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2. Corrigendum

Author

Zhan, Yao, Guo, Jun, Yang, William, Goncalves, Christophe, Rzymski, Tomasz, Dreas, Agnieszka, Zylkiewicz, Eliza, Mikulski, Maciej, Brzozka, Krzysztof, Golas, Aniela, Kong, Yan, Ma, Meng, Huang, Fan, Huor, Bonnie, Guo, Qianyu, da Silva, Sabrina Daniela, Torres, Jose, Cai, Yutian, Topisirovic, Ivan, Su, Jie, Bijian, Krikor, Alaoui-Jamali, Moulay A., Huang, Sidong, Journe, Fabrice, Ghanem, Ghanem E., Miller, Wilson H., Jr., and del Rincon, Sonia V.

Subjects
Health care industry
Abstract

Original citation: J Clin Invest. 2017;127(11):4179-4192. https://doi.org/10.1172/JCI91258. Citation for this corrigendum: J Clin Invest. 2024;134(8):e181338. https://doi.org/10.1172/JCI181338. The authors recently became aware that in the original Figure 2, A and C, [...]

Published
2024
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3. Large-scale Gender/Age Prediction of Tumblr Users

Author

Zhan, Yao, Hu, Changwei, Hu, Yifan, Kasturi, Tejaswi, Ramasamy, Shanmugam, Gillingham, Matt, and Yamamoto, Keith

Subjects
Computer Science - Machine Learning, Computer Science - Social and Information Networks, Statistics - Machine Learning
Abstract

Tumblr, as a leading content provider and social media, attracts 371 million monthly visits, 280 million blogs and 53.3 million daily posts. The popularity of Tumblr provides great opportunities for advertisers to promote their products through sponsored posts. However, it is a challenging task to target specific demographic groups for ads, since Tumblr does not require user information like gender and ages during their registration. Hence, to promote ad targeting, it is essential to predict user's demography using rich content such as posts, images and social connections. In this paper, we propose graph based and deep learning models for age and gender predictions, which take into account user activities and content features. For graph based models, we come up with two approaches, network embedding and label propagation, to generate connection features as well as directly infer user's demography. For deep learning models, we leverage convolutional neural network (CNN) and multilayer perceptron (MLP) to prediction users' age and gender. Experimental results on real Tumblr daily dataset, with hundreds of millions of active users and billions of following relations, demonstrate that our approaches significantly outperform the baseline model, by improving the accuracy relatively by 81% for age, and the AUC and accuracy by 5\% for gender.

Published
2020

4. Abundant dynamics of group velocity locked vector solitons from Er-doped fiber laser based on GO/PVA film

Author

Lin Ja-Hon, Zhang Zhan-Yao, Li Zhen-Ying, Peng Peng-Chun, Song Yu-Feng, and Zhang Han

Subjects
dual wavelength, graphene oxide, group velocity locked vector solitons, lyot filter, multiple soliton, Physics, QC1-999
Abstract

With the insertion a segment of polarization-maintaining fiber (PMF) inside the cavity, abundant dynamics of group velocity locked vector solitons (GVLVSs) in Er-doped fiber laser have been investigated by using graphene oxide/polyvinyl alcohol (GO/PVA) film as a saturable absorber (SA). The generated Kelly sidebands in emission spectra reveal peak-valley or valley-peak alternation and slightly shift in two orthogonal components, which are the characteristics of GVLVSs. Through proper adjustment of polarization controllers (PCs) inside the EDFLs cavity, versatile vector soliton dynamics such as polarization locked GVLVSs (PL-GVLVSs), polarization rotation GVLVSs (PR-GVLVSs), dual wavelength GVLVSs, bound state GVLVSs, bunch GVLVSs and harmonic mode-locking GVLVSs (HML-GVLVSs) have been observed. The separation between two emission peaks from the dual wavelength GVLVSs was controlled by the Lyot filter and related to the insertion length of PMF inside the cavity. Unlike PL-GVLVSs, the period-doubling phenomenon has been found in two orthogonal components of the PR-GVLVSs. Besides, the bound state GVLVSs were generated showing strongly modulated interference fringes in emission spectrum. For the bunch and HML GVLVSs, the number of solitons inside the cavity increased with the pump power, and it showed the quintuple solitons and the 7th HML-GVLVSs at the highest pump power.

Published
2022
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5. Correction: MNK1/NODAL Signaling Promotes Invasive Progression of Breast Ductal Carcinoma In Situ

Author

Guo, Qianyu, primary, Li, Vivian Z., additional, Nichol, Jessica N., additional, Huang, Fan, additional, Yang, William, additional, Preston, Samuel E.J., additional, Talat, Zahra, additional, Lefrère, Hanne, additional, Yu, Henry, additional, Zhang, Guihua, additional, Basik, Mark, additional, Gonçalves, Christophe, additional, Zhan, Yao, additional, Plourde, Dany, additional, Su, Jie, additional, Torres, Jose, additional, Marques, Maud, additional, Habyan, Sara Al, additional, Bijian, Krikor, additional, Amant, Frédéric, additional, Wichter, Michael, additional, Behbod, Fariba, additional, McCaffrey, Luke, additional, Alaoui-Jamali, Moulay, additional, Giannakopoulos, Nadia V., additional, Brackstone, Muriel, additional, Postovit, Lynne-Marie, additional, del Rincón, Sonia V., additional, and Miller, William H., additional

Published
2024
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6. MNK1/2 inhibition limits oncogenicity and metastasis of KIT-mutant melanoma

Author

Zhan, Yao, primary, Guo, Jun, additional, Yang, William, additional, Goncalves, Christophe, additional, Rzymski, Tomasz, additional, Dreas, Agnieszka, additional, Żyłkiewicz, Eliza, additional, Mikulski, Maciej, additional, Brzózka, Krzysztof, additional, Golas, Aniela, additional, Kong, Yan, additional, Ma, Meng, additional, Huang, Fan, additional, Huor, Bonnie, additional, Guo, Qianyu, additional, da Silva, Sabrina Daniela, additional, Torres, Jose, additional, Cai, Yutian, additional, Topisirovic, Ivan, additional, Su, Jie, additional, Bijian, Krikor, additional, Alaoui-Jamali, Moulay A., additional, Huang, Sidong, additional, Journe, Fabrice, additional, Ghanem, Ghanem E., additional, Miller, Wilson H., additional, and del Rincón, Sonia V., additional

Published
2024
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8. Impact of the model of long‐term follow‐up care on adherence to guideline‐recommended surveillance among survivors of adolescent and young adult cancers

Author

Dalia Kagramanov, Rinku Sutradhar, Cindy Lau, Zhan Yao, Jason D. Pole, Nancy N. Baxter, Sumit Gupta, and Paul C. Nathan

Subjects
adolescent and young adult, cancer survivor, follow‐up care, surveillance, survivorship, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Abstract Purpose Adolescent and young adult cancer survivors require lifelong healthcare to address the late effects of therapy. We examined the impact of different provider models of long‐term follow‐up (LTFU) care on adherence to recommended surveillance. Methods We conducted a retrospective cohort study using administrative health databases in Ontario, Canada. Five‐year survivors were identified from IMPACT, a database of patients aged 15–20.9 years at diagnosis of six cancers between 1992 and 2010. We defined three models of LTFU care hierarchically: specialized survivor clinics (SCCs), general cancer clinics (GCCs), and family physician (FP). We assessed adherence to the Children's Oncology Group surveillance guidelines for cardiomyopathy and breast cancer. Multistate models assessed adherence transitions and impacts of LTFU attendance. Results A total of 1574 survivors were followed for a mean of 9.2 years (range 4.3–13.9 years) from index (5‐year survival). The highest level of LTFU attended in the first 2‐years post‐index was a GCC (47%); only 16.7% attended a SCC. By the end of study, 72% no longer attended any of the models of care and only 2% still attended an SCC. Among 188 survivors requiring breast cancer surveillance, 6.9% were adherent to their first required surveillance testing. Attendance at a SCC in the previous year and higher cumulative FP or GCC visits increased the rate of subsequently becoming adherent. Among 857 survivors requiring cardiomyopathy surveillance, 11% were adherent at study entry. Each subsequent SCC visit led to an 11.3% (95% CI: 1.05–1.18) increase in the rate of becoming adherent. Conclusion LTFU attendance and surveillance adherence are sub‐optimal. SCC follow‐up is associated with greater adherence, but few survivors receive such care, and this proportion diminished over time. Interventions are needed to improve LTFU attendance and promote surveillance adherence.

Published
2021
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9. Mutant-selective degradation by BRAF-targeting PROTACs

Author

Shanique Alabi, Saul Jaime-Figueroa, Zhan Yao, Yijun Gao, John Hines, Kusal T. G. Samarasinghe, Lea Vogt, Neal Rosen, and Craig M. Crews

Subjects
Science
Abstract

Hundreds of BRAF mutations have been identified in patients with cancer but currently approved drugs only target BRAF V600 mutants. Here, the authors develop a vemurafenib-based PROTAC that induces degradation of all classes of BRAF mutants without affecting wild-type RAF proteins.

Published
2021
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10. RAF dimer inhibition enhances the antitumor activity of MEK inhibitors in K‐RAS mutant tumors

Author

Xi Yuan, Zhiyu Tang, Rong Du, Zhan Yao, Shing‐Hu Cheung, Xinwen Zhang, Jing Wei, Yuan Zhao, Yunguang Du, Ye Liu, Xiaoxia Hu, Wenfeng Gong, Yong Liu, Yajuan Gao, Zhiyue Huang, Zongfu Cao, Min Wei, Changyou Zhou, Lai Wang, Neal Rosen, Paul D. Smith, and Lusong Luo

Subjects
combination therapy, MEK inhibitor, RAF dimer inhibitor, RAS‐mutated cancer, synergy, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

The mutation of K‐RAS represents one of the most frequent genetic alterations in cancer. Targeting of downstream effectors of RAS, including of MEK and ERK, has limited clinical success in cancer patients with K‐RAS mutations. The reduced sensitivity of K‐RAS‐mutated cells to certain MEK inhibitors (MEKi) is associated with the feedback phosphorylation of MEK by C‐RAF and with the reactivation of mitogen‐activated protein kinase (MAPK) signaling. Here, we report that the RAF dimer inhibitors lifirafenib (BGB‐283) and compound C show a strong synergistic effect with MEKi, including mirdametinib (PD‐0325901) and selumetinib, in suppressing the proliferation of K‐RAS‐mutated non‐small‐cell lung cancer and colorectal cancer (CRC) cell lines. This synergistic effect was not observed with the B‐RAFV600E selective inhibitor vemurafenib. Our mechanistic analysis revealed that RAF dimer inhibition suppresses RAF‐dependent MEK reactivation and leads to the sustained inhibition of MAPK signaling in K‐RAS‐mutated cells. This synergistic effect was also observed in several K‐RAS mutant mouse xenograft models. A pharmacodynamic analysis supported a role for the synergistic phospho‐ERK blockade in enhancing the antitumor activity observed in the K‐RAS mutant models. These findings support a vertical inhibition strategy in which RAF dimer and MEKi are combined to target K‐RAS‐mutated cancers, and have led to a Phase 1b/2 combination therapy study of lifirafenib and mirdametinib in solid tumor patients with K‐RAS mutations and other MAPK pathway aberrations.

Published
2020
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13. Efficacy and Safety of Tranexamic Acid in Reducing Blood Loss of Lower Extremity Osteotomy in Peri‐acetabulum and High Tibia: A Systematic Review and Meta‐analysis

Author

Ru‐zhan Yao, Wei‐qiang Gao, Bing‐wu Wang, Guang‐lin Wang, Cheng‐xi Wu, and Yi‐da A‐mu

Subjects
Blood loss, High tibial osteotomy, Meta‐analysis, Periacetabular osteotomy, Tranexamic acid, Orthopedic surgery, RD701-811
Abstract

Objective To assess the efficacy of tranexamic acid (TXA) in reducing total blood loss and transfusion, and the risk of thromboembolic events in patients undergoing periacetabular osteotomy (PAO) and high tibial osteotomy (HTO). Methods A systematic literature search was performed using PubMed, the Cochrane Central Register of Controlled Trials (CENTRAL), Embase (Ovid), Medline (Ovid), and Web of Science. ClinicalTrials.gov, American Academy of Orthopaedic Surgeons (AAOS), and Orthopaedic Trauma Association (OTA) conference proceedings were also searched to gain more eligible studies. The primary outcome measure was total blood loss and the blood transfusion rate of the TXA group versus control. The meta‐analysis was conducted using the RevMan 5.3 and Stata 14.0 software. Results A total of six studies were included involving 665 patients. Three studies were PAO, and the other three were HTO. The total blood loss in PAO (WMD, −330.49; 95% CI, −390.16 to −270.83; P

Published
2019
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14. Clinical study on hematoma puncture and catheter drainage in treatment of intracerebral hemorrhage under CT real-time guide

Author

Zhong-zheng HE, Zhan-yao WANG, Hong WANG, Yan-ping YANG, An-sheng WANG, Qian-fa LONG, Wen-feng NING, Xiao-ping WU, and Shu-yuan YUE

Subjects
Cerebral hemorrhage, Drainage, Tomography, X-ray computed, Neurology. Diseases of the nervous system, RC346-429
Abstract

Objective To study the efficacy and safety of hematoma puncture catheter drainage under CT real-time guide for treatment of intracerebral hemorrhage (ICH). Methods A total of 80 ICH patients with hematoma volume 15-30 ml were given conservative treatment (control group, 40 cases including 6 cases with hematoma volume 15-20 ml and 34 cases with hematoma volume > 20-30 ml) and hematoma puncture and catheter drainage under CT real-time guide (operation group, 40 cases with hematoma volume > 20-30 ml). Conscious states were evaluated by Glasgow Coma Scale (GCS) on admission and 3 d after onset. Neurological deficits of patients were evaluated by National Institutes of Health Stroke Scale (NIHSS) on admission and discharge. Hospitalization days and complications (including rebleeding, epilepsy, intracranial infection, severe pulmonary infection and bleeding caused by digestive tract stress ulcer) were recorded. Results The GCS scores 3 d after onset (P = 0.000) and NIHSS scores on discharge (P = 0.000) of 2 groups were significantly lower than those on admission. The GCS score of operation group was significantly higher (P = 0.003) and NIHSS score was significantly lower (P = 0.000) than that of control group. The hospitalization time of operation group was significantly lower than those of control group [(10.53 ± 2.64) d vs. (17.30 ± 4.92) d; t = 7.673, P = 0.000]. Complications including rebleeding, intracranial infection, severe pulmonary infection and bleeding caused by digestive tract stress ulcer did not occur in patients of 2 groups. Conclusions For supratentorial hemorrhage patients withhematoma volume 15-30 ml, in comparison with conservative treatment, operation with hematoma puncture and catheter drainage under CT real-time guide can save hospitalization days, relieve edema peak response and improve the prognosis. DOI: 10.3969/j.issn.1672-6731.2018.11.007

Published
2018
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15. A population-based study of the risk of osteoporosis and fracture with dutasteride and finasteride

Author

Tony Antoniou, Erin M. Macdonald, Zhan Yao, Tara Gomes, Mina Tadrous, Joanne M.-W. Ho, Muhammad M. Mamdani, David N. Juurlink, and for the Canadian Drug Safety and Effectiveness Research Network

Subjects
5-alpha Reductase inhibitors/adverse effects, Osteoporosis/physiopathology, Dutasteride, Finasteride, Diseases of the musculoskeletal system, RC925-935
Abstract

Abstract Background Dutasteride is a potent inhibitor of 5-alpha reductase enzymes that reduces concentrations of dihydrotestosterone to a greater extent than finasteride. Whether this has adverse implications for bone health is unknown. We compared the risk of osteoporosis and fractures in older men treated with dutasteride or finasteride. Methods We conducted a population-based retrospective cohort study with high-dimensional propensity score matching of Ontario men aged 66 years or older who started treatment with dutasteride or finasteride between January 1, 2006 and December 31, 2012. The primary outcome was a diagnosis of osteoporosis within 2 years of treatment initiation. A secondary outcome was osteoporotic or fragility fractures. Results We studied 31,615 men treated with dutasteride and an equal number of men treated with finasteride. Dutasteride-treated patients had a lower incidence of osteoporosis than those receiving finasteride [2.2 versus 2.6 per 100 person years; hazard ratio (HR) 0.82; 95% confidence interval (CI) 0.72 to 0.93]. This effect was no longer statistically significant following adjustment for specialty of prescribing physician (HR 0.90; 95% CI 0.78 to 1.02)]. There was no differential risk of fractures with dutasteride (HR 1.04; 95% 0.86 to 1.25). Conclusions Despite differential effects on 5-alpha reductase, dutasteride is not associated with an increased risk of osteoporosis or fractures in older men relative to finasteride. These findings suggest that dutasteride does not adversely affect bone health.

Published
2018
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16. Abundant dynamics of group velocity locked vector solitons from Er-doped fiber laser based on GO/PVA film

Author

Ja-Hon Lin, Zhan-Yao Zhang, Zhen-Ying Li, Peng-Chun Peng, Yu-Feng Song, and Han Zhang

Subjects
Electrical and Electronic Engineering, Atomic and Molecular Physics, and Optics, Electronic, Optical and Magnetic Materials, Biotechnology
Abstract

With the insertion a segment of polarization-maintaining fiber (PMF) inside the cavity, abundant dynamics of group velocity locked vector solitons (GVLVSs) in Er-doped fiber laser have been investigated by using graphene oxide/polyvinyl alcohol (GO/PVA) film as a saturable absorber (SA). The generated Kelly sidebands in emission spectra reveal peak-valley or valley-peak alternation and slightly shift in two orthogonal components, which are the characteristics of GVLVSs. Through proper adjustment of polarization controllers (PCs) inside the EDFLs cavity, versatile vector soliton dynamics such as polarization locked GVLVSs (PL-GVLVSs), polarization rotation GVLVSs (PR-GVLVSs), dual wavelength GVLVSs, bound state GVLVSs, bunch GVLVSs and harmonic mode-locking GVLVSs (HML-GVLVSs) have been observed. The separation between two emission peaks from the dual wavelength GVLVSs was controlled by the Lyot filter and related to the insertion length of PMF inside the cavity. Unlike PL-GVLVSs, the period-doubling phenomenon has been found in two orthogonal components of the PR-GVLVSs. Besides, the bound state GVLVSs were generated showing strongly modulated interference fringes in emission spectrum. For the bunch and HML GVLVSs, the number of solitons inside the cavity increased with the pump power, and it showed the quintuple solitons and the 7th HML-GVLVSs at the highest pump power.

Published
2022

17. Back Frame Optimization of a Large Radio Telescope Based on Force Cone Method

Author

Qinglong WU, Zhan YAO, Tanhui WU, Houfei FANG, and Yangqing HOU

Subjects
Multidisciplinary
Abstract

A new research perspective is proposed to optimize the topology of truss structure by force cone method, which involves force cone drawing rules and growth rules. Through the comparison with the mature variable density topology optimization method, the effectiveness of force cone method is verified. This kind of new method is simple and easy to understand (no need to master complex structural optimization design theory). Besides, it is time-saving in finite element calculations, and can obtain an optimized truss layout easily. By drawing the force cone, its application on a large radio telescope's back frame structure shows that, compared with the existing one in terms of structural stiffness, Root Mean Square (RMS) precision, and beam stress distribution, the optimized back frame using the force cone method has higher stiffness, better RMS, more uniform stress, and lighter weight.

Published
2022

18. Rare BRAF mutations in pancreatic neuroendocrine tumors may predict response to RAF and MEK inhibition.

Author

Amy Allen, Alice Can Ran Qin, Nitya Raj, Jiawan Wang, Sharmeen Uddin, Zhan Yao, Laura Tang, Paul A Meyers, Barry S Taylor, Michael F Berger, Rona Yaeger, Diane Reidy-Lagunes, and Christine A Pratilas

Subjects
Medicine, Science
Abstract

The clinical significance of BRAF alterations in well-differentiated (WD) metastatic pancreatic neuroendocrine tumor (panNET) is unknown, but BRAF-mutated panNET could represent a subset characterized by an identifiable and clinically actionable driver. Following the identification of two patients with WD metastatic panNET whose tumors harbored BRAF mutations, we queried the MSK-IMPACT series of 80 patients with WD metastatic panNET for additional mutations in BRAF, and in other genes involved in RAS/ RTK/ PI3K signaling pathways. BRAF mutations were identified in six samples (7.5%): two tumors harbored V600E mutations, one tumor each expressed K601E, T599K, and T310I mutations, and one tumor expressed both G596D and E451K BRAF. Few additional actionable driver alterations were identified. To determine the ERK activating capability of four BRAF mutations not previously characterized, mutant constructs were tested in model systems. Biochemical characterization of BRAF mutations revealed both high and low activity mutants. Engineered cells expressing BRAF K601E and V600E were used for in vitro drug testing of RAF and MEK inhibitors currently in clinical use. BRAF K601E demonstrated reduced sensitivity to dabrafenib compared to BRAF V600E, but the combination of RAF plus MEK inhibition was effective in cells expressing this mutation. Herein, we describe the clinical course of a patient with BRAF K601E and a patient with BRAF V600E WD metastatic panNET, and the identification of four mutations in BRAF not previously characterized. The combined clinical and biochemical data support a potential role for RAF and MEK inhibitors, or a combination of these, in a selected panNET population.

Published
2019
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19. Prediction of Chemical Composition in Tea Based on Image Processing Technology

Author

Zhan Yao

Subjects
Chemical engineering, TP155-156, Computer engineering. Computer hardware, TK7885-7895
Abstract

The most prevalent method used for tea production makes it difficult to guarantee the tea quality due to the fact that the natural environment is bad and artificial technology level is poor. There is a pressing need to find a feasible way that can estimate tea production schedule and quality. Against this backdrop, this paper introduces the image processing technology into the quality judgment in the tea production to predict chemical constituent changes in tea such that the most appropriate production model will be available. In this study, image processing technology extracts the tea color information in the production process. PCA (principal component analysis) simulates the relationship between the color change information and the chemical composition, based on which to train the BP neural network, and also successfully predict the contents of sugars, starch, total nitrogen, alkalis, and other principal chemical components in the phases of the tea production process. This study provides a reference for tea quality judgment.

Published
2018
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20. Supplementary Methods, Figures 1 - 5, Tables 1 - 5 from Diverse and Targetable Kinase Alterations Drive Histiocytic Neoplasms

Author

Omar Abdel-Wahab, Tanja A. Gruber, Neal Rosen, Jean-Francois Emile, Ahmet Dogan, Zahir Amoura, Christopher Y. Park, Barry S. Taylor, Filip Janku, José Baselga, David M. Hyman, David B. Solit, Jean Donadieu, Sebastien Héritier, Jared Block, Omotayo Fasan, Samuel R. Briggs, Siraj M. Ali, Jeffrey S. Ross, Vincent A. Miller, Philip J. Stephens, William A. Gahl, Mario Lacouture, Juvianee Estrada-Veras, David W. Ellison, James D. Dalton, Chezi Ganzel, Joy Nakitandwe, Paul Zappile, Adriana Heguy, Olga Aminova, Igor Dolgalev, Brooke Sylvester, Michael P. Walsh, Patrick Campbell, Jean-Baptiste Micol, Yijun Gao, Stanley Chun-Wei Lee, Fleur Cohen-Aubart, Eunhee Kim, John Choi, Zhaoming Wang, Sameer A. Parikh, Jing Ma, Zhan Yao, Julien Haroche, Benjamin H. Durham, and Eli L. Diamond

Abstract

Supplementary Figure 1. Somatic mutations detected in histiocytic neoplasms. Supplementary Figure 2. Frequencies of known activating kinase mutations in histiocytic neoplasms. Supplementary Figure 3. ARAF mutations and variants of unknown significance detected in BRAFV600E-wildtype, non-Langerhans Cell Histiocytic neoplasms. Supplementary Figure 4. Clinical and histological images of the non-Langerhans cell histiocytosis (non-LCH) lesions from index patients with kinase fusions identified by RNA-seq. Supplementary Figure 5. Gene expression analysis of histiocytic neoplasms by RNA-seq. Supplementary Table 1. Characteristics of patient samples with histiocytic neoplasms used in this study and genomic analysis utilized for each sample. Supplementary Table 2. Whole exome sequencing metrics. Supplementary Table 3. Somatic variants identified by whole exome and whole transcriptome sequencing and validated by droplet-digital PCR and/or custom-capture targeted next-generation sequencing with variant allele frequencies (VAFs). Supplementary Table 4. List of the top 1% of differentially expressed genes across histiocytic samples from mRNA sequencing. Supplementary Table 5. PCR primers with M13F2 and M13R2 tails (blue) for Sanger sequencing used in the targeted sequencing recurrence testing for MAP2K1 exons 2 and 3 and all coding regions of ARAF.

Published
2023

21. Data from Rapid Induction of Apoptosis by PI3K Inhibitors Is Dependent upon Their Transient Inhibition of RAS–ERK Signaling

Author

Neal Rosen, Sarat Chandarlapaty, Ningshu Liu, José Baselga, Elisa de Stanchina, Xuejun Jiang, Prashant Monian, Xiaodong Huang, Claudia Schneider, Vanessa Rodrik-Outmezguine, Zhan Yao, Weiyi Toy, Alice Can Ran Qin, and Marie Will

Abstract

The effects of selective phosphoinositide 3-kinase (PI3K) and AKT inhibitors were compared in human tumor cell lines in which the pathway is dysregulated. Both caused inhibition of AKT, relief of feedback inhibition of receptor tyrosine kinases, and growth arrest. However, only the PI3K inhibitors caused rapid induction of cell death. In seeking a mechanism for this phenomenon, we found that PI3K inhibition, but not AKT inhibition, causes rapid inhibition of wild-type RAS and of RAF–MEK–ERK signaling. Inhibition of RAS–ERK signaling is transient, rebounding a few hours after drug addition, and is required for rapid induction of apoptosis. Combined MEK and AKT inhibition also promotes cell death, and in murine models of HER2+ cancer, either pulsatile PI3K inhibition or combined MEK and AKT inhibition causes tumor regression. We conclude that PI3K is upstream of RAS and AKT and that pulsatile inhibition of both pathways is sufficient for effective antitumor activity.Significance: We show that the RAS–ERK pathway is a key downstream effector pathway of oncogenic PI3K. Coordinate downregulation of AKT and ERK is necessary for induction of apoptosis and antitumor activity and can be accomplished with pulsatile dosing, which will likely decrease toxicity and allow administration of therapeutic doses. Cancer Discov; 4(3); 334–47. ©2014 AACR.This article is highlighted in the In This Issue feature, p. 259

Published
2023

22. Supplementary Material from A Secondary Mutation in BRAF Confers Resistance to RAF Inhibition in a BRAFV600E-Mutant Brain Tumor

Author

Christine A. Pratilas, Barry S. Taylor, Neal Rosen, David J. Pisapia, Marc K. Rosenblum, Sofia Haque, Katia Manova, Mary Petriccione, Ira J. Dunkel, Sharmeen Uddin, Alice Can Ran Qin, Amy N. Allen, Philip Jonsson, Zhan Yao, and Jiawan Wang

Abstract

Supplementary Figure S1: Representative H&E, phospho-ERK and FISH images of pre-dabrafenib (3) and post-dabrafenib (4) tumors. Supplementary Figure S2: WES analysis of copy number variation in pre- and postdabrafenib tumors. Supplementary Figure S3: Whole copy number profiles from WES of pre- and posttreatment tumors. Supplementary Figure S4: Homology alignment of BRAF p. L514 with residues in other tyrosine kinases. Supplementary Figure S5: Relative frequency of BRAF variant alleles in SK-BT-DR cells determined by individual clone sequencing. Supplementary Figure S6: BRAF V600E/L514V reduces dabrafenib sensitivity in NIH- 3T3 cells, related to Figure 2. Supplementary Figure S7: BRAF V600E/L514V confers biochemical resistance to dabrafenib over a time course, related to Figure 2G. Supplementary Figure S8: Comparison of IC50, IC75 and IC90 of dabrafenib against A375 cells expressing BRAF V600E and BRAF V600E/L514V, related to Figure 2H. Supplementary Figure S9: The BRAF V600E/L514V double mutant promotes homodimerization, related to Figure 3A and B. Supplementary Figure S10: BRAF L514V alone is hypoactive and associated with decreased ERK signaling that is not sensitive to dabrafenib. Supplementary Figure S11: BRAF V600E/L514V is inhibited by dabrafenib in a purified kinase assay, indicating that it is not a gatekeeper mutation. Supplementary Figure S12: Quantitation of p-MEK and p-ERK immunoblots, related to Figure 4B. Supplementary Figure S13: Comparison of IC50, IC75 and IC90 of trametinib against A375 expressing BRAF V600E and BRAF V600E/L514V, related to Figure 4C. Supplementary Figure S14: The BRAF V600E/L514V mutant mediates resistance to dabrafenib that cannot be completely overcome by trametinib or dabrafenib plus trametinib, related to Figure 4D. Supplementary Figure S15: V5, p-MEK, total MEK immunoblots, and quantitation of p-ERK immunoblots, related to Figure 5A. Supplementary Figure S16: Novel RAF dimer inhibitors, MEK inhibitor and ERK inhibitor equipotently inhibit cell growth in BRAF V600E and V600E/L514V expressing cells. Supplementary Figure S17: Novel RAF dimer inhibitor, MEK inhibitor and ERK inhibitor equipotently inhibit ERK signaling in BRAF V600E and V600E/L514V expressing cells. Supplementary Figure S18: BGB3245 binds mutant BRAF V600E monomer and second site of V600E/L514V dimer with similar affinity. Supplementary Table S1: Mutations identified by WES of pre-dabrafenib and postdabrafenib tumors. Supplementary Table S2: Secondary mutations associated with acquired resistance and occurring in residues homologous with L514 in BRAF. Supplementary Table S3: BRAF L514V allele frequency determined by ddPCR.

Published
2023

23. Supplementary Materials and Methods from Rapid Induction of Apoptosis by PI3K Inhibitors Is Dependent upon Their Transient Inhibition of RAS–ERK Signaling

Author

Neal Rosen, Sarat Chandarlapaty, Ningshu Liu, José Baselga, Elisa de Stanchina, Xuejun Jiang, Prashant Monian, Xiaodong Huang, Claudia Schneider, Vanessa Rodrik-Outmezguine, Zhan Yao, Weiyi Toy, Alice Can Ran Qin, and Marie Will

Abstract

PDF file 93K, This file contains detailed description of experimental procedures as well as reagents utilized

Published
2023

24. Supplementary Figure S6 from Rapid Induction of Apoptosis by PI3K Inhibitors Is Dependent upon Their Transient Inhibition of RAS–ERK Signaling

Author

Neal Rosen, Sarat Chandarlapaty, Ningshu Liu, José Baselga, Elisa de Stanchina, Xuejun Jiang, Prashant Monian, Xiaodong Huang, Claudia Schneider, Vanessa Rodrik-Outmezguine, Zhan Yao, Weiyi Toy, Alice Can Ran Qin, and Marie Will

Abstract

PDF file 40K, Supplementary Figure S6. Induction of apoptosis by PI3K inhibition in HER2-amplified cells. Related to main Figure 6

Published
2023

26. Data from Allele-Specific Mechanisms of Activation of MEK1 Mutants Determine Their Properties

Author

Neal Rosen, Zhan Yao, Barry S. Taylor, Omar Abdel-Wahab, David B. Solit, Henrik Moebitz, Darrin Stuart, Giordano Caponigro, Mariano Barbacid, Matthias Drosten, Keven Muniz, Neilawattie M. Torres, Rona Yaeger, Bing Zhou, Na Na, Daniel McKay, Matthew T. Chang, and Yijun Gao

Abstract

Mutations at multiple sites in MEK1 occur in cancer, suggesting that their mechanisms of activation might be different. We analyzed 17 tumor-associated MEK1 mutants and found that they drove ERK signaling autonomously or in a RAS/RAF-dependent manner. The latter are sensitive to feedback inhibition of RAF, which limits their functional output, and often cooccur with RAS or RAF mutations. They act as amplifiers of RAF signaling. In contrast, another class of mutants deletes a hitherto unrecognized negative regulatory segment of MEK1, is RAF- and phosphorylation-independent, is unaffected by feedback inhibition of upstream signaling, and drives high ERK output and transformation in the absence of RAF activity. Moreover, these RAF-independent mutants are insensitive to allosteric MEK inhibitors, which preferentially bind to the inactivated form of MEK1. All the mutants are sensitive to an ATP-competitive MEK inhibitor. Thus, our study comprises a novel therapeutic strategy for tumors driven by RAF-independent MEK1 mutants.Significance: Mutants with which MEK1 mutants coexist and their sensitivity to inhibitors are determined by allele-specific properties. This study shows the importance of functional characterization of mutant alleles in single oncogenes and identifies a new class of MEK1 mutants, insensitive to current MEK1 inhibitors but treatable with a new ATP-competitive inhibitor. Cancer Discov; 8(5); 648–61. ©2018 AACR.See related commentary by Maust et al., p. 534.This article is highlighted in the In This Issue feature, p. 517

Published
2023

27. Supplementary Figure Legends from Rapid Induction of Apoptosis by PI3K Inhibitors Is Dependent upon Their Transient Inhibition of RAS–ERK Signaling

Author

Neal Rosen, Sarat Chandarlapaty, Ningshu Liu, José Baselga, Elisa de Stanchina, Xuejun Jiang, Prashant Monian, Xiaodong Huang, Claudia Schneider, Vanessa Rodrik-Outmezguine, Zhan Yao, Weiyi Toy, Alice Can Ran Qin, and Marie Will

Abstract

PDF file 67K, This file contains legends for supplementary figures S1-S7. It describes in detail what's included in each figure

Published
2023

30. Data from V211D Mutation in MEK1 Causes Resistance to MEK Inhibitors in Colon Cancer

Author

Rona Yaeger, Zhan Yao, Neal Rosen, Elisa de Stanchina, Jorge S. Reis-Filho, HuiYong Zhao, Barry S. Taylor, Britta Weigelt, Robert A. Lefkowitz, Julianne Carson, Jaclyn F. Hechtman, Alexander N. Gorelick, Arnaud da Cruz Paula, Na Na, Ann Maria, and Yijun Gao

Abstract

We report the emergence of the novel MEK1V211D gatekeeper mutation in a patient with BRAFK601E colon cancer treated with the allosteric MEK inhibitor binimetinib and the anti-EGFR antibody panitumumab. The MEK1V211D mutation concurrently occurs in the same cell with BRAFK601E and leads to RAF-independent activity but remains regulated by RAF. The V211D mutation causes resistance to binimetinib by both increasing the catalytic activity of MEK1 and reducing its affinity for the drug. Moreover, the mutant exhibits reduced sensitivity to all the allosteric MEK inhibitors tested. Thus, this mutation serves as a general resistance mutation for current MEK inhibitors; however, it is sensitive to a newly reported ATP-competitive MEK inhibitor, which therefore could be used to overcome drug resistance.Significance:We report a resistance mechanism to allosteric MEK inhibitors in the clinic. A MEK1V211D mutation developed in a patient with BRAFK601E colon cancer on MEK and EGFR inhibitors. This mutant increases the catalytic activity of MEK1 and reduces its affinity for binimetinib, but remains sensitive to ATP-competitive MEK inhibitors.This article is highlighted in the In This Issue feature, p. 1143

Published
2023

32. Supplementary Data from Leveraging Systematic Functional Analysis to Benchmark an In Silico Framework Distinguishes Driver from Passenger MEK Mutants in Cancer

Author

David B. Solit, Barry S. Taylor, Neal Rosen, Michael F. Berger, Taha Merghoub, Omar Abdel-Wahab, Agnes Viale, Shakuntala Tiwari, Alexander N. Shoushtari, Elena I. Gavrila, Hannah C. Wise, Wenhuo Hu, Yijun Gao, Zhan Yao, Abigail N. Poteshman, Clare A. Nimura, Moriah H. Nissan, Amber J. Kiliti, Alexis M. Jones, Alexander N. Gorelick, Sizhi P. Gao, Dong Xu, Ye Liu, Weiwei Han, Jianjiong Gao, Arijh Elzein, Matthew T. Chang, Brooke E. Sylvester, and Aphrothiti J. Hanrahan

Abstract

This supplementary data file contains 5 figures pertaining to the tumor distribution of MEK1 hotspot mutations, functional characterization of further MEK1/2 mutants with and without MEK or ERK inhibitor treatment, and the sequence paralogy alignment of MEK1 and MEK2. This file also contains 4 tables detailing hotspot analysis q values for MEK1/2 mutants, tumor incidence of MEK1 in-frame deletions, and a summary of MEK1/2 paralogous residues and their concordant activation status.

Published
2023

33. Data from Mechanisms of Acquired Resistance to BRAF V600E Inhibition in Colon Cancers Converge on RAF Dimerization and Are Sensitive to Its Inhibition

Author

Neal Rosen, David B. Solit, Michael F. Berger, Leonard Saltz, Elisa de Stanchina, Jose Baselga, Andrea Cercek, Andrew Joelson, Lu Wang, Wenjing Su, HuiYong Zhao, Efsevia Vakiani, Jaclyn F. Hechtman, David M. Hyman, Zhan Yao, and Rona Yaeger

Abstract

BRAF V600E colorectal cancers are insensitive to RAF inhibitor monotherapy due to feedback reactivation of receptor tyrosine kinase signaling. Combined RAF and EGFR inhibition exerts a therapeutic effect, but resistance invariably develops through undefined mechanisms. In this study, we determined that colorectal cancer progression specimens invariably harbored lesions in elements of the RAS–RAF–MEK–ERK pathway. Genetic amplification of wild-type RAS was a recurrent mechanism of resistance in colorectal cancer patients that was not seen in similarly resistant melanomas. We show that wild-type RAS amplification increases receptor tyrosine kinase-dependent activation of RAS more potently in colorectal cancer than in melanoma and causes resistance only in the former. Currently approved RAF inhibitors inhibit RAF monomers but not dimers. All the drug-resistant lesions we identified activate BRAF V600E dimerization directly or by elevating RAS-GTP. Overall, our results show that mechanisms of resistance converge on formation of RAF dimers and that inhibiting EGFR and RAF dimers can effectively suppress ERK-driven growth of resistant colorectal cancer. Cancer Res; 77(23); 6513–23. ©2017 AACR.

Published
2023

34. Supplementary figures from Mechanisms of Acquired Resistance to BRAF V600E Inhibition in Colon Cancers Converge on RAF Dimerization and Are Sensitive to Its Inhibition

Author

Neal Rosen, David B. Solit, Michael F. Berger, Leonard Saltz, Elisa de Stanchina, Jose Baselga, Andrea Cercek, Andrew Joelson, Lu Wang, Wenjing Su, HuiYong Zhao, Efsevia Vakiani, Jaclyn F. Hechtman, David M. Hyman, Zhan Yao, and Rona Yaeger

Abstract

Supplementary Figures 1-5: Supplementary Figure 1 - validation and characterization of acquired genomic alterations, Supplementary Figure 2 - RAS amplification leads to increased RAS-GTP and dimerization of RAF, Supplementary Figure 3 - Increase in NRAS expression is sufficient to cause resistance to RAF/EGFR inhibition in vitro in CRC, Supplementary Figure 4 - Increase in NRAS expression does not cause resistance to RAF inhibition in melanoma, Supplementary Figure 5 - Combined EGFR and RAF dimer inhibitors lead to better inhibition of signaling and tumor growth than RAF dimer inhibitor alone in BRAF V600E CRC.

Published
2023

35. Data from Leveraging Systematic Functional Analysis to Benchmark an In Silico Framework Distinguishes Driver from Passenger MEK Mutants in Cancer

Author

David B. Solit, Barry S. Taylor, Neal Rosen, Michael F. Berger, Taha Merghoub, Omar Abdel-Wahab, Agnes Viale, Shakuntala Tiwari, Alexander N. Shoushtari, Elena I. Gavrila, Hannah C. Wise, Wenhuo Hu, Yijun Gao, Zhan Yao, Abigail N. Poteshman, Clare A. Nimura, Moriah H. Nissan, Amber J. Kiliti, Alexis M. Jones, Alexander N. Gorelick, Sizhi P. Gao, Dong Xu, Ye Liu, Weiwei Han, Jianjiong Gao, Arijh Elzein, Matthew T. Chang, Brooke E. Sylvester, and Aphrothiti J. Hanrahan

Abstract

Despite significant advances in cancer precision medicine, a significant hurdle to its broader adoption remains the multitude of variants of unknown significance identified by clinical tumor sequencing and the lack of biologically validated methods to distinguish between functional and benign variants. Here we used functional data on MAP2K1 and MAP2K2 mutations generated in real-time within a co-clinical trial framework to benchmark the predictive value of a three-part in silico methodology. Our computational approach to variant classification incorporated hotspot analysis, three-dimensional molecular dynamics simulation, and sequence paralogy. In silico prediction accurately distinguished functional from benign MAP2K1 and MAP2K2 mutants, yet drug sensitivity varied widely among activating mutant alleles. These results suggest that multifaceted in silico modeling can inform patient accrual to MEK/ERK inhibitor clinical trials, but computational methods need to be paired with laboratory- and clinic-based efforts designed to unravel variabilities in drug response.Significance:Leveraging prospective functional characterization of MEK1/2 mutants, it was found that hotspot analysis, molecular dynamics simulation, and sequence paralogy are complementary tools that can robustly prioritize variants for biologic, therapeutic, and clinical validation.See related commentary by Whitehead and Sebolt-Leopold, p. 4042

Published
2023

36. Data from Combined Inhibition of SHP2 and MEK Is Effective in Models of NF1-Deficient Malignant Peripheral Nerve Sheath Tumors

Author

Christine A. Pratilas, Fausto J. Rodriguez, Zhan Yao, Dirk Pijnenburg, Tushar Tomar, Amy N. Allen, Kai Pollard, and Jiawan Wang

Abstract

Loss of the RAS GTPase-activating protein (RAS-GAP) NF1 drives aberrant activation of RAS/MEK/ERK signaling and other effector pathways in the majority of malignant peripheral nerve sheath tumors (MPNST). These dysregulated pathways represent potential targets for therapeutic intervention. However, studies of novel single agents including MEK inhibitors (MEKi) have demonstrated limited efficacy both preclinically and clinically, with little advancement in overall patient survival. By interrogation of kinome activity through an unbiased screen and targeted evaluation of the signaling response to MEK inhibition, we have identified global activation of upstream receptor tyrosine kinases (RTK) that converges on activation of RAS as a mechanism to limit sensitivity to MEK inhibition. As no direct inhibitors of pan-RAS were available, an inhibitor of the protein tyrosine phosphatase SHP2, a critical mediator of RAS signal transduction downstream of multiple RTK, represented an alternate strategy. The combination of MEKi plus SHP099 was superior to MEKi alone in models of NF1-MPNST, including those with acquired resistance to MEKi. Our findings have immediate translational implications and may inform future clinical trials for patients with MPNST harboring alterations in NF1.Significance:Combined inhibition of MEK and SHP2 is effective in models of NF1-MPNST, both those naïve to and those resistant to MEKi, as well as in the MPNST precursor lesion plexiform neurofibroma.

Published
2023

38. Supplementary Figure Legends from Mechanisms of Acquired Resistance to BRAF V600E Inhibition in Colon Cancers Converge on RAF Dimerization and Are Sensitive to Its Inhibition

Author

Neal Rosen, David B. Solit, Michael F. Berger, Leonard Saltz, Elisa de Stanchina, Jose Baselga, Andrea Cercek, Andrew Joelson, Lu Wang, Wenjing Su, HuiYong Zhao, Efsevia Vakiani, Jaclyn F. Hechtman, David M. Hyman, Zhan Yao, and Rona Yaeger

Abstract

Supplementary Figure Legends: Supplementary Figure 1 - validation and characterization of acquired genomic alterations, Supplementary Figure 2 - RAS amplification leads to increased RAS-GTP and dimerization of RAF, Supplementary Figure 3 - Increase in NRAS expression is sufficient to cause resistance to RAF/EGFR inhibition in vitro in CRC, Supplementary Figure 4 - Increase in NRAS expression does not cause resistance to RAF inhibition in melanoma, Supplementary Figure 5 - Combined EGFR and RAF dimer inhibitors lead to better inhibition of signaling and tumor growth than RAF dimer inhibitor alone in BRAF V600E CRC.

Published
2023

39. Data Supplement from Loss of NF1 in Cutaneous Melanoma Is Associated with RAS Activation and MEK Dependence

Author

David B. Solit, Neal Rosen, Michael F. Berger, Nikolaus Schultz, Barry S. Taylor, Rona Yaeger, Paul B. Chapman, Antoni Ribas, Taha Merghoub, Zhan Yao, Aphrothiti J. Hanrahan, Li Kong, Shakuntala Tiwari, Cailian Liu, Helen Won, Ricardo Ramirez, Alexis M. Jones, Christine A. Pratilas, and Moriah H. Nissan

Abstract

Supplementary Figures S1-S8. Levels of RAS-GTP in melanoma cell lines (S1); Changes in pERK and cyclin D1 levels as function of time in cells treated with the MEK inhibitor PD0325901 (S2); Sk-Mel-113 (NF1 null) melanoma cells are resistant to AKT inhibition (S3); Variability in induction of pMEK levels following exposure to four allosteric MEK inhibitors (S4); Exon-capture deep sequencing via IMPACT of the NF1 gene in M308 shows a nonsense Q1070* mutation (S5); Expression of activated RAS is sufficient to confer resistance to vemurafenib in Sk-Mel-239 (BRAF V600E) cells (S6); Sensitivity of A375 (BRAF V600E) cells to vemurafenib (S7); The MAPK pathway and the inhibitors used in the study of NF1-null cells (S8).

Published
2023

40. Inhibiting the MNK1/2-eIF4E axis impairs melanoma phenotype switching and potentiates antitumor immune responses

Author

Huang, Fan, Goncalves, Christophe, Bartish, Margarita, Remy-Sarrazin, Joelle, Issa, Mark E., Cordeiro, Brendan, Guo, Qianyu, Emond, Audrey, Attias, Mikhael, Yang, William, Plourde, Dany, Su, Jie, Gimeno, Marina Godoy, Zhan, Yao, Galan, Alba, Rzymski, Tomasz, Mazan, Milena, Masiejczyk, Magdalena, Faber, Jacek, Khoury, Elie, Benoit, Alexandre, Gagnon, Natascha, Dankort, David, Journe, Fabrice, Ghanem, Ghanem E., Krawczyk, Connie M., Saragovi, H. Uri, Piccirillo, Ciriaco A., Sonenberg, Nahum, Topisirovic, Ivan, Rudd, Christopher E., Miller, Wilson H., Jr., and del Rincon, Sonia V.

Subjects
Immune response -- Genetic aspects, Phosphotransferases -- Health aspects, Melanoma -- Genetic aspects -- Development and progression -- Care and treatment, Phenotype -- Health aspects, Health care industry
Abstract

Melanomas commonly undergo a phenotype switch, from a proliferative to an invasive state. Such tumor cell plasticity contributes to immunotherapy resistance; however, the mechanisms are not completely understood and thus are therapeutically unexploited. Using melanoma mouse models, we demonstrated that blocking the MNK1/2-eIF4E axis inhibited melanoma phenotype switching and sensitized melanoma to anti-PD-1 immunotherapy. We showed that phosphoeIF4E-deficient murine melanomas expressed high levels of melanocytic antigens, with similar results verified in patient melanomas. Mechanistically, we identified phospho-eIF4E-mediated translational control of NGFR, a critical effector of phenotype switching. Genetic ablation of phospho-eIF4E reprogrammed the immunosuppressive microenvironment, exemplified by lowered production of inflammatory factors, decreased PD-L1 expression on dendritic cells and myeloid-derived suppressor cells, and increased [CD8.sup.+] T cell infiltrates. Finally, dual blockade of the MNK1/2-eIF4E axis and the PD-1/ PD-L1 immune checkpoint demonstrated efficacy in multiple melanoma models regardless of their genomic classification. An increase in the presence of intratumoral stem-like [TCF1.sup.+][PD-1.sup.+][CD8.sup.+] T cells, a characteristic essential for durable antitumor immunity, was detected in mice given a MNK1/2 inhibitor and anti-PD-1 therapy. Using MNK1/2 inhibitors to repress phospho-eIF4E thus offers a strategy to inhibit melanoma plasticity and improve response to anti-PD-1 immunotherapy., Introduction Malignant melanoma is the deadliest form of skin cancer. In melanoma, the major signaling pathways, RAS/RAF/MAPK and PI3K/AKT, are constitutively activated through numerous avenues, including genetic alterations in BRAF [...]

Published
2021
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41. MNK1/2 inhibition limits oncogenicity and metastasis of KIT-mutant melanoma

Author

Zhan, Yao, Guo, Jun, Yang, William, Goncalves, Christophe, Rzymski, Tomasz, Dreas, Agnieszka, Zyfkiewicz, Eliza, Mikulski, Maciej, Brzozka, Krzysztof, Golas, Aniela, Kong, Yan, Ma, Meng, Huang, Fan, Huor, Bonnie, Guo, Qianyu, Daniela da Silva, Sabrina, Torres, Jose, Cai, Yutian, Topisirovic, Ivan, Su, Jie, Bijian, Krikor, Alaoui-Jamali, Moulay A., Huang, Sidong, Journe, Fabrice, Ghanem, Ghanem E., H. Miller Jr., Wilson, and del Rincon, Sonia V.

Subjects
Phosphorylation -- Research, Gene mutation -- Research, Cell migration -- Research, Melanoma -- Diagnosis -- Care and treatment, Health care industry
Abstract

Melanoma can be stratified into unique subtypes based on distinct pathologies. The acral/mucosal melanoma subtype is characterized by aberrant and constitutive activation of the proto-oncogene receptor tyrosine kinase C-KIT, which drives tumorigenesis. Treatment of these melanoma patients with C-KIT inhibitors has proven challenging, prompting us to investigate the downstream effectors of the C-KIT receptor. We determined that C-KIT stimulates MAP kinase-interacting serine/threonine kinases 1 and 2 (MNK1/2), which phosphorylate eukaryotic translation initiation factor 4E (eIF4E) and render it oncogenic. Depletion of MNK1/2 in melanoma cells with oncogenic C-KIT inhibited cell migration and mRNA translation of the transcriptional repressor SNA/1 and the cell cycle gene CCNE1. This suggested that blocking MNK1/2 activity may inhibit tumor progression, at least in part, by blocking translation initiation of mRNAs encoding cell migration proteins. Moreover, we developed an MNK1/2 inhibitor (SEL201), and found that SEL201-treated KIT-mutant melanoma cells had lower oncogenicity and reduced metastatic ability. Clinically, tumors from melanoma patients harboring K/T mutations displayed a marked increase in MNK1 and phospho-eIF4E. Thus, our studies indicate that blocking MNK1/2 exerts potent antimelanoma effects and support blocking MNK1/2 as a potential strategy to treat patients positive for K/T mutations., Introduction Early-stage melanoma can be cured by surgery, but patients often develop advanced disease that requires effective systemic treatment. Melanoma arising on acral and mucosal anatomical sites accounts for about [...]

Published
2017
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43. Impact of the model of long‐term follow‐up care on adherence to guideline‐recommended surveillance among survivors of adolescent and young adult cancers

Author

Jason D. Pole, Zhan Yao, Rinku Sutradhar, Paul C. Nathan, Dalia Kagramanov, Sumit Gupta, Nancy N. Baxter, and Cindy Lau

Subjects
Male, Cancer Research, Pediatrics, medicine.medical_specialty, Neoplasms, Radiation-Induced, Adolescent, Databases, Factual, cancer survivor, Aftercare, Breast Neoplasms, Cancer Care Facilities, Young Adult, Breast cancer, Cancer Survivors, Quality of life, Health care, Humans, Medicine, Radiology, Nuclear Medicine and imaging, Young adult, Research Articles, RC254-282, Retrospective Studies, Ontario, Cancer survivor, business.industry, adolescent and young adult, Attendance, Clinical Cancer Research, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Retrospective cohort study, Guideline, medicine.disease, follow‐up care, Oncology, Population Surveillance, surveillance, Female, Guideline Adherence, Cardiomyopathies, Family Practice, business, survivorship, Research Article, Mammography
Abstract

Purpose Adolescent and young adult cancer survivors require lifelong healthcare to address the late effects of therapy. We examined the impact of different provider models of long‐term follow‐up (LTFU) care on adherence to recommended surveillance. Methods We conducted a retrospective cohort study using administrative health databases in Ontario, Canada. Five‐year survivors were identified from IMPACT, a database of patients aged 15–20.9 years at diagnosis of six cancers between 1992 and 2010. We defined three models of LTFU care hierarchically: specialized survivor clinics (SCCs), general cancer clinics (GCCs), and family physician (FP). We assessed adherence to the Children's Oncology Group surveillance guidelines for cardiomyopathy and breast cancer. Multistate models assessed adherence transitions and impacts of LTFU attendance. Results A total of 1574 survivors were followed for a mean of 9.2 years (range 4.3–13.9 years) from index (5‐year survival). The highest level of LTFU attended in the first 2‐years post‐index was a GCC (47%); only 16.7% attended a SCC. By the end of study, 72% no longer attended any of the models of care and only 2% still attended an SCC. Among 188 survivors requiring breast cancer surveillance, 6.9% were adherent to their first required surveillance testing. Attendance at a SCC in the previous year and higher cumulative FP or GCC visits increased the rate of subsequently becoming adherent. Among 857 survivors requiring cardiomyopathy surveillance, 11% were adherent at study entry. Each subsequent SCC visit led to an 11.3% (95% CI: 1.05–1.18) increase in the rate of becoming adherent. Conclusion LTFU attendance and surveillance adherence are sub‐optimal. SCC follow‐up is associated with greater adherence, but few survivors receive such care, and this proportion diminished over time. Interventions are needed to improve LTFU attendance and promote surveillance adherence., Long‐term follow‐up care attendance and surveillance adherence are sub‐optimal among adolescent and young adult cancer survivors. Specialized survivor clinic follow‐up is associated with greater adherence, but few survivors receive such care, and this proportion diminished over time. Interventions are needed to improve the long‐term follow‐up care attendance and promote surveillance adherence.

Published
2021

44. Procyanidin A1 improves sepsis-induced liver injury by inhibiting inflammation.

Author

Zhan Yao, Shuna Liu, Chunmei Zheng, Qiangwu Li, and Liya Wang

Subjects
*SEPSIS, *PROCYANIDINS, *LIVER injuries, *LIVER cells, *ASPARTATE aminotransferase, *ALANINE aminotransferase
Abstract

Purpose: To determine the effect of procyanidin A1 (PCA1) on sepsis. Methods: Dulbecco's Modified Eagle Medium (DMEM) was employed to incubate mouse hepatic cell line AML12. The AML12 cells treated with lipopolysaccharide (LPS, 50 µg/mL) was used to establish a sepsis cell model. Cell viability was evaluated using CCK-8 assay, while cell apoptosis was assessed by flow cytometry. Aspartate transaminase (AST), alanine aminotransferase (ALT), IL-6 and TNF-a levels were evaluated by enzyme linked immunosorbent assay (ELISA). Protein expressions were assessed using western blot assay. Results: The viability of AML12 cells decreased following treatment with IL-1ß, but this change was offset by PCA1 treatment (40 or 80 µM). Similarly, cell apoptosis was enhanced after LPS treatment, but this change was attenuated by PCA1 treatment. The AST, ALT, IL-6 and TNF-a levels were all elevated after LPS treatment, but these changes were also reversed by PCA1 treatment, indicating that PCA1 suppressed LPS-induced liver injury and inflammation. Furthermore, the protein levels of p-p65/p65 and p-IκBa increased, and IκBa lowered following LPS treatment, but these effects were reversed by PCA1 treatment, indicating that PCA1 retarded NF-κB pathway. Conclusion: PCA1 alleviates sepsis-induced liver injury by inhibiting inflammation through NF-κB pathway. This suggestes that PCA1 may be an therapeutic agent for the treatment of sepsis. [ABSTRACT FROM AUTHOR]

Published
2023
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46. TGF-β reduces DNA ds-break repair mechanisms to heighten genetic diversity and adaptability of CD44+/CD24− cancer cells

Author

Debjani Pal, Anja Pertot, Nitin H Shirole, Zhan Yao, Naishitha Anaparthy, Tyler Garvin, Hilary Cox, Kenneth Chang, Fred Rollins, Jude Kendall, Leyla Edwards, Vijay A Singh, Gary C Stone, Michael C Schatz, James Hicks, Gregory J Hannon, and Raffaella Sordella

Subjects
genetic diversity, drug adaptability, intra-tumor heterogeneity, tumor evolution, tumor fitness, copy number alteration, Medicine, Science, Biology (General), QH301-705.5
Abstract

Many lines of evidence have indicated that both genetic and non-genetic determinants can contribute to intra-tumor heterogeneity and influence cancer outcomes. Among the best described sub-population of cancer cells generated by non-genetic mechanisms are cells characterized by a CD44+/CD24− cell surface marker profile. Here, we report that human CD44+/CD24− cancer cells are genetically highly unstable because of intrinsic defects in their DNA-repair capabilities. In fact, in CD44+/CD24− cells, constitutive activation of the TGF-beta axis was both necessary and sufficient to reduce the expression of genes that are crucial in coordinating DNA damage repair mechanisms. Consequently, we observed that cancer cells that reside in a CD44+/CD24− state are characterized by increased accumulation of DNA copy number alterations, greater genetic diversity and improved adaptability to drug treatment. Together, these data suggest that the transition into a CD44+/CD24− cell state can promote intra-tumor genetic heterogeneity, spur tumor evolution and increase tumor fitness.

Published
2017
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48. The Role of Intrathecal Morphine for Postoperative Analgesia in Primary Total Joint Arthroplasty under Spinal Anesthesia: A Systematic Review and Meta-Analysis

Author

Zhen Zhang, Ru-Zhan Yao, Guanglin Wang, and Limin Wang

Subjects
medicine.medical_treatment, Analgesic, Placebo, Anesthesia, Spinal, law.invention, 03 medical and health sciences, 0302 clinical medicine, Randomized controlled trial, 030202 anesthesiology, law, medicine, Humans, Arthroplasty, Replacement, Knee, Injections, Spinal, Pain, Postoperative, Morphine, Urinary retention, business.industry, General Medicine, Arthroplasty, Analgesics, Opioid, Anesthesiology and Pain Medicine, Meta-analysis, Anesthesia, Vomiting, Neurology (clinical), Analgesia, medicine.symptom, business, 030217 neurology & neurosurgery, medicine.drug
Abstract

Objective To assess the efficacy and safety of intrathecal morphine (ITM) for postoperative analgesia in primary total joint arthroplasty (TJA) under spinal anesthesia and to explore the dose-response relationship for analgesic efficacy or risk of side effects. Methods We searched MEDLINE, EMBASE, Web of Science, Cochrane Central Register of Controlled Trials and ClinicalTrials.gov for any studies meeting the inclusion criteria. All the data were summarized using the random effects model. Subgroup analyses were performed based on the surgical procedure and dose of ITM. Meta-regression was used to explore the dose-response relationship. Results Eighteen randomized controlled trials were included. Compared with the placebo or blank control, ITM reduced the postoperative 24-h morphine consumption by 10.07 mg and prolonged the duration of analgesia. However, ITM significantly increased the risk of pruritus by 2.79 fold, with a tendency to increase the risk of postoperative nausea and/or vomiting (P = 0.08). No difference was observed regarding the length of stay (LOS) and incidence of respiratory depression or urinary retention. Furthermore, meta-regression showed a linear dose-response relationship for the postoperative 24-h morphine consumption but no linear dose-response relationship for the risk of side effects. Conclusions Adding morphine to intrathecal anesthetics provides a prolonged and robust analgesic effect without significantly increasing the risk of side effects other than pruritus. Although we found a linear dose-response relationship for the postoperative 24-h morphine consumption, the optimal dose of ITM remains to be further explored in high-quality RCTs with a large sample size.

Published
2021

49. Health care costs associated with chronic hepatitis C virus infection in Ontario, Canada: a retrospective cohort study

Author

Zhan Yao, Murray Krahn, Beate Sander, Karen E. Bremner, William Wong, Andrew Calzavara, Nicholas Mitsakakis, Alex Haines, Jeffrey C. Kwong, and Hla-Hla Thein

Subjects
Adult, Liver Cirrhosis, Male, medicine.medical_specialty, Carcinoma, Hepatocellular, Cirrhosis, Adolescent, Hepatitis C virus, medicine.medical_treatment, Population, Liver transplantation, medicine.disease_cause, Antiviral Agents, Cohort Studies, Young Adult, Internal medicine, medicine, Humans, education, Aged, Retrospective Studies, Aged, 80 and over, Ontario, education.field_of_study, business.industry, Research, Liver Neoplasms, Retrospective cohort study, Health Care Costs, General Medicine, Hepatitis C, Chronic, Middle Aged, medicine.disease, Comorbidity, Confidence interval, Liver Transplantation, Hepatocellular carcinoma, Female, business
Abstract

Background High-quality estimates of health care costs are required to understand the burden of illness and to inform economic models. We estimated the costs associated with hepatitis C virus (HCV) infection from the public payer perspective in Ontario, Canada. Methods In this population-based retrospective cohort study, we identified patients aged 18-105 years diagnosed with chronic HCV infection in Ontario from 2003 to 2014 using linked administrative data. We allocated the time from diagnosis until death or the end of follow-up (Dec. 31, 2016) to 9 mutually exclusive health states using validated algorithms: no cirrhosis, no cirrhosis (RNA negative) (i.e., cured HCV infection), compensated cirrhosis, decompensated cirrhosis, hepatocellular carcinoma, both decompensated cirrhosis and hepatocellular carcinoma, liver transplantation, terminal (liver-related) and terminal (non-liver-related). We estimated direct medical costs (in 2018 Canadian dollars) per 30 days per health state and used regression models to identify predictors of the costs. Results We identified 48 239 patients with chronic hepatitis C, of whom 30 763 (63.8%) were men and 35 891 (74.4%) were aged 30-59 years at diagnosis. The mean 30-day costs were $798 (95% confidence interval [CI] $780-$816) (n = 43 568) for no cirrhosis, $661 (95% CI $630-$692) (n = 6422) for no cirrhosis (RNA negative), $1487 (95% CI $1375-$1599) (n = 4970) for compensated cirrhosis, $3659 (95% CI $3279-$4039) (n = 3151) for decompensated cirrhosis, $4238 (95% CI $3480-$4996) (n = 550) for hepatocellular carcinoma, $8753 (95% CI $7130-$10 377) (n = 485) for both decompensated cirrhosis and hepatocellular carcinoma, $4539 (95% CI $3746-$5333) (n = 372) for liver transplantation, $11 202 (95% CI $10 645-$11 760) (n = 3201) for terminal (liver-related) and $8801 (95% CI $8331-$9271) (n = 5278) for terminal (non-liver-related) health states. Comorbidity was the most significant predictor of total costs for all health states. Interpretation Our findings suggest that the financial burden of HCV infection is substantially higher than previously estimated in Canada. Our comprehensive, up-to-date cost estimates for clinically defined health states of HCV infection should be useful for future economic evaluations related to this disorder.

Published
2021

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