Mark Manzano
Asssistant Professor
University of Arkansas for Medical Sciences
faculty
Microbiology & Immunology, College of Medicine
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Biography and Research Information
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Mark Manzano's laboratory investigates host-pathogen interactions and biological processes, employing functional genomics, particularly CRISPR screens, to link genotype to phenotype on a genome-wide scale. His research focuses on primary effusion lymphoma (PEL), an aggressive B cell cancer associated with the Kaposi’s sarcoma-associated herpesvirus (KSHV/HHV8). PEL cells depend on virally encoded genes that alter host gene expression to promote tumor cell proliferation and survival. Previous genome-wide CRISPR/Cas9 screens conducted by Manzano's lab identified 210 host genes essential for PEL cell proliferation and survival.
Further research aims to elucidate the functions of these identified host genes in B cell lymphoma. Utilizing CRISPR/Cas9, CRISPRi, and CRISPRa-based synthetic lethality and rescue screens, the lab seeks to uncover functional genetic interactions. This unbiased approach is expected to reveal novel therapeutic targets and mechanisms of KSHV latency and oncogenesis. Manzano's work has been supported by four federal grants totaling over $1.3 million, including funding from the NIH/National Institute of Allergy and Infectious Diseases, NIH/National Cancer Institute, and NIH/National Institute of Dental and Craniofacial Research. He has published 32 works, accumulating 1,280 citations, and maintains an h-index of 15.
Metrics
- h-index: 15
- Publications: 32
- Citations: 1,280
Selected Publications
- Cytotoxicity of activator expression in CRISPR-based transcriptional activation systems (2025) DOI
- Intrinsic p53 activation restricts gammaherpesvirus driven germinal center B cell expansion during latency establishment (2025) DOI
- The Mitochondrial Ubiquitin Ligase MARCHF5 Cooperates with MCL1 to Inhibit Apoptosis in KSHV-Transformed Primary Effusion Lymphoma Cell Lines (2024) DOI
- Cytotoxicity of Activator Expression in CRISPR-based Transcriptional Activation Systems (2024) DOI
- Molecular Mechanisms of KSHV Latency Establishment and Maintenance (2024) DOI
- Suppression of TRIP13 Induces Metabolic Changes and Potentiates Ferroptosis in Multiple Myeloma (2023) DOI
- Intrinsic p53 Activation Restricts Gammaherpesvirus-Driven Germinal Center B Cell Expansion during Latency Establishment (2023) DOI
- CRISPR screens identify novel regulators of cFLIP dependency and ligand-independent, TRAIL-R1-mediated cell death (2023) DOI
- Expression Ratios of the Antiapoptotic BCL2 Family Members Dictate the Selective Addiction of Kaposi’s Sarcoma-Associated Herpesvirus-Transformed Primary Effusion Lymphoma Cell Lines to MCL1 (2022) DOI
- Expression Ratios of the Anti-Apoptotic BCL2 Family Members Dictate the Selective Addiction of KSHV-Transformed Primary Effusion Lymphoma Cell Lines to MCL1 (2022) DOI
- CRISPR Screens Identify Novel Regulators of cFLIP Dependency and Ligand-Independent, TRAIL-R1-Mediated Cell Death (2022) DOI
Federal Grants 4 $1,340,840 total
Lytic viral genes in the pathogenesis of oncogenic gammaherpesviruses
Role of a latent OriLyt RNA in KSHV latency in primary effusion lymphoma
Oncogenic Roles and Therapeutic Potential of MCL1 Addiction in Primary Effusion Lymphoma
Grants & Funding
- Epigenetic Regulation of KSHV Latency NIH/Nat. Inst. of Dental & Craniofacial Research Principal Investigator
- Epigenetic Regulation of KSHV Latency NIH/Nat. Inst. of Dental & Craniofacial Research Principal Investigator
- Role of a latent OriLyt RNA in KSHV latency in primary effusion lymphoma NIH/Nat. Cancer Institute Principal Investigator
- Role of a latent OriLyt RNA in KSHV latency in primary effusion lymphoma NIH/Nat. Cancer Institute Principal Investigator
- Epigenetic Regulation of KSHV Latency NIH/Nat. Inst. of Dental & Craniofacial Research Principal Investigator
- Epigenetic Regulation of KSHV Latency NIH/Nat. Inst. of Dental & Craniofacial Research Principal Investigator
- Oncogenic Roles and Therapeutic Potential of MCL1 Addiction in Primary Effusion Lymphoma NIH/Nat. Cancer Institute Principal Investigator
- Role of a latent OriLyt RNA in KSHV latency in primary effusion lymphoma NIH/Nat. Cancer Institute Principal Investigator
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