Your search keyword '"Joseph Pangallo"' showing total 7 results

1. Coordinated missplicing of TMEM14C and ABCB7 causes ring sideroblast formation in SF3B1-mutant myelodysplastic syndrome

Author

Robert K. Bradley, Patrick Nugent, Khrystyna North, Jasmine Naru, Eunhee Kim, Janine O. Ilagan, Joseph Pangallo, Sergei Doulatov, Martina Sarchi, Derek L. Stirewalt, Arvind R. Subramaniam, Rochelle Bergantinos, Massiel Chavez Stolla, Omar Abdel-Wahab, Janis L. Abkowitz, and Courtnee Clough

Subjects

Untranslated region, Immunology, Mutant, Mitochondrion, Mitochondrial Membrane Transport Proteins, Biochemistry, Mitochondrial Proteins, Splicing factor, Humans, Protoporphyrinogen Oxidase, Induced pluripotent stem cell, Flavoproteins, biology, Chemistry, Cell Differentiation, Cell Biology, Hematology, Phosphoproteins, ABCB7, Cell biology, Haematopoiesis, Myelodysplastic Syndromes, Mutation, RNA splicing, biology.protein, ATP-Binding Cassette Transporters, RNA Splicing Factors

Abstract

SF3B1 splicing factor mutations are near-universally found in myelodysplastic syndromes (MDS) with ring sideroblasts (RS), a clonal hematopoietic disorder characterized by abnormal erythroid cells with iron-loaded mitochondria. Despite this remarkably strong genotype-to-phenotype correlation, the mechanism by which mutant SF3B1 dysregulates iron metabolism to cause RS remains unclear due to an absence of physiological models of RS formation. Here, we report an induced pluripotent stem cell model of SF3B1-mutant MDS that for the first time recapitulates robust RS formation during in vitro erythroid differentiation. Mutant SF3B1 induces missplicing of ∼100 genes throughout erythroid differentiation, including proposed RS driver genes TMEM14C, PPOX, and ABCB7. All 3 missplicing events reduce protein expression, notably occurring via 5′ UTR alteration, and reduced translation efficiency for TMEM14C. Functional rescue of TMEM14C and ABCB7, but not the non–rate-limiting enzyme PPOX, markedly decreased RS, and their combined rescue nearly abolished RS formation. Our study demonstrates that coordinated missplicing of mitochondrial transporters TMEM14C and ABCB7 by mutant SF3B1 sequesters iron in mitochondria, causing RS formation.

Published

2022

2. Synthetic introns enable splicing factor mutation-dependent targeting of cancer cells

Author

Khrystyna North, Salima Benbarche, Bo Liu, Joseph Pangallo, Sisi Chen, Maximilian Stahl, Jan Philipp Bewersdorf, Robert F. Stanley, Caroline Erickson, Hana Cho, Jose Mario Bello Pineda, James D. Thomas, Jacob T. Polaski, Andrea E. Belleville, Austin M. Gabel, Dylan B. Udy, Olivier Humbert, Hans-Peter Kiem, Omar Abdel-Wahab, and Robert K. Bradley

Subjects

Uveal Neoplasms, Leukemia, Biomedical Engineering, Breast Neoplasms, Bioengineering, Genetic Therapy, Antiviral Agents, Thymidine Kinase, Applied Microbiology and Biotechnology, Introns, Mice, Mutation, Animals, Humans, Molecular Medicine, Female, RNA Splicing Factors, Ganciclovir, Melanoma, Biotechnology

Abstract

Many cancers carry recurrent, change-of-function mutations affecting RNA splicing factors. Here, we describe a method to harness this abnormal splicing activity to drive splicing factor mutation-dependent gene expression to selectively eliminate tumor cells. We engineered synthetic introns that were efficiently spliced in cancer cells bearing SF3B1 mutations, but unspliced in otherwise isogenic wild-type cells, to yield mutation-dependent protein production. A massively parallel screen of 8,878 introns delineated ideal intronic size and mapped elements underlying mutation-dependent splicing. Synthetic introns enabled mutation-dependent expression of herpes simplex virus-thymidine kinase (HSV-TK) and subsequent ganciclovir (GCV)-mediated killing of SF3B1-mutant leukemia, breast cancer, uveal melanoma and pancreatic cancer cells in vitro, while leaving wild-type cells unaffected. Delivery of synthetic intron-containing HSV-TK constructs to leukemia, breast cancer and uveal melanoma cells and GCV treatment in vivo significantly suppressed the growth of these otherwise lethal xenografts and improved mouse host survival. Synthetic introns provide a means to exploit tumor-specific changes in RNA splicing for cancer gene therapy.

Published

2022

3. Spliceosomal disruption of the non-canonical BAF complex in cancer

Author

Sydney X. Lu, Yu Chen, Daichi Inoue, Justin Taylor, Ariele Block, Robert K. Bradley, Cigall Kadoch, Alex Penson, Andrew R. D’Avino, Khrystyna North, Bo Liu, Brittany C. Michel, Hana Cho, Tyler D. Hitchman, Guo-Liang Chew, Stanley Chun-Wei Lee, Akihide Yoshimi, Joseph Pangallo, Luisa F. Escobar-Hoyos, Omar Abdel-Wahab, Lillian Bitner, and Amanda R. Moore

Subjects

0301 basic medicine, Chromosomal Proteins, Non-Histone, RNA Splicing, Mutant, Mutagenesis (molecular biology technique), Biology, medicine.disease_cause, Article, law.invention, 03 medical and health sciences, Exon, Mice, 0302 clinical medicine, law, Cell Line, Tumor, Neoplasms, medicine, Animals, Humans, Psychological repression, Multidisciplinary, Alternative splicing, Chromatin Assembly and Disassembly, Phosphoproteins, 3. Good health, Cell biology, 030104 developmental biology, 030220 oncology & carcinogenesis, RNA splicing, Spliceosomes, Suppressor, RNA Splicing Factors, Carcinogenesis, Neoplasm Transplantation, Transcription Factors

Abstract

SF3B1 is the most commonly mutated RNA splicing factor in cancer1–4, but the mechanisms by which SF3B1 mutations promote malignancy are poorly understood. Here we integrated pan-cancer splicing analyses with a positive-enrichment CRISPR screen to prioritize splicing alterations that promote tumorigenesis. We report that diverse SF3B1 mutations converge on repression of BRD9, which is a core component of the recently described non-canonical BAF chromatin-remodelling complex that also contains GLTSCR1 and GLTSCR1L5–7. Mutant SF3B1 recognizes an aberrant, deep intronic branchpoint within BRD9 and thereby induces the inclusion of a poison exon that is derived from an endogenous retroviral element and subsequent degradation of BRD9 mRNA. Depletion of BRD9 causes the loss of non-canonical BAF at CTCF-associated loci and promotes melanomagenesis. BRD9 is a potent tumour suppressor in uveal melanoma, such that correcting mis-splicing of BRD9 in SF3B1-mutant cells using antisense oligonucleotides or CRISPR-directed mutagenesis suppresses tumour growth. Our results implicate the disruption of non-canonical BAF in the diverse cancer types that carry SF3B1 mutations and suggest a mechanism-based therapeutic approach for treating these malignancies. A range of SF3B1 mutations promote tumorigenesis through the repression of BRD9, a core component of the non-canonical BAF complex, and correcting BRD9 mis-splicing in these SF3B1-mutant cells suppresses tumour growth.

Published

2019

4. Single-cell genomics reveals the genetic and molecular bases for escape from mutational epistasis in myeloid neoplasms

Author

Daniel H. Wiseman, Michael Haddadin, Katherine Knorr, Alexander V Penson, Terra L. Lasho, Xiaoli Mi, Joseph Pangallo, Bo Liu, Ayalew Tefferi, Robert K. Bradley, Yang Liang, Justin Taylor, Khrystyna North, Salima Benbarche, Stephanie Halene, Omar Abdel-Wahab, Moritz Binder, and Mrinal M. Patnaik

Subjects

0301 basic medicine, RNA Splicing Factors, Myeloid, RNA Splicing, Immunology, DNA Mutational Analysis, Genomics, Biology, Biochemistry, 03 medical and health sciences, Splicing factor, 0302 clinical medicine, medicine, Humans, Allele, Gene, Alleles, Genetics, Epistasis, Genetic, Cell Biology, Hematology, 030104 developmental biology, medicine.anatomical_structure, Leukemia, Myeloid, 030220 oncology & carcinogenesis, Hematologic Neoplasms, RNA splicing, Mutation, Epistasis, Single-Cell Analysis

Abstract

Large-scale sequencing studies of hematologic malignancies have revealed notable epistasis among high-frequency mutations. One of the most striking examples of epistasis occurs for mutations in RNA splicing factors. These lesions are among the most common alterations in myeloid neoplasms and generally occur in a mutually exclusive manner, a finding attributed to their synthetic lethal interactions and/or convergent effects. Curiously, however, patients with multiple-concomitant splicing factor mutations have been observed, challenging our understanding of one of the most common examples of epistasis in hematologic malignancies. In this study, we performed bulk and single-cell analyses of patients with myeloid malignancy who were harboring ≥2 splicing factor mutations, to understand the frequency and basis for the coexistence of these mutations. Although mutations in splicing factors were strongly mutually exclusive across 4231 patients (q < .001), 0.85% harbored 2 concomitant bona fide splicing factor mutations, ∼50% of which were present in the same individual cells. However, the distribution of mutations in patients with double mutations deviated from that in those with single mutations, with selection against the most common alleles, SF3B1K700E and SRSF2P95H/L/R, and selection for less common alleles, such as SF3B1 non-K700E mutations, rare amino acid substitutions at SRSF2P95, and combined U2AF1S34/Q157 mutations. SF3B1 and SRSF2 alleles enriched in those with double-mutations had reduced effects on RNA splicing and/or binding compared with the most common alleles. Moreover, dual U2AF1 mutations occurred in cis with preservation of the wild-type allele. These data highlight allele-specific differences as critical in regulating the molecular effects of splicing factor mutations as well as their cooccurrences/exclusivities with one another.

Published

2020

5. Rare and private spliceosomal gene mutations drive partial, complete, and dual phenocopies of hotspot alterations

Author

Joseph Pangallo, Omar Abdel-Wahab, Bruno Cassinat, Robert K. Bradley, Jacob T. Polaski, Jean-Jacques Kiladjian, Khrystyna North, Justin Taylor, and Aline Renneville

Subjects

0301 basic medicine, RNA Splicing Factors, RNA Splicing, Immunology, Penetrance, Biology, Gene mutation, Biochemistry, 03 medical and health sciences, Exon, 0302 clinical medicine, Cell Line, Tumor, Missense mutation, Humans, Gene, Genetic Association Studies, Genetics, Phenocopy, Gene Expression Profiling, Computational Biology, Cell Biology, Hematology, Exons, Isogenic human disease models, 030104 developmental biology, Phenotype, RNA splicing, Mutation, Spliceosomes, RNA Splice Sites, Transcriptome, 030215 immunology

Abstract

Genes encoding the RNA splicing factors SF3B1, SRSF2, and U2AF1 are subject to frequent missense mutations in clonal hematopoiesis and diverse neoplastic diseases. Most "spliceosomal" mutations affect specific hotspot residues, resulting in splicing changes that promote disease pathophysiology. However, a subset of patients carry spliceosomal mutations that affect non-hotspot residues, whose potential functional contributions to disease are unstudied. Here, we undertook a systematic characterization of diverse rare and private spliceosomal mutations to infer their likely disease relevance. We utilized isogenic cell lines and primary patient materials to discover that 11 of 14 studied rare and private mutations in SRSF2 and U2AF1 induced distinct splicing alterations, including partially or completely phenocopying the alterations in exon and splice site recognition induced by hotspot mutations or driving "dual" phenocopies that mimicked two co-occurring hotspot mutations. Our data suggest that many rare and private spliceosomal mutations contribute to disease pathogenesis and illustrate the utility of molecular assays to inform precision medicine by inferring the potential disease relevance of newly discovered mutations.

Published

2019

6. Interferon lambda 4 expression is suppressed by the host during viral infection

Author

Shuanghu Liu, Yueh Ming Loo, Joseph Pangallo, Chrissie Lim, Curt H. Hagedorn, Michael Gale, Ram Savan, Alison M. Kell, Abigail Jarret, Mee Ae Hong, and Johannes Schwerk

Subjects

0301 basic medicine, Polyadenylation, Hepatitis C virus, Immunology, Intracellular Space, Hepacivirus, Biology, medicine.disease_cause, Antiviral Agents, Models, Biological, 03 medical and health sciences, 0302 clinical medicine, Immune system, Interferon, Cell Line, Tumor, Polysome, medicine, Animals, Humans, Protein Isoforms, Immunology and Allergy, Receptors, Cytokine, Frameshift Mutation, Research Articles, Receptors, Interferon, Messenger RNA, Base Sequence, Cell Death, Effector, Interleukins, Pathogen-Associated Molecular Pattern Molecules, Brief Definitive Report, Translation (biology), Virology, Recombinant Proteins, 3. Good health, Alternative Splicing, 030104 developmental biology, Virus Diseases, Protein Biosynthesis, 030220 oncology & carcinogenesis, Host-Pathogen Interactions, Interferons, Extracellular Space, Signal Transduction, medicine.drug

Abstract

Hong et al. show that IFNλ4 exhibits similar antiviral activity to IFNλ3. Humans deploy several mechanisms to limit expression of functional IFNλ4 through noncoding splice variants and nonfunctional protein isoforms., Interferon (IFN) lambdas are critical antiviral effectors in hepatic and mucosal infections. Although IFNλ1, IFNλ2, and IFNλ3 act antiviral, genetic association studies have shown that expression of the recently discovered IFNL4 is detrimental to hepatitis C virus (HCV) infection through a yet unknown mechanism. Intriguingly, human IFNL4 harbors a genetic variant that introduces a premature stop codon. We performed a molecular and biochemical characterization of IFNλ4 to determine its role and regulation of expression. We found that IFNλ4 exhibits similar antiviral activity to IFNλ3 without negatively affecting antiviral IFN activity or cell survival. We show that humans deploy several mechanisms to limit expression of functional IFNλ4 through noncoding splice variants and nonfunctional protein isoforms. Furthermore, protein-coding IFNL4 mRNA are not loaded onto polyribosomes and lack a strong polyadenylation signal, resulting in poor translation efficiency. This study provides mechanistic evidence that humans suppress IFNλ4 expression, suggesting that immune function is dependent on other IFNL family members.

Published

2016

7. Progressive engineering of a homing endonuclease genome editing reagent for the murine X-linked immunodeficiency locus

Author

David Baker, Andrew M. Scharenberg, Sandrine Boissel, Iram F. Khan, Yupeng Wang, Summer B. Thyme, David J. Rawlings, Joseph Pangallo, and Jordan Jarjour

Subjects

Homing endonuclease, Genome engineering, Endonuclease, Mice, Genome editing, Genetics, Agammaglobulinaemia Tyrosine Kinase, Bruton's tyrosine kinase, Animals, Humans, DNA Cleavage, Endodeoxyribonucleases, Homologous Recombination, Gene, Cells, Cultured, biology, Nucleic Acid Enzymes, DNA-binding domain, Genomics, Protein-Tyrosine Kinases, Protein Structure, Tertiary, DNA-Binding Proteins, HEK293 Cells, Genetic Loci, Mutation, biology.protein, Indicators and Reagents, Directed Molecular Evolution

Abstract

LAGLIDADG homing endonucleases (LHEs) are compact endonucleases with 20–22 bp recognition sites, and thus are ideal scaffolds for engineering site-specific DNA cleavage enzymes for genome editing applications. Here, we describe a general approach to LHE engineering that combines rational design with directed evolution, using a yeast surface display high-throughput cleavage selection. This approach was employed to alter the binding and cleavage specificity of the I-Anil LHE to recognize a mutation in the mouse Bruton tyrosine kinase (Btk) gene causative for mouse X-linked immunodeficiency (XID)—a model of human X-linked agammaglobulinemia (XLA). The required re-targeting of I-AniI involved progressive resculpting of the DNA contact interface to accommodate nine base differences from the native cleavage sequence. The enzyme emerging from the progressive engineering process was specific for the XID mutant allele versus the wild-type (WT) allele, and exhibited activity equivalent to WT I-AniI in vitro and in cellulo reporter assays. Fusion of the enzyme to a site-specific DNA binding domain of transcription activator-like effector (TALE) resulted in a further enhancement of gene editing efficiency. These results illustrate the potential of LHE enzymes as specific and efficient tools for therapeutic genome engineering.

Published

2014