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578 results on '"Boggon, Titus J."'

101. CDC42 binds PAK4 via an extended GTPase-effector interface.

Author

Byung Hak Ha and Boggon, Titus J.

Subjects
*PROTEIN kinases, *THREONINE, *PROTEIN-protein interactions, *RHO GTPases, *CELLULAR signal transduction, *CELL cycle
Abstract

The p21-activated kinase (PAK) group of serine/threonine kinases are downstream effectors of RHO GTPases and play important roles in regulation of the actin cytoskeleton, cell growth, survival, polarity, and development. Here we probe the interaction of the type II PAK, PAK4, with RHO GTPases. Using solution scattering we find that the full-length PAK4 heterodimer with CDC42 adopts primarily a compact organization. X-ray crystallography reveals the molecular nature of the interaction between PAK4 and CDC42 and shows that in addition to the canonical PAK4 CDC42/RAC interactive binding (CRIB) domain binding to CDC42 there are unexpected contacts involving the PAK4 kinase C-lobe, CDC42, and the PAK4 polybasic region. These additional interactions modulate kinase activity and increase the binding affinity of CDC42 for full-length PAK4 compared with the CRIB domain alone. We therefore show that the interaction of CDC42 with PAK4 can influence kinase activity in a previously unappreciated manner. [ABSTRACT FROM AUTHOR]

Published
2018
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105. Metabolic Rewiring by Oncogenic BRAF V600E Links Ketogenesis Pathway to BRAF-MEK1 Signaling

Author

Kang, Hee-Bum, primary, Fan, Jun, additional, Lin, Ruiting, additional, Elf, Shannon, additional, Ji, Quanjiang, additional, Zhao, Liang, additional, Jin, Lingtao, additional, Seo, Jae Ho, additional, Shan, Changliang, additional, Arbiser, Jack L., additional, Cohen, Cynthia, additional, Brat, Daniel, additional, Miziorko, Henry M., additional, Kim, Eunhee, additional, Abdel-Wahab, Omar, additional, Merghoub, Taha, additional, Fröhling, Stefan, additional, Scholl, Claudia, additional, Tamayo, Pablo, additional, Barbie, David A., additional, Zhou, Lu, additional, Pollack, Brian P., additional, Fisher, Kevin, additional, Kudchadkar, Ragini R., additional, Lawson, David H., additional, Sica, Gabriel, additional, Rossi, Michael, additional, Lonial, Sagar, additional, Khoury, Hanna J., additional, Khuri, Fadlo R., additional, Lee, Benjamin H., additional, Boggon, Titus J., additional, He, Chuan, additional, Kang, Sumin, additional, and Chen, Jing, additional

Published
2015
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109. Glutamate Dehydrogenase 1 Signals through Antioxidant Glutathione Peroxidase 1 to Regulate Redox Homeostasis and Tumor Growth

Author

Jin, Lingtao, primary, Li, Dan, additional, Alesi, Gina N., additional, Fan, Jun, additional, Kang, Hee-Bum, additional, Lu, Zhou, additional, Boggon, Titus J., additional, Jin, Peng, additional, Yi, Hong, additional, Wright, Elizabeth R., additional, Duong, Duc, additional, Seyfried, Nicholas T., additional, Egnatchik, Robert, additional, DeBerardinis, Ralph J., additional, Magliocca, Kelly R., additional, He, Chuan, additional, Arellano, Martha L., additional, Khoury, Hanna J., additional, Shin, Dong M., additional, Khuri, Fadlo R., additional, and Kang, Sumin, additional

Published
2015
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113. Mutation of NLRC4 causes a syndrome of enterocolitis and autoinflammation

Author

Romberg, Neil, primary, Al Moussawi, Khatoun, additional, Nelson-Williams, Carol, additional, Stiegler, Amy L, additional, Loring, Erin, additional, Choi, Murim, additional, Overton, John, additional, Meffre, Eric, additional, Khokha, Mustafa K, additional, Huttner, Anita J, additional, West, Brian, additional, Podoltsev, Nikolai A, additional, Boggon, Titus J, additional, Kazmierczak, Barbara I, additional, and Lifton, Richard P, additional

Published
2014
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114. Tyr-301 Phosphorylation Inhibits Pyruvate Dehydrogenase by Blocking Substrate Binding and Promotes the Warburg Effect

Author

Fan, Jun, primary, Kang, Hee-Bum, additional, Shan, Changliang, additional, Elf, Shannon, additional, Lin, Ruiting, additional, Xie, Jianxin, additional, Gu, Ting-Lei, additional, Aguiar, Mike, additional, Lonning, Scott, additional, Chung, Tae-Wook, additional, Arellano, Martha, additional, Khoury, Hanna J., additional, Shin, Dong M., additional, Khuri, Fadlo R., additional, Boggon, Titus J., additional, Kang, Sumin, additional, and Chen, Jing, additional

Published
2014
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117. Tyr-94 Phosphorylation Inhibits Pyruvate Dehydrogenase Phosphatase 1 and Promotes Tumor Growth

Author

Shan, Changliang, primary, Kang, Hee-Bum, additional, Elf, Shannon, additional, Xie, Jianxin, additional, Gu, Ting-Lei, additional, Aguiar, Mike, additional, Lonning, Scott, additional, Hitosugi, Taro, additional, Chung, Tae-Wook, additional, Arellano, Martha, additional, Khoury, Hanna J., additional, Shin, Dong M., additional, Khuri, Fadlo R., additional, Boggon, Titus J., additional, and Fan, Jun, additional

Published
2014
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118. Lysine Acetylation Activates 6-Phosphogluconate Dehydrogenase to Promote Tumor Growth

Author

Shan, Changliang, primary, Elf, Shannon, additional, Ji, Quanjiang, additional, Kang, Hee-Bum, additional, Zhou, Lu, additional, Hitosugi, Taro, additional, Jin, Lingtao, additional, Lin, Ruiting, additional, Zhang, Liang, additional, Seo, Jae Ho, additional, Xie, Jianxin, additional, Tucker, Meghan, additional, Gu, Ting-Lei, additional, Sudderth, Jessica, additional, Jiang, Lei, additional, DeBerardinis, Ralph J., additional, Wu, Shaoxiong, additional, Li, Yuancheng, additional, Mao, Hui, additional, Chen, Peng R., additional, Wang, Dongsheng, additional, Chen, Georgia Zhuo, additional, Lonial, Sagar, additional, Arellano, Martha L., additional, Khoury, Hanna J., additional, Khuri, Fadlo R., additional, Lee, Benjamin H., additional, Brat, Daniel J., additional, Ye, Keqiang, additional, Boggon, Titus J., additional, He, Chuan, additional, Kang, Sumin, additional, Fan, Jun, additional, and Chen, Jing, additional

Published
2014
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120. Tyr Phosphorylation of PDP1 Toggles Recruitment between ACAT1 and SIRT3 to Regulate the Pyruvate Dehydrogenase Complex

Author

Fan, Jun, primary, Shan, Changliang, additional, Kang, Hee-Bum, additional, Elf, Shannon, additional, Xie, Jianxin, additional, Tucker, Meghan, additional, Gu, Ting-Lei, additional, Aguiar, Mike, additional, Lonning, Scott, additional, Chen, Huaibin, additional, Mohammadi, Moosa, additional, Britton, Laura-Mae P., additional, Garcia, Benjamin A., additional, Alečković, Maša, additional, Kang, Yibin, additional, Kaluz, Stefan, additional, Devi, Narra, additional, Van Meir, Erwin G., additional, Hitosugi, Taro, additional, Seo, Jae Ho, additional, Lonial, Sagar, additional, Gaddh, Manila, additional, Arellano, Martha, additional, Khoury, Hanna J., additional, Khuri, Fadlo R., additional, Boggon, Titus J., additional, Kang, Sumin, additional, and Chen, Jing, additional

Published
2014
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121. Identification of a Major Determinant for Serine-Threonine Kinase Phosphoacceptor Specificity

Author

Chen, Catherine, primary, Ha, Byung Hak, additional, Thévenin, Anastasia F., additional, Lou, Hua Jane, additional, Zhang, Rong, additional, Yip, Kevin Y., additional, Peterson, Jeffrey R., additional, Gerstein, Mark, additional, Kim, Philip M., additional, Filippakopoulos, Panagis, additional, Knapp, Stefan, additional, Boggon, Titus J., additional, and Turk, Benjamin E., additional

Published
2014
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127. Tyr26 phosphorylation of PGAM1 provides a metabolic advantage to tumours by stabilizing the active conformation

Author

Hitosugi, Taro, primary, Zhou, Lu, additional, Fan, Jun, additional, Elf, Shannon, additional, Zhang, Liang, additional, Xie, Jianxin, additional, Wang, Yi, additional, Gu, Ting-Lei, additional, Alečković, Masa, additional, LeRoy, Gary, additional, Kang, Yibin, additional, Kang, Hee-Bum, additional, Seo, Jae-Ho, additional, Shan, Changliang, additional, Jin, Peng, additional, Gong, Weimin, additional, Lonial, Sagar, additional, Arellano, Martha L., additional, Khoury, Hanna J., additional, Chen, Georgia Z., additional, Shin, Dong M., additional, Khuri, Fadlo R., additional, Boggon, Titus J., additional, Kang, Sumin, additional, He, Chuan, additional, and Chen, Jing, additional

Published
2013
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129. Abstract 2925: p90RSK2 coordinates pro-apoptotic and anti-apoptotic signaling pathways to protect cancer cells from anoikis.

Author

Jin, Lingtao, primary, Li, Dan, additional, Lee, Jongseok, additional, Alesi, Gina N., additional, Fan, Jun, additional, Kang, Hee-Bum, additional, Wang, Dongsheng, additional, Fu, Haian, additional, Taunton, Jack, additional, Boggon, Titus J., additional, Tucker, Meghan, additional, Gu, Ting-Lei, additional, Chen, Zhuo G., additional, Shin, Dong M., additional, Khuri, Fadlo R., additional, and Kang, Sumin, additional

Published
2013
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134. Mutational landscape of uterine and ovarian carcinosarcomas implicates histone genes in epithelial-mesenchymal transition.

Author

Falchetti, Marcella, Siming Zhao, Thakral, Durga, Jungmin Choi, Bi, Mark, Mane, Shrikant, Bilgüvar, Kaya, Lifton, Richard P., Edraki, Babak, Lee, Moses, Choi, Murim, Stiegler, Amy L., Boggon, Titus J., Schlessinger, Joseph, Birrer, Michael J., Kohn, Elise, Bellone, Stefania, Lopez, Salvatore, Schwab, Carlton, and English, Diana P.

Subjects
CARCINOSARCOMAS, UTERINE cancer, OVARIAN cancer, EXONS (Genetics), EPITHELIAL cell culture
Abstract

Carcinosarcomas (CSs) of the uterus and ovary are highly aggressive neoplasms containing both carcinomatous and sarcomatous elements. We analyzed the mutational landscape of 68 uterine and ovarian CSs by whole-exome sequencing. We also performed multiregion whole-exome sequencing comprising two carcinoma and sarcoma samples from six tumors to resolve their evolutionary histories. The results demonstrated that carcinomatous and sarcomatous elements derive from a common precursor having mutations typical of carcinomas. In addition to mutations in cancer genes previously identified in uterine and ovarian carcinomas such as TP53, PIK3CA, PPP2R1A, KRAS, PTEN, CHD4, and BCOR, we found an excess of mutations in genes encoding histone H2A and H2B, as well as significant amplification of the segment of chromosome 6p harboring the histone gene cluster containing these genes. We also found frequent deletions of the genes TP53 and MBD3 (a member with CHD4 of the nucleosome remodeling deacetylase complex) and frequent amplification of chromosome segments containing the genes PIK3CA, TERT, and MYC. Stable transgenic expression of H2A and H2B in a uterine serous carcinoma cell line demonstrated that mutant, but not wild-type, histones increased expression of markers of epithelial-mesenchymal transition (EMT) as well as tumor migratory and invasive properties, suggesting a role in sarcomatous transformation. Comparison of the phylogenetic relationships of carcinomatous and sarcomatous elements of the same tumors demonstrated separate lineages leading to these two components. These findings define the genetic landscape of CSs and suggest therapeutic targets for these highly aggressive neoplasms. [ABSTRACT FROM AUTHOR]

Published
2016
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135. PAK6 targets to cell-cell adhesions through its N-terminus in a Cdc42-dependent manner to drive epithelial colony escape.

Author

Morse, Elizabeth M., Xiaowen Sun, Olberding, Jordan R., Byung Hak Ha, Boggon, Titus J., and Calderwood, David A.

Subjects
CELL-matrix adhesions, KINASES, CELL adhesion, PROSTATE cancer, COSTAMERES
Abstract

The six serine/threonine kinases in the p21-activated kinase (PAK) family are important regulators of cell adhesion, motility and survival. PAK6, which is overexpressed in prostate cancer, was recently reported to localize to cell-cell adhesions and to drive epithelial cell colony escape. Here we report that PAK6 targeting to cell-cell adhesions occurs through its N-terminus, requiring both its Cdc42/ Rac interactive binding (CRIB) domain and an adjacent polybasic region for maximal targeting efficiency. We find PAK6 localization to cell-cell adhesions is Cdc42-dependent, as Cdc42 knockdown inhibits PAK6 targeting to cell-cell adhesions. We further find the ability of PAK6 to drive epithelial cell colony escape requires kinase activity and is disrupted by mutations that perturb PAK6 cell-cell adhesion targeting. Finally, we demonstrate that all type II PAKs (PAK4, PAK5 and PAK6) target to cell-cell adhesions, albeit to differing extents, but PAK1 (a type I PAK) does not. Notably, the ability of a PAK isoform to drive epithelial colony escape correlates with its targeting to cell-cell adhesions. We conclude that PAKs have a broader role in the regulation of cell-cell adhesions than previously appreciated. [ABSTRACT FROM AUTHOR]

Published
2016
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137. Diverse p120RasGAP interactions with doubly phosphorylated partners EphB4, p190RhoGAP, and Dok1.

Author

Vish, Kimberly J., Stiegler, Amy L., and Boggon, Titus J.

Subjects
*GTPASE-activating protein, *CATALYTIC activity, *SMALL-angle X-ray scattering, *X-ray scattering
Abstract

RasGAP (p120RasGAP), the founding member of the GTPase-activating protein (GAP) family, is one of only nine human proteins to contain two SH2 domains and is essential for proper vascular development. Despite its importance, its interactions with key binding partners remains unclear. In this study we provide a detailed viewpoint of RasGAP recruitment to various binding partners and assess their impact on RasGAP activity. We reveal the RasGAP SH2 domains generate distinct binding interactions with three well-known doubly phosphorylated binding partners: p190RhoGAP, Dok1, and EphB4. Affinity measurements demonstrate a 100-fold weakened affinity for RasGAP-EphB4 binding compared to RasGAP-p190RhoGAP or RasGAP-Dok1 binding, possibly driven by single versus dual SH2 domain engagement with a dominant N-terminal SH2 interaction. Small-angle X-ray scattering reveals conformational differences between RasGAP-EphB4 binding and RasGAPp190RhoGAP binding. Importantly, these interactions do not impact catalytic activity, implying RasGAP utilizes its SH2 domains to achieve diverse spatial-temporal regulation of Ras signaling in a previously unrecognized fashion. [ABSTRACT FROM AUTHOR]

Published
2023
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139. Activation of the AXL kinase causes resistance to EGFR-targeted therapy in lung cancer

Author

Zhang, Zhenfeng, primary, Lee, Jae Cheol, additional, Lin, Luping, additional, Olivas, Victor, additional, Au, Valerie, additional, LaFramboise, Thomas, additional, Abdel-Rahman, Mohamed, additional, Wang, Xiaoqi, additional, Levine, Alan D, additional, Rho, Jin Kyung, additional, Choi, Yun Jung, additional, Choi, Chang-Min, additional, Kim, Sang-We, additional, Jang, Se Jin, additional, Park, Young Soo, additional, Kim, Woo Sung, additional, Lee, Dae Ho, additional, Lee, Jung-Shin, additional, Miller, Vincent A, additional, Arcila, Maria, additional, Ladanyi, Marc, additional, Moonsamy, Philicia, additional, Sawyers, Charles, additional, Boggon, Titus J, additional, Ma, Patrick C, additional, Costa, Carlota, additional, Taron, Miquel, additional, Rosell, Rafael, additional, Halmos, Balazs, additional, and Bivona, Trever G, additional

Published
2012
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144. Genomic analysis of 220 CTCLs identifies a novel recurrent gain-of-function alteration in RLTPR (p.Q575E)

Author

Park, Joonhee, Yang, Jingyi, Wenzel, Alexander T., Ramachandran, Akshaya, Lee, Wung J., Daniels, Jay C., Kim, Juhyun, Martinez-Escala, Estela, Amankulor, Nduka, Pro, Barbara, Guitart, Joan, Mendillo, Marc L., Savas, Jeffrey N., Boggon, Titus J., and Choi, Jaehyuk

Abstract

Cutaneous T-cell lymphoma (CTCL) is an incurable non-Hodgkin lymphoma of the skin-homing T cell. In early-stage disease, lesions are limited to the skin, but in later-stage disease, the tumor cells can escape into the blood, the lymph nodes, and at times the visceral organs. To clarify the genomic basis of CTCL, we performed genomic analysis of 220 CTCLs. Our analyses identify 55 putative driver genes, including 17 genes not previously implicated in CTCL. These novel mutations are predicted to affect chromatin (BCOR, KDM6A, SMARCB1, TRRAP), immune surveillance (CD58, RFXAP), MAPK signaling (MAP2K1, NF1), NF-κB signaling (PRKCB, CSNK1A1), PI-3-kinase signaling (PIK3R1, VAV1), RHOA/cytoskeleton remodeling (ARHGEF3), RNA splicing (U2AF1), T-cell receptor signaling (PTPRN2, RLTPR), and T-cell differentiation (RARA). Our analyses identify recurrent mutations in 4 genes not previously identified in cancer. These include CK1α (encoded by CSNK1A1) (p.S27F; p.S27C), PTPRN2 (p.G526E), RARA (p.G303S), and RLTPR (p.Q575E). Last, we functionally validate CSNK1A1and RLTPRas putative oncogenes. RLTPRencodes a recently described scaffolding protein in the T-cell receptor signaling pathway. We show that RLTPR (p.Q575E) increases binding of RLTPR to downstream components of the NF-κB signaling pathway, selectively upregulates the NF-κB pathway in activated T cells, and ultimately augments T-cell-receptor-dependent production of interleukin 2 by 34-fold. Collectively, our analysis provides novel insights into CTCL pathogenesis and elucidates the landscape of potentially targetable gene mutations.

Published
2017
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145. Tyrosine Phosphorylation of Lactate Dehydrogenase A Is Important for NADH/NAD+ Redox Homeostasis in Cancer Cells

Author

Fan, Jun, primary, Hitosugi, Taro, additional, Chung, Tae-Wook, additional, Xie, Jianxin, additional, Ge, Qingyuan, additional, Gu, Ting-Lei, additional, Polakiewicz, Roberto D., additional, Chen, Georgia Z., additional, Boggon, Titus J., additional, Lonial, Sagar, additional, Khuri, Fadlo R., additional, Kang, Sumin, additional, and Chen, Jing, additional

Published
2011
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146. Tyrosine Phosphorylation of Mitochondrial Pyruvate Dehydrogenase Kinase 1 Is Important for Cancer Metabolism

Author

Hitosugi, Taro, primary, Fan, Jun, additional, Chung, Tae-Wook, additional, Lythgoe, Katherine, additional, Wang, Xu, additional, Xie, Jianxin, additional, Ge, Qingyuan, additional, Gu, Ting-Lei, additional, Polakiewicz, Roberto D., additional, Roesel, Johannes L., additional, Chen, Georgia Z., additional, Boggon, Titus J., additional, Lonial, Sagar, additional, Fu, Haian, additional, Khuri, Fadlo R., additional, Kang, Sumin, additional, and Chen, Jing, additional

Published
2011
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