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1. Inhibition and degradation of NRAS with a pan-NRAS monobody.

Author

Whaby, Michael, Ketavarapu, Gayatri, Koide, Akiko, Mazzei, Megan, Mintoo, Mubashir, Glasser, Eliezra, Patel, Unnatiben, Nasarre, Cecile, Sale, Matthew, Mccormick, Frank, Koide, Shohei, and OBryan, John

Subjects
Humans, GTP Phosphohydrolases, Membrane Proteins, Mutation, Melanoma, Cell Line, Tumor, Signal Transduction, Animals, Proteolysis, Mice, Guanosine Triphosphate, Proto-Oncogene Proteins p21(ras)
Abstract

The RAS family GTPases are the most frequently mutated oncogene family in human cancers. Activating mutations in either of the three RAS isoforms (HRAS, KRAS, or NRAS) are found in nearly 20% of all human tumors with NRAS mutated in ~25% of melanomas. Despite remarkable advancements in therapies targeted against mutant KRAS, NRAS-specific pharmacologics are lacking. Thus, development of inhibitors of NRAS would address a critical unmet need to treating primary tumors harboring NRAS mutations as well as BRAF-mutant melanomas, which frequently develop resistance to clinically approved BRAF inhibitors through NRAS mutation. Building upon our previous studies with the monobody NS1 that recognizes HRAS and KRAS but not NRAS, here we report the development of a monobody that specifically binds to both GDP and GTP-bound states of NRAS and inhibits NRAS-mediated signaling in a mutation-agnostic manner. Further, this monobody can be formatted into a genetically encoded NRAS-specific degrader. Our study highlights the feasibility of developing NRAS selective inhibitors for therapeutic efforts.

Published
2024

2. The prominent pervasive oncogenic role and tissue specific permissiveness of RAS gene mutations.

Author

Yi, Ming, Soppet, Daniel, McCormick, Frank, and Nissley, Dwight

Subjects
Humans, Mutation, Organ Specificity, Neoplasms, Genes, ras, Proto-Oncogene Proteins p21(ras), Membrane Proteins, GTP Phosphohydrolases, Cell Line, Tumor, Carcinogenesis, Oncogenes
Abstract

In cancer research, RAS biology has been focused on only a handful of tumor types. While RAS genes have long been suspected as common contributors to a wide spectrum of cancer types, robust evidence is required to firmly establish their critical oncogenic significance. We present a data mining study using DepMap genome-wide CRISPR screening data, which provide substantial evidence to support the prominent pervasive oncogenic role and tissue-specific permissiveness of RAS gene mutations. Differential analysis of CRISPR effect scores identifies K- or N-RAS genes as the most differential gene in contrasts of (K-, N-, combined) RAS mutant versus wild-type cell lines across multiple tissue types. The distinguished tissue-specific pattern of KRAS vs. NRAS as top differential genes in subsets of tissue types and evidence from genome data supported the idea of KRAS- and NRAS-engaged tissue types. To our knowledge, this is the first report of prominent pervasive oncogenic role of RAS mutations revealed by gene dependency data that is beyond the current understanding of the oncogenic role of RAS genes and their well-known involved tissue types. Our findings strongly support RAS mutations as primary oncogenic drivers beyond traditionally recognized cancer types and offer insights into their tissue-specific permissiveness.

Published
2024

3. A Top-Down Proteomic Assay to Evaluate KRAS4B-Compound Engagement.

Author

DIppolito, Robert, Rabara, Dana, Blanco, Maria, Alberico, Emily, Drew, Matthew, Ramakrishnan, Nitya, Sontan, Dara, Widmeyer, Stephanie, Scheidemantle, Grace, Messing, Simon, Turner, David, Nissley, Dwight, DeHart, Caroline, Maciag, Anna, Stephen, Andrew, Esposito, Dominic, Mccormick, Frank, and Arkin, Michelle

Subjects
Proteomics, Proto-Oncogene Proteins p21(ras), Mutation, Binding Sites
Abstract

Development of new targeted inhibitors for oncogenic KRAS mutants may benefit from insight into how a given mutation influences the accessibility of protein residues and how compounds interact with mutant or wild-type KRAS proteins. Targeted proteomic analysis, a key validation step in the KRAS inhibitor development process, typically involves both intact mass- and peptide-based methods to confirm compound localization or quantify binding. However, these methods may not always provide a clear picture of the compound binding affinity for KRAS, how specific the compound is to the target KRAS residue, and how experimental conditions may impact these factors. To address this, we have developed a novel top-down proteomic assay to evaluate in vitro KRAS4B-compound engagement while assessing relative quantitation in parallel. We present two applications to demonstrate the capabilities of our assay: maleimide-biotin labeling of a KRAS4BG12D cysteine mutant panel and treatment of three KRAS4B proteins (WT, G12C, and G13C) with small molecule compounds. Our results show the time- or concentration-dependence of KRAS4B-compound engagement in context of the intact protein molecule while directly mapping the compound binding site.

Published
2024

4. Structural dynamics of RAF1-HSP90-CDC37 and HSP90 complexes reveal asymmetric client interactions and key structural elements.

Author

Finci, Lorenzo, Chakrabarti, Mayukh, Gulten, Gulcin, Finney, Joseph, Grose, Carissa, Fox, Tara, Yang, Renbin, Nissley, Dwight, Esposito, Dominic, Balius, Trent, Simanshu, Dhirendra, and Mccormick, Frank

Subjects
Humans, Cell Cycle Proteins, Protein Binding, Chaperonins, Molecular Chaperones, HSP90 Heat-Shock Proteins
Abstract

RAF kinases are integral to the RAS-MAPK signaling pathway, and proper RAF1 folding relies on its interaction with the chaperone HSP90 and the cochaperone CDC37. Understanding the intricate molecular interactions governing RAF1 folding is crucial for comprehending this process. Here, we present a cryo-EM structure of the closed-state RAF1-HSP90-CDC37 complex, where the C-lobe of the RAF1 kinase domain binds to one side of the HSP90 dimer, and an unfolded N-lobe segment of the RAF1 kinase domain threads through the center of the HSP90 dimer. CDC37 binds to the kinase C-lobe, mimicking the N-lobe with its HxNI motif. We also describe structures of HSP90 dimers without RAF1 and CDC37, displaying only N-terminal and middle domains, which we term the semi-open state. Employing 1 μs atomistic simulations, energetic decomposition, and comparative structural analysis, we elucidate the dynamics and interactions within these complexes. Our quantitative analysis reveals that CDC37 bridges the HSP90-RAF1 interaction, RAF1 binds HSP90 asymmetrically, and that HSP90 structural elements engage RAF1s unfolded region. Additionally, N- and C-terminal interactions stabilize HSP90 dimers, and molecular interactions in HSP90 dimers rearrange between the closed and semi-open states. Our findings provide valuable insight into the contributions of HSP90 and CDC37 in mediating client folding.

Published
2024

5. Comparative analysis of KRAS4a and KRAS4b splice variants reveals distinctive structural and functional properties.

Author

Whitley, Matthew, Tran, Timothy, Rigby, Megan, Yi, Ming, Dharmaiah, Srisathiyanarayanan, Waybright, Timothy, Ramakrishnan, Nitya, Perkins, Shelley, Taylor, Troy, Messing, Simon, Esposito, Dominic, Nissley, Dwight, Mccormick, Frank, Stephen, Andrew, Turbyville, Thomas, Cornilescu, Gabriel, and Simanshu, Dhirendra

Subjects
Humans, Molecular Conformation, Neoplasms, Protein Isoforms, Proto-Oncogene Proteins p21(ras)
Abstract

KRAS, the most frequently mutated oncogene in human cancer, produces two isoforms, KRAS4a and KRAS4b, through alternative splicing. These isoforms differ in exon 4, which encodes the final 15 residues of the G-domain and hypervariable regions (HVRs), vital for trafficking and membrane localization. While KRAS4b has been extensively studied, KRAS4a has been largely overlooked. Our multidisciplinary study compared the structural and functional characteristics of KRAS4a and KRAS4b, revealing distinct structural properties and thermal stability. Position 151 influences KRAS4as thermal stability, while position 153 affects binding to RAF1 CRD protein. Nuclear magnetic resonance analysis identified localized structural differences near sequence variations and provided a solution-state conformational ensemble. Notably, KRAS4a exhibits substantial transcript abundance in bile ducts, liver, and stomach, with transcript levels approaching KRAS4b in the colon and rectum. Functional disparities were observed in full-length KRAS variants, highlighting the impact of HVR variations on interaction with trafficking proteins and downstream effectors like RAF and PI3K within cells.

Published
2024

6. Revealing the mechanism of action of a first-in-class covalent inhibitor of KRASG12C (ON) and other functional properties of oncogenic KRAS by 31P NMR.

Author

Maciag, Anna, Sharma, Alok, Pei, Jun, Yang, Yue, Dyba, Marcin, Smith, Brian, Rabara, Dana, Larsen, Erik, Lightstone, Felice, Esposito, Dominic, Stephen, Andrew, Wang, Bin, Beltran, Pedro, Wallace, Eli, Nissley, Dwight, and Mccormick, Frank

Subjects
(31)P NMR, GTP, GTPase KRAS, GppNHp, KRAS G12C selective small-molecule inhibitor, cancer, nucleotide, protein complex, state 1 (inactive) conformation, state 2 (active) conformation, Proto-Oncogene Proteins p21(ras), ras Proteins, Guanosine Triphosphate, Magnetic Resonance Spectroscopy, Signal Transduction, Mutation
Abstract

Individual oncogenic KRAS mutants confer distinct differences in biochemical properties and signaling for reasons that are not well understood. KRAS activity is closely coupled to protein dynamics and is regulated through two interconverting conformations: state 1 (inactive, effector binding deficient) and state 2 (active, effector binding enabled). Here, we use 31P NMR to delineate the differences in state 1 and state 2 populations present in WT and common KRAS oncogenic mutants (G12C, G12D, G12V, G13D, and Q61L) bound to its natural substrate GTP or a commonly used nonhydrolyzable analog GppNHp (guanosine-5-[(β,γ)-imido] triphosphate). Our results show that GppNHp-bound proteins exhibit significant state 1 population, whereas GTP-bound KRAS is primarily (90% or more) in state 2 conformation. This observation suggests that the predominance of state 1 shown here and in other studies is related to GppNHp and is most likely nonexistent in cells. We characterize the impact of this differential conformational equilibrium of oncogenic KRAS on RAF1 kinase effector RAS-binding domain and intrinsic hydrolysis. Through a KRAS G12C drug discovery, we have identified a novel small-molecule inhibitor, BBO-8956, which is effective against both GDP- and GTP-bound KRAS G12C. We show that binding of this inhibitor significantly perturbs state 1-state 2 equilibrium and induces an inactive state 1 conformation in GTP-bound KRAS G12C. In the presence of BBO-8956, RAF1-RAS-binding domain is unable to induce a signaling competent state 2 conformation within the ternary complex, demonstrating the mechanism of action for this novel and active-conformation inhibitor.

Published
2024

7. Functional interactions between neurofibromatosis tumor suppressors underlie Schwann cell tumor de-differentiation and treatment resistance

Author

Vasudevan, Harish N., Payne, Emily, Delley, Cyrille L., John Liu, S., Mirchia, Kanish, Sale, Matthew J., Lastella, Sydney, Nunez, Maria Sacconi, Lucas, Calixto-Hope G., Eaton, Charlotte D., Casey-Clyde, Tim, Magill, Stephen T., Chen, William C., Braunstein, Steve E., Perry, Arie, Jacques, Line, Reddy, Alyssa T., Pekmezci, Melike, Abate, Adam R., McCormick, Frank, and Raleigh, David R.

Published
2024
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9. RAS Signaling Gone Awry in the Skin: The Complex Role of RAS in Cutaneous Neurofibroma Pathogenesis, Emerging Biological Insights.

Author

Rhodes, Steven, Mccormick, Frank, Cagan, Ross, Bakker, Annette, Staedtke, Verena, Ly, Ina, Steensma, Matthew, Lee, Sang, Romo, Carlos, Blakeley, Jaishri, and Sarin, Kavita

Subjects
Humans, Neurofibroma, Neurofibromatosis 1, Skin Neoplasms, Signal Transduction
Abstract

Cutaneous neurofibromas (cNFs) are the most common tumor in people with the rasopathy neurofibromatosis type 1. They number in hundreds or even thousands throughout the body, and currently, there are no effective interventions to prevent or treat these skin tumors. To facilitate the identification of novel and effective therapies, essential studies including a more refined understanding of cNF biology and the role of RAS signaling and downstream effector pathways responsible for cNF initiation, growth, and maintenance are needed. This review highlights the current state of knowledge of RAS signaling in cNF pathogenesis and therapeutic development for cNF treatment.

Published
2023

10. A Call for Discovery and Therapeutic Development for Cutaneous Neurofibromas

Author

Blakeley, Jaishri O, Le, Lu Q, Lee, Sang Y, Ly, Ina, Rhodes, Steven D, Romo, Carlos G, Sarin, Kavita Y, Staedtke, Verena, Steensma, Matthew R, Wolkenstein, Pierre, Participants, 2022 NTAP Cutaneous Neurofibroma Symposium, Largaespada, David, Serra, Eduard, Haniffa, Muzlifah, Bakker, Annette, McCormick, Frank, Cagan, Ross L, Ju, William, Stemmer-Rachamimov, Anat, Grimes, Kevin, Topilko, Piotr, Kornacki, Deanna, Kelly, Kristen M, Gottesman, Sally, York, Zachary, and Epps, Roselyn

Subjects
Humans, Neurofibroma, Neurofibromatosis 1, Skin Neoplasms, Connective Tissue Diseases, NTAP Cutaneous Neurofibroma Symposium Participants, Clinical Sciences, Oncology and Carcinogenesis, Dermatology & Venereal Diseases
Published
2023

12. RAS-dependent RAF-MAPK hyperactivation by pathogenic RIT1 is a therapeutic target in Noonan syndrome-associated cardiac hypertrophy.

Author

Cuevas-Navarro, Antonio, Wagner, Morgan, Van, Richard, Swain, Monalisa, Mo, Stephanie, Columbus, John, Allison, Madeline, Cheng, Alice, Messing, Simon, Turbyville, Thomas, Simanshu, Dhirendra, Sale, Matthew, Stephen, Andrew, Castel, Pau, and Mccormick, Frank

Subjects
Animals, Mice, Noonan Syndrome, Mitogen-Activated Protein Kinases, Cardiomegaly, Signal Transduction, Lung Neoplasms
Abstract

RIT1 is a RAS guanosine triphosphatase (GTPase) that regulates different aspects of signal transduction and is mutated in lung cancer, leukemia, and in the germline of individuals with Noonan syndrome. Pathogenic RIT1 proteins promote mitogen-activated protein kinase (MAPK) hyperactivation; however, this mechanism remains poorly understood. Here, we show that RAF kinases are direct effectors of membrane-bound mutant RIT1 necessary for MAPK activation. We identify critical residues in RIT1 that facilitate interaction with membrane lipids and show that these are necessary for association with RAF kinases and MAPK activation. Although mutant RIT1 binds to RAF kinases directly, it fails to activate MAPK signaling in the absence of classical RAS proteins. Consistent with aberrant RAF/MAPK activation as a driver of disease, we show that pathway inhibition alleviates cardiac hypertrophy in a mouse model of RIT1 mutant Noonan syndrome. These data shed light on the function of pathogenic RIT1 and identify avenues for therapeutic intervention.

Published
2023

13. The ribosomal S6 kinase 2 (RSK2)–SPRED2 complex regulates the phosphorylation of RSK substrates and MAPK signaling

Author

Lopez, Jocelyne, Bonsor, Daniel A, Sale, Matthew J, Urisman, Anatoly, Mehalko, Jennifer L, Cabanski-Dunning, Miranda, Castel, Pau, Simanshu, Dhirendra K, and McCormick, Frank

Subjects
Biochemistry and Cell Biology, Biological Sciences, Cancer, 2.1 Biological and endogenous factors, 1.1 Normal biological development and functioning, Generic health relevance, Mitogen-Activated Protein Kinases, Phosphorylation, Ribosomal Protein S6 Kinases, 90-kDa, Signal Transduction, Humans, Cell Line, Protein Domains, Repressor Proteins, Gene Knockdown Techniques, Protein Transport, Protein Binding, Protein Structure, Tertiary, Models, Molecular, Neurofibromin 1, RAS signaling, RASopathy, RSK2, SPRED2, kinase, neurofibromin, Chemical Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences
Abstract

Sprouty-related EVH-1 domain-containing (SPRED) proteins are a family of proteins that negatively regulate the RAS-Mitogen-Activated Protein Kinase (MAPK) pathway, which is involved in the regulation of the mitogenic response and cell proliferation. However, the mechanism by which these proteins affect RAS-MAPK signaling has not been elucidated. Patients with mutations in SPRED give rise to unique disease phenotypes; thus, we hypothesized that distinct interactions across SPRED proteins may account for alternative nodes of regulation. To characterize the SPRED interactome and evaluate how members of the SPRED family function through unique binding partners, we performed affinity purification mass spectrometry. We identified 90-kDa ribosomal S6 kinase 2 (RSK2) as a specific interactor of SPRED2 but not SPRED1 or SPRED3. We identified that the N-terminal kinase domain of RSK2 mediates the interaction between amino acids 123 to 201 of SPRED2. Using X-ray crystallography, we determined the structure of the SPRED2-RSK2 complex and identified the SPRED2 motif, F145A, as critical for interaction. We found that the formation of this interaction is regulated by MAPK signaling events. We also find that this interaction between SPRED2 and RSK2 has functional consequences, whereby the knockdown of SPRED2 resulted in increased phosphorylation of RSK substrates, YB1 and CREB. Furthermore, SPRED2 knockdown hindered phospho-RSK membrane and nuclear subcellular localization. We report that disruption of the SPRED2-RSK complex has effects on RAS-MAPK signaling dynamics. Our analysis reveals that members of the SPRED family have unique protein binding partners and describes the molecular and functional determinants of SPRED2-RSK2 complex dynamics.

Published
2023

14. Reduced dynamic complexity allows structure elucidation of an excited state of KRASG13D.

Author

Chao, Fa-An, Chan, Albert H, Dharmaiah, Srisathiyanarayanan, Schwieters, Charles D, Tran, Timothy H, Taylor, Troy, Ramakrishnan, Nitya, Esposito, Dominic, Nissley, Dwight V, McCormick, Frank, Simanshu, Dhirendra K, and Cornilescu, Gabriel

Subjects
ras Proteins, Magnetic Resonance Spectroscopy, Binding Sites, Protein Conformation, Proto-Oncogene Proteins p21(ras), Underpinning research, 1.1 Normal biological development and functioning, Generic health relevance
Abstract

Localized dynamics of RAS, including regions distal to the nucleotide-binding site, is of high interest for elucidating the mechanisms by which RAS proteins interact with effectors and regulators and for designing inhibitors. Among several oncogenic mutants, methyl relaxation dispersion experiments reveal highly synchronized conformational dynamics in the active (GMPPNP-bound) KRASG13D, which suggests an exchange between two conformational states in solution. Methyl and 31P NMR spectra of active KRASG13D in solution confirm a two-state ensemble interconverting on the millisecond timescale, with a major Pγ atom peak corresponding to the dominant State 1 conformation and a secondary peak indicating an intermediate state different from the known State 2 conformation recognized by RAS effectors. High-resolution crystal structures of active KRASG13D and KRASG13D-RAF1 RBD complex provide snapshots of the State 1 and 2 conformations, respectively. We use residual dipolar couplings to solve and cross-validate the structure of the intermediate state of active KRASG13D, showing a conformation distinct from those of States 1 and 2 outside the known flexible switch regions. The dynamic coupling between the conformational exchange in the effector lobe and the breathing motion in the allosteric lobe is further validated by a secondary mutation in the allosteric lobe, which affects the conformational population equilibrium.

Published
2023

16. Destabilizing NF1 variants act in a dominant negative manner through neurofibromin dimerization.

Author

Young, Lucy C, Goldstein de Salazar, Ruby, Han, Sae-Won, Huang, Zi Yi Stephanie, Merk, Alan, Drew, Matthew, Darling, Joseph, Wall, Vanessa, Grisshammer, Reinhard, Cheng, Alice, Allison, Madeline R, Sale, Matthew J, Nissley, Dwight V, Esposito, Dominic, Ognjenovic, Jana, and McCormick, Frank

Subjects
Humans, Neurofibromatosis 1, Neurofibromin 1, Dimerization, Mutation, Mutation, Missense, NFI, cryo-EM, neurofibromatosis type I, Genetics, Rare Diseases, Neurosciences, Neurofibromatosis, Aetiology, 2.1 Biological and endogenous factors
Abstract

The majority of pathogenic mutations in the neurofibromatosis type I (NF1) gene reduce total neurofibromin protein expression through premature truncation or microdeletion, but it is less well understood how loss-of-function missense variants drive NF1 disease. We have found that patient variants in codons 844 to 848, which correlate with a severe phenotype, cause protein instability and exert an additional dominant-negative action whereby wild-type neurofibromin also becomes destabilized through protein dimerization. We have used our neurofibromin cryogenic electron microscopy structure to predict and validate other patient variants that act through a similar mechanism. This provides a foundation for understanding genotype-phenotype correlations and has important implications for patient counseling, disease management, and therapeutics.

Published
2023

17. Impaired proteolysis of non-canonical RAS proteins drives clonal hematopoietic transformation

Author

Chen, Sisi, Vedula, Rahul S, Cuevas-Navarro, Antonio, Lu, Bin, Hogg, Simon J, Wang, Eric, Benbarche, Salima, Knorr, Katherine, Kim, Won Jun, Stanley, Robert F, Cho, Hana, Erickson, Caroline, Singer, Michael, Cui, Dan, Tittley, Steven, Durham, Benjamin H, Pavletich, Tatiana S, Fiala, Elise, Walsh, Michael F, Inoue, Daichi, Monette, Sebastien, Taylor, Justin, Rosen, Neal, McCormick, Frank, Lindsley, R Coleman, Castel, Pau, and Abdel-Wahab, Omar

Subjects
Rare Diseases, Cancer, Hematology, Stem Cell Research, 2.1 Biological and endogenous factors, Aetiology, Cullin Proteins, Guanosine Triphosphate, Humans, Leukemia, Protein Kinase Inhibitors, Proteolysis, Proto-Oncogene Proteins p21(ras), Transcription Factors, ras Proteins, Oncology and Carcinogenesis
Abstract

Recently, screens for mediators of resistance to FLT3 and ABL kinase inhibitors in leukemia resulted in the discovery of LZTR1 as an adapter of a Cullin-3 RING E3 ubiquitin ligase complex responsible for the degradation of RAS GTPases. In parallel, dysregulated LZTR1 expression via aberrant splicing and mutations was identified in clonal hematopoietic conditions. Here we identify that loss of LZTR1, or leukemia-associated mutants in the LZTR1 substrate and RAS GTPase RIT1 that escape degradation, drives hematopoietic stem cell (HSC) expansion and leukemia in vivo. Although RIT1 stabilization was sufficient to drive hematopoietic transformation, transformation mediated by LZTR1 loss required MRAS. Proteolysis targeting chimeras (PROTAC) against RAS or reduction of GTP-loaded RAS overcomes LZTR1 loss-mediated resistance to FLT3 inhibitors. These data reveal proteolysis of noncanonical RAS proteins as novel regulators of HSC self-renewal, define the function of RIT1 and LZTR1 mutations in leukemia, and identify means to overcome drug resistance due to LZTR1 downregulation.SignificanceHere we identify that impairing proteolysis of the noncanonical RAS GTPases RIT1 and MRAS via LZTR1 downregulation or leukemia-associated mutations stabilizing RIT1 enhances MAP kinase activation and drives leukemogenesis. Reducing the abundance of GTP-bound KRAS and NRAS overcomes the resistance to FLT3 kinase inhibitors associated with LZTR1 downregulation in leukemia. This article is highlighted in the In This Issue feature, p. 2221.

Published
2022

18. Structure of the SHOC2-MRAS-PP1C complex provides insights into RAF activation and Noonan syndrome.

Author

Bonsor, Daniel, Alexander, Patrick, Snead, Kelly, Hartig, Nicole, Drew, Matthew, Messing, Simon, Finci, Lorenzo, Nissley, Dwight, Esposito, Dominic, Rodriguez-Viciana, Pablo, Stephen, Andrew, Simanshu, Dhirendra, and Mccormick, Frank

Subjects
Humans, Intracellular Signaling Peptides and Proteins, MAP Kinase Signaling System, Mitogen-Activated Protein Kinase Kinases, Noonan Syndrome, Phosphoserine, Protein Phosphatase 1, Proto-Oncogene Proteins p21(ras), raf Kinases, ras Proteins
Abstract

SHOC2 acts as a strong synthetic lethal interactor with MEK inhibitors in multiple KRAS cancer cell lines. SHOC2 forms a heterotrimeric complex with MRAS and PP1C that is essential for regulating RAF and MAPK-pathway activation by dephosphorylating a specific phosphoserine on RAF kinases. Here we present the high-resolution crystal structure of the SHOC2-MRAS-PP1C (SMP) complex and apo-SHOC2. Our structures reveal that SHOC2, MRAS, and PP1C form a stable ternary complex in which all three proteins synergistically interact with each other. Our results show that dephosphorylation of RAF substrates by PP1C is enhanced upon interacting with SHOC2 and MRAS. The SMP complex forms only when MRAS is in an active state and is dependent on SHOC2 functioning as a scaffolding protein in the complex by bringing PP1C and MRAS together. Our results provide structural insights into the role of the SMP complex in RAF activation and how mutations found in Noonan syndrome enhance complex formation, and reveal new avenues for therapeutic interventions.

Published
2022

19. Structure–function analysis of the SHOC2–MRAS–PP1C holophosphatase complex

Author

Kwon, Jason J, Hajian, Behnoush, Bian, Yuemin, Young, Lucy C, Amor, Alvaro J, Fuller, James R, Fraley, Cara V, Sykes, Abbey M, So, Jonathan, Pan, Joshua, Baker, Laura, Lee, Sun Joo, Wheeler, Douglas B, Mayhew, David L, Persky, Nicole S, Yang, Xiaoping, Root, David E, Barsotti, Anthony M, Stamford, Andrew W, Perry, Charles K, Burgin, Alex, McCormick, Frank, Lemke, Christopher T, Hahn, William C, and Aguirre, Andrew J

Subjects
2.1 Biological and endogenous factors, Underpinning research, Aetiology, 1.1 Normal biological development and functioning, Generic health relevance, Cancer, Amino Acid Motifs, Binding Sites, Cryoelectron Microscopy, Guanosine Triphosphate, Humans, Intracellular Signaling Peptides and Proteins, MAP Kinase Signaling System, Multiprotein Complexes, Mutation, Missense, Phosphorylation, Protein Binding, Protein Phosphatase 1, Protein Stability, raf Kinases, ras Proteins, General Science & Technology
Abstract

Receptor tyrosine kinase (RTK)-RAS signalling through the downstream mitogen-activated protein kinase (MAPK) cascade regulates cell proliferation and survival. The SHOC2-MRAS-PP1C holophosphatase complex functions as a key regulator of RTK-RAS signalling by removing an inhibitory phosphorylation event on the RAF family of proteins to potentiate MAPK signalling1. SHOC2 forms a ternary complex with MRAS and PP1C, and human germline gain-of-function mutations in this complex result in congenital RASopathy syndromes2-5. However, the structure and assembly of this complex are poorly understood. Here we use cryo-electron microscopy to resolve the structure of the SHOC2-MRAS-PP1C complex. We define the biophysical principles of holoenzyme interactions, elucidate the assembly order of the complex, and systematically interrogate the functional consequence of nearly all of the possible missense variants of SHOC2 through deep mutational scanning. We show that SHOC2 binds PP1C and MRAS through the concave surface of the leucine-rich repeat region and further engages PP1C through the N-terminal disordered region that contains a cryptic RVXF motif. Complex formation is initially mediated by interactions between SHOC2 and PP1C and is stabilized by the binding of GTP-loaded MRAS. These observations explain how mutant versions of SHOC2 in RASopathies and cancer stabilize the interactions of complex members to enhance holophosphatase activity. Together, this integrative structure-function model comprehensively defines key binding interactions within the SHOC2-MRAS-PP1C holophosphatase complex and will inform therapeutic development .

Published
2022

21. ARAF protein kinase activates RAS by antagonizing its binding to RASGAP NF1

Author

Su, Wenjing, Mukherjee, Radha, Yaeger, Rona, Son, Jieun, Xu, Jianing, Na, Na, Merna Timaul, Neilawattie, Hechtman, Jaclyn, Paroder, Viktoriya, Lin, Mika, Mattar, Marissa, Qiu, Juan, Chang, Qing, Zhao, Huiyong, Zhang, Jonathan, Little, Megan, Adachi, Yuta, Han, Sae-Won, Taylor, Barry S, Ebi, Hiromichi, Abdel-Wahab, Omar, de Stanchina, Elisa, Rudin, Charles M, Jänne, Pasi A, McCormick, Frank, Yao, Zhan, and Rosen, Neal

Subjects
Cancer, Rare Diseases, Lung, ErbB Receptors, Guanosine Triphosphate, Humans, Neurofibromin 1, Protein Binding, Proto-Oncogene Proteins A-raf, Signal Transduction, ras GTPase-Activating Proteins, ARAF, ERK signaling, NF1, RAS-GTP, drug sensitivity, receptor tyrosine kinase inhibitor, Biological Sciences, Medical and Health Sciences, Developmental Biology
Abstract

RAF protein kinases are effectors of the GTP-bound form of small guanosine triphosphatase RAS and function by phosphorylating MEK. We showed here that the expression of ARAF activated RAS in a kinase-independent manner. Binding of ARAF to RAS displaced the GTPase-activating protein NF1 and antagonized NF1-mediated inhibition of RAS. This reduced ERK-dependent inhibition of RAS and increased RAS-GTP. By this mechanism, ARAF regulated the duration and consequences of RTK-induced RAS activation and supported the RAS output of RTK-dependent tumor cells. In human lung cancers with EGFR mutation, amplification of ARAF was associated with acquired resistance to EGFR inhibitors, which was overcome by combining EGFR inhibitors with an inhibitor of the protein tyrosine phosphatase SHP2 to enhance inhibition of nucleotide exchange and RAS activation.

Published
2022

22. Targeting CD70 in cutaneous T-cell lymphoma using an antibody-drug conjugate in patient-derived xenograft models

Author

Wu, Chi-Heng, Wang, Linlin, Yang, Chen-Yen, Wen, Kwun Wah, Hinds, Brian R, Gill, Ryan, McCormick, Frank, Moasser, Mark, Pincus, Laura, and Ai, Weiyun Z

Subjects
Hematology, Orphan Drug, Clinical Research, Clinical Trials and Supportive Activities, Cancer, Rare Diseases, Lymphoma, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Animals, CD27 Ligand, Heterografts, Humans, Immunoconjugates, Lymphoma, T-Cell, Cutaneous, Skin Neoplasms
Abstract

CD70 is a member of the tumor necrosis factor receptor superfamily. Emerging data indicate that CD70 may be a suitable target for various malignancies. We investigated the expression of CD70 in cutaneous and systemic T-cell lymphomas and conducted preclinical studies of SGN-CD70A, a CD70-directed antibody-drug conjugate (ADC), using patient-derived xenograft cutaneous T-cell lymphoma (CTCL PDX) models. CD70 expression was examined by immunohistochemical (IHC) stains in 49 diagnostic specimens of T-cell lymphomas. The activities of SGN-CD70A in growth inhibition and apoptosis induction were examined in CTCL cell lines and primary CTCL tumor cells. Using previously established CTCL PDXs, we conducted a dose-finding trial followed by a phase 2-like trial to evaluate the optimal dosing and the efficacy of SGN-CD70A in tumor-bearing PDX animals. The therapeutic efficacy of SGN-CD70A was measured by tumor-associated cell-free DNA (cfDNA) and survival of treated PDXs. We found that CD70 is highly expressed in T-cell lymphomas, especially in CTCL. SGN-CD70A inhibited cell growth and induced apoptosis in CD70-expressing CTCL cell lines and primary tumors cells. Additionally, SGN-CD70A at 100 μg/kg and 300 μg/kg prolonged the survival of PDXs in a dose-dependent manner. Finally, treatment with 3 doses of SGN-CD70A at 300 μg/kg was superior to a single-dose treatment in survival prolongation (median survival: 111 days vs 39 days; P = .017). Most importantly, multiple dosing of SGN-CD70A induced complete eradication of established tumors in PDXs measured by cfDNA. Our results demonstrated marked antitumor activity of SGN-CD70A in CTCL PDXs, providing compelling support for its clinical investigation.

Published
2022

23. NMR 1H, 13C, 15N backbone resonance assignments of the T35S and oncogenic T35S/Q61L mutants of human KRAS4b in the active, GppNHp-bound conformation

Author

Sharma, Alok K, Dyba, Marcin, Tonelli, Marco, Smith, Brian, Gillette, William K, Esposito, Dominic, Nissley, Dwight V, McCormick, Frank, and Maciag, Anna E

Subjects
Biochemistry and Cell Biology, Biological Sciences, Cancer, Digestive Diseases, Guanosine Triphosphate, Humans, Magnetic Resonance Spectroscopy, Nuclear Magnetic Resonance, Biomolecular, Protein Conformation, Proto-Oncogene Proteins p21(ras), GTPase KRAS, GppNHp, HSQC, T35S, Q61L, CSP, Biophysics, Biochemistry and cell biology
Abstract

RAS proteins cycling between the active-form (GTP-bound) and inactive-form (GDP-bound) play a key role in cell signaling pathways that control cell survival, proliferation, and differentiation. Mutations at codon 12, 13, and 61 in RAS are known to attenuate its GTPase activity favoring the RAS active state and constitutively active downstream signaling. This hyperactivation accounts for various malignancies including pancreatic, lung, and colorectal cancers. Active KRAS is found to exist in equilibrium between two rapidly interconverting conformational states (State1-State2) in solution. Due to this dynamic feature of the protein, the 1H-15N correlation cross-peak signals of several amino acid (AA) residues of KRAS belonging to the flexible loop regions are absent from its 2D 1H-15N HSQC spectrum within and near physiological solution pH. A threonine to serine mutation at position 35 (T35S) shifts the interconverting equilibrium to State1 conformation and enables the emergence of such residues in the 2D 1H-15N HSQC spectrum due to gained conformational rigidity. We report here the 1HN, 15N, and 13C backbone resonance assignments for the 19.2 kDa (AA 1-169) protein constructs of KRAS-GppNHp harboring T35S mutation (KRAST35S/C118S-GppNHp) and of its oncogenic counterpart harboring the Q61L mutation (KRAST35S/Q61L/C118S-GppNHp) using heteronuclear, multidimensional NMR spectroscopy at 298 K. High resolution NMR data allowed the unambiguous assignments of 1H-15N correlation cross-peaks for all the residues except for Met1. Furthermore, 2D 1H-15N HSQC overlay of two proteins assisted in determination of Q61L mutation-induced chemical shift perturbations for select residues in the regions of P-loop, Switch-II, and helix α3.

Published
2022

24. Cross-species analysis of LZTR1 loss-of-function mutants demonstrates dependency to RIT1 orthologs.

Author

Cuevas-Navarro, Antonio, Rodriguez-Muñoz, Laura, Grego-Bessa, Joaquim, Cheng, Alice, Rauen, Katherine A, Urisman, Anatoly, McCormick, Frank, Jimenez, Gerardo, and Castel, Pau

Subjects
Animals, Mice, ras Proteins, Adaptor Proteins, Signal Transducing, Drosophila Proteins, Transcription Factors, Signal Transduction, Cell Proliferation, Ubiquitination, CG3711, D. melanogaster, LZTR1, RASopathy, RIC, RIT1, cancer biology, genetics, genomics, human, mouse, noonan syndrome, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, D, melanogaster, Human, Mouse, Biochemistry and Cell Biology
Abstract

RAS GTPases are highly conserved proteins involved in the regulation of mitogenic signaling. We have previously described a novel Cullin 3 RING E3 ubiquitin ligase complex formed by the substrate adaptor protein LZTR1 that binds, ubiquitinates, and promotes proteasomal degradation of the RAS GTPase RIT1. In addition, others have described that this complex is also responsible for the ubiquitination of classical RAS GTPases. Here, we have analyzed the phenotypes of Lztr1 loss-of-function mutants in both fruit flies and mice and have demonstrated a biochemical preference for their RIT1 orthologs. Moreover, we show that Lztr1 is haplosufficient in mice and that embryonic lethality of the homozygous null allele can be rescued by deletion of Rit1. Overall, our results indicate that, in model organisms, RIT1 orthologs are the preferred substrates of LZTR1.

Published
2022

25. Insights into the Cross Talk between Effector and Allosteric Lobes of KRAS from Methyl Conformational Dynamics.

Author

Chao, Fa-An, Dharmaiah, Srisathiyanarayanan, Taylor, Troy, Messing, Simon, Gillette, William, Esposito, Dominic, Nissley, Dwight, Byrd, R, Simanshu, Dhirendra, Cornilescu, Gabriel, and Mccormick, Frank

Subjects
Cell Physiological Phenomena, Humans, Molecular Conformation, Neoplasms, Proto-Oncogene Proteins p21(ras), ras Proteins
Abstract

KRAS is the most frequently mutated RAS protein in cancer patients, and it is estimated that about 20% of the cancer patients in the United States carried mutant RAS proteins. To accelerate therapeutic development, structures and dynamics of RAS proteins had been extensively studied by various biophysical techniques for decades. Although 31P NMR studies revealed population equilibrium of the two major states in the active GMPPNP-bound form, more complex conformational dynamics in RAS proteins and oncogenic mutants subtly modulate the interactions with their downstream effectors. We established a set of customized NMR relaxation dispersion techniques to efficiently and systematically examine the ms-μs conformational dynamics of RAS proteins. This method allowed us to observe varying synchronized motions that connect the effector and allosteric lobes in KRAS. We demonstrated the role of conformational dynamics of KRAS in controlling its interaction with the Ras-binding domain of the downstream effector RAF1, the first kinase in the MAPK pathway. This allows one to explain, as well as to predict, the altered binding affinities of various KRAS mutants, which was neither previously reported nor apparent from the structural perspective.

Published
2022

26. Classical RAS proteins are not essential for paradoxical ERK activation induced by RAF inhibitors

Author

Lai, Lick Pui, Fer, Nicole, Burgan, William, Wall, Vanessa E, Xu, Bingfang, Soppet, Daniel, Esposito, Dominic, Nissley, Dwight V, and McCormick, Frank

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Cancer, Lung, Rare Diseases, Animals, Antineoplastic Agents, Cell Line, Tumor, Cell Proliferation, Fibroblasts, Intracellular Signaling Peptides and Proteins, MAP Kinase Signaling System, Mice, Mouse Embryonic Stem Cells, Mutation, Phosphorylation, Protein Kinase Inhibitors, Proto-Oncogene Proteins B-raf, Proto-Oncogene Proteins c-raf, Signal Transduction, raf Kinases, ras Proteins, MRAS, paradoxical ERK activation, RAF inhibitors, RAS GTPase, RAS-related GTPase
Abstract

RAF inhibitors unexpectedly induce ERK signaling in normal and tumor cells with elevated RAS activity. Paradoxical activation is believed to be RAS dependent. In this study, we showed that LY3009120, a pan-RAF inhibitor, can unexpectedly cause paradoxical ERK activation in KRASG12C-dependent lung cancer cell lines, when KRAS is inhibited by ARS1620, a KRASG12C inhibitor. Using H/N/KRAS-less mouse embryonic fibroblasts, we discovered that classical RAS proteins are not essential for RAF inhibitor-induced paradoxical ERK signaling. In their absence, RAF inhibitors can induce ERK phosphorylation, ERK target gene transcription, and cell proliferation. We further showed that the MRAS/SHOC2 complex is required for this process. This study highlights the complexity of the allosteric RAF regulation by RAF inhibitors, and the importance of other RAS-related proteins in this process.

Published
2022

27. Machine learning–driven multiscale modeling reveals lipid-dependent dynamics of RAS signaling proteins

Author

Ingólfsson, Helgi I, Neale, Chris, Carpenter, Timothy S, Shrestha, Rebika, López, Cesar A, Tran, Timothy H, Oppelstrup, Tomas, Bhatia, Harsh, Stanton, Liam G, Zhang, Xiaohua, Sundram, Shiv, Di Natale, Francesco, Agarwal, Animesh, Dharuman, Gautham, Kokkila Schumacher, Sara IL, Turbyville, Thomas, Gulten, Gulcin, Van, Que N, Goswami, Debanjan, Jean-Francois, Frantz, Agamasu, Constance, Chen, De, Hettige, Jeevapani J, Travers, Timothy, Sarkar, Sumantra, Surh, Michael P, Yang, Yue, Moody, Adam, Liu, Shusen, Van Essen, Brian C, Voter, Arthur F, Ramanathan, Arvind, Hengartner, Nicolas W, Simanshu, Dhirendra K, Stephen, Andrew G, Bremer, Peer-Timo, Gnanakaran, S, Glosli, James N, Lightstone, Felice C, McCormick, Frank, Nissley, Dwight V, and Streitz, Frederick H

Subjects
Networking and Information Technology R&D (NITRD), Generic health relevance, Cell Membrane, Humans, Lipids, Machine Learning, Molecular Dynamics Simulation, Protein Multimerization, Proto-Oncogene Proteins p21(ras), Signal Transduction, RAS dynamics, RAS-membrane biology, multiscale modeling, massive parallel simulations, multiscale infrastructure
Abstract

RAS is a signaling protein associated with the cell membrane that is mutated in up to 30% of human cancers. RAS signaling has been proposed to be regulated by dynamic heterogeneity of the cell membrane. Investigating such a mechanism requires near-atomistic detail at macroscopic temporal and spatial scales, which is not possible with conventional computational or experimental techniques. We demonstrate here a multiscale simulation infrastructure that uses machine learning to create a scale-bridging ensemble of over 100,000 simulations of active wild-type KRAS on a complex, asymmetric membrane. Initialized and validated with experimental data (including a new structure of active wild-type KRAS), these simulations represent a substantial advance in the ability to characterize RAS-membrane biology. We report distinctive patterns of local lipid composition that correlate with interfacially promiscuous RAS multimerization. These lipid fingerprints are coupled to RAS dynamics, predicted to influence effector binding, and therefore may be a mechanism for regulating cell signaling cascades.

Published
2022

28. Novel Regulators of Macropinocytosis-Dependent Growth Revealed by Informer Set Library Screening in Pancreatic Cancer Cells

Author

Kim, Sang Hoon, Song, Jae Ho, Kim, Min Ji, Song, Mun Gu, Ku, Angel A, Bandyopadhyay, Sourav, McCormick, Frank, and Kim, Sung Eun

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Biological Sciences, Rare Diseases, Biotechnology, Pancreatic Cancer, Cancer, Digestive Diseases, macropinocytosis, pancreatic cancer, Informer set library screening, cancer metabolism, nutrient scavenging, Analytical Chemistry, Clinical Sciences, Biochemistry and cell biology, Medical biochemistry and metabolomics, Analytical chemistry
Abstract

Cancer cells utilize multiple nutrient scavenging mechanisms to support growth and survival in nutrient-poor, hypoxic tumor microenvironments. Among these mechanisms, macropinocytosis has emerged as an important pathway of extracellular nutrient acquisition in cancer cells, particularly in tumors with activated RAS signaling, such as pancreatic cancer. However, the absence of a clinically available inhibitor, as well as the gap of knowledge in macropinocytosis regulation, remain a hurdle for its use for cancer therapy. Here, we use the Informer set library to identify novel regulators of macropinocytosis-dependent growth in pancreatic cancer cells. Understanding how these regulators function will allow us to provide novel opportunities for therapeutic intervention.

Published
2022

30. Surgical Technique: Arthroscopic Labral Management

Author

Parvaresh, Kevin C., McCormick, Frank, Federer, Andrew E., Nho, Shane J., Nwachukwu, Benedict U., Section editor, Nho, Shane J., editor, Bedi, Asheesh, editor, Salata, Michael J., editor, Mather III, Richard C., editor, and Kelly, Bryan T., editor

Published
2022
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32. How to End the Kidney Shortage

Author

McCormick, Frank and Held, Philip J.

Subjects
Kidneys -- Transplantation, Donation of organs, tissues, etc. -- Social aspects -- Forecasts and trends, Market trend/market analysis, Business, Government, Law
Abstract

News stories abound of kind people--relatives, close friends, and even complete strangers--who donate a kidney to someone suffering from kidney failure. These stories usually explain that people whose kidneys have [...]

Published
2023

33. Synergistic effects of RPT1G, a first-in-class small molecule NAMPT inhibitor, with venetoclax and olaparib in hematological malignancies.

Author

Crimmins, Gregory, primary, Wu, Min, additional, Roushar, Francis, additional, Bhurruth-Alcor, Yushma, additional, Jarvela, Timothy, additional, Digel, James, additional, Robb, Caroline, additional, Moghaddam-Taaheri, Parisa, additional, De Jesus-Diaz, Dennise, additional, and McCormick, Frank, additional

Published
2024
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35. The Cost of Procuring Deceased Donor Livers: Evidence From US Organ Procurement Organization Cost Reports, 2013–2018.

Author

Bragg‐Gresham, Jennifer L., Peters, Thomas G., Vaughan, William P., Held, Philip, McCormick, Frank, and Roberts, John P.

Subjects
COST of living, OVERHEAD costs, HOSPITAL costs, LIVER transplantation, COST estimates
Abstract

Deceased donor organs for transplantation are costly. Expenses include donor assessment, pre‐operative care of acceptable donors, surgical organ recovery, preservation and transport, and other costs. US Organ Procurement Organizations (OPOs) serve defined geographic areas in which each OPO has exclusive organ recovery responsibilities including detailed reporting of costs. We sought to determine the costs of procuring deceased donor livers by examining reported organ acquisition costs from OPO cost reports. Using 6 years of US OPO cost report data for each OPO (2013–2018), we determined the average cost of recovering a viable (i.e., transplanted) liver for each of the 51 independent US OPOs. We examined predictors of these costs including the number of livers procured, the percent of nonviable livers, direct procurement costs, coordinator salaries, professional education, and local cost of living. A cost curve estimated the relationship between the cost of livers and the number of locally procured livers. The average cost of procured livers by individual OPO‐year varied widely from $11 393 to $65 556 (average $31 659) over the six study years. An increase in the overall number of procured livers was associated with lower direct costs, administrative, and procurement overhead costs, but this association differed for imported livers. Cost per local liver decreased linearly for each additional liver, while importing more livers was only cost saving until 200 livers, with imported livers costing more ($39K vs. $31.7K). The largest predictor of variation in cost was the aggregate of direct costs (e.g., hospital costs) to recover the organ (57%). Cost increases were 2.5% per year (+$766/year). This information may be valuable in determining how OPOs might improve service to transplant centers and the patients they serve. [ABSTRACT FROM AUTHOR]

Published
2024
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36. A Top-Down Proteomic Assay to Evaluate KRAS4B-Compound Engagement

Author

D’Ippolito, Robert A., primary, Rabara, Dana, additional, Blanco, Maria Abreu, additional, Alberico, Emily, additional, Drew, Matthew R., additional, Ramakrishnan, Nitya, additional, Sontan, Dara, additional, Widmeyer, Stephanie R. T., additional, Scheidemantle, Grace M., additional, Messing, Simon, additional, Turner, David, additional, Arkin, Michelle, additional, Maciag, Anna E., additional, Stephen, Andrew G., additional, Esposito, Dominic, additional, McCormick, Frank, additional, Nissley, Dwight V., additional, and DeHart, Caroline J., additional

Published
2024
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39. A Top-Down Proteomic Assay to Evaluate KRAS4B-Compound Engagement.

Author

D'Ippolito, Robert A., Rabara, Dana, Blanco, Maria Abreu, Alberico, Emily, Drew, Matthew R., Ramakrishnan, Nitya, Sontan, Dara, Widmeyer, Stephanie R. T., Scheidemantle, Grace M., Messing, Simon, Turner, David, Arkin, Michelle, Maciag, Anna E., Stephen, Andrew G., Esposito, Dominic, McCormick, Frank, Nissley, Dwight V., and DeHart, Caroline J.

Published
2024
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40. Long-term ecological research in freshwaters enabled by regional biodiversity collections, stable isotope analysis, and environmental informatics

Author

Turner, Thomas F, primary, Bart Jr, Henry L, additional, McCormick, Frank, additional, Besser, Alexi C, additional, Bowes, Rachel E, additional, Capps, Krista A, additional, DeArmon, Emily S, additional, Dillman, Casey B, additional, Driscoll, Katelyn P, additional, Dugger, Aubrey, additional, Hamilton, Gregor L, additional, Harris, Phillip M, additional, Hendrickson, Dean A, additional, Hoffman, Joel, additional, Knouft, Jason H, additional, Lepak, Ryan F, additional, López-Fernández, Hernán, additional, Montaña, Carmen G, additional, Newsome, Seth D, additional, Pease, Allison A, additional, Smith, W Leo, additional, Taylor, Christopher A, additional, and Welicky, Rachel L, additional

Published
2023
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41. Abstract A016: Expanded RAS proteoform landscape in malignant cell lines revealed by top-down mass spectrometry

Author

DeHart, Caroline J., primary, D'Ippolito, Robert A., additional, Sharma, Kanika, additional, Fer, Nicole, additional, Smith, Brian, additional, Meyer, Mackenzie, additional, Eury, Scott, additional, Neish, Abigail, additional, Powell, Katie, additional, Wall, Vanessa, additional, Burgan, William, additional, Esposito, Dominic, additional, Maciag, Anna E., additional, McCormick, Frank, additional, and Nissley, Dwight V., additional

Published
2023
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42. Abstract A018: A top-down proteomic assay to evaluate KRAS4B-compound engagement

Author

D'Ippolito, Robert A., primary, DeHart, Caroline J., additional, Rabara, Dana, additional, Blanco, Maria Abreu, additional, Alberico, Emily, additional, Ramakrishnan, Nitya, additional, Widmeyer, Stephanie, additional, Messing, Simon, additional, Turner, David, additional, Arkin, Michelle, additional, Maciag, Anna, additional, Stephen, Andrew, additional, Esposito, Dominic, additional, McCormick, Frank, additional, and Nissley, Dwight V., additional

Published
2023
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47. Abstract A028: An isogenic H/N/KRAS-less mouse embryonic fibroblast cell line panel derived from a size sorted diploid clonal parent

Author

Burgan, William E., primary, Fer, Nicole, additional, Powell, Katie, additional, Xu, Bingfang, additional, Meyer, Mackenzie, additional, Eury, Scott, additional, Neish, Abigail, additional, Soppet, Daniel, additional, Esposito, Dominic, additional, McCormick, Frank, additional, and Nissley, Dwight V., additional

Published
2023
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48. Report From a Multidisciplinary Symposium on the Future of Living Kidney Donor Transplantation.

Author

Peters, Thomas G., Fung, John J., Radcliffe-Richards, Janet, Satel, Sally, Roth, Alvin E., McCormick, Frank, Gershun, Martha, Matas, Arthur J., Roberts, John P., Morrison, Josh, Chertow, Glenn M., Lee, Laurie D., Held, Philip J., and Ojo, Akinlolu

Subjects
HEALTH policy, CHRONIC kidney failure, HEALTH services accessibility, ETHICS, CONFERENCES & conventions, KIDNEY transplantation, MEDICAL care costs, COST benefit analysis, REWARD (Psychology), PATIENT education, ORGAN donors, PATIENT safety
Abstract

Virtually all clinicians agree that living donor renal transplantation is the optimal treatment for permanent loss of kidney function. Yet, living donor kidney transplantation has not grown in the United States for more than 2 decades. A virtual symposium gathered experts to examine this shortcoming and to stimulate and clarify issues salient to improving living donation. The ethical principles of rewarding kidney donors and the limits of altruism as the exclusive compelling stimulus for donation were emphasized. Concepts that donor incentives could save up to 40 000 lives annually and considerable taxpayer dollars were examined, and survey data confirmed voter support for donor compensation. Objections to rewarding donors were also presented. Living donor kidney exchanges and limited numbers of deceased donor kidneys were reviewed. Discussants found consensus that attempts to increase living donation should include removing artificial barriers in donor evaluation, expansion of living donor chains, affirming the safety of live kidney donation, and assurance that donors incur no expense. If the current legal and practice standards persist, living kidney donation will fail to achieve its true potential to save lives. [ABSTRACT FROM AUTHOR]

Published
2023
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49. Supplementary Data from Inhibition of MET Signaling with Ficlatuzumab in Combination with Chemotherapy in Refractory AML: Clinical Outcomes and High-Dimensional Analysis

Author

Wang, Victoria E., primary, Blaser, Bradley W., primary, Patel, Ravi K., primary, Behbehani, Gregory K., primary, Rao, Arjun A., primary, Durbin-Johnson, Blythe, primary, Jiang, Tommy, primary, Logan, Aaron C., primary, Settles, Matthew, primary, Mannis, Gabriel N., primary, Olin, Rebecca, primary, Damon, Lloyd E., primary, Martin, Thomas G., primary, Sayre, Peter H., primary, Gaensler, Karin M., primary, McMahon, Emma, primary, Flanders, Michael, primary, Weinberg, Vivian, primary, Ye, Chun J., primary, Carbone, David P., primary, Munster, Pamela N., primary, Fragiadakis, Gabriela K., primary, McCormick, Frank, primary, and Andreadis, Charalambos, primary

Published
2023
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50. Data from Inhibition of MET Signaling with Ficlatuzumab in Combination with Chemotherapy in Refractory AML: Clinical Outcomes and High-Dimensional Analysis

Author

Wang, Victoria E., primary, Blaser, Bradley W., primary, Patel, Ravi K., primary, Behbehani, Gregory K., primary, Rao, Arjun A., primary, Durbin-Johnson, Blythe, primary, Jiang, Tommy, primary, Logan, Aaron C., primary, Settles, Matthew, primary, Mannis, Gabriel N., primary, Olin, Rebecca, primary, Damon, Lloyd E., primary, Martin, Thomas G., primary, Sayre, Peter H., primary, Gaensler, Karin M., primary, McMahon, Emma, primary, Flanders, Michael, primary, Weinberg, Vivian, primary, Ye, Chun J., primary, Carbone, David P., primary, Munster, Pamela N., primary, Fragiadakis, Gabriela K., primary, McCormick, Frank, primary, and Andreadis, Charalambos, primary

Published
2023
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