keyword
https://read.qxmd.com/read/38592721/anti-egfr-rechallenge-in-patients-with-refractory-ctdna-ras-braf-wt-metastatic-colorectal-cancer-a-nonrandomized-controlled-trial
#21
JOURNAL ARTICLE
Davide Ciardiello, Erika Martinelli, Teresa Troiani, Gianluca Mauri, Daniele Rossini, Giulia Martini, Stefania Napolitano, Vincenzo Famiglietti, Sara Del Tufo, Gianluca Masi, Daniele Santini, Antonio Avallone, Filippo Pietrantonio, Sara Lonardi, Massimo Di Maio, Maria Giulia Zampino, Nicola Fazio, Alberto Bardelli, Salvatore Siena, Chiara Cremolini, Andrea Sartore-Bianchi, Fortunato Ciardiello
IMPORTANCE: The available evidence regarding anti-epidermal growth factor receptor (EGFR) inhibitor rechallenge in patients with refractory circulating tumor DNA (ctDNA) RAS/BRAF wild-type (wt) metastatic colorectal cancer (mCRC) is derived from small retrospective and prospective studies. OBJECTIVE: To evaluate the efficacy of anti-EGFR rechallenge in patients with refractory ctDNA RAS/BRAF wt mCRC. DESIGN, SETTING, AND PARTICIPANTS: This nonrandomized controlled trial used a pooled analysis of individual patient data from patients with RAS/BRAF wt ctDNA mCRC enrolled in 4 Italian trials (CAVE, VELO, CRICKET, and CHRONOS) and treated with anti-EGFR rechallenge between 2015 and 2022 (median [IQR] follow-up, 28...
April 1, 2024: JAMA Network Open
https://read.qxmd.com/read/38589732/rhes-a-striatal-enriched-protein-regulates-post-translational-small-ubiquitin-like-modifier-sumo-modification-of-nuclear-proteins-and-alters-gene-expression
#22
JOURNAL ARTICLE
Oscar Rivera, Manish Sharma, Sunayana Dagar, Neelam Shahani, Uri Nimrod Ramĺrez-Jarquĺn, Gogce Crynen, Pabalu Karunadharma, Francis McManus, Eric Bonneil, Thibault Pierre, Srinivasa Subramaniam
Rhes (Ras homolog enriched in the striatum), a multifunctional protein that regulates striatal functions associated with motor behaviors and neurological diseases, can shuttle from cell to cell via the formation of tunneling-like nanotubes (TNTs). However, the mechanisms by which Rhes mediates diverse functions remain unclear. Rhes is a small GTPase family member which contains a unique C-terminal Small Ubiquitin-like Modifier (SUMO) E3-like domain that promotes SUMO post-translational modification of proteins (SUMOylation) by promoting "cross-SUMOylation" of the SUMO enzyme SUMO E1 (Aos1/Uba2) and SUMO E2 ligase (Ubc-9)...
April 8, 2024: Cellular and Molecular Life Sciences: CMLS
https://read.qxmd.com/read/38586390/cell-cycle-associated-protein-1-associates-with-immune-infiltration-and-ferroptosis-in-gastrointestinal-cancer
#23
JOURNAL ARTICLE
Yan Gao, Ruimin Wu, Zhijun Pei, Changbin Ke, Daobing Zeng, Xiaohui Li, Yanmin Zhang
BACKGROUND: Cell Cycle-Associated Protein 1 (CAPRIN1) play an important role in cell proliferation, oxidative stress, and inflammatory response. Nonetheless, its role in tumor immunity and ferroptosis is largely unknown in gastrointestinal cancer patients. METHODS: Through comprehensive bioinformatics, we investigate CAPRIN1 expression patterns and its role in diagnosis, functional signaling pathways, tumor immune infiltration and ferroptosis of different gastrointestinal cancer subtypes...
April 15, 2024: Heliyon
https://read.qxmd.com/read/38583246/targeted-genetic-and-small-molecule-disruption-of-n-ras-caax-cleavage-alters-its-localization-and-oncogenic-potential
#24
JOURNAL ARTICLE
Emily R Hildebrandt, Shaneela A Hussain, Michelle A Sieburg, Rajani Ravishankar, Nadeem Asad, Sangram Gore, Takahiro Ito, James L Hougland, Timothy M Dore, Walter K Schmidt
Ras GTPases and other CaaX proteins undergo multiple post-translational modifications at their carboxyl-terminus. These events initiate with prenylation of a cysteine and are followed by endoproteolytic removal of the 'aaX' tripeptide and carboxylmethylation. Some CaaX proteins are only subject to prenylation, however, due to the presence of an uncleavable sequence. In this study, uncleavable sequences were used to stage Ras isoforms in a farnesylated and uncleaved state to address the impact of CaaX proteolysis on protein localization and function...
March 27, 2024: Bioorganic Chemistry
https://read.qxmd.com/read/38581120/a-new-tandem-repeat-enriched-lncrna-xloc_008672-promotes-gastric-carcinogenesis-by-regulating-g3bp1-expression
#25
JOURNAL ARTICLE
Li Li, Shijun Yu, Ning Dou, Xiao Wang, Yong Gao, Yandong Li
Aberrant expression of forkhead box transcription factor 1 (FOXM1) plays critical roles in a variety of human malignancies and predicts poor prognosis. However, little is known about the crosstalk between FOXM1 and long noncoding RNAs (lncRNAs) in tumorigenesis. The present study identifies a previously uncharacterized lncRNA XLOC_008672 in gastric cancer (GC), which is regulated by FOXM1 and possesses multiple copies of tandem repetitive sequences. LncRNA microarrays are used to screen differentially expressed lncRNAs in FOXM1 knockdown GC cells, and then the highest fold downregulation lncRNA XLOC_008672 is screened out...
April 5, 2024: Cancer Science
https://read.qxmd.com/read/38578356/astaxanthin-and-dha-supplementation-modulates-the-maternal-undernutrition-induced-impairment-of-cognitive-behavior-and-synaptic-plasticity-in-adult-life-of-offspring-s-exploring-the-molecular-mechanism
#26
JOURNAL ARTICLE
Megha Bhat Agni, Pramukh Subrahmanya Hegde, Praveen Rai, Monika Sadananda, Damodara Gowda K M
Maternal nutrition was recognized as a significant part of brain growth and maturation in most mammalian species. Timely intervention with suitable nutraceuticals would provide long-term health benefits. We aim to unravel the molecular mechanisms of perinatal undernutrition-induced impairments in cognition and synaptic plasticity, employing animal model based on dietary nutraceutical supplementation. We treated undernourished dams at their gestational, lactational, and at both the time point with Astaxanthin (AsX) and Docosahexaenoic acid (DHA), and their pups were used as experimental animals...
April 5, 2024: Molecular Neurobiology
https://read.qxmd.com/read/38577921/adipose-tissue-plasticity-mediated-by-the-counterregulatory-axis-of-the-renin-angiotensin-system-role-of-mas-and-mrgd-receptors
#27
REVIEW
Ana Beatriz Proença, Gabriela Rodrigues Medeiros, Guilherme Dos Santos Reis, Luiza da França Losito, Luiza Mazzali Ferraz, Thereza Cristina Lonzetti Bargut, Nícia Pedreira Soares, Beatriz Alexandre-Santos, Maria Jose Campagnole-Santos, D'Angelo Carlo Magliano, Antonio Claudio Lucas da Nobrega, Robson Augusto Souza Santos, Eliete Dalla Corte Frantz
The renin-angiotensin system (RAS) is an endocrine system composed of two main axes: the classical and the counterregulatory, very often displaying opposing effects. The classical axis, primarily mediated by angiotensin receptors type 1 (AT1R), is linked to obesity-associated metabolic effects. On the other hand, the counterregulatory axis appears to exert antiobesity effects through the activation of two receptors, the G protein-coupled receptor (MasR) and Mas-related receptor type D (MrgD). The local RAS in adipose organ has prompted extensive research into white adipose tissue and brown adipose tissue (BAT), with a key role in regulating the cellular and metabolic plasticity of these tissues...
April 5, 2024: Journal of Cellular Physiology
https://read.qxmd.com/read/38576721/genetically-encodable-biosensors-for-ras-activity
#28
REVIEW
Ryan Weeks, Sohum Mehta, Jin Zhang
Genetically encoded Ras biosensors have been instrumental in illuminating the spatiotemporal dynamics of Ras activity since the beginning of the imaging revolution of the early 21st century. In general, these sensors employ Ras sensing units coupled with fluorescent proteins. These biosensors have not only helped elucidate Ras signalling dynamics at the plasma membrane but also revealed novel roles for Ras signalling within subcellular compartments such as the Golgi apparatus. In this review, we discuss the different classes of biosensors used to measure Ras activity and discuss their importance in uncovering new roles for Ras activity in cellular signalling and behavior...
April 3, 2024: RSC chemical biology
https://read.qxmd.com/read/38576709/targeting-kras-mutations-in-pancreatic-cancer-opportunities-for-future-strategies
#29
REVIEW
Anna Linehan, Mary O'Reilly, Ray McDermott, Grainne M O'Kane
Targeting the RAS pathway remains the holy grail of precision oncology. In the case of pancreatic ductal adenocarcinomas (PDAC), 90-92% harbor mutations in the oncogene KRAS, triggering canonical MAPK signaling. The smooth structure of the altered KRAS protein without a binding pocket and its affinity for GTP have, in the past, hampered drug development. The emergence of KRASG12C covalent inhibitors has provided renewed enthusiasm for targeting KRAS. The numerous pathways implicated in RAS activation do, however, lead to the development of early resistance...
2024: Frontiers in Medicine
https://read.qxmd.com/read/38574162/point-mutations-in-arf1-reveal-cooperative-effects-of-the-n-terminal-extension-and-myristate-for-gtpase-activating-protein-catalytic-activity
#30
JOURNAL ARTICLE
Eric M Rosenberg, Xiaoying Jian, Olivier Soubias, Rebekah A Jackson, Erin Gladu, Emily Andersen, Lothar Esser, Alexander J Sodt, Di Xia, R Andrew Byrd, Paul A Randazzo
The ADP-ribosylation factors (Arfs) constitute a family of small GTPases within the Ras superfamily, with a distinguishing structural feature of a hypervariable N-terminal extension of the G domain modified with myristate. Arf proteins, including Arf1, have roles in membrane trafficking and cytoskeletal dynamics. While screening for Arf1:small molecule co-crystals, we serendipitously solved the crystal structure of the non-myristoylated engineered mutation [L8K]Arf1 in complex with a GDP analogue. Like wild-type (WT) non-myristoylated Arf1•GDP, we observed that [L8K]Arf1 exhibited an N-terminal helix that occludes the hydrophobic cavity that is occupied by the myristoyl group in the GDP-bound state of the native protein...
2024: PloS One
https://read.qxmd.com/read/38570469/flag-kras4b-as-a-model-system-for-kras4b-proteoform-and-ptm-evaluation-by-mass-spectrometry
#31
JOURNAL ARTICLE
Robert A D'Ippolito, Grace M Scheidemantle, Brian P Smith, Katie Powell, Scott Eury, Abigail Neish, Jennifer Mehalko, Lauren Beaumont, Nicole Fer, Vanessa Wall, William Burgan, Anna E Maciag, Dominic Esposito, Caroline J DeHart
Prior analysis of intact and modified protein forms (proteoforms) of KRAS4B isolated from cell lines and tumor samples by top-down mass spectrometry revealed the presence of novel posttranslational modifications (PTMs) and potential evidence of context-specific KRAS4B modifications. However, low endogenous proteoform signal resulted in ineffective characterization, making it difficult to visualize less abundant PTMs or perform follow-up PTM validation using standard proteomic workflows. The NCI RAS Initiative has developed a model system, whereby KRAS4B bearing an N-terminal FLAG tag can be stably expressed within a panel of cancer cell lines...
2024: Methods in Molecular Biology
https://read.qxmd.com/read/38570468/a-method-to-conditionally-measure-target-engagement-at-intracellular-ras-and-raf-complexes
#32
JOURNAL ARTICLE
James D Vasta, Ani Michaud, J Aaron Crapster, Matthew B Robers
Dysfunction of the RAS/mitogen-activated protein kinase (MAPK) pathway is a common driver of human cancers. As such, both the master regulator of the pathway, RAS, and its proximal kinase effectors, RAFs, have been of interest as drug targets for decades. Importantly, signaling within the RAS/MAPK pathway is highly coordinated due to the formation of a higher-order complex called the RAS/RAF signalosome, which may minimally contain dimers of both RAS and RAF protomers. In the disease state, RAS and RAF assemble in homo- and/or heterodimeric forms...
2024: Methods in Molecular Biology
https://read.qxmd.com/read/38570466/flim-fret-protein-protein-interaction-assay
#33
JOURNAL ARTICLE
Pedro Andrade Bonilla, Rebika Shrestha
Fluorescence lifetime imaging performed under FRET conditions between two interacting molecules is a sensitive and robust way to quantify intermolecular interactions in cells. The fluorescence lifetime, an inherent property of the fluorophore, remains unaffected by factors such as concentration, laser intensity, and other photophysical artifacts. In the context of FLIM-FRET, the focus lies on measuring the fluorescence lifetime of the donor molecule, which diminishes upon interaction with a neighboring acceptor molecule...
2024: Methods in Molecular Biology
https://read.qxmd.com/read/38570465/studying-ras-interactions-in-live-cells-with-bret
#34
JOURNAL ARTICLE
John Columbus, Thomas Turbyville
Bioluminescence resonance energy transfer (BRET) is a valuable technique for studying protein-protein interactions (PPIs) within live cells (Pfleger and Eidne, Nat Methods 3:165-174, 2006). Among the various BRET methodologies, a recent addition called NanoBRET has emerged, leveraging advancements in donor and acceptor technologies (Machleidt and Woodroofe, ACS Chem Biol 10:1797-1804, 2015). In this study, we present a developed methodology designed to measure PPIs involving the RAS protein family and their effectors and interactors at the plasma membrane...
2024: Methods in Molecular Biology
https://read.qxmd.com/read/38570464/real-time-monitoring-of-ras-activity-using-in-vitro-and-in-cell-nmr-spectroscopy
#35
JOURNAL ARTICLE
Qingci Zhao, Ichio Shimada, Noritaka Nishida
The activation level of RAS can be determined by GTP hydrolysis rate (khy ) and GDP-GTP exchange rates (kex ). Either impaired GTP hydrolysis or enhanced GDP-GTP exchange causes the aberrant activation of RAS in oncogenic mutants. Therefore, it is important to quantify the khy and kex for understanding the mechanisms of RAS oncogenesis and drug development. Conventional methods have individually measured the kex and khy of RAS. However, within the intracellular environment, GTP hydrolysis and GDP-GTP exchange reactions occur simultaneously under conditions where GTP concentration is kept constant...
2024: Methods in Molecular Biology
https://read.qxmd.com/read/38570462/probing-ras-function-using-monobody-and-nanobit-technologies
#36
JOURNAL ARTICLE
Michael Whaby, Rakesh Sathish Nair, John P O'Bryan
Missense mutations in the RAS family of oncogenes (HRAS, KRAS, and NRAS) are present in approximately 20% of human cancers, making RAS a valuable therapeutic target (Prior et al., Cancer Res 80:2969-2974, 2020). Although decades of research efforts to develop therapeutic inhibitors of RAS were unsuccessful, there has been success in recent years with the entrance of FDA-approved KRASG12C -specific inhibitors to the clinic (Skoulidis et al., N Engl J Med 384:2371-2381, 2021; Jänne et al., N Engl J Med 387:120-131, 2022)...
2024: Methods in Molecular Biology
https://read.qxmd.com/read/38570461/profiling-complex-ras-effector-interactions-using-nmr-spectroscopy
#37
JOURNAL ARTICLE
Regina Strakhova, Matthew J Smith
Knowledge of how effectors interact with RAS GTPases is key to understanding how these switch-like proteins function in cells. Effectors bind specifically to GTP-loaded RAS using RAS association (RA) or RAS binding domains (RBDs) that show wide-ranging affinities and thermodynamic characteristics. Both normal development and RAS-induced tumorigenesis depend on multiple distinct effector proteins that are frequently co-expressed and co-localized, suggesting an antagonistic nature to signaling whereby multiple proteins compete for a limited pool of activated GTPase...
2024: Methods in Molecular Biology
https://read.qxmd.com/read/38570460/biophysical-characterization-of-ras-sos-complexes-by-native-mass-spectrometry
#38
JOURNAL ARTICLE
Sangho Yun, Elena Scott, Arthur Laganowsky
RAS is regulated by specific guanine nucleotide exchange factors, such as Son of Sevenless (SOS), that activates RAS by facilitating the exchange of inactive, GDP-bound RAS with GTP. The catalytic activity of SOS is known to be allosterically modulated by an active, GTP-bound RAS. However, it remains poorly understood how oncogenic RAS mutants interact with SOS and modulate its activity. In this chapter, we describe the application of native mass spectrometry (MS) to monitor the assembly of the catalytic domain of SOS (SOScat ) with RAS and cancer-associated mutants...
2024: Methods in Molecular Biology
https://read.qxmd.com/read/38570459/kras4b-raf-1-homogenous-time-resolved-fluorescence-resonance-energy-transfer-assay-for-drug-discovery
#39
JOURNAL ARTICLE
Erik K Larsen, Maria Abreu-Blanco, Dana Rabara, Andrew G Stephen
Homogenous time-resolved FRET (HTRF) assays have become one of the most popular tools for pharmaceutical drug screening efforts over the last two decades. Large Stokes shifts and long fluorescent lifetimes of lanthanide chelates lead to robust signal to noise, as well as decreased false positive rates compared to traditional assay techniques. In this chapter, we describe an HTRF protein-protein interaction (PPI) assay for the KRAS4b G-domain in the GppNHp-bound state and the RAF-1-RBD currently used for drug screens...
2024: Methods in Molecular Biology
https://read.qxmd.com/read/38570455/affinity-measurement-of-non-covalent-interactions-of-the-covalent-kras-g12c-gdp-inhibitor-mrtx849-to-ras-isoforms-using-surface-plasmon-resonance
#40
JOURNAL ARTICLE
Patrick Alexander, Andrew G Stephen
Surface plasmon resonance (SPR) is an optical effect at an electron-rich surface that enables affinity measurements of biomolecules in real time. It is label free and versatile, not limited to proteins, nucleic acids, and small molecules. SPR is a widely accepted method to measure not only affinity of molecular interactions but also association and dissociation rates of such interactions. In this chapter, we describe a general method to measure the affinity of a small molecule drug, MRTX849, to GDP bound HRAS, KRAS, and NRAS...
2024: Methods in Molecular Biology
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