Preclinical development and qualification of ZFN-mediated CCR5 disruption in human hematopoietic stem/progenitor cells

DiGiusto, David; Cannon, Paula M.; Holmes, Michael C.; Li, Lijing; Rao, Anil V.; Wang, Jianbin; Lee, Gary; Gregory, Philip D.; Kim, Kenneth; Hayward, Samuel B.; Meyer, Kathleen; Exline, Colin M.; Lopez, Evan; Henley, Jill; González, Norma; Bedell, Victoria; Stan, Rodica; Zaia, John A.

doi:10.1038/mtm.2016.67

Cited by 97 publications

(61 citation statements)

References 38 publications

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“…With the first genome editing of autologous HSCs clinical trial being approved by the FDA for the treatment of HIV using ZFNs targeting CCR5 40 , the new paradigm within cell and gene therapy has begun. Now with the variety of genome editing tools in the toolbox, we can easily typeset the genetic code with base pair precision to: 1) reactivate silenced genes through enhancer disruption, 2) replace good genes with bad genes and 3) revert disease-causing nucleotide substitutions, and with that ease of modification, comes great responsibility for all the researchers and clinicians involved.…”

Section: Resultsmentioning

confidence: 99%

The changing landscape of gene editing in hematopoietic stem cells: a step towards Cas9 clinical translation

Dever

Porteus²

2017

Current Opinion in Hematology

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Purpose of review Since the discovery two decades ago that programmable endonucleases can be engineered to modify human cells at single nucleotide resolution, the concept of genome editing was born. Now these technologies are being applied to therapeutically relevant cell types, including hematopotieic stem cells (HSC), which posses the power to repopulate an entire blood and immune system. The purpose of this review is to discuss the changing landscape of genome editing in hematopotieic stem cells (GE-HSC) from the discovery stage to the preclinical stage, with the imminent goal of clinical translational for the treatment of serious genetic diseases of the blood and immune system. Recent Findings With the discovery that the RNA-programmable (sgRNA) clustered regularly interspace short palindromic repeats (CRISPR)-Cas9 nuclease (Cas9/sgRNA) systems can be easily used to precisely modify the human genome in 2012, a genome editing revolution of hematopotieic stem cells (HSC) has bloomed. We have observed that over the last two years, academic institutions and small biotech companies are developing HSC-based Cas9/sgRNA genome editing curative strategies to treat monogenic disorders, including β-hemoglobinopathies and primary immunodeficiencies. We will focus on recent publications (within the past 2 years) that employ different genome editing strategies to “hijack” the cell’s endogenous double strand repair pathways to confer a disease-specific therapeutic advantage. Summary The number of genome editing strategies in HSCs that could offer therapeutic potential for diseases of the blood and immune system have dramatically risen over the past two years. The HSC-based genome-editing field is primed to enter clinical trials in the subsequent years. We will summarize the major advancements for the development of novel autologous GE-HSC cell and gene therapy strategies for hematopotieic diseases that are candidates for curative allogeneic bone marrow transplantation.

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Section: Resultsmentioning

confidence: 99%

The changing landscape of gene editing in hematopoietic stem cells: a step towards Cas9 clinical translation

Dever

Porteus²

2017

Current Opinion in Hematology

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“…Wang et al, 2015). Trials targeting BCL11A are approaching the clinic (Chang et al, 2017) and several early phase clinical trials have been completed using ZFNs to modify the CCR5 gene in HIV-infected patient peripheral blood T-cells (Tebas et al, 2014) or HSCs (DiGiusto et al, 2016). …”

Section: Gene Editing Strategiesmentioning

confidence: 99%

Hematopoietic Stem Cell Gene Therapy: Progress and Lessons Learned

et al. 2017

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The use of allogeneic hematopoietic stem cells (HSCs) to treat genetic blood cell diseases has become a clinical standard but is limited by availability of suitable matched donors and potential immunologic complications. Gene therapy using autologous HSCs should avoid these limitations and thus may be safer. Progressive improvements in techniques for genetic correction of HSCs, by either vector gene addition or gene editing, are facilitating successful treatments for an increasing number of diseases. We highlight the progress, successes, and remaining challenges toward development of HSC gene therapies and discuss lessons they provide for development of future clinical stem cell therapies.

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“…Editing HSPCs instead of CD4 + T cells has the potential to provide a long-lasting source of modified cells. Success of this strategy has been established in preclinical studies [23] and a recent clinical trial (#NCT02500849) has been initiated using this approach. Programs to disrupt CCR5 in T cells and HSPCs, using the other nuclease platforms that include TALENs, CRISPR/Cas9 and megaTALs (a meganuclease fused to TAL effector modules), are also underway; these are at the pre-clinical stage.…”

Section: First-in-human Studymentioning

confidence: 99%

“…The method of ZFN delivery could also vary depending on the human cell types. For example, Ad5/F35-mediated delivery of ZFNs was very efficient in CD4 + T cells while it was less efficient in HSPCs [23]. The nontoxic mRNA electroporation has been efficient for the introduction of ZFNs into HSPCs.…”

Section: Challenges Facing Zfn-based Gene Editing Before Routine Tranmentioning

confidence: 99%

Recent advances in the use of ZFN-mediated gene editing for human gene therapy

Chandrasegaran¹

2017

Cell Gene Therapy Insights

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Targeted genome editing with programmable nucleases has revolutionized biomedical research. The ability to make site-specific modifications to the human genome, has invoked a paradigm shift in gene therapy. Using gene editing technologies, the sequence in the human genome can now be precisely engineered to achieve a therapeutic effect. Zinc finger nucleases (ZFNs) were the first programmable nucleases designed to target and cleave custom sites. This article summarizes the advances in the use of ZFN-mediated gene editing for human gene therapy and discusses the challenges associated with translating this gene editing technology into clinical use.

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Preclinical development and qualification of ZFN-mediated CCR5 disruption in human hematopoietic stem/progenitor cells

Cited by 97 publications

References 38 publications

The changing landscape of gene editing in hematopoietic stem cells: a step towards Cas9 clinical translation

The changing landscape of gene editing in hematopoietic stem cells: a step towards Cas9 clinical translation

Hematopoietic Stem Cell Gene Therapy: Progress and Lessons Learned

Recent advances in the use of ZFN-mediated gene editing for human gene therapy

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