Your search keyword '"Huang, Shixia"' showing total 388 results

1. The IL6/JAK/STAT3 signaling axis is a therapeutic vulnerability in SMARCB1-deficient bladder cancer

Author

Amara, Chandra Sekhar, Kami Reddy, Karthik Reddy, Yuntao, Yang, Chan, Yuen San, Piyarathna, Danthasinghe Waduge Badrajee, Dobrolecki, Lacey Elizabeth, Shih, David J. H., Shi, Zhongcheng, Xu, Jun, Huang, Shixia, Ellis, Matthew J., Apolo, Andrea B., Ballester, Leomar Y., Gao, Jianjun, Hansel, Donna E., Lotan, Yair, Hodges, H. Courtney, Lerner, Seth P., Creighton, Chad J., Sreekumar, Arun, Zheng, W. Jim, Msaouel, Pavlos, Kavuri, Shyam M., and Putluri, Nagireddy

Published

2024

2. The IFITM5 mutation in osteogenesis imperfecta type V is associated with an ERK/SOX9-dependent osteoprogenitor differentiation defect

Author

Marom, Ronit, Song, I-Wen, Busse, Emily C., Washington, Megan E., Berrier, Ava S., Rossi, Vittoria C., Ortinau, Laura, Jeong, Youngjae, Jiang, Ming-Ming, Dawson, Brian C., Adeyeye, Mary, Leynes, Carolina, Lietman, Caressa D., Stroup, Bridget M., Batkovskyte, Dominyka, Jain, Mahim, Chen, Yuqing, Cela, Racel, Castellon, Alexis, Tran, Alyssa A., Lorenzo, Isabel, Meyers, D. Nicole, Huang, Shixia, Turner, Alicia, Shenava, Vinitha, Wallace, Maegen, Orwoll, Eric, Park, Dongsu, Ambrose, Catherine G., Nagamani, Sandesh C.S., Heaney, Jason D., and Lee, Brendan H.

Subjects

Osteogenesis imperfecta -- Genetic aspects -- Risk factors -- Development and progression, Membrane proteins -- Analysis -- Health aspects, Health care industry

Abstract

Osteogenesis imperfecta (OI) type V is the second most common form of OI, distinguished by hyperplastic callus formation and calcification of the interosseous membranes, in addition to the bone fragility. It is caused by a recurrent, dominant pathogenic variant (c.-14C>T) in interferon-induced transmembrane protein 5 (IFITM5). Here, we generated a conditional Roso26-knockin mouse model to study the mechanistic consequences of the recurrent mutation. Expression of the mutant Ifitm5 in osteo-chondroprogenitor or chondrogenic cells resulted in low bone mass and growth retardation. Mutant limbs showed impaired endochondral ossification, cartilage overgrowth, and abnormal growth plate architecture. The cartilage phenotype correlates with the pathology reported in patients with OI type V. Surprisingly, expression of mutant Ifitm5 in mature osteoblasts caused no obvious skeletal abnormalities. In contrast, earlier expression in osteo-chondroprogenitors was associated with an increase in the skeletal progenitor cell population within the periosteum. Lineage tracing showed that chondrogenic cells expressing the mutant Ifitm5 had decreased differentiation into osteoblastic cells in diaphyseal bone. Moreover, mutant IFITM5 disrupted early skeletal homeostasis in part by activating ERK signaling and downstream SOX9 protein, and inhibition of these pathways partially rescued the phenotype in mutant animals. These data identify the contribution of a signaling defect altering osteo-chondroprogenitor differentiation as a driver in the pathogenesis of OI type V., Introduction Osteogenesis imperfecta (OI) is an inherited multi-systemic disorder characterized by low bone mass, recurrent fractures, growth deficiency, and skeletal deformities (1-3). Extraskeletal manifestations may include muscle weakness, dentinogenesis imperfecta, [...]

Published

2024

3. BST2 facilitates activation of hematopoietic stem cells through ERK signaling

Author

Florez, Marcus A., Thatavarty, Apoorva, Le, Duy T., Hill, Holly A., Jeong, Youngjae, Ho, Brian M., Kus, Pawel, Wathan, Trisha K., Kain, Bailee N., Huang, Shixia, Park, Dongsu, and King, Katherine Y.

Published

2024

4. Sirt6 protects retinal ganglion cells and optic nerve from degeneration during aging and glaucoma

Author

Xia, Fan, Shi, Shuizhen, Palacios, Erick, Liu, Wei, Buscho, Seth E., Li, Joseph, Huang, Shixia, Vizzeri, Gianmarco, Dong, Xiaocheng Charlie, Motamedi, Massoud, Zhang, Wenbo, and Liu, Hua

Published

2024

5. CD24 negativity reprograms mitochondrial metabolism to PPARα and NF-κB-driven fatty acid β-oxidation in triple-negative breast cancer

Author

Murthy, Divya, Dutta, Debasmita, Attri, Kuldeep S., Samanta, Tagari, Yang, Sukjin, Jung, Kwang Hwa, Latario, Sarah G., Putluri, Vasanta, Huang, Shixia, Putluri, Nagireddy, Park, Jun Hyoung, and Kaipparettu, Benny Abraham

Published

2024

6. Inhibition of GATA2 in prostate cancer by a clinically available small molecule.

Author

Kaochar, Salma, Rusin, Aleksandra, Foley, Christopher, Rajapakshe, Kimal, Robertson, Matthew, Skapura, Darlene, Mason, Cammy, Berman De Ruiz, Karen, Tyryshkin, Alexey, Deng, Jenny, Shin, Jin, Fiskus, Warren, Dong, Jianrong, Huang, Shixia, Navone, Nora, Davis, Christel, Ehli, Erik, Coarfa, Cristian, and Mitsiades, Nicholas

Subjects

Dilazep, GATA2, c-MYC, castration-resistance, prostate cancer, Cell Line, Tumor, Chromatin, Dilazep, GATA2 Transcription Factor, Gene Expression Regulation, Neoplastic, Humans, Male, Oncogenes, Prostatic Neoplasms, Castration-Resistant, Receptors, Androgen

Abstract

Castration-resistant prostate cancer (CRPC) remains highly lethal and in need of novel, actionable therapeutic targets. The pioneer factor GATA2 is a significant prostate cancer (PC) driver and is linked to poor prognosis. GATA2 directly promotes androgen receptor (AR) gene expression (both full-length and splice-variant) and facilitates AR binding to chromatin, recruitment of coregulators, and target gene transcription. Unfortunately, there is no clinically applicable GATA2 inhibitor available at the moment. Using a bioinformatics algorithm, we screened in silico 2650 clinically relevant drugs for a potential GATA2 inhibitor. Validation studies used cytotoxicity and proliferation assays, global gene expression analysis, RT-qPCR, reporter assay, reverse phase protein array analysis (RPPA), and immunoblotting. We examined target engagement via cellular thermal shift assay (CETSA), ChIP-qPCR, and GATA2 DNA-binding assay. We identified the vasodilator dilazep as a potential GATA2 inhibitor and confirmed on-target activity via CETSA. Dilazep exerted anticancer activity across a broad panel of GATA2-dependent PC cell lines in vitro and in a PDX model in vivo. Dilazep inhibited GATA2 recruitment to chromatin and suppressed the cell-cycle program, transcriptional programs driven by GATA2, AR, and c-MYC, and the expression of several oncogenic drivers, including AR, c-MYC, FOXM1, CENPF, EZH2, UBE2C, and RRM2, as well as of several mediators of metastasis, DNA damage repair, and stemness. In conclusion, we provide, via an extensive compendium of methodologies, proof-of-principle that a small molecule can inhibit GATA2 function and suppress its downstream AR, c-MYC, and other PC-driving effectors. We propose GATA2 as a therapeutic target in CRPC.

Published

2021

7. LncRNA PVT-1 promotes osteosarcoma cancer stem-like properties through direct interaction with TRIM28 and TSC2 ubiquitination

Author

Tsang, Susan V., Rainusso, Nino, Liu, Meng, Nomura, Motonari, Patel, Tajhal D., Nakahata, Kengo, Kim, Ha Ram, Huang, Shixia, Rajapakshe, Kimal, Coarfa, Cristian, Man, Tsz-Kwong, Rao, Pulivarthi H., and Yustein, Jason T.

Published

2022

8. Regorafenib is effective against neuroblastoma in vitro and in vivo and inhibits the RAS/MAPK, PI3K/Akt/mTOR and Fos/Jun pathways.

Author

Subramonian, Divya, Phanhthilath, Nikki, Rinehardt, Hannah, Mo, Qianxing, Huang, Shixia, Lesperance, Jacqueline, Huo, Yuchen, Zhang, Jing, Messer, Karen, Zage, Peter, and Flynn, Sean

Subjects

Animals, Cell Cycle, Cell Line, Tumor, Cell Proliferation, Cell Survival, Drug Synergism, Female, Gene Expression Regulation, Neoplastic, Humans, Isotretinoin, Mice, Mitogen-Activated Protein Kinases, Neuroblastoma, Phenylurea Compounds, Phosphatidylinositol 3-Kinases, Protein Kinase Inhibitors, Proto-Oncogene Proteins c-akt, Proto-Oncogene Proteins c-fos, Proto-Oncogene Proteins c-jun, Pyridines, Signal Transduction, TOR Serine-Threonine Kinases, Xenograft Model Antitumor Assays, ras Proteins

Abstract

BACKGROUND: Regorafenib is an inhibitor of multiple kinases with aberrant expression and activity in neuroblastoma tumours that have potential roles in neuroblastoma pathogenesis. METHODS: We evaluated neuroblastoma cells treated with regorafenib for cell viability and confluence, and analysed treated cells for apoptosis and cell cycle progression. We evaluated the efficacy of regorafenib in vivo using an orthotopic xenograft model. We evaluated regorafenib-mediated inhibition of kinase targets and performed reverse-phase protein array (RPPA) analysis of neuroblastoma cells treated with regorafenib. Lastly, we evaluated the efficacy and effects of the combination of regorafenib and 13-cis-retinoic acid on intracellular signalling. RESULTS: Regorafenib treatment resulted in reduced neuroblastoma cell viability and confluence, with both induction of apoptosis and of cell cycle arrest. Regorafenib treatment inhibits known receptor tyrosine kinase targets RET and PDGFRβ and intracellular signalling through the RAS/MAPK, PI3K/Akt/mTOR and Fos/Jun pathways. Regorafenib is effective against neuroblastoma tumours in vivo, and the combination of regorafenib and 13-cis-retinoic acid demonstrates enhanced efficacy compared with regorafenib alone. CONCLUSIONS: The effects of regorafenib on multiple intracellular signalling pathways and the potential additional efficacy when combined with 13-cis-retinoic acid represent opportunities to develop treatment regimens incorporating regorafenib for children with neuroblastoma.

Published

2020

9. STAT5 confers lactogenic properties in breast tumorigenesis and restricts metastatic potential

Author

Lin, Meng, Ku, Amy T., Dong, Jie, Yue, Fei, Jiang, Weiyu, Ibrahim, Ahmed Atef, Peng, Fanglue, Creighton, Chad J., Nagi, Chandandeep, Gutierrez, Carolina, Rosen, Jeffrey M., Zhang, Xiang H.-F., Hilsenbeck, Susan G., Chen, Xi, Du, Yi-Chieh Nancy, Huang, Shixia, Shi, Aiping, Fan, Zhimin, and Li, Yi

Published

2022

10. AIMp1 Potentiates TH1 Polarization and Is Critical for Effective Antitumor and Antiviral Immunity

Author

Liang, Dan, Tian, Lin, You, Ran, Halpert, Matthew M, Konduri, Vanaja, Baig, Yunyu C, Paust, Silke, Kim, Doyeun, Kim, Sunghoon, Jia, Fuli, Huang, Shixia, Zhang, Xiang, Kheradmand, Farrah, Corry, David B, Gilbert, Brian E, Levitt, Jonathan M, and Decker, William K

Subjects

Immunization, Infectious Diseases, Vaccine Related, Cancer, Emerging Infectious Diseases, Infection, Inflammatory and immune system, dendritic cell, AI Mp1, TH1 immunity, IL-12, antitumor immunity, antiviral immunity, p38 MAPK signaling, AIMp1, Immunology, Medical Microbiology

Abstract

Dendritic cells (DCs) must integrate a broad array of environmental cues to exact control over downstream immune responses including TH polarization. The multienzyme aminoacyl-tRNA synthetase complex component AIMp1/p43 responds to cellular stress and exerts pro-inflammatory functions; however, a role for DC-expressed AIMp1 in TH polarization has not previously been shown. Here, we demonstrate that the absence of AIMp1 in bone marrow-derived DC (BMDC) significantly impairs cytokine and costimulatory molecule expression, p38 MAPK signaling, and TH1 polarization of cocultured T-cells while significantly dysregulating immune-related gene expression. These deficits resulted in significantly compromised BMDC vaccine-mediated protection against melanoma. AIMp1 within the host was also critical for innate and adaptive antiviral immunity against influenza virus infection in vivo. Cancer patients with AIMp1 expression levels in the highest tertiles exhibited a 70% survival advantage at 15-year postdiagnosis as determined by bioinformatics analysis of nearly 9,000 primary human tumor samples in The Cancer Genome Atlas database. These data establish the importance of AIMp1 for the effective governance of antitumor and antiviral immune responses.

Published

2018

11. Supplementary Figure S1 from Selective CDK7 Inhibition Suppresses Cell Cycle Progression and MYC Signaling While Enhancing Apoptosis in Therapy-resistant Estrogen Receptor–positive Breast Cancer

Author

Guarducci, Cristina, primary, Nardone, Agostina, primary, Russo, Douglas, primary, Nagy, Zsuzsanna, primary, Heraud, Capucine, primary, Grinshpun, Albert, primary, Zhang, Qi, primary, Freelander, Allegra, primary, Leventhal, Mathew Joseph, primary, Feit, Avery, primary, Cohen Feit, Gabriella, primary, Feiglin, Ariel, primary, Liu, Weihan, primary, Hermida-Prado, Francisco, primary, Kesten, Nikolas, primary, Ma, Wen, primary, De Angelis, Carmine, primary, Morlando, Antonio, primary, O'Donnell, Madison, primary, Naumenko, Sergey, primary, Huang, Shixia, primary, Nguyen, Quang-Dé, primary, Huang, Ying, primary, Malorni, Luca, primary, Bergholz, Johann S., primary, Zhao, Jean J., primary, Fraenkel, Ernest, primary, Lim, Elgene, primary, Schiff, Rachel, primary, Shapiro, Geoffrey I., primary, and Jeselsohn, Rinath, primary

Published

2024

12. Data from Selective CDK7 Inhibition Suppresses Cell Cycle Progression and MYC Signaling While Enhancing Apoptosis in Therapy-resistant Estrogen Receptor–positive Breast Cancer

Author

Guarducci, Cristina, primary, Nardone, Agostina, primary, Russo, Douglas, primary, Nagy, Zsuzsanna, primary, Heraud, Capucine, primary, Grinshpun, Albert, primary, Zhang, Qi, primary, Freelander, Allegra, primary, Leventhal, Mathew Joseph, primary, Feit, Avery, primary, Cohen Feit, Gabriella, primary, Feiglin, Ariel, primary, Liu, Weihan, primary, Hermida-Prado, Francisco, primary, Kesten, Nikolas, primary, Ma, Wen, primary, De Angelis, Carmine, primary, Morlando, Antonio, primary, O'Donnell, Madison, primary, Naumenko, Sergey, primary, Huang, Shixia, primary, Nguyen, Quang-Dé, primary, Huang, Ying, primary, Malorni, Luca, primary, Bergholz, Johann S., primary, Zhao, Jean J., primary, Fraenkel, Ernest, primary, Lim, Elgene, primary, Schiff, Rachel, primary, Shapiro, Geoffrey I., primary, and Jeselsohn, Rinath, primary

Published

2024

13. Supplementary Tables S1-8 from Selective CDK7 Inhibition Suppresses Cell Cycle Progression and MYC Signaling While Enhancing Apoptosis in Therapy-resistant Estrogen Receptor–positive Breast Cancer

Author

Guarducci, Cristina, primary, Nardone, Agostina, primary, Russo, Douglas, primary, Nagy, Zsuzsanna, primary, Heraud, Capucine, primary, Grinshpun, Albert, primary, Zhang, Qi, primary, Freelander, Allegra, primary, Leventhal, Mathew Joseph, primary, Feit, Avery, primary, Cohen Feit, Gabriella, primary, Feiglin, Ariel, primary, Liu, Weihan, primary, Hermida-Prado, Francisco, primary, Kesten, Nikolas, primary, Ma, Wen, primary, De Angelis, Carmine, primary, Morlando, Antonio, primary, O'Donnell, Madison, primary, Naumenko, Sergey, primary, Huang, Shixia, primary, Nguyen, Quang-Dé, primary, Huang, Ying, primary, Malorni, Luca, primary, Bergholz, Johann S., primary, Zhao, Jean J., primary, Fraenkel, Ernest, primary, Lim, Elgene, primary, Schiff, Rachel, primary, Shapiro, Geoffrey I., primary, and Jeselsohn, Rinath, primary

Published

2024

14. Selective CDK7 Inhibition Suppresses Cell Cycle Progression and MYC Signaling While Enhancing Apoptosis in Therapy-resistant Estrogen Receptor–positive Breast Cancer

Author

Guarducci, Cristina, primary, Nardone, Agostina, additional, Russo, Douglas, additional, Nagy, Zsuzsanna, additional, Heraud, Capucine, additional, Grinshpun, Albert, additional, Zhang, Qi, additional, Freelander, Allegra, additional, Leventhal, Mathew Joseph, additional, Feit, Avery, additional, Cohen Feit, Gabriella, additional, Feiglin, Ariel, additional, Liu, Weihan, additional, Hermida-Prado, Francisco, additional, Kesten, Nikolas, additional, Ma, Wen, additional, De Angelis, Carmine, additional, Morlando, Antonio, additional, O'Donnell, Madison, additional, Naumenko, Sergey, additional, Huang, Shixia, additional, Nguyen, Quang-Dé, additional, Huang, Ying, additional, Malorni, Luca, additional, Bergholz, Johann S., additional, Zhao, Jean J., additional, Fraenkel, Ernest, additional, Lim, Elgene, additional, Schiff, Rachel, additional, Shapiro, Geoffrey I., additional, and Jeselsohn, Rinath, additional

Published

2024

15. Estimation of leaf color variances of Cotinus coggygria based on geographic and environmental variables

Author

Tan, Xing, Wu, Jiaojiao, Liu, Yun, Huang, Shixia, Gao, Lan, and Zhang, Wen

Published

2021

16. miR-431 Promotes Metastasis of Pancreatic Neuroendocrine Tumors by Targeting DAB2 Interacting Protein, a Ras GTPase Activating Protein Tumor Suppressor

Author

Zhang, Tiantian, Choi, Soyoung, Zhang, Tuo, Chen, Zhengming, Chi, Yudan, Huang, Shixia, Xiang, Jenny Z., and Du, Yi-Chieh Nancy

Published

2020

17. Abstract PR02: Modeling breast cancer through somatic precision gene editing with high flexibility and efficiency

Author

Bu, Wen, primary, Li, Yi, additional, Creighton, Chad J, additional, Heavener, Kelsey S, additional, Gutierrez, Carolina, additional, Dou, Yongchao, additional, Jiang, Weiyu, additional, Zhang, Bing, additional, Ku, Amy T, additional, and Huang, Shixia, additional

Published

2024

18. Metformin and an insulin/IGF-1 receptor inhibitor are synergistic in blocking growth of triple-negative breast cancer

Author

Xue, Lei, Chen, Fengju, Yue, Fei, Camacho, Laura, Kothapalli, Sushma, Wei, Guanyun, Huang, Shixia, Mo, Qianxing, Ma, Fei, Li, Yi, and Jiralerspong, Sao

Published

2021

19. Inhibition of the hexosamine biosynthetic pathway promotes castration-resistant prostate cancer.

Author

Kaushik, Akash, Shojaie, Ali, Panzitt, Katrin, Sonavane, Rajni, Venghatakrishnan, Harene, Manikkam, Mohan, Zaslavsky, Alexander, Putluri, Vasanta, Vasu, Vihas, Zhang, Yiqing, Khan, Ayesha, Lloyd, Stacy, Szafran, Adam, Dasgupta, Subhamoy, Bader, David, Stossi, Fabio, Li, Hangwen, Samanta, Susmita, Cao, Xuhong, Tsouko, Efrosini, Huang, Shixia, Frigo, Daniel, Chan, Lawrence, Edwards, Dean, Kaipparettu, Benny, Mitsiades, Nicholas, Weigel, Nancy, Mancini, Michael, McGuire, Sean, Mehra, Rohit, Ittmann, Michael, Chinnaiyan, Arul, Putluri, Nagireddy, Palapattu, Ganesh, Michailidis, George, and Sreekumar, Arun

Subjects

Animals, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, Cell Line, Hexosamines, Humans, Male, Mice, Mice, SCID, Phosphatidylinositol 3-Kinases, Prostatic Neoplasms, Castration-Resistant, Proto-Oncogene Proteins c-akt

Abstract

The precise molecular alterations driving castration-resistant prostate cancer (CRPC) are not clearly understood. Using a novel network-based integrative approach, here, we show distinct alterations in the hexosamine biosynthetic pathway (HBP) to be critical for CRPC. Expression of HBP enzyme glucosamine-phosphate N-acetyltransferase 1 (GNPNAT1) is found to be significantly decreased in CRPC compared with localized prostate cancer (PCa). Genetic loss-of-function of GNPNAT1 in CRPC-like cells increases proliferation and aggressiveness, in vitro and in vivo. This is mediated by either activation of the PI3K-AKT pathway in cells expressing full-length androgen receptor (AR) or by specific protein 1 (SP1)-regulated expression of carbohydrate response element-binding protein (ChREBP) in cells containing AR-V7 variant. Strikingly, addition of the HBP metabolite UDP-N-acetylglucosamine (UDP-GlcNAc) to CRPC-like cells significantly decreases cell proliferation, both in-vitro and in animal studies, while also demonstrates additive efficacy when combined with enzalutamide in-vitro. These observations demonstrate the therapeutic value of targeting HBP in CRPC.

Published

2016

20. The REGγ-proteasome forms a regulatory circuit with IκBɛ and NFκB in experimental colitis.

Author

Xu, Jinjin, Zhou, Lei, Ji, Lei, Chen, Fengyuan, Fortmann, Karen, Zhang, Kun, Liu, Qingwu, Li, Ke, Wang, Weicang, Wang, Hao, Xie, Wei, Wang, Qingwei, Liu, Jiang, Zheng, Biao, Zhang, Pei, Huang, Shixia, Shi, Tieliu, Zhang, Biaohong, Dang, Yongyan, Chen, Jiwu, O'Malley, Bert W, Moses, Robb E, Wang, Ping, Li, Lei, Xiao, Jianru, Hoffmann, Alexander, and Li, Xiaotao

Subjects

Intestinal Mucosa, HCT116 Cells, Animals, Mice, Inbred C57BL, Mice, Knockout, Humans, Colonic Neoplasms, Colitis, Proteasome Endopeptidase Complex, Dextran Sulfate, NF-kappa B, Autoantigens, I-kappa B Kinase, HEK293 Cells, Mice, Inbred C57BL, Knockout, Crohn's Disease, Digestive Diseases, Autoimmune Disease, Inflammatory Bowel Disease, 2.1 Biological and endogenous factors, Cancer, Oral and Gastrointestinal

Abstract

Increasing incidence of inflammatory bowel disorders demands a better understanding of the molecular mechanisms underlying its multifactorial aetiology. Here we demonstrate that mice deficient for REGγ, a proteasome activator, show significantly attenuated intestinal inflammation and colitis-associated cancer in dextran sodium sulfate model. Bone marrow transplantation experiments suggest that REGγ's function in non-haematopoietic cells primarily contributes to the phenotype. Elevated expression of REGγ exacerbates local inflammation and promotes a reciprocal regulatory loop with NFκB involving ubiquitin-independent degradation of IκBɛ. Additional deletion of IκBɛ restored colitis phenotypes and inflammatory gene expression in REGγ-deficient mice. In sum, this study identifies REGγ-mediated control of IκBɛ as a molecular mechanism that contributes to NFκB activation and promotes bowel inflammation and associated tumour formation in response to chronic injury.

Published

2016

21. High-Throughput Evaluation of Metabolic Activities Using Reverse Phase Protein Array Technology

Author

Lu, Hsin-Yi, primary, Xiong, Jian, additional, Perera, Dimuthu Nuwan, additional, Rajapakshe, Kimal, additional, Wang, Xuan, additional, Costello, Myra, additional, Holloway, Kimberly R., additional, Ramos, Carlos, additional, Grimm, Sandra L., additional, Wulfkuhle, Julia, additional, Coarfa, Cristian, additional, Edwards, Dean P., additional, Zhu, Michael X., additional, and Huang, Shixia, additional

Published

2021

22. SOD1 is a synthetic lethal target in PPM1D-mutant leukemia cells

Author

Zhang, Linda, primary, Hsu, Joanne I., additional, Braekeleer, Etienne D., additional, Chen, Chun-Wei, additional, Patel, Tajhal D., additional, Urya, Hidetaka, additional, Guzman, Anna G., additional, Martell, Alejandra G., additional, Waldvogel, Sarah M., additional, Tovy, Ayala, additional, Callen, Elsa, additional, Murdaugh, Rebecca, additional, Richard, Rosemary, additional, Jansen, Sandra, additional, Vissers, Lisenka, additional, de Vries, Bert B.A., additional, Nussenzweig, Andre, additional, Huang, Shixia, additional, Coarfa, Cristian, additional, Anastas, Jamie N., additional, Takahashi, Koichi, additional, Vassiliou, George, additional, and Goodell, Margaret A., additional

Published

2023

23. Author Response: SOD1 is a synthetic lethal target in PPM1D-mutant leukemia cells

Author

Zhang, Linda, primary, Hsu, Joanne I., additional, Braekeleer, Etienne D., additional, Chen, Chun-Wei, additional, Patel, Tajhal D., additional, Urya, Hidetaka, additional, Guzman, Anna G., additional, Martell, Alejandra G., additional, Waldvogel, Sarah M., additional, Tovy, Ayala, additional, Callen, Elsa, additional, Murdaugh, Rebecca, additional, Richard, Rosemary, additional, Jansen, Sandra, additional, Vissers, Lisenka, additional, de Vries, Bert B.A., additional, Nussenzweig, Andre, additional, Huang, Shixia, additional, Coarfa, Cristian, additional, Anastas, Jamie N., additional, Takahashi, Koichi, additional, Vassiliou, George, additional, and Goodell, Margaret A., additional

Published

2023

24. Targeting TGF-[beta] for treatment of osteogenesis imperfecta

Author

Song, I-Wen, Nagamani, Sandesh C.S., Nguyen, Dianne, Grafe, Ingo, Sutton, Vernon Reid, Gannon, Francis H., Munivez, Elda, Jiang, Ming-Ming, Tran, Alyssa, Wallace, Maegen, Esposito, Paul, Musaad, Salma, Strudthoff, Elizabeth, McGuire, Sharon, Thornton, Michele, Shenava, Vinitha, Rosenfeld, Scott, Huang, Shixia, Shypailo, Roman, Orwoll, Eric, and Lee, Brendan

Subjects

Osteogenesis imperfecta -- Genetic aspects -- Care and treatment -- Development and progression, Transforming growth factors -- Health aspects -- Genetic aspects, Cellular signal transduction -- Genetic aspects -- Health aspects, Molecular targeted therapy -- Methods -- Testing, Monoclonal antibodies -- Testing, Health care industry

Abstract

BACKGROUND. Currently, there is no disease-specific therapy for osteogenesis imperfecta (OI). Preclinical studies demonstrate that excessive TGF-[beta] signaling is a pathogenic mechanism in OI. Here, we evaluated TGF-[beta] signaling in children with OI and conducted a phase I clinical trial of TGF-[beta] inhibition in adults with OI. METHODS. Histology and RNA-Seq were performed on bones obtained from children. Gene Ontology (GO) enrichment assay, gene set enrichment analysis (GSEA), and Ingenuity Pathway Analysis (IPA) were used to identify dysregulated pathways. Reverse-phase protein array, Western blot, and IHC were performed to evaluate protein expression. A phase I study of fresolimumab, a TGF-[beta] neutralizing antibody, was conducted in 8 adults with OI. Safety and effects on bone remodeling markers and lumbar spine areal bone mineral density (LS aBMD) were assessed. RESULTS. OI bone demonstrated woven structure, increased osteocytes, high turnover, and reduced maturation. SMAD phosphorylation was the most significantly upregulated GO molecular event. GSEA identified the TGF-[beta] pathway as the top activated signaling pathway, and IPA showed that TGF-[beta]1 was the most significant activated upstream regulator mediating the global changes identified in OI bone. Treatment with fresolimumab was well-tolerated and associated with increases in LS aBMD in participants with OI type IV, whereas participants with OI type III and VIII had unchanged or decreased LS aBMD. CONCLUSION. Increased TGF-[beta] signaling is a driver pathogenic mechanism in OI. Anti-TGF-[beta] therapy could be a potential disease-specific therapy, with dose-dependent effects on bone mass and turnover. TRIAL REGISTRATION. ClinicalTrials.gov NCT03064074. FUNDING. Brittle Bone Disorders Consortium (U54AR068069), Clinical Translational Core of Baylor College of Medicine Intellectual and Developmental Disabilities Research Center (P50HD103555) from National Institute of Child Health and Human Development, USDA/ARS (cooperative agreement 58-6250-6-001), and Sanofi Genzyme., Introduction Osteogenesis imperfecta (OI) is a genetically and phenotypically heterogeneous Mendelian disorder of connective tissue that has an estimated prevalence of 1 in 10,000 to 20,000 births. Skeletal manifestations of [...]

Published

2022

25. BCL9/STAT3 regulation of transcriptional enhancer networks promote DCIS progression

Author

Elsarraj, Hanan S., Hong, Yan, Limback, Darlene, Zhao, Ruonan, Berger, Jenna, Bishop, Stephanie C., Sabbagh, Aria, Oppenheimer, Linzi, Harper, Haleigh E., Tsimelzon, Anna, Huang, Shixia, Hilsenbeck, Susan G., Edwards, Dean P., Fontes, Joseph, Fan, Fang, Madan, Rashna, Fangman, Ben, Ellis, Ashley, Tawfik, Ossama, Persons, Diane L., Fields, Timothy, Godwin, Andrew K., Hagan, Christy R., Swenson-Fields, Katherine, Coarfa, Cristian, Thompson, Jeffrey, and Behbod, Fariba

Published

2020

26. Dimethyl Sulfoxide Inhibits Bile Acid Synthesis in Healthy Mice but Does Not Protect Mice from Bile-Acid-Induced Liver Damage

Author

Chen, Xi, primary, Li, Huiqiao, additional, Liu, Yu’e, additional, Qi, Jing, additional, Dong, Bingning, additional, Huang, Shixia, additional, Zhao, Shangang, additional, and Zhu, Yi, additional

Published

2023

27. Evidence That Transgenes Encoding Components of the Wnt Signaling Pathway Preferentially Induce Mammary Cancers from Progenitor Cells

Author

Li, Yi, Welm, Bryan, Podsypanina, Katrina, Huang, Shixia, Chamorro, Mario, Zhang, Xiaomei, Rowlands, Tracey, Egeblad, Mikala, Cowin, Pam, Werb, Zena, Tan, Lee K., Rosen, Jeffrey M., and Varmus, Harold E.

Published

2003

28. Bempegaldesleukin selectively depletes intratumoral Tregs and potentiates T cell-mediated cancer therapy

Author

Sharma, Meenu, Khong, Hiep, Fa’ak, Faisal, Bentebibel, Salah-Eddine, Janssen, Louise M. E., Chesson, Brent C., Creasy, Caitlin A., Forget, Marie-Andrée, Kahn, Laura Maria S., Pazdrak, Barbara, Karki, Binisha, Hailemichael, Yared, Singh, Manisha, Vianden, Christina, Vennam, Srinivas, Bharadwaj, Uddalak, Tweardy, David J., Haymaker, Cara, Bernatchez, Chantale, Huang, Shixia, Rajapakshe, Kimal, Coarfa, Cristian, Hurwitz, Michael E., Sznol, Mario, Hwu, Patrick, Hoch, Ute, Addepalli, Murali, Charych, Deborah H., Zalevsky, Jonathan, Diab, Adi, and Overwijk, Willem W.

Published

2020

29. CGRRF1, a growth suppressor, regulates EGFR ubiquitination in breast cancer

Author

Lee, Yu-Ju, Ho, Shiuh-Rong, Graves, Joshua D., Xiao, Yang, Huang, Shixia, and Lin, Weei-Chin

Published

2019

30. Chapter 2 - Profiling histone posttranslational modifications and chromatin-modifying proteins by high-throughput reverse phase protein array

Author

Wang, Xuan, Shi, Zhongcheng, Young, Nicolas L., Edwards, Dean P., and Huang, Shixia

Published

2024

31. Changes in gene expression during the development of mammary tumors in MMTV-Wnt-1transgenic mice

Author

Huang, Shixia, Li, Yi, Chen, Yidong, Podsypanina, Katrina, Chamorro, Mario, Olshen, Adam B, Desai, Kartiki V, Tann, Anne, Petersen, David, Green, Jeffrey E, and Varmus, Harold E

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Breast Cancer, Biotechnology, Genetics, 2.1 Biological and endogenous factors, Aetiology, Animals, Gene Expression Profiling, Gene Expression Regulation, Neoplastic, Genes, Neoplasm, Genotype, Hyperplasia, Mammary Glands, Animal, Mammary Neoplasms, Animal, Mammary Tumor Virus, Mouse, Mice, Mice, Transgenic, Wnt1 Protein, Environmental Sciences, Information and Computing Sciences, Bioinformatics

Abstract

BackgroundIn human breast cancer normal mammary cells typically develop into hyperplasia, ductal carcinoma in situ, invasive cancer, and metastasis. The changes in gene expression associated with this stepwise progression are unclear. Mice transgenic for mouse mammary tumor virus (MMTV)-Wnt-1 exhibit discrete steps of mammary tumorigenesis, including hyperplasia, invasive ductal carcinoma, and distant metastasis. These mice might therefore be useful models for discovering changes in gene expression during cancer development.ResultsWe used cDNA microarrays to determine the expression profiles of five normal mammary glands, seven hyperplastic mammary glands and 23 mammary tumors from MMTV-Wnt-1 transgenic mice, and 12 mammary tumors from MMTV-Neu transgenic mice. Adipose tissues were used to control for fat cells in the vicinity of the mammary glands. In these analyses, we found that the progression of normal virgin mammary glands to hyperplastic tissues and to mammary tumors is accompanied by differences in the expression of several hundred genes at each step. Some of these differences appear to be unique to the effects of Wnt signaling; others seem to be common to tumors induced by both Neu and Wnt-1 oncogenes.ConclusionWe described gene-expression patterns associated with breast-cancer development in mice, and identified genes that may be significant targets for oncogenic events. The expression data developed provide a resource for illuminating the molecular mechanisms involved in breast cancer development, especially through the identification of genes that are critical in cancer initiation and progression.

Published

2005

32. Changes in gene expression during the development of mammary tumors in MMTV-Wnt-1 transgenic mice.

Author

Huang, Shixia, Li, Yi, Chen, Yidong, Podsypanina, Katrina, Chamorro, Mario, Olshen, Adam B, Desai, Kartiki V, Tann, Anne, Petersen, David, Green, Jeffrey E, and Varmus, Harold E

Subjects

Mammary Glands, Animal, Animals, Mice, Transgenic, Mice, Mammary Tumor Virus, Mouse, Mammary Neoplasms, Animal, Hyperplasia, Gene Expression Profiling, Gene Expression Regulation, Neoplastic, Genotype, Wnt1 Protein, Genes, Neoplasm, Mammary Glands, Animal, Transgenic, Mammary Tumor Virus, Mouse, Mammary Neoplasms, Gene Expression Regulation, Neoplastic, Genes, Neoplasm, Bioinformatics, Environmental Sciences, Biological Sciences, Information and Computing Sciences

Abstract

BackgroundIn human breast cancer normal mammary cells typically develop into hyperplasia, ductal carcinoma in situ, invasive cancer, and metastasis. The changes in gene expression associated with this stepwise progression are unclear. Mice transgenic for mouse mammary tumor virus (MMTV)-Wnt-1 exhibit discrete steps of mammary tumorigenesis, including hyperplasia, invasive ductal carcinoma, and distant metastasis. These mice might therefore be useful models for discovering changes in gene expression during cancer development.ResultsWe used cDNA microarrays to determine the expression profiles of five normal mammary glands, seven hyperplastic mammary glands and 23 mammary tumors from MMTV-Wnt-1 transgenic mice, and 12 mammary tumors from MMTV-Neu transgenic mice. Adipose tissues were used to control for fat cells in the vicinity of the mammary glands. In these analyses, we found that the progression of normal virgin mammary glands to hyperplastic tissues and to mammary tumors is accompanied by differences in the expression of several hundred genes at each step. Some of these differences appear to be unique to the effects of Wnt signaling; others seem to be common to tumors induced by both Neu and Wnt-1 oncogenes.ConclusionWe described gene-expression patterns associated with breast-cancer development in mice, and identified genes that may be significant targets for oncogenic events. The expression data developed provide a resource for illuminating the molecular mechanisms involved in breast cancer development, especially through the identification of genes that are critical in cancer initiation and progression.

Published

2005

33. TRAF4-mediated ubiquitination of NGF receptor TrkA regulates prostate cancer metastasis

Author

Singh, Ramesh, Karri, Dileep, Shen, Hong, Shao, Jiangyong, Dasgupta, Subhamoy, Huang, Shixia, Edwards, Dean P., Ittmann, Michael M., O'Malley, Bert W., and Yi, Ping

Subjects

Nerve growth factor -- Research, Tyrosine -- Research, Prostate cancer -- Genetic aspects -- Drug therapy -- Research, Gene expression -- Research, Health care industry

Abstract

Receptor tyrosine kinases (RTKs) are important drivers of cancers. In addition to genomic alterations, aberrant activation of WT RTKs plays an important role in driving cancer progression. However, the mechanisms underlying how RTKs drive prostate cancer remain incompletely characterized. Here we show that non-proteolytic ubiquitination of RTK regulates its kinase activity and contributes to RTK-mediated prostate cancer metastasis. TRAF4, an E3 ubiquitin ligase, is highly expressed in metastatic prostate cancer. We demonstrated here that it is a key player in regulating RTK-mediated prostate cancer metastasis. We further identified TrkA, a neurotrophin RTK, as a TRAF4-targeted ubiquitination substrate that promotes cancer cell invasion and found that inhibition of TrkA activity abolished TRAF4-dependent cell invasion. TRAF4 promoted K27- and K29-linked ubiquitination at the TrkA kinase domain and increased its kinase activity. Mutation of TRAF4-targeted ubiquitination sites abolished TrkA tyrosine autophosphorylation and its interaction with downstream proteins. TRAF4 knockdown also suppressed nerve growth factor (NGF) stimulated TrkA downstream p38 MAPK activation and invasion-associated gene expression. Furthermore, elevated TRAF4 levels significantly correlated with increased NGF-stimulated invasion-associated gene expression in prostate cancer patients, indicating that this signaling axis is significantly activated during oncogenesis. Our results revealed a posttranslational modification mechanism contributing to aberrant non-mutated RTK activation in cancer cells., Introduction Ubiquitination is an important posttranslational modification regulating protein degradation, trafficking, and activity, as well as protein-protein interaction. Dysregulation of the ubiquitin pathways has been implicated in a number of [...]

Published

2018

34. Caspase-2 is essential for proliferation and self-renewal of nucleophosmin-mutated acute myeloid leukemia.

Author

Sakthivel, Dharaniya, primary, Brown-Suedel, Alexandra N., additional, Keane, Francesca, additional, Huang, Shixia, additional, Mc Sherry, Kenneth, additional, Charendoff, Chloé I, additional, Dunne, Kevin P., additional, Robichaux, Dexter J, additional, Le, BaoChau, additional, Shin, Crystal S., additional, Carisey, Alexandre F, additional, Flanagan, Jonathan M., additional, and Bouchier-Hayes, Lisa, additional

Published

2023

35. Efficient cancer modeling through CRISPR-Cas9/HDR-based somatic precision gene editing in mice

Author

Bu, Wen, primary, Creighton, Chad J., additional, Heavener, Kelsey S., additional, Gutierrez, Carolina, additional, Dou, Yongchao, additional, Ku, Amy T., additional, Zhang, Yiqun, additional, Jiang, Weiyu, additional, Urrutia, Jazmin, additional, Jiang, Wen, additional, Yue, Fei, additional, Jia, Luyu, additional, Ibrahim, Ahmed Atef, additional, Zhang, Bing, additional, Huang, Shixia, additional, and Li, Yi, additional

Published

2023

36. Data from Loss of MutL Disrupts CHK2-Dependent Cell-Cycle Control through CDK4/6 to Promote Intrinsic Endocrine Therapy Resistance in Primary Breast Cancer

Author

Haricharan, Svasti, primary, Punturi, Nindo, primary, Singh, Purba, primary, Holloway, Kimberly R., primary, Anurag, Meenakshi, primary, Schmelz, Jacob, primary, Schmidt, Cheryl, primary, Lei, Jonathan T., primary, Suman, Vera, primary, Hunt, Kelly, primary, Olson, John A., primary, Hoog, Jeremy, primary, Li, Shunqiang, primary, Huang, Shixia, primary, Edwards, Dean P., primary, Kavuri, Shyam M., primary, Bainbridge, Matthew N., primary, Ma, Cynthia X., primary, and Ellis, Matthew J., primary

Published

2023

37. Figures S1-7 from Loss of MutL Disrupts CHK2-Dependent Cell-Cycle Control through CDK4/6 to Promote Intrinsic Endocrine Therapy Resistance in Primary Breast Cancer

Author

Haricharan, Svasti, primary, Punturi, Nindo, primary, Singh, Purba, primary, Holloway, Kimberly R., primary, Anurag, Meenakshi, primary, Schmelz, Jacob, primary, Schmidt, Cheryl, primary, Lei, Jonathan T., primary, Suman, Vera, primary, Hunt, Kelly, primary, Olson, John A., primary, Hoog, Jeremy, primary, Li, Shunqiang, primary, Huang, Shixia, primary, Edwards, Dean P., primary, Kavuri, Shyam M., primary, Bainbridge, Matthew N., primary, Ma, Cynthia X., primary, and Ellis, Matthew J., primary

Published

2023

38. Data from CCR2 Chemokine Receptors Enhance Growth and Cell-Cycle Progression of Breast Cancer Cells through SRC and PKC Activation

Author

Yao, Min, primary, Fang, Wei, primary, Smart, Curtis, primary, Hu, Qingting, primary, Huang, Shixia, primary, Alvarez, Nehemiah, primary, Fields, Patrick, primary, and Cheng, Nikki, primary

Published

2023

39. Supplementary Data from CCR2 Chemokine Receptors Enhance Growth and Cell-Cycle Progression of Breast Cancer Cells through SRC and PKC Activation

Author

Yao, Min, primary, Fang, Wei, primary, Smart, Curtis, primary, Hu, Qingting, primary, Huang, Shixia, primary, Alvarez, Nehemiah, primary, Fields, Patrick, primary, and Cheng, Nikki, primary

Published

2023

40. Data from Mammary Precancerous Stem and Non-Stem Cells Evolve into Cancers of Distinct Subtypes

Author

Bu, Wen, primary, Liu, Zhenyu, primary, Jiang, Weiyu, primary, Nagi, Chandandeep, primary, Huang, Shixia, primary, Edwards, Dean P., primary, Jo, Eunji, primary, Mo, Qianxing, primary, Creighton, Chad J., primary, Hilsenbeck, Susan G., primary, Leavitt, Andrew D., primary, Lewis, Michael T., primary, Wong, Stephen T. C., primary, and Li, Yi, primary

Published

2023

41. Supplementary File 5 from Mass Spectrometry–Based Proteomics Reveals Potential Roles of NEK9 and MAP2K4 in Resistance to PI3K Inhibition in Triple-Negative Breast Cancers

Author

Mundt, Filip, primary, Rajput, Sandeep, primary, Li, Shunqiang, primary, Ruggles, Kelly V., primary, Mooradian, Arshag D., primary, Mertins, Philipp, primary, Gillette, Michael A., primary, Krug, Karsten, primary, Guo, Zhanfang, primary, Hoog, Jeremy, primary, Erdmann-Gilmore, Petra, primary, Primeau, Tina, primary, Huang, Shixia, primary, Edwards, Dean P., primary, Wang, Xiaowei, primary, Wang, Xuya, primary, Kawaler, Emily, primary, Mani, D.R., primary, Clauser, Karl R., primary, Gao, Feng, primary, Luo, Jingqin, primary, Davies, Sherri R., primary, Johnson, Gary L., primary, Huang, Kuan-lin, primary, Yoon, Christopher J., primary, Ding, Li, primary, Fenyö, David, primary, Ellis, Matthew J., primary, Townsend, R. Reid, primary, Held, Jason M., primary, Carr, Steven A., primary, and Ma, Cynthia X., primary

Published

2023

42. Supplementary File 1 from Mass Spectrometry–Based Proteomics Reveals Potential Roles of NEK9 and MAP2K4 in Resistance to PI3K Inhibition in Triple-Negative Breast Cancers

Author

Mundt, Filip, primary, Rajput, Sandeep, primary, Li, Shunqiang, primary, Ruggles, Kelly V., primary, Mooradian, Arshag D., primary, Mertins, Philipp, primary, Gillette, Michael A., primary, Krug, Karsten, primary, Guo, Zhanfang, primary, Hoog, Jeremy, primary, Erdmann-Gilmore, Petra, primary, Primeau, Tina, primary, Huang, Shixia, primary, Edwards, Dean P., primary, Wang, Xiaowei, primary, Wang, Xuya, primary, Kawaler, Emily, primary, Mani, D.R., primary, Clauser, Karl R., primary, Gao, Feng, primary, Luo, Jingqin, primary, Davies, Sherri R., primary, Johnson, Gary L., primary, Huang, Kuan-lin, primary, Yoon, Christopher J., primary, Ding, Li, primary, Fenyö, David, primary, Ellis, Matthew J., primary, Townsend, R. Reid, primary, Held, Jason M., primary, Carr, Steven A., primary, and Ma, Cynthia X., primary

Published

2023

43. Supplementary File 2 from Mass Spectrometry–Based Proteomics Reveals Potential Roles of NEK9 and MAP2K4 in Resistance to PI3K Inhibition in Triple-Negative Breast Cancers

Author

Mundt, Filip, primary, Rajput, Sandeep, primary, Li, Shunqiang, primary, Ruggles, Kelly V., primary, Mooradian, Arshag D., primary, Mertins, Philipp, primary, Gillette, Michael A., primary, Krug, Karsten, primary, Guo, Zhanfang, primary, Hoog, Jeremy, primary, Erdmann-Gilmore, Petra, primary, Primeau, Tina, primary, Huang, Shixia, primary, Edwards, Dean P., primary, Wang, Xiaowei, primary, Wang, Xuya, primary, Kawaler, Emily, primary, Mani, D.R., primary, Clauser, Karl R., primary, Gao, Feng, primary, Luo, Jingqin, primary, Davies, Sherri R., primary, Johnson, Gary L., primary, Huang, Kuan-lin, primary, Yoon, Christopher J., primary, Ding, Li, primary, Fenyö, David, primary, Ellis, Matthew J., primary, Townsend, R. Reid, primary, Held, Jason M., primary, Carr, Steven A., primary, and Ma, Cynthia X., primary

Published

2023

44. Extended Methods from Mass Spectrometry–Based Proteomics Reveals Potential Roles of NEK9 and MAP2K4 in Resistance to PI3K Inhibition in Triple-Negative Breast Cancers

Author

Mundt, Filip, primary, Rajput, Sandeep, primary, Li, Shunqiang, primary, Ruggles, Kelly V., primary, Mooradian, Arshag D., primary, Mertins, Philipp, primary, Gillette, Michael A., primary, Krug, Karsten, primary, Guo, Zhanfang, primary, Hoog, Jeremy, primary, Erdmann-Gilmore, Petra, primary, Primeau, Tina, primary, Huang, Shixia, primary, Edwards, Dean P., primary, Wang, Xiaowei, primary, Wang, Xuya, primary, Kawaler, Emily, primary, Mani, D.R., primary, Clauser, Karl R., primary, Gao, Feng, primary, Luo, Jingqin, primary, Davies, Sherri R., primary, Johnson, Gary L., primary, Huang, Kuan-lin, primary, Yoon, Christopher J., primary, Ding, Li, primary, Fenyö, David, primary, Ellis, Matthew J., primary, Townsend, R. Reid, primary, Held, Jason M., primary, Carr, Steven A., primary, and Ma, Cynthia X., primary

Published

2023

45. Supplementary File 3 from Mass Spectrometry–Based Proteomics Reveals Potential Roles of NEK9 and MAP2K4 in Resistance to PI3K Inhibition in Triple-Negative Breast Cancers

Author

Mundt, Filip, primary, Rajput, Sandeep, primary, Li, Shunqiang, primary, Ruggles, Kelly V., primary, Mooradian, Arshag D., primary, Mertins, Philipp, primary, Gillette, Michael A., primary, Krug, Karsten, primary, Guo, Zhanfang, primary, Hoog, Jeremy, primary, Erdmann-Gilmore, Petra, primary, Primeau, Tina, primary, Huang, Shixia, primary, Edwards, Dean P., primary, Wang, Xiaowei, primary, Wang, Xuya, primary, Kawaler, Emily, primary, Mani, D.R., primary, Clauser, Karl R., primary, Gao, Feng, primary, Luo, Jingqin, primary, Davies, Sherri R., primary, Johnson, Gary L., primary, Huang, Kuan-lin, primary, Yoon, Christopher J., primary, Ding, Li, primary, Fenyö, David, primary, Ellis, Matthew J., primary, Townsend, R. Reid, primary, Held, Jason M., primary, Carr, Steven A., primary, and Ma, Cynthia X., primary

Published

2023

46. Supplementary Figures from Mass Spectrometry–Based Proteomics Reveals Potential Roles of NEK9 and MAP2K4 in Resistance to PI3K Inhibition in Triple-Negative Breast Cancers

Author

Mundt, Filip, primary, Rajput, Sandeep, primary, Li, Shunqiang, primary, Ruggles, Kelly V., primary, Mooradian, Arshag D., primary, Mertins, Philipp, primary, Gillette, Michael A., primary, Krug, Karsten, primary, Guo, Zhanfang, primary, Hoog, Jeremy, primary, Erdmann-Gilmore, Petra, primary, Primeau, Tina, primary, Huang, Shixia, primary, Edwards, Dean P., primary, Wang, Xiaowei, primary, Wang, Xuya, primary, Kawaler, Emily, primary, Mani, D.R., primary, Clauser, Karl R., primary, Gao, Feng, primary, Luo, Jingqin, primary, Davies, Sherri R., primary, Johnson, Gary L., primary, Huang, Kuan-lin, primary, Yoon, Christopher J., primary, Ding, Li, primary, Fenyö, David, primary, Ellis, Matthew J., primary, Townsend, R. Reid, primary, Held, Jason M., primary, Carr, Steven A., primary, and Ma, Cynthia X., primary

Published

2023

47. Figure S8 from Mammary Precancerous Stem and Non-Stem Cells Evolve into Cancers of Distinct Subtypes

Author

Bu, Wen, primary, Liu, Zhenyu, primary, Jiang, Weiyu, primary, Nagi, Chandandeep, primary, Huang, Shixia, primary, Edwards, Dean P., primary, Jo, Eunji, primary, Mo, Qianxing, primary, Creighton, Chad J., primary, Hilsenbeck, Susan G., primary, Leavitt, Andrew D., primary, Lewis, Michael T., primary, Wong, Stephen T. C., primary, and Li, Yi, primary

Published

2023

48. Supplementary Data from A Phase II Study of Cabozantinib and Androgen Ablation in Patients with Hormone-Naïve Metastatic Prostate Cancer

Author

Corn, Paul G., primary, Zhang, Miao, primary, Nogueras-Gonzalez, Graciela M., primary, Xiao, Lianchun, primary, Zurita, Amado J., primary, Subudhi, Sumit K., primary, Tu, Shi-Ming, primary, Aparicio, Ana M., primary, Coarfa, Cristian, primary, Rajapakshe, Kimal, primary, Huang, Shixia, primary, Navone, Nora M., primary, Lin, Sue-Hwa, primary, Wang, Guocan, primary, Ramachandran, Sumankalai, primary, Titus, Mark A., primary, Panaretakis, Theocharis, primary, Gallick, Gary E., primary, Efstathiou, Eleni, primary, Troncoso, Patricia, primary, and Logothetis, Christopher, primary

Published

2023

49. Supplementary tables 1 and 2 from Mass Spectrometry–Based Proteomics Reveals Potential Roles of NEK9 and MAP2K4 in Resistance to PI3K Inhibition in Triple-Negative Breast Cancers

Author

Mundt, Filip, primary, Rajput, Sandeep, primary, Li, Shunqiang, primary, Ruggles, Kelly V., primary, Mooradian, Arshag D., primary, Mertins, Philipp, primary, Gillette, Michael A., primary, Krug, Karsten, primary, Guo, Zhanfang, primary, Hoog, Jeremy, primary, Erdmann-Gilmore, Petra, primary, Primeau, Tina, primary, Huang, Shixia, primary, Edwards, Dean P., primary, Wang, Xiaowei, primary, Wang, Xuya, primary, Kawaler, Emily, primary, Mani, D.R., primary, Clauser, Karl R., primary, Gao, Feng, primary, Luo, Jingqin, primary, Davies, Sherri R., primary, Johnson, Gary L., primary, Huang, Kuan-lin, primary, Yoon, Christopher J., primary, Ding, Li, primary, Fenyö, David, primary, Ellis, Matthew J., primary, Townsend, R. Reid, primary, Held, Jason M., primary, Carr, Steven A., primary, and Ma, Cynthia X., primary

Published

2023

50. Data from A Wnt-Independent LGR4–EGFR Signaling Axis in Cancer Metastasis

Author

Yue, Fei, primary, Jiang, Weiyu, primary, Ku, Amy T., primary, Young, Adelaide I.J., primary, Zhang, Weijie, primary, Souto, Eric P., primary, Gao, Yankun, primary, Yu, Zihan, primary, Wang, Yi, primary, Creighton, Chad J., primary, Nagi, Chandandeep, primary, Wang, Tao, primary, Hilsenbeck, Susan G., primary, Feng, Xin-Hua, primary, Huang, Shixia, primary, Coarfa, Cristian, primary, Zhang, Xiang H.-F., primary, Liu, Qingyun, primary, Lin, Xia, primary, and Li, Yi, primary

Published

2023