizabeth A. Griffiths, MDPublished Online: Jul 27, 2015

 

Krishan Maggon 's curator insight, July 30, 2015 4:02 AM

Targeted Oncology

 

Engineered T Cells for Leukemia: A Review of Current Approaches and Applications

 

Pallawi Torka, MD, and Elizabeth A. Griffiths, MDPublished Online: Jul 27, 2015

 

Rescooped by Gilbert C FAURE from Cancer Immunotherapy Review and Collection
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The development of potential antibody-based therapies for myeloma - Blood Reviews

The development of potential antibody-based therapies for myeloma - Blood Reviews | Hematology | Scoop.it

Abstract

With optimal target antigen selection antibody-based therapeutics can be very effective agents for hematologic malignancies, but none have yet been approved for myeloma. Rituximab and brentuximab vedotin are examples of success for the naked antibody and antibody–drug conjugate classes, respectively. Plasma cell myeloma is an attractive disease for antibody-based targeting due to target cell accessibility and the complementary mechanism of action with approved therapies. Initial antibodies tested in myeloma were disappointing. However, recent results from targeting well-characterized antigens have been more encouraging. In particular, the CD38 and CD138 targeted therapies are showing single-agent activity in early phase clinical trials. Here we will review the development pipeline for naked antibodies and antibody–drug conjugates for myeloma. There is clear clinical need for new treatments, as myeloma inevitably becomes refractory to standard agents. The full impact is yet to be established, but we are optimistic that the first FDA-approved antibody therapeutic(s) for this disease will emerge in the near future.


Via Krishan Maggon
Krishan Maggon 's curator insight, March 30, 2015 4:49 AM
Blood Reviews

Volume 29, Issue 2, March 2015, Pages 81–91

REVIEW The development of potential antibody-based therapies for myelomaDaniel W. Sherbenoub, c, Christopher R. Behrensa, Yang Sua, Jeffrey L. Wolfb, c, Thomas G. Martin IIIb, c,Bin Liua, c, 
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New Era for Monoclonal Antibodies on Horizon in Multiple Myeloma

New Era for Monoclonal Antibodies on Horizon in Multiple Myeloma | Hematology | Scoop.it
The prospects for mAbs to change the treatment paradigm for multiple myeloma have grown considerably brighter as early-phase clinical trial results suggest that emerging agents with novel mechanisms of action are capable of delivering significant efficacy.

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B-cell activating factor in the pathophysiology of multiple myeloma: a target ... - Nature.com

B-cell activating factor in the pathophysiology of multiple myeloma: a target ... - Nature.com | Hematology | Scoop.it

Abstract

Multiple myeloma (MM) is a currently incurable malignancy of plasma cells. Malignant myeloma cells (MMCs) are heavily dependent upon the bone marrow (BM) microenvironment for their survival. One component of this tumor microenvironment, B-Cell Activating Factor (BAFF), has been implicated as a key player in this interaction. This review discusses the role of BAFF in the pathophysiology of MM, and the potential of BAFF-inhibitory therapy for the treatment of MM. Multiple studies have shown that BAFF functions as a survival factor for MMCs. Furthermore, MMCs express several BAFF-binding receptors. Of these, only Transmembrane Activator and CAML Interactor (TACI) correlates with the MMC’s capability to ligate BAFF. Additionally, the level of expression of TACI correlates with the level of the MMC’s BM dependency. Ligation of BAFF receptors on MMCs causes activation of the Nuclear Factor of κ-B (NF-κB) pathway, a crucial pathway for the pathogenesis of many B-cell malignancies. Serum BAFF levels are significantly elevated in MM patients when compared to healthy controls, and correlate inversely with overall survival. BAFF signaling is thus an interesting target for the treatment of MM. Several BAFF-inhibitory drugs are currently under evaluation for the treatment of MM. These include BAFF-monoclonal antibodies (tabalumab) and antibody-drug conjugates (GSK2857916).


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Krishan Maggon 's curator insight, March 1, 2015 5:36 AM
Review

Citation: Blood Cancer Journal (2015) 5, e282; doi:10.1038/bcj.2015.3
Published online 27 February 2015

B-cell activating factor in the pathophysiology of multiple myeloma: a target for therapy?
OPEN

P J Hengeveld1 and M J Kersten1

1Department of Hematology, Academic Medical Center, Amsterdam, The Netherlands

Correspondence: PJ Hengeveld, Department of Hematology, F4-224, Academic Medical Center, Meibergdreef 9, Amsterdam 1105 AZ, The Netherlands. E-mail: P.J.Hengeveld@amc.uva.nl

Received 3 November 2014; Revised 2 January 2015; Accepted 21 January 2015