Clinical Pathology - Research Publications

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Author: George, Amee × Start date: 2020 × End date: 2022 ×

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    Nuclear stabilization of p53 requires a functional nucleolar surveillance pathway
    Hannan, KM ; Soo, P ; Wong, MS ; Lee, JK ; Hein, N ; Poh, P ; Wysoke, KD ; Williams, TD ; Montellese, C ; Smith, LK ; Al-Obaidi, SJ ; Nunez-Villacis, L ; Pavy, M ; He, J-S ; Parsons, KM ; Loring, KE ; Morrison, T ; Diesch, J ; Burgio, G ; Ferreira, R ; Feng, Z-P ; Gould, CM ; Madhamshettiwar, PB ; Flygare, J ; Gonda, TJ ; Simpson, KJ ; Kutay, U ; Pearson, RB ; Engel, C ; Watkins, NJ ; Hannan, RD ; George, AJ (CELL PRESS, 2022-11-01)
    The nucleolar surveillance pathway monitors nucleolar integrity and responds to nucleolar stress by mediating binding of ribosomal proteins to MDM2, resulting in p53 accumulation. Inappropriate pathway activation is implicated in the pathogenesis of ribosomopathies, while drugs selectively activating the pathway are in trials for cancer. Despite this, the molecular mechanism(s) regulating this process are poorly understood. Using genome-wide loss-of-function screens, we demonstrate the ribosome biogenesis axis as the most potent class of genes whose disruption stabilizes p53. Mechanistically, we identify genes critical for regulation of this pathway, including HEATR3. By selectively disabling the nucleolar surveillance pathway, we demonstrate that it is essential for the ability of all nuclear-acting stresses, including DNA damage, to induce p53 accumulation. Our data support a paradigm whereby the nucleolar surveillance pathway is the central integrator of stresses that regulate nuclear p53 abundance, ensuring that ribosome biogenesis is hardwired to cellular proliferative capacity.
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    Identification and characterization of a novel SNAT2 (SLC38A2) inhibitor reveals synergy with glucose transport inhibition in cancer cells
    Gauthier-Coles, G ; Broer, A ; McLeod, MD ; George, AJ ; Hannan, RD ; Broer, S (FRONTIERS MEDIA SA, 2022-09-21)
    SNAT2 (SLC38A2) is a sodium-dependent neutral amino acid transporter, which is important for the accumulation of amino acids as nutrients, the maintenance of cellular osmolarity, and the activation of mTORC1. It also provides net glutamine for glutaminolysis and consequently presents as a potential target to treat cancer. A high-throughput screening assay was developed to identify new inhibitors of SNAT2 making use of the inducible nature of SNAT2 and its electrogenic mechanism. Using an optimized FLIPR membrane potential (FMP) assay, a curated scaffold library of 33934 compounds was screened to identify 3-(N-methyl (4-methylphenyl)sulfonamido)-N-(2-trifluoromethylbenzyl)thiophene-2-carboxamide as a potent inhibitor of SNAT2. In two different assays an IC50 of 0.8-3 µM was determined. The compound discriminated against the close transporter homologue SNAT1. MDA-MB-231 breast cancer and HPAFII pancreatic cancer cell lines tolerated the SNAT2 inhibitor up to a concentration of 100 µM but in combination with tolerable doses of the glucose transport inhibitor Bay-876, proliferative growth of both cell lines was halted. This points to synergy between inhibition of glycolysis and glutaminolysis in cancer cells.
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    Cohesin mutations are synthetic lethal with stimulation of WNT signaling
    Chin, CV ; Antony, J ; Ketharnathan, S ; Labudina, A ; Gimenez, G ; Parsons, KM ; He, J ; George, AJ ; Pallotta, MM ; Musio, A ; Braithwaite, A ; Guilford, P ; Hannan, RD ; Horsfield, JA (ELIFE SCIENCES PUBLICATIONS LTD, 2020-12-07)
    Mutations in genes encoding subunits of the cohesin complex are common in several cancers, but may also expose druggable vulnerabilities. We generated isogenic MCF10A cell lines with deletion mutations of genes encoding cohesin subunits SMC3, RAD21, and STAG2 and screened for synthetic lethality with 3009 FDA-approved compounds. The screen identified several compounds that interfere with transcription, DNA damage repair and the cell cycle. Unexpectedly, one of the top 'hits' was a GSK3 inhibitor, an agonist of Wnt signaling. We show that sensitivity to GSK3 inhibition is likely due to stabilization of β-catenin in cohesin-mutant cells, and that Wnt-responsive gene expression is highly sensitized in STAG2-mutant CMK leukemia cells. Moreover, Wnt activity is enhanced in zebrafish mutant for cohesin subunits stag2b and rad21. Our results suggest that cohesin mutations could progress oncogenesis by enhancing Wnt signaling, and that targeting the Wnt pathway may represent a novel therapeutic strategy for cohesin-mutant cancers.
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    A Dual-Antigen Enzyme-Linked Immunosorbent Assay Allows the Assessment of Severe Acute Respiratory Syndrome Coronavirus 2 Antibody Seroprevalence in a Low-Transmission Setting
    Hicks, SM ; Pohl, K ; Neeman, T ; McNamara, HA ; Parsons, KM ; He, J-S ; Ali, SA ; Nazir, S ; Rowntree, LC ; Nguyen, THO ; Kedzierska, K ; Doolan, DL ; Vinuesa, CG ; Cook, MC ; Coatsworth, N ; Myles, PS ; Kurth, F ; Sander, LE ; Mann, GJ ; Gruen, RL ; George, AJ ; Gardiner, EE ; Cockburn, IA (OXFORD UNIV PRESS INC, 2021-01-01)
    Estimates of seroprevalence of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) antibodies have been hampered by inadequate assay sensitivity and specificity. Using an enzyme-linked immunosorbent assay-based approach that combines data about immunoglobulin G responses to both the nucleocapsid and spike receptor binding domain antigens, we show that excellent sensitivity and specificity can be achieved. We used this assay to assess the frequency of virus-specific antibodies in a cohort of elective surgery patients in Australia and estimated seroprevalence in Australia to be 0.28% (95% Confidence Interval, 0-1.15%). These data confirm the low level of transmission of SARS-CoV-2 in Australia before July 2020 and validate the specificity of our assay.
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    A dual antigen ELISA allows the assessment of SARS-CoV-2 antibody seroprevalence in a low transmission setting
    Hicks, S ; Pohl, K ; Neeman, T ; McNamara, H ; Parsons, K ; He, J-S ; Ali, S ; Nazir, S ; Rowntree, L ; Nguyen, T ; Kedzierska, K ; Doolan, D ; Vinueas, C ; Cook, M ; Coatsworth, N ; Myles, P ; Kurth, F ; Sander, L ; Mann, G ; Gruen, R ; George, A ; Gardiner, E ; Cockburn, I ; the SARS-CoV-2 Testing in Elective Surgery Collaborators, (Cold Spring Harbor Laboratory, 2020)
    Estimates of seroprevalence of SARS-CoV-2 antibodies have been hampered by inadequate assay sensitivity and specificity. Using an ELISA-based approach to that combines data about IgG responses to both the Nucleocapsid and Spike-receptor binding domain antigens, we show that near-optimal sensitivity and specificity can be achieved. We used this assay to assess the frequency of virus-specific antibodies in a cohort of elective surgery patients in Australia and estimated seroprevalence in Australia to be 0.28% (0 to 0.72%). These data confirm the low level of transmission of SARS-CoV-2 in Australia before July 2020 and validate the specificity of our assay.