Your search keyword '"Michelle S. Prew"' showing total 19 results

1. Targeting MCL-1 triggers DNA damage and an anti-proliferative response independent from apoptosis induction

Author

Utsarga Adhikary, Joao A. Paulo, Marina Godes, Shrabasti Roychoudhury, Michelle S. Prew, Yael Ben-Nun, Ellen W. Yu, Amit Budhraja, Joseph T. Opferman, Dipanjan Chowdhury, Steven P. Gygi, and Loren D. Walensky

Subjects

CP: Molecular biology, CP: Cancer, Biology (General), QH301-705.5

Abstract

Summary: MCL-1 is a high-priority target due to its dominant role in the pathogenesis and chemoresistance of cancer, yet clinical trials of MCL-1 inhibitors are revealing toxic side effects. MCL-1 biology is complex, extending beyond apoptotic regulation and confounded by its multiple isoforms, its domains of unresolved structure and function, and challenges in distinguishing noncanonical activities from the apoptotic response. We find that, in the presence or absence of an intact mitochondrial apoptotic pathway, genetic deletion or pharmacologic targeting of MCL-1 induces DNA damage and retards cell proliferation. Indeed, the cancer cell susceptibility profile of MCL-1 inhibitors better matches that of anti-proliferative than pro-apoptotic drugs, expanding their potential therapeutic applications, including synergistic combinations, but heightening therapeutic window concerns. Proteomic profiling provides a resource for mechanistic dissection and reveals the minichromosome maintenance DNA helicase as an interacting nuclear protein complex that links MCL-1 to the regulation of DNA integrity and cell-cycle progression.

Published

2023

2. Structural basis for defective membrane targeting of mutant enzyme in human VLCAD deficiency

Author

Michelle S. Prew, Christina M. Camara, Thomas Botzanowski, Jamie A. Moroco, Noah B. Bloch, Hannah R. Levy, Hyuk-Soo Seo, Sirano Dhe-Paganon, Gregory H. Bird, Henry D. Herce, Micah A. Gygi, Silvia Escudero, Thomas E. Wales, John R. Engen, and Loren D. Walensky

Subjects

Science

Abstract

Prew et al. uncovered a structural basis for human VLCAD deficiency that arises from point mutations within the enzyme’s membrane-binding region, which was shown to fold as a putative α-helical hairpin. Helix-breaking mutations selectively disrupt membrane interaction and thus homeostatic function.

Published

2022

3. The conformational stability of pro-apoptotic BAX is dictated by discrete residues of the protein core

Author

Noah B. Bloch, Thomas E. Wales, Michelle S. Prew, Hannah R. Levy, John R. Engen, and Loren D. Walensky

Subjects

Science

Abstract

The pro-apoptotic BAX protein is a monomer under homeostatic conditions and, in response to stress, transforms into oligomers that induce apoptosis. Here, the authors characterize structural features of BAX that individually stabilize the monomer while collectively contributing to oligomerization.

Published

2021

4. MCL-1 is a master regulator of cancer dependency on fatty acid oxidation

Author

Michelle S. Prew, Utsarga Adhikary, Dong Wook Choi, Erika P. Portero, Joao A. Paulo, Pruthvi Gowda, Amit Budhraja, Joseph T. Opferman, Steven P. Gygi, Nika N. Danial, and Loren D. Walensky

Subjects

CP: Cancer, CP: Metabolism, Biology (General), QH301-705.5

Abstract

Summary: MCL-1 is an anti-apoptotic BCL-2 family protein essential for survival of diverse cell types and is a major driver of cancer and chemoresistance. The mechanistic basis for the oncogenic supremacy of MCL-1 among its anti-apoptotic homologs is unclear and implicates physiologic roles of MCL-1 beyond apoptotic suppression. Here we find that MCL-1-dependent hematologic cancer cells specifically rely on fatty acid oxidation (FAO) as a fuel source because of metabolic wiring enforced by MCL-1 itself. We demonstrate that FAO regulation by MCL-1 is independent of its anti-apoptotic activity, based on metabolomic, proteomic, and genomic profiling of MCL-1-dependent leukemia cells lacking an intact apoptotic pathway. Genetic deletion of Mcl-1 results in transcriptional downregulation of FAO pathway proteins such that glucose withdrawal triggers cell death despite apoptotic blockade. Our data reveal that MCL-1 is a master regulator of FAO, rendering MCL-1-driven cancer cells uniquely susceptible to treatment with FAO inhibitors.

Published

2022

5. Precision Targeting of BFL-1/A1 and an ATM Co-dependency in Human Cancer

Author

Rachel M. Guerra, Gregory H. Bird, Edward P. Harvey, Neekesh V. Dharia, Kyle J. Korshavn, Michelle S. Prew, Kimberly Stegmaier, and Loren D. Walensky

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Cancer cells overexpress a diversity of anti-apoptotic BCL-2 family proteins, such as BCL-2, MCL-1, and BFL-1/A1, to enforce cellular immortality. Thus, intensive drug development efforts have focused on targeting this class of oncogenic proteins to overcome treatment resistance. Whereas a selective BCL-2 inhibitor has been FDA approved and several small molecule inhibitors of MCL-1 have recently entered phase I clinical testing, BFL-1/A1 remains undrugged. Here, we developed a series of stapled peptide design principles to engineer a functionally selective and cell-permeable BFL-1/A1 inhibitor that is specifically cytotoxic to BFL-1/A1-dependent human cancer cells. Because cancers harbor a diversity of resistance mechanisms and typically require multi-agent treatment, we further investigated BFL-1/A1 co-dependencies by mining a genome-scale CRISPR-Cas9 screen. We identified ataxia-telangiectasia-mutated (ATM) kinase as a BFL-1/A1 co-dependency in acute myeloid leukemia (AML), which informed the validation of BFL-1/A1 and ATM inhibitor co-treatment as a synergistic approach to subverting apoptotic resistance in cancer. : Guerra et al. constructed an exquisitely selective BFL-1 inhibitor capable of covalent BFL-1 targeting and cellular penetrance without membrane disruption. Mining a genetic dependency database revealed a spectrum of BFL-1 dependency in cancer and an ATM co-dependency in AML, prompting the combination of BFL-1 and ATM inhibitors to achieve synergistic cytotoxicity. Keywords: BFL-1, A1, BCL-2 family, apoptosis, stapled peptide, covalent inhibitor, dependency, ATM, AML, cancer

Published

2018

6. Targeting a helix-in-groove interaction between E1 and E2 blocks ubiquitin transfer

Author

Loren D. Walensky, Ann M. Cathcart, Henry D. Herce, Tun Oo, Thomas E. Wales, John R. Engen, Susan Lee, Michelle S. Prew, Utsarga Adhikary, Zachary J. Hauseman, Gregory H. Bird, Catherine E. Newman, and Edward P. Harvey

Subjects

Proteasome Endopeptidase Complex, Conformational change, Molecular Conformation, Druggability, Ubiquitin-Activating Enzymes, Article, Structure-Activity Relationship, 03 medical and health sciences, Adenosine Triphosphate, Ubiquitin, Cell Line, Tumor, Humans, Amino Acid Sequence, Molecular Biology, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Binding Sites, biology, Chemistry, 030302 biochemistry & molecular biology, Ubiquitination, Cell Biology, Small molecule, Cell biology, Molecular Docking Simulation, Enzyme, Drug Resistance, Neoplasm, Drug Design, Helix, Cancer cell, biology.protein, Peptides, Alpha helix, Protein Binding

Abstract

The ubiquitin-proteasome system (UPS) is a highly regulated protein disposal process critical to cell survival. Inhibiting the pathway induces proteotoxic stress and can be an effective cancer treatment. The therapeutic window observed upon proteasomal blockade has motivated multiple UPS-targeting strategies, including preventing ubiquitination altogether. E1 initiates the cascade by transferring ubiquitin to E2 enzymes. A small molecule that engages the E1 ATP-binding site and derivatizes ubiquitin disrupts enzymatic activity and kills cancer cells. However, binding-site mutations cause resistance, motivating alternative approaches to block this promising target. We identified an interaction between the E2 N-terminal alpha-1 helix and a pocket within the E1 ubiquitin-fold domain as a potentially druggable site. Stapled peptides modeled after the E2 alpha-1 helix bound to the E1 groove, induced a consequential conformational change and inhibited E1 ubiquitin thiotransfer, disrupting E2 ubiquitin charging and ubiquitination of cellular proteins. Thus, we provide a blueprint for a distinct E1-targeting strategy to treat cancer.

Published

2020

7. Structural basis for defective membrane targeting of mutant enzyme in human VLCAD deficiency

Author

Michelle S, Prew, Christina M, Camara, Thomas, Botzanowski, Jamie A, Moroco, Noah B, Bloch, Hannah R, Levy, Hyuk-Soo, Seo, Sirano, Dhe-Paganon, Gregory H, Bird, Henry D, Herce, Micah A, Gygi, Silvia, Escudero, Thomas E, Wales, John R, Engen, and Loren D, Walensky

Subjects

Mitochondrial Diseases, Muscular Diseases, Acyl-CoA Dehydrogenase, Long-Chain, Congenital Bone Marrow Failure Syndromes, Humans, Lipid Metabolism, Inborn Errors

Abstract

Very long-chain acyl-CoA dehydrogenase (VLCAD) is an inner mitochondrial membrane enzyme that catalyzes the first and rate-limiting step of long-chain fatty acid oxidation. Point mutations in human VLCAD can produce an inborn error of metabolism called VLCAD deficiency that can lead to severe pathophysiologic consequences, including cardiomyopathy, hypoglycemia, and rhabdomyolysis. Discrete mutations in a structurally-uncharacterized C-terminal domain region of VLCAD cause enzymatic deficiency by an incompletely defined mechanism. Here, we conducted a structure-function study, incorporating X-ray crystallography, hydrogen-deuterium exchange mass spectrometry, computational modeling, and biochemical analyses, to characterize a specific membrane interaction defect of full-length, human VLCAD bearing the clinically-observed mutations, A450P or L462P. By disrupting a predicted α-helical hairpin, these mutations either partially or completely impair direct interaction with the membrane itself. Thus, our data support a structural basis for VLCAD deficiency in patients with discrete mutations in an α-helical membrane-binding motif, resulting in pathologic enzyme mislocalization.

Published

2021

8. The conformational stability of pro-apoptotic BAX is dictated by discrete residues of the protein core

Author

Thomas E. Wales, John R. Engen, Noah B. Bloch, Hannah R. Levy, Michelle S. Prew, and Loren D. Walensky

Subjects

Models, Molecular, Conformational change, Protein Conformation, Science, Cell, General Physics and Astronomy, Apoptosis, Mitochondrion, Article, General Biochemistry, Genetics and Molecular Biology, Cytosol, medicine, Animals, Humans, Amino Acids, Cells, Cultured, bcl-2-Associated X Protein, Mice, Knockout, Binding Sites, Multidisciplinary, Mass spectrometry, Chemistry, Protein core, General Chemistry, Oncogene proteins, Mitochondria, Cell biology, medicine.anatomical_structure, Mutation, Helix, Conformational stability, Protein Multimerization, Structural biology, Protein Binding, Signal Transduction

Abstract

BAX is a pro-apoptotic member of the BCL-2 family, which regulates the balance between cellular life and death. During homeostasis, BAX predominantly resides in the cytosol as a latent monomer but, in response to stress, transforms into an oligomeric protein that permeabilizes the mitochondria, leading to apoptosis. Because renegade BAX activation poses a grave risk to the cell, the architecture of BAX must ensure monomeric stability yet enable conformational change upon stress signaling. The specific structural features that afford both stability and dynamic flexibility remain ill-defined and represent a critical control point of BAX regulation. We identify a nexus of interactions involving four residues of the BAX core α5 helix that are individually essential to maintaining the structure and latency of monomeric BAX and are collectively required for dimeric assembly. The dual yet distinct roles of these residues reveals the intricacy of BAX conformational regulation and opportunities for therapeutic modulation., The pro-apoptotic BAX protein is a monomer under homeostatic conditions and, in response to stress, transforms into oligomers that induce apoptosis. Here, the authors characterize structural features of BAX that individually stabilize the monomer while collectively contributing to oligomerization.

Published

2021

9. Cell-based artificial APC resistant to lentiviral transduction for efficient generation of CAR-T cells from various cell sources

Author

Amanda A. Bouffard, Michelle S. Prew, Rebecca C. Larson, Felipe Bedoya, Leah C Marsh, J. Keith Joung, Mark B. Leick, Marcela V. Maus, Matthew J. Frigault, Michael Kann, Angela C. Boroughs, Sonika Vatsa, Bryan D. Choi, Stefanie R. Bailey, Irene Scarfò, Andrea Schmidts, Ambike A Srivastava, and Benjamin P. Kleinstiver

Subjects

0301 basic medicine, Cancer Research, T cell, Immunology, Antigen presentation, Cell, Antigen-Presenting Cells, Biology, Viral vector, Cell therapy, 03 medical and health sciences, Transduction (genetics), 0302 clinical medicine, Transduction, Genetic, immunotherapy, adoptive, medicine, Humans, Immunology and Allergy, B cell, RC254-282, Pharmacology, Immune Cell Therapies and Immune Cell Engineering, Lentivirus, receptors, chimeric antigen, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Chimeric antigen receptor, antigen presentation, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cancer research, Molecular Medicine

Abstract

BackgroundAdoptive cell therapy with chimeric antigen receptor T cells (CAR-T) has become a standard treatment for patients with certain aggressive B cell malignancies and holds promise to improve the care of patients suffering from numerous other cancers in the future. However, the high manufacturing cost of CAR-T cell therapies poses a major barrier to their broader clinical application. Among the key cost drivers of CAR-T production are single-use reagents for T cell activation and clinical-grade viral vector. The presence of variable amounts of contaminating monocytes in the starting material poses an additional challenge to CAR-T manufacturing, since they can impede T cell stimulation and transduction, resulting in manufacturing failure.MethodsWe created K562-based artificial antigen-presenting cells (aAPC) with genetically encoded T cell stimulation and costimulation that represent an inexhaustible source for T cell activation. We additionally disrupted endogenous expression of the low-density lipoprotein receptor (LDLR) on these aAPC (aAPC-ΔLDLR) using CRISPR-Cas9 gene editing nucleases to prevent inadvertent lentiviral transduction and avoid the sink effect on viral vector during transduction. Using various T cell sources, we produced CD19-directed CAR-T cells via aAPC-ΔLDLR-based activation and tested their in vitro and in vivo antitumor potency against B cell malignancies.ResultsWe found that lack of LDLR expression on our aAPC-ΔLDLR conferred resistance to lentiviral transduction during CAR-T production. Using aAPC-ΔLDLR, we achieved efficient expansion of CAR-T cells even from unpurified starting material like peripheral blood mononuclear cells or unmanipulated leukapheresis product, containing substantial proportions of monocytes. CD19-directed CAR-T cells that we produced via aAPC-ΔLDLR-based expansion demonstrated potent antitumor responses in preclinical models of acute lymphoblastic leukemia and B-cell lymphoma.ConclusionsOur aAPC-ΔLDLR represent an attractive approach for manufacturing of lentivirally transduced T cells that may be simpler and more cost efficient than currently available methods.

Published

2020

10. Precision Targeting of BFL-1/A1 and an ATM Co-dependency in Human Cancer

Author

Neekesh V. Dharia, Rachel M. Guerra, Kyle J. Korshavn, Loren D. Walensky, Michelle S. Prew, Edward P. Harvey, Gregory H. Bird, and Kimberly Stegmaier

Subjects

0301 basic medicine, Male, Antineoplastic Agents, Ataxia Telangiectasia Mutated Proteins, General Biochemistry, Genetics and Molecular Biology, Article, Minor Histocompatibility Antigens, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, medicine, Cytotoxic T cell, Humans, lcsh:QH301-705.5, Binding Sites, Kinase, business.industry, Bcl-2 family, Myeloid leukemia, Cancer, medicine.disease, Leukemia, Myeloid, Acute, 030104 developmental biology, HEK293 Cells, Drug development, lcsh:Biology (General), Proto-Oncogene Proteins c-bcl-2, Apoptosis, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Female, business, Protein Binding

Abstract

Summary: Cancer cells overexpress a diversity of anti-apoptotic BCL-2 family proteins, such as BCL-2, MCL-1, and BFL-1/A1, to enforce cellular immortality. Thus, intensive drug development efforts have focused on targeting this class of oncogenic proteins to overcome treatment resistance. Whereas a selective BCL-2 inhibitor has been FDA approved and several small molecule inhibitors of MCL-1 have recently entered phase I clinical testing, BFL-1/A1 remains undrugged. Here, we developed a series of stapled peptide design principles to engineer a functionally selective and cell-permeable BFL-1/A1 inhibitor that is specifically cytotoxic to BFL-1/A1-dependent human cancer cells. Because cancers harbor a diversity of resistance mechanisms and typically require multi-agent treatment, we further investigated BFL-1/A1 co-dependencies by mining a genome-scale CRISPR-Cas9 screen. We identified ataxia-telangiectasia-mutated (ATM) kinase as a BFL-1/A1 co-dependency in acute myeloid leukemia (AML), which informed the validation of BFL-1/A1 and ATM inhibitor co-treatment as a synergistic approach to subverting apoptotic resistance in cancer. : Guerra et al. constructed an exquisitely selective BFL-1 inhibitor capable of covalent BFL-1 targeting and cellular penetrance without membrane disruption. Mining a genetic dependency database revealed a spectrum of BFL-1 dependency in cancer and an ATM co-dependency in AML, prompting the combination of BFL-1 and ATM inhibitors to achieve synergistic cytotoxicity. Keywords: BFL-1, A1, BCL-2 family, apoptosis, stapled peptide, covalent inhibitor, dependency, ATM, AML, cancer

Published

2018

11. Allele-Specific CRISPR-Cas9 Genome Editing of the Single-Base P23H Mutation for Rhodopsin-Associated Dominant Retinitis Pigmentosa

Author

Qin Liu, Michelle S. Prew, J. Keith Joung, Scott H. Greenwald, Benjamin P. Kleinstiver, Mihoko Leon, Pingjuan Li, Eric A. Pierce, and Daniel Navarro-Gomez

Subjects

0301 basic medicine, Genetics, Mutation, Mutant, Biology, medicine.disease_cause, medicine.disease, 03 medical and health sciences, Protospacer adjacent motif, 030104 developmental biology, 0302 clinical medicine, Genome editing, Retinitis pigmentosa, medicine, Gene silencing, CRISPR, sense organs, Allele, 030217 neurology & neurosurgery, Research Articles, Biotechnology

Abstract

Treatment strategies for dominantly inherited disorders typically involve silencing or ablating the pathogenic allele. CRISPR-Cas nucleases have shown promise in allele-specific knockout approaches when the dominant allele creates unique protospacer adjacent motifs that can lead to allele-restricted targeting. Here, we present a spacer-mediated allele-specific knockout approach that utilizes both SpCas9 variants and truncated single-guide RNAs to achieve efficient discrimination of a single-nucleotide mutation in rhodopsin (Rho)-P23H mice, a model of dominant retinitis pigmentosa. We found that approximately 45% of the mutant P23H allele was edited at the DNA level and that the relative RNA expression of wild-type Rho was about 2.8 times more than that of mutant Rho in treated retinas. Furthermore, the progression of photoreceptor cell degeneration in outer nuclear layer was significantly delayed in treated regions of the Rho-P23H retinas at 5 weeks of age. Our proof-of-concept study therefore outlines a general strategy that could potentially be expanded to examine the therapeutic benefit of allele-specific gene editing approach to treat human P23H patients. Our study also extends allele-specific editing strategies beyond discrimination within the protospacer adjacent motif sites, with potentially broad applicability to other dominant diseases.

Published

2018

12. High-fidelity CRISPR–Cas9 nucleases with no detectable genome-wide off-target effects

Author

Shengdar Q. Tsai, J. Keith Joung, Vikram Pattanayak, Michelle S. Prew, Nhu T. Nguyen, Zongli Zheng, and Benjamin P. Kleinstiver

Subjects

0301 basic medicine, Streptococcus pyogenes, CRISPR-Associated Proteins, Biology, medicine.disease_cause, DNA-binding protein, Genome, Substrate Specificity, 03 medical and health sciences, Genome editing, medicine, Humans, CRISPR, Clustered Regularly Interspaced Short Palindromic Repeats, Genetics, Mutation, Multidisciplinary, Base Sequence, Genome, Human, Cas9, Reproducibility of Results, DNA, Sequence Analysis, DNA, Endonucleases, DNA-Binding Proteins, Protospacer adjacent motif, 030104 developmental biology, RNA, Human genome, CRISPR-Cas Systems, Genetic Engineering, Protein Binding

Abstract

CRISPR-Cas9 nucleases are widely used for genome editing but can induce unwanted off-target mutations. Existing strategies for reducing genome-wide off-target effects of the widely used Streptococcus pyogenes Cas9 (SpCas9) are imperfect, possessing only partial or unproven efficacies and other limitations that constrain their use. Here we describe SpCas9-HF1, a high-fidelity variant harbouring alterations designed to reduce non-specific DNA contacts. SpCas9-HF1 retains on-target activities comparable to wild-type SpCas9 with >85% of single-guide RNAs (sgRNAs) tested in human cells. Notably, with sgRNAs targeted to standard non-repetitive sequences, SpCas9-HF1 rendered all or nearly all off-target events undetectable by genome-wide break capture and targeted sequencing methods. Even for atypical, repetitive target sites, the vast majority of off-target mutations induced by wild-type SpCas9 were not detected with SpCas9-HF1. With its exceptional precision, SpCas9-HF1 provides an alternative to wild-type SpCas9 for research and therapeutic applications. More broadly, our results suggest a general strategy for optimizing genome-wide specificities of other CRISPR-RNA-guided nucleases.

Published

2016

13. Broadening the targeting range of Staphylococcus aureus CRISPR-Cas9 by modifying PAM recognition

Author

Shengdar Q. Tsai, Benjamin P. Kleinstiver, Zongli Zheng, J. Keith Joung, Michelle S. Prew, Ved V Topkar, and Nhu T. Nguyen

Subjects

Genetics, Cas9, Biomedical Engineering, Bioengineering, Biology, medicine.disease_cause, Applied Microbiology and Biotechnology, DNA sequencing, Protospacer adjacent motif, Genome editing, Molecular evolution, Staphylococcus aureus, parasitic diseases, medicine, Molecular Medicine, CRISPR, Guide RNA, Biotechnology

Abstract

CRISPR-Cas9 nucleases target specific DNA sequences using a guide RNA but also require recognition of a protospacer adjacent motif (PAM) by the Cas9 protein. Although longer PAMs can potentially improve the specificity of genome editing, they limit the range of sequences that Cas9 orthologs can target. One potential strategy to relieve this restriction is to relax the PAM recognition specificity of Cas9. Here we used molecular evolution to modify the NNGRRT PAM of Staphylococcus aureus Cas9 (SaCas9). One variant we identified, referred to as KKH SaCas9, showed robust genome editing activities at endogenous human target sites with NNNRRT PAMs, thereby increasing SaCas9 targeting range by two- to fourfold. Using GUIDE-seq, we show that wild-type and KKH SaCas9 induce comparable numbers of off-target effects in human cells. Our strategy for evolving PAM specificity does not require structural information and therefore should be applicable to a wide range of Cas9 orthologs.

Published

2015

14. Engineered CRISPR-Cas9 nucleases with altered PAM specificities

Author

Benjamin P. Kleinstiver, Michelle S. Prew, Shengdar Q. Tsai, Ved V. Topkar, Nhu T. Nguyen, Zongli Zheng, Andrew P. W. Gonzales, Zhuyun Li, Randall T. Peterson, Jing-Ruey Joanna Yeh, Martin J. Aryee, and J. Keith Joung

Subjects

Staphylococcus aureus, Streptococcus pyogenes, CRISPR-Associated Proteins, Computational biology, Biology, Protein Engineering, medicine.disease_cause, Genome, Article, Cell Line, Substrate Specificity, Molecular engineering, stomatognathic system, parasitic diseases, medicine, Animals, Humans, Streptococcus thermophilus, CRISPR, Clustered Regularly Interspaced Short Palindromic Repeats, Nucleotide Motifs, Zebrafish, Epigenomics, Genetics, Mutation, Multidisciplinary, Protein engineering, Protospacer adjacent motif, Genomic engineering, Amino Acid Substitution, CRISPR-Cas Systems, Directed Molecular Evolution

Abstract

Although CRISPR-Cas9 nucleases are widely used for genome editing1, 2, the range of sequences that Cas9 can recognize is constrained by the need for a specific protospacer adjacent motif (PAM)3–6. As a result, it can often be difficult to target double-stranded breaks (DSBs) with the precision that is necessary for various genome editing applications. The ability to engineer Cas9 derivatives with purposefully altered PAM specificities would address this limitation. Here we show that the commonly used Streptococcus pyogenes Cas9 (SpCas9) can be modified to recognize alternative PAM sequences using structural information, bacterial selection-based directed evolution, and combinatorial design. These altered PAM specificity variants enable robust editing of endogenous gene sites in zebrafish and human cells not currently targetable by wild-type SpCas9, and their genome-wide specificities are comparable to wild-type SpCas9 as judged by GUIDE-Seq analysis7. In addition, we identified and characterized another SpCas9 variant that exhibits improved specificity in human cells, possessing better discrimination against off-target sites with non-canonical NAG and NGA PAMs and/or mismatched spacers. We also found that two smaller-size Cas9 orthologues, Streptococcus thermophilus Cas9 (St1Cas9) and Staphylococcus aureus Cas9 (SaCas9), function efficiently in the bacterial selection systems and in human cells, suggesting that our engineering strategies could be extended to Cas9s from other species. Our findings provide broadly useful SpCas9 variants and, more importantly, establish the feasibility of engineering a wide range of Cas9s with altered and improved PAM specificities.

Published

2015

15. Allele-specific CRISPR/Cas9 genome editing of the single-base P23H mutation for rhodopsin associated dominant retinitis pigmentosa

Author

J. Keith Joung, Qin Liu, Benjamin P. Kleinstiver, Scott H. Greenwald, Mihoko Leon, Michelle S. Prew, Pingjuan Li, Eric A. Pierce, and Daniel Navarro-Gomez

Subjects

Genetics, Mutation, Mutant, Biology, medicine.disease_cause, medicine.disease, Genome editing, Retinitis pigmentosa, medicine, CRISPR, Gene silencing, Guide RNA, sense organs, Allele

Abstract

Treatment strategies for dominantly inherited disorders typically involve silencing or ablating the pathogenic allele. CRISPR/Cas nucleases have shown promise in allele-specific knockout approaches when the dominant allele creates unique protospacer adjacent motifs (PAMs) that can lead to allele restricted targeting. Here, we present a spacer-mediated allele-specific knockout approach that utilizes both SpCas9 variants and truncated single guide RNAs (trusgRNAs) to achieve efficient discrimination of a single-nucleotide mutation in rhodopsin (Rho)-P23H mice, a model of dominant retinitis pigmentosa (RP). We found that approximately 45% of the mutant P23H allele was edited at DNA level, and that the relative RNA expression of wild-type Rho was about 2.8 times more than that of mutant Rho in treated retinas. Furthermore, the progression of photoreceptor cell degeneration in outer nuclear layer was significantly delayed in treated regions of the Rho-P23H retinas at five weeks of age. Our proof-of-concept study therefore outlines a general strategy that could potentially be expanded to examine the therapeutic benefit of allele-specific gene editing approach to treat human P23H patient. Our study also extends allele-specific editing strategies beyond discrimination within the PAM sites, with potentially broad applicability to other dominant diseases.

Published

2017

16. Genome-wide specificity profiles of CRISPR-Cas Cpf1 nucleases in human cells

Author

J. Keith Joung, Michelle S. Prew, Nhu T. Nguyen, Moira M. Welch, Jose Malagon Lopez, Martin J. Aryee, Zachary R. McCaw, Benjamin P. Kleinstiver, and Shengdar Q. Tsai

Subjects

Trans-activating crRNA, 0303 health sciences, Cas9, RNA, Computational biology, Biology, medicine.disease_cause, Genome, Deep sequencing, 03 medical and health sciences, 0302 clinical medicine, Genome editing, Streptococcus pyogenes, medicine, CRISPR, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

CRISPR-Cas Cpf1 nucleases have recently been described as an alternative genome-editing platform, yet their activities and genome-wide specificities remain largely undefined. Here we show that two Cpf1 nucleases function robustly in human cells with on-target efficiencies comparable to those of the widely used Streptococcus pyogenes Cas9 (SpCas9). We also demonstrate that four to six bases at the 39 end of the short CRISPR RNA (crRNA) used to program Cpf1 are insensitive to single base mismatches but that many of the other bases within the crRNA targeting region are highly sensitive to single or double substitutions. Consistent with these results, GUIDE-seq and targeted deep sequencing analyses of two Cpf1 nucleases revealed no detectable off-target cleavage for over half of 20 different crRNAs we examined. Our results suggest that the two Cpf1 nucleases we characterized generally possess high specificities in human cells, a finding that should encourage broader use of these genome editing enzymes.

Published

2016

17. 731. High-Fidelity CRISPR-Cas9 Nucleases with No Detectable Genome-Wide Off-Target Effects

Author

Vikram Pattanayak, Michelle S. Prew, J. Keith Joung, Benjamin P. Kleinstiver, Shengdar Q. Tsai, and Nhu T. Nguyen

Subjects

0301 basic medicine, Pharmacology, Genetics, Cas9, Biology, medicine.disease_cause, Genome, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, chemistry, Genome editing, Drug Discovery, Streptococcus pyogenes, medicine, Molecular Medicine, CRISPR, Molecular Biology, Peptide sequence, DNA

Abstract

CRISPR-Cas9 nucleases are widely used for genome editing but can induce unwanted off-target mutations at genomic locations that resemble the intended target. These so-called off-target effects can confound research applications and are important considerations for potential therapeutic use. Existing strategies for reducing genome-wide off-targets of the broadly used Streptococcus pyogenes Cas9 (SpCas9) have thus far proven to be imperfect by possessing only partial efficacy and/or other limitations that constrain their use. Here we describe a high-fidelity variant of SpCas9, called SpCas9-HF1, that contains alterations in the amino acid sequence designed to reduce non-specific contacts to the target strand DNA. SpCas9-HF1 retains on-target activities comparable to wild-type SpCas9 with >85% of the 37 single-guide RNAs (sgRNAs) tested in human cells. Strikingly, with eight different sgRNAs targeted to standard non-repetitive sequences in human cells, SpCas9-HF1 rendered all or nearly all off-target events imperceptible by genome-wide break capture and targeted sequencing methods. Even for atypical, repetitive target sites, the vast majority of off-targets induced by SpCas9-HF1 were not detected. With its exceptional precision, SpCas9-HF1 provides an important and easily employed alternative to wild-type SpCas9 that can eliminate off-target effects when using CRISPR-Cas9 for research and therapeutic applications. Our findings also suggest a general strategy for improving or optimizing the genome-wide specificities of other Cas9 orthologues and engineered variants.

Published

2016

18. 58. Engineered Cas9 Variants with Novel PAM Specificities Expand the Targeting Range of CRISPR/Cas Nucleases

Author

Shengdar Q. Tsai, Michelle S. Prew, Ved V Topkar, Benjamin P. Kleinstiver, and Jae Keith Joung

Subjects

Pharmacology, Genetics, Nuclease, biology, Cas9, Heterologous, medicine.disease_cause, Genome, Protospacer adjacent motif, Drug Discovery, Streptococcus pyogenes, biology.protein, medicine, Molecular Medicine, CRISPR, Molecular Biology, Gene

Abstract

Specificity and targeting range are important considerations when selecting an engineered nuclease platform for functional studies or therapeutic applications. The use of CRISPR/Cas9 to edit virtually any genome has enabled researchers to rapidly knock out genes or to introduce precise genomic changes. A number of studies have explored and improved the specificity of the CRISPR/Cas9 platform but the targeting range remains limited to certain sequences. The most widely used Cas9 from Streptococcus pyogenes (SpCas9) recognizes a protospacer adjacent motif (PAM) of the form NGG, a constraint that restricts the range of sequences that can be edited. Combined with the 5’ nucleotide requirement for guide-RNA expression from a polIII promoter, this restriction can be limiting particularly when one is using CRISPR/Cas9 nucleases to introduce precise mutations by homology-directed repair (HDR), which requires that double-strand breaks be introduced very closely to the site of sequence alteration.To address this challenge, we developed a heterologous genetic system that enabled us to rapidly screen libraries of Cas9 clones and identify variants with distinct cleavage specificities. Using this technology, we identified and optimized two different Cas9 variants that recognize novel PAMs. We demonstrate that these variants enable targeting of sites with non-canonical PAM sequences that were previously inaccessible with wild-type SpCas9, more than doubling the total range of sequences that can be edited by HDR and by error-prone non-homologous end-joining (NHEJ). We demonstrate that these variants can robustly modify endogenous genes in human cells and that they are compatible with previously described specificity improvements to SpCas9 such as truncated gRNAs.Furthermore, we also show Cas9 nucleases from other bacterial species such as Staphylococcus aureus and Streptococcus thermophilus can also be assessed for activity in our heterologous genetic system, suggesting that these alternative Cas9s might also be modified in their PAM specificities using the same approach we undertook with SpCas9. These orthogonal Cas9 nucleases offer the advantage of being substantially smaller in size than SpCas9, an important factor when considering packaging limits for viral delivery of CRISPR/Cas9 components. Taken together, our results more than double the targeting range of CRISPR/Cas9 nuclease platform and improve the prospects for translation of these reagents to clinical settings.

Published

2015

19. Cell-based artificial APC resistant to lentiviral transduction for efficient generation of CAR-T cells from various cell sources

Author

Irene Scarfò, Marcela V Maus, Andrea Schmidts, Leah C Marsh, Ambike A Srivastava, Amanda A Bouffard, Angela C Boroughs, Rebecca C Larson, Felipe Bedoya, Bryan D Choi, Matthew J Frigault, Stefanie R Bailey, Mark B Leick, Sonika Vatsa, Michael C Kann, Michelle S Prew, Benjamin P Kleinstiver, and J Keith Joung

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background Adoptive cell therapy with chimeric antigen receptor T cells (CAR-T) has become a standard treatment for patients with certain aggressive B cell malignancies and holds promise to improve the care of patients suffering from numerous other cancers in the future. However, the high manufacturing cost of CAR-T cell therapies poses a major barrier to their broader clinical application. Among the key cost drivers of CAR-T production are single-use reagents for T cell activation and clinical-grade viral vector. The presence of variable amounts of contaminating monocytes in the starting material poses an additional challenge to CAR-T manufacturing, since they can impede T cell stimulation and transduction, resulting in manufacturing failure.Methods We created K562-based artificial antigen-presenting cells (aAPC) with genetically encoded T cell stimulation and costimulation that represent an inexhaustible source for T cell activation. We additionally disrupted endogenous expression of the low-density lipoprotein receptor (LDLR) on these aAPC (aAPC-ΔLDLR) using CRISPR-Cas9 gene editing nucleases to prevent inadvertent lentiviral transduction and avoid the sink effect on viral vector during transduction. Using various T cell sources, we produced CD19-directed CAR-T cells via aAPC-ΔLDLR-based activation and tested their in vitro and in vivo antitumor potency against B cell malignancies.Results We found that lack of LDLR expression on our aAPC-ΔLDLR conferred resistance to lentiviral transduction during CAR-T production. Using aAPC-ΔLDLR, we achieved efficient expansion of CAR-T cells even from unpurified starting material like peripheral blood mononuclear cells or unmanipulated leukapheresis product, containing substantial proportions of monocytes. CD19-directed CAR-T cells that we produced via aAPC-ΔLDLR-based expansion demonstrated potent antitumor responses in preclinical models of acute lymphoblastic leukemia and B-cell lymphoma.Conclusions Our aAPC-ΔLDLR represent an attractive approach for manufacturing of lentivirally transduced T cells that may be simpler and more cost efficient than currently available methods.

Published

2020