Your search keyword '"CRISPR screen"' showing total 9 results

1. CRISPR Screen Reveals PACT as a Pro-Viral Factor for Dengue Viral Replication.

Author

Shivaprasad, Shwetha, Qiao, Wenjie, Weng, Kuo-Feng, Umashankar, Pavithra, Carette, Jan E., and Sarnow, Peter

Subjects

*DENGUE viruses, *VIRAL replication, *MEDICAL screening, *CRISPRS, *GENE expression, *DENGUE, *CUCUMBER mosaic virus, *FENITROTHION

Abstract

The dengue virus is a single-stranded, positive-sense RNA virus that infects ~400 million people worldwide. Currently, there are no approved antivirals available. CRISPR-based screening methods have greatly accelerated the discovery of host factors that are essential for DENV infection and that can be targeted in host-directed antiviral interventions. In the present study, we performed a focused CRISPR (Clustered Regularly Interspaced Palindromic Repeats) library screen to discover the key host factors that are essential for DENV infection in human Huh7 cells and identified the Protein Activator of Interferon-Induced Protein Kinase (PACT) as a novel pro-viral factor for DENV. PACT is a double-stranded RNA-binding protein generally known to activate antiviral responses in virus-infected cells and block viral replication. However, in our studies, we observed that PACT plays a pro-viral role in DENV infection and specifically promotes viral RNA replication. Knockout of PACT resulted in a significant decrease in DENV RNA and protein abundances in infected cells, which was rescued upon ectopic expression of full-length PACT. An analysis of global gene expression changes indicated that several ER-associated pro-viral genes such as ERN1, DDIT3, HERPUD1, and EIF2AK3 are not upregulated in DENV-infected PACT knockout cells as compared to infected wildtype cells. Thus, our study demonstrates a novel role for PACT in promoting DENV replication, possibly through modulating the expression of ER-associated pro-viral genes. [ABSTRACT FROM AUTHOR]

Published

2024

2. CRISPR Screen Identifies the RNA-Binding Protein Eef1a1 as a Key Regulator of Myogenesis.

Author

Liu, Weiwei, Wang, Wei, Wang, Zishuai, Fan, Xinhao, Li, Wangchang, Huang, Yuxin, Yang, Xiaogan, and Tang, Zhonglin

Subjects

*RNA-binding proteins, *MYOGENESIS, *CRISPRS, *GENETIC regulation, *NON-coding RNA

Abstract

Skeletal muscle myogenesis hinges on gene regulation, meticulously orchestrated by molecular mechanisms. While the roles of transcription factors and non-coding RNAs in myogenesis are widely known, the contribution of RNA-binding proteins (RBPs) has remained unclear until now. Therefore, to investigate the functions of post-transcriptional regulators in myogenesis and uncover new functional RBPs regulating myogenesis, we employed CRISPR high-throughput RBP-KO (RBP-wide knockout) library screening. Through this approach, we successfully identified Eef1a1 as a novel regulatory factor in myogenesis. Using CRISPR knockout (CRISPRko) and CRISPR interference (CRISPRi) technologies, we successfully established cellular models for both CRISPRko and CRISPRi. Our findings demonstrated that Eef1a1 plays a crucial role in promoting proliferation in C2C12 myoblasts. Through siRNA inhibition and overexpression methods, we further elucidated the involvement of Eef1a1 in promoting proliferation and suppressing differentiation processes. RIP (RNA immunoprecipitation), miRNA pull-down, and Dual-luciferase reporter assays confirmed that miR-133a-3p targets Eef1a1. Co-transfection experiments indicated that miR-133a-3p can rescue the effect of Eef1a1 on C2C12 myoblasts. In summary, our study utilized CRISPR library high-throughput screening to unveil a novel RBP, Eef1a1, involved in regulating myogenesis. Eef1a1 promotes the proliferation of myoblasts while inhibiting the differentiation process. Additionally, it acts as an antagonist to miR-133a-3p, thus modulating the process of myogenesis. [ABSTRACT FROM AUTHOR]

Published

2024

3. The Current Situation and Development Prospect of Whole-Genome Screening.

Author

Yang, Caiting, Lei, Yu, Ren, Tinglin, and Yao, Mingze

Subjects

*GENETIC testing, *GENETIC techniques, *GENOME editing, *RNA interference, *SMALL interfering RNA

Abstract

High-throughput genetic screening is useful for discovering critical genes or gene sequences that trigger specific cell functions and/or phenotypes. Loss-of-function genetic screening is mainly achieved through RNA interference (RNAi), CRISPR knock-out (CRISPRko), and CRISPR interference (CRISPRi) technologies. Gain-of-function genetic screening mainly depends on the overexpression of a cDNA library and CRISPR activation (CRISPRa). Base editing can perform both gain- and loss-of-function genetic screening. This review discusses genetic screening techniques based on Cas9 nuclease, including Cas9-mediated genome knock-out and dCas9-based gene activation and interference. We compare these methods with previous genetic screening techniques based on RNAi and cDNA library overexpression and propose future prospects and applications for CRISPR screening. [ABSTRACT FROM AUTHOR]

Published

2024

4. CRISPR-Cas9 Genetic Analysis of Virus-Host Interactions.

Author

Gebre, Makda, Nomburg, Jason L., and Gewurz, Benjamin E.

Subjects

*CRISPRS, *GENOMES, *VIRUSES, *PATHOGENIC microorganisms, *COMBINATORIAL dynamics

Abstract

Clustered regularly interspaced short palindromic repeats (CRISPR) has greatly expanded the ability to genetically probe virus-host interactions. CRISPR systems enable focused or systematic, genomewide studies of nearly all aspects of a virus lifecycle. Combined with its relative ease of use and high reproducibility, CRISPR is becoming an essential tool in studies of the host factors important for viral pathogenesis. Here, we review the use of CRISPR-Cas9 for the loss-of-function analysis of host dependency factors. We focus on the use of CRISPR-pooled screens for the systematic identification of host dependency factors, particularly in Epstein-Barr virus-transformed B cells. We also discuss the use of CRISPR interference (CRISPRi) and gain-of-function CRISPR activation (CRISPRa) approaches to probe virus-host interactions. Finally, we comment on the future directions enabled by combinatorial CRISPR screens. [ABSTRACT FROM AUTHOR]

Published

2018

5. CRISPR Screens in Synthetic Lethality and Combinatorial Therapies for Cancer

Author

Castells-Roca, L, Tejero, E, Rodriguez-Santiago, B, and Surralles, J

Subjects

combinatorial therapy, cancer therapeutic resistance, synthetic lethality, CRISPR screen

Abstract

Simple Summary The synthetic lethality (SL) clinical success of PARP inhibitors in homologous recombinant deficient tumors has established a new concept for cancer treatment. For decades, efforts have centered on identifying genetic interactions for determining essential tumoral genes, and more recently, SL interactions to determine combinational treatments against persistent cancer reappearance. Currently, the feasibility of CRISPR screen methodology has emerged as the state of the art for uncovering new SL or viable interactors in the biology and treatment of cancers. We present the up-to-date research of numerous laboratories that take advantage of the genome-wide forward genetic CRISPR screen tools and protocols to identify cancer biomarkers, genetic interactions and novel therapies. Indeed, investigations are nowadays focused on defining innovative combinatorial treatments based on SL interactions. By coupling different drugs, concentration treatments can be lowered and therefore toxicity reduced. CRISPR screen technologies have deeply impacted cancer research to promote a robust advance in combined therapies. Cancer is a complex disease resulting from the accumulation of genetic dysfunctions. Tumor heterogeneity causes the molecular variety that divergently controls responses to chemotherapy, leading to the recurrent problem of cancer reappearance. For many decades, efforts have focused on identifying essential tumoral genes and cancer driver mutations. More recently, prompted by the clinical success of the synthetic lethality (SL)-based therapy of the PARP inhibitors in homologous recombinant deficient tumors, scientists have centered their novel research on SL interactions (SLI). The state of the art to find new genetic interactions are currently large-scale forward genetic CRISPR screens. CRISPR technology has rapidly evolved to be a common tool in the vast majority of laboratories, as tools to implement CRISPR screen protocols are available to all researchers. Taking advantage of SLI, combinatorial therapies have become the ultimate model to treat cancer with lower toxicity, and therefore better efficiency. This review explores the CRISPR screen methodology, integrates the up-to-date published findings on CRISPR screens in the cancer field and proposes future directions to uncover cancer regulation and individual responses to chemotherapy.

Published

2021

6. A Genome-Wide CRISPR Activation Screen Identifies Genes Involved in Protection from Zika Virus Infection

Author

Markus Fricke, Jae U. Jung, Nabila Jabrane-Ferrat, Qian Chen, Ella H. Sklan, Manja Marz, Kevin Lamkiewicz, and Anna Dukhovny

Subjects

Programmed cell death, biology, Transmission (medicine), lcsh:A, biology.organism_classification, Genome, Virology, Zika virus, CRISPR screen, interferon-stimulated genes, Interferon, medicine, CRISPR, lcsh:General Works, Gene, Pathogen, medicine.drug

Abstract

Zika virus (ZIKV) is an arthropod-borne emerging pathogen causing febrile illness. ZIKV is associated with the Guillain–Barré syndrome and other neurological complications. The vertical transmission of ZIKV can cause fetus demise, stillbirths or severe congenital abnormalities and neurological complications. There is still no vaccine or specific treatment for ZIKV infection. To identify the host factors that can rescue cells from ZIKV infection, we used a genome-scale CRISPR activation screen. Our highly ranking hits included a short list of interferon-stimulated genes (ISGs) previously reported to have antiviral activity. Validation of the screen results highlighted interferon lambda 2 (IFN-lamda2) and interferon alpha-inducible protein 6 (IFI6) as genes providing high levels of protection from ZIKV infection. The activation of these genes had an effect at an early stage in the viral infection. In addition, infected cells expressing single guide RNAs (sgRNAs) for both of these genes displayed lower levels of cell death than did the controls. Furthermore, the identified genes were significantly induced in ZIKV-infected placenta explants. These results highlighted a set of ISGs directly relevant for rescuing cells from ZIKV infection or its associated cell death, thus substantiating CRISPR activation screens as a valid tool for identifying host factors impeding pathogen infection.

Published

2020

7. CRISPR Screen Contributes to Novel Target Discovery in Prostate Cancer.

Author

Tsujino, Takuya, Komura, Kazumasa, Inamoto, Teruo, and Azuma, Haruhito

Subjects

*PROSTATE cancer, *CRISPRS, *DRUG resistance in cancer cells, *DRUG target, *MEDICAL personnel, *GENOME editing

Abstract

Prostate cancer (PCa) is one of the common malignancies in male adults. Recent advances in omics technology, especially in next-generation sequencing, have increased the opportunity to identify genes that correlate with cancer diseases, including PCa. In addition, a genetic screen based on CRISPR/Cas9 technology has elucidated the mechanisms of cancer progression and drug resistance, which in turn has enabled the discovery of new targets as potential genes for new therapeutic targets. In the era of precision medicine, such knowledge is crucial for clinicians in their decision-making regarding patient treatment. In this review, we focus on how CRISPR screen for PCa performed to date has contributed to the identification of biologically critical and clinically relevant target genes. [ABSTRACT FROM AUTHOR]

Published

2021

8. CRISPR–Cas9 Genetic Analysis of Virus–Host Interactions

Author

Makda S. Gebre, Benjamin E. Gewurz, and Jason Nomburg

Subjects

0301 basic medicine, Herpesvirus 4, Human, Viral pathogenesis, lcsh:QR1-502, Computational biology, Review, Virus Physiological Phenomena, Biology, combinatorial CRISPR, Genetic analysis, lcsh:Microbiology, Genome engineering, CRISPR screen, Epstein–Barr virus, 03 medical and health sciences, Genome editing, host dependency factor, Virology, CRISPR, Humans, Viral Regulatory and Accessory Proteins, Genetic Testing, Cas9, CRISPR interference, Gene Editing, B-Lymphocytes, CRISPR activation, 030104 developmental biology, Infectious Diseases, Gene Targeting, Host-Pathogen Interactions, CRISPR-Cas Systems, genome engineering

Abstract

Clustered regularly interspaced short palindromic repeats (CRISPR) has greatly expanded the ability to genetically probe virus-host interactions. CRISPR systems enable focused or systematic, genomewide studies of nearly all aspects of a virus lifecycle. Combined with its relative ease of use and high reproducibility, CRISPR is becoming an essential tool in studies of the host factors important for viral pathogenesis. Here, we review the use of CRISPR-Cas9 for the loss-of-function analysis of host dependency factors. We focus on the use of CRISPR-pooled screens for the systematic identification of host dependency factors, particularly in Epstein-Barr virus-transformed B cells. We also discuss the use of CRISPR interference (CRISPRi) and gain-of-function CRISPR activation (CRISPRa) approaches to probe virus-host interactions. Finally, we comment on the future directions enabled by combinatorial CRISPR screens.

Published

2018

9. CRISPR Screens in Synthetic Lethality and Combinatorial Therapies for Cancer.

Author

Castells-Roca L, Tejero E, Rodríguez-Santiago B, and Surrallés J

Abstract

Cancer is a complex disease resulting from the accumulation of genetic dysfunctions. Tumor heterogeneity causes the molecular variety that divergently controls responses to chemotherapy, leading to the recurrent problem of cancer reappearance. For many decades, efforts have focused on identifying essential tumoral genes and cancer driver mutations. More recently, prompted by the clinical success of the synthetic lethality (SL)-based therapy of the PARP inhibitors in homologous recombinant deficient tumors, scientists have centered their novel research on SL interactions (SLI). The state of the art to find new genetic interactions are currently large-scale forward genetic CRISPR screens. CRISPR technology has rapidly evolved to be a common tool in the vast majority of laboratories, as tools to implement CRISPR screen protocols are available to all researchers. Taking advantage of SLI, combinatorial therapies have become the ultimate model to treat cancer with lower toxicity, and therefore better efficiency. This review explores the CRISPR screen methodology, integrates the up-to-date published findings on CRISPR screens in the cancer field and proposes future directions to uncover cancer regulation and individual responses to chemotherapy.

Published

2021