Toward eliminating HLA class I expression to generate universal cells from allogeneic donors

Torikai, Hiroki; Reik, Andreas; Soldner, Frank; Warren, Edus H.; Yuen, Carrie; Zhou, Yuanyue; Crossland, Denise L.; Huls, Helen; Littman, Nicholas; Zhang, Ziying; Tykodi, Scott S.; Kebriaei, Partow; Lee, Dean A.; Miller, Jeffrey C.; Rebar, Edward J.; Holmes, Michael C.; Jaenisch, Rudolf; Champlin, Richard E.; Gregory, Philip D.; Cooper, Laurence J.N.

doi:10.1182/blood-2013-03-478255

Cited by 260 publications

(208 citation statements)

References 48 publications

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“…On the basis of these analyses, we conclude that TALEN-mediated genome editing can be incorporated into a large-scale T-cell culture process as a practical and safe approach to the manufacturing of third-party CAR T cells for use in adoptive T-cell immunotherapies. Zinc finger nucleases have previously been applied for gene editing in human T cells, including inactivation of both the TCRa and TCRb genes for enabling allogeneic "off-the-shelf" and TCR replacement strategies and inactivation of an HLA class I gene (34)(35)(36). Our observations, regarding the functional capabilities of TRAC KO T cells, are consistent with the results described in the aforementioned publications; T cells lacking a TCR component lose CD3 expression and all capacity for activation via either the TCR or through the CD3 complex.…”

Section: Discussionmentioning

confidence: 99%

Multiplex Genome-Edited T-cell Manufacturing Platform for “Off-the-Shelf” Adoptive T-cell Immunotherapies

et al. 2015

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Adoptive immunotherapy using autologous T cells endowed with chimeric antigen receptors (CAR) has emerged as a powerful means of treating cancer. However, a limitation of this approach is that autologous CAR T cells must be generated on a custom-made basis. Here we show that electroporation of transcription activator-like effector nuclease (TALEN) mRNA allows highly efficient multiplex gene editing in primary human T cells. We use this TALEN-mediated editing approach to develop a process for the large-scale manufacturing of T cells deficient in expression of both their ab T-cell receptor (TCR) and CD52, a protein targeted by alemtuzumab, a chemotherapeutic agent. Functionally, T cells manufactured with this process do not mediate graft-versus-host reactions and are rendered resistant to destruction by alemtuzumab. These characteristics enable the administration of alemtuzumab concurrently or prior to engineered T cells, supporting their engraftment. Furthermore, endowing the TALEN-engineered cells with a CD19 CAR led to efficient destruction of CD19 þ tumor targets even in the presence of the chemotherapeutic agent. These results demonstrate the applicability of TALEN-mediated genome editing to a scalable process, which enables the manufacturing of third-party CAR T-cell immunotherapies against arbitrary targets. As such, CAR T-cell immunotherapies can therefore be used in an "off-the-shelf" manner akin to other biologic immunopharmaceuticals. Cancer Res; 75(18); 3853-64. Ó2015 AACR.

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Section: Discussionmentioning

confidence: 99%

Multiplex Genome-Edited T-cell Manufacturing Platform for “Off-the-Shelf” Adoptive T-cell Immunotherapies

et al. 2015

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“…Moreover, a recent report demonstrated that reconstitution of NKTs in peripheral blood is associated with long-term remission in pediatric leukemia patients receiving haploidentical stem cell transplantation (71,72). Hence, unlike donor-derived CAR-T cells, CAR-NKTs can be given early after HSCT when the disease burden is minimal and the curative potential of immunotherapy jci.org Volume 126 Number 6 June 2016 system as previously described (76). A clone with an intermediate level of CD1d expression induced the highest rate of NKT proliferation and was further modified with lentiviral vectors encoding CD86, 4-1BBL, or OX40L followed by single cell sorting and clonal expansion.…”

Section: Nkt Isolation Transduction Expansion and Sortingmentioning

confidence: 99%

“…We rendered K562 cells HLA null by eliminating the HLA-C gene from the K562 cell genome using an HLA-Cspecific ZFN as previously described (76). Briefly, ZFNs containing 5 or 6 fingers were designed and assembled using an established archive of prevalidated 2-finger and 1-finger modules (Sangamo BioScience).…”

Section: Author Contributionsmentioning

confidence: 99%

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CD62L+ NKT cells have prolonged persistence and antitumor activity in vivo

Tian¹,

Courtney²,

Jena³

et al. 2016

Journal of Clinical Investigation

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“…Regarding applicability of engineered T cells, strategies are being developed to generate "universal" T cells that could be manufactured from one donor and administered to multiple patients. For instance, this could be done by eliminating the expression of endogenous TCR to generate T cells devoid of alloreactive TCRs (27). Finally, ACT efficacy may be improved by generating and/or selecting T cells with enhanced proliferative and antitumor capacity.…”

Section: Tcr T Cells Some On-target Toxicities Have Been Observed Wimentioning

confidence: 99%

T-cell–based Immunotherapy: Adoptive Cell Transfer and Checkpoint Inhibition

Houot

Schultz

Marabelle

et al. 2015

Cancer Immunology Research

163

121

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Tumor immunotherapy has had demonstrable efficacy in patients with cancer. The most promising results have been with T-cell-based therapies. These include adoptive cell transfer of tumor-infiltrating lymphocytes, genetically engineered T cells, and immune checkpoint inhibitor antibodies. In this review, we describe the different T-cell-based strategies currently in clinical trials and put their applications, present and future, into perspective.

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Toward eliminating HLA class I expression to generate universal cells from allogeneic donors

Abstract: Key Points Allogeneic-donor–derived cells can be genetically modified to eliminate expression of HLA-A. HLA-A disruption from donor cells is a step toward generating allogeneic cells as an off-the-shelf therapeutic.

Cited by 260 publications

References 48 publications

Multiplex Genome-Edited T-cell Manufacturing Platform for “Off-the-Shelf” Adoptive T-cell Immunotherapies

Multiplex Genome-Edited T-cell Manufacturing Platform for “Off-the-Shelf” Adoptive T-cell Immunotherapies

CD62L+ NKT cells have prolonged persistence and antitumor activity in vivo

T-cell–based Immunotherapy: Adoptive Cell Transfer and Checkpoint Inhibition

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