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126 results on '"Cheng, Jijun"'

1. CoNIC Challenge: Pushing the Frontiers of Nuclear Detection, Segmentation, Classification and Counting

Author

Graham, Simon, Vu, Quoc Dang, Jahanifar, Mostafa, Weigert, Martin, Schmidt, Uwe, Zhang, Wenhua, Zhang, Jun, Yang, Sen, Xiang, Jinxi, Wang, Xiyue, Rumberger, Josef Lorenz, Baumann, Elias, Hirsch, Peter, Liu, Lihao, Hong, Chenyang, Aviles-Rivero, Angelica I., Jain, Ayushi, Ahn, Heeyoung, Hong, Yiyu, Azzuni, Hussam, Xu, Min, Yaqub, Mohammad, Blache, Marie-Claire, Piégu, Benoît, Vernay, Bertrand, Scherr, Tim, Böhland, Moritz, Löffler, Katharina, Li, Jiachen, Ying, Weiqin, Wang, Chixin, Kainmueller, Dagmar, Schönlieb, Carola-Bibiane, Liu, Shuolin, Talsania, Dhairya, Meda, Yughender, Mishra, Prakash, Ridzuan, Muhammad, Neumann, Oliver, Schilling, Marcel P., Reischl, Markus, Mikut, Ralf, Huang, Banban, Chien, Hsiang-Chin, Wang, Ching-Ping, Lee, Chia-Yen, Lin, Hong-Kun, Liu, Zaiyi, Pan, Xipeng, Han, Chu, Cheng, Jijun, Dawood, Muhammad, Deshpande, Srijay, Bashir, Raja Muhammad Saad, Shephard, Adam, Costa, Pedro, Nunes, João D., Campilho, Aurélio, Cardoso, Jaime S., S, Hrishikesh P, Puthussery, Densen, G, Devika R, C V, Jiji, Zhang, Ye, Fang, Zijie, Lin, Zhifan, Zhang, Yongbing, Lin, Chunhui, Zhang, Liukun, Mao, Lijian, Wu, Min, Vo, Vi Thi-Tuong, Kim, Soo-Hyung, Lee, Taebum, Kondo, Satoshi, Kasai, Satoshi, Dumbhare, Pranay, Phuse, Vedant, Dubey, Yash, Jamthikar, Ankush, Vuong, Trinh Thi Le, Kwak, Jin Tae, Ziaei, Dorsa, Jung, Hyun, Miao, Tianyi, Snead, David, Raza, Shan E Ahmed, Minhas, Fayyaz, and Rajpoot, Nasir M.

Subjects
Computer Science - Computer Vision and Pattern Recognition, Computer Science - Machine Learning
Abstract

Nuclear detection, segmentation and morphometric profiling are essential in helping us further understand the relationship between histology and patient outcome. To drive innovation in this area, we setup a community-wide challenge using the largest available dataset of its kind to assess nuclear segmentation and cellular composition. Our challenge, named CoNIC, stimulated the development of reproducible algorithms for cellular recognition with real-time result inspection on public leaderboards. We conducted an extensive post-challenge analysis based on the top-performing models using 1,658 whole-slide images of colon tissue. With around 700 million detected nuclei per model, associated features were used for dysplasia grading and survival analysis, where we demonstrated that the challenge's improvement over the previous state-of-the-art led to significant boosts in downstream performance. Our findings also suggest that eosinophils and neutrophils play an important role in the tumour microevironment. We release challenge models and WSI-level results to foster the development of further methods for biomarker discovery.

Published
2023

2. RECO: Rotation Equivariant COnvolutional Neural Network for Human Trajectory Forecasting

Author

Cheng, Jijun, Wang, Hao, Shao, Dongheng, Yang, Jian, Chen, Mingsong, Wei, Xian, Tang, Xuan, Goos, Gerhard, Founding Editor, Hartmanis, Juris, Founding Editor, Bertino, Elisa, Editorial Board Member, Gao, Wen, Editorial Board Member, Steffen, Bernhard, Editorial Board Member, Yung, Moti, Editorial Board Member, Liu, Qingshan, editor, Wang, Hanzi, editor, Ma, Zhanyu, editor, Zheng, Weishi, editor, Zha, Hongbin, editor, Chen, Xilin, editor, Wang, Liang, editor, and Ji, Rongrong, editor

Published
2024
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4. A Standardized Pipeline for Colon Nuclei Identification and Counting Challenge

Author

Cheng, Jijun, Pan, Xipeng, Hou, Feihu, Zhao, Bingchao, Lin, Jiatai, Liu, Zhenbing, Liu, Zaiyi, and Han, Chu

Subjects
Electrical Engineering and Systems Science - Image and Video Processing, Computer Science - Computer Vision and Pattern Recognition, Quantitative Biology - Quantitative Methods
Abstract

Nuclear segmentation and classification is an essential step for computational pathology. TIA lab from Warwick University organized a nuclear segmentation and classification challenge (CoNIC) for H&E stained histopathology images in colorectal cancer with two highly correlated tasks, nuclei segmentation and classification task and cellular composition task. There are a few obstacles we have to address in this challenge, 1) limited training samples, 2) color variation, 3) imbalanced annotations, 4) similar morphological appearance among classes. To deal with these challenges, we proposed a standardized pipeline for nuclear segmentation and classification by integrating several pluggable components. First, we built a GAN-based model to automatically generate pseudo images for data augmentation. Then we trained a self-supervised stain normalization model to solve the color variation problem. Next we constructed a baseline model HoVer-Net with cost-sensitive loss to encourage the model pay more attention on the minority classes. According to the results of the leaderboard, our proposed pipeline achieves 0.40665 mPQ+ (Rank 49th) and 0.62199 r2 (Rank 10th) in the preliminary test phase.

Published
2022

19. Single-cell microRNA/mRNA co-sequencing reveals non-genetic heterogeneity and novel regulatory mechanisms

Author

Wang, Nayi, primary, Zheng, Ji, additional, Chen, Zhuo, additional, Liu, Yang, additional, Dura, Burak, additional, Kwak, Minsuk, additional, Xavier-Ferrucio, Juliana, additional, Lu, Yi-Chien, additional, Zhang, Miaomiao, additional, Roden, Christine, additional, Cheng, Jijun, additional, Krause, Diane, additional, Ding, Ye, additional, Fan, Rong, additional, and Lu, Jun, additional

Published
2018
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24. The DNA Methylcytosine Dioxygenase Tet2 Sustains Immunosuppressive Function of Tumor-Infiltrating Myeloid Cells to Promote Melanoma Progression

Author

Pan, Wen, primary, Zhu, Shu, additional, Qu, Kun, additional, Meeth, Katrina, additional, Cheng, Jijun, additional, He, Kaixin, additional, Ma, Hongdi, additional, Liao, Yan, additional, Wen, Xizhi, additional, Roden, Christine, additional, Tobiasova, Zuzana, additional, Wei, Zheng, additional, Zhao, Jun, additional, Liu, Jun, additional, Zheng, Ji, additional, Guo, Bo, additional, Khan, Sajid A., additional, Bosenberg, Marcus, additional, Flavell, Richard A., additional, and Lu, Jun, additional

Published
2017
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25. Novel determinants of mammalian primary microRNA processing revealed by systematic evaluation of hairpin-containing transcripts and human genetic variation

Author

Roden, Christine, primary, Gaillard, Jonathan, additional, Kanoria, Shaveta, additional, Rennie, William, additional, Barish, Syndi, additional, Cheng, Jijun, additional, Pan, Wen, additional, Liu, Jun, additional, Cotsapas, Chris, additional, Ding, Ye, additional, and Lu, Jun, additional

Published
2017
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30. Regulation of the DNA Methylation Landscape in Human Somatic Cell Reprogramming by the miR-29 Family

Author

Hysolli, Eriona, primary, Tanaka, Yoshiaki, additional, Su, Juan, additional, Kim, Kun-Yong, additional, Zhong, Tianyu, additional, Janknecht, Ralf, additional, Zhou, Xiao-Ling, additional, Geng, Lin, additional, Qiu, Caihong, additional, Pan, Xinghua, additional, Jung, Yong-Wook, additional, Cheng, Jijun, additional, Lu, Jun, additional, Zhong, Mei, additional, Weissman, Sherman M., additional, and Park, In-Hyun, additional

Published
2016
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32. A Molecular Chipper technology for CRISPR sgRNA library generation and functional mapping of noncoding regions

Author

Cheng, Jijun, primary, Roden, Christine A., additional, Pan, Wen, additional, Zhu, Shu, additional, Baccei, Anna, additional, Pan, Xinghua, additional, Jiang, Tingting, additional, Kluger, Yuval, additional, Weissman, Sherman M., additional, Guo, Shangqin, additional, Flavell, Richard A., additional, Ding, Ye, additional, and Lu, Jun, additional

Published
2016
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35. Nonstochastic Reprogramming from a Privileged Somatic Cell State

Author

Guo, Shangqin, primary, Zi, Xiaoyuan, additional, Schulz, Vincent P., additional, Cheng, Jijun, additional, Zhong, Mei, additional, Koochaki, Sebastian H.J., additional, Megyola, Cynthia M., additional, Pan, Xinghua, additional, Heydari, Kartoosh, additional, Weissman, Sherman M., additional, Gallagher, Patrick G., additional, Krause, Diane S., additional, Fan, Rong, additional, and Lu, Jun, additional

Published
2014
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36. An Extensive Network of TET2-Targeting MicroRNAs Regulates Malignant Hematopoiesis

Author

Cheng, Jijun, primary, Guo, Shangqin, additional, Chen, Suning, additional, Mastriano, Stephen J., additional, Liu, Chaochun, additional, D’Alessio, Ana C., additional, Hysolli, Eriona, additional, Guo, Yanwen, additional, Yao, Hong, additional, Megyola, Cynthia M., additional, Li, Dan, additional, Liu, Jun, additional, Pan, Wen, additional, Roden, Christine A., additional, Zhou, Xiao-Ling, additional, Heydari, Kartoosh, additional, Chen, Jianjun, additional, Park, In-Hyun, additional, Ding, Ye, additional, Zhang, Yi, additional, and Lu, Jun, additional

Published
2013
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39. miR-125bpromotes MLL-AF9–driven murine acute myeloid leukemia involving a VEGFA-mediated non–cell-intrinsic mechanism

Author

Liu, Jun, Guo, Bo, Chen, Zhuo, Wang, Nayi, Iacovino, Michelina, Cheng, Jijun, Roden, Christine, Pan, Wen, Khan, Sajid, Chen, Suning, Kyba, Michael, Fan, Rong, Guo, Shangqin, and Lu, Jun

Abstract

The hematopoietic stem cell–enriched miR-125family microRNAs (miRNAs) are critical regulators of hematopoiesis. Overexpression of miR-125aor miR-125bis frequent in human acute myeloid leukemia (AML), and the overexpression of these miRNAs in mice leads to expansion of hematopoietic stem cells accompanied by perturbed hematopoiesis with mostly myeloproliferative phenotypes. However, whether and how miR-125family miRNAs cooperate with known AML oncogenes in vivo, and how the resultant leukemia is dependent on miR-125overexpression, are not well understood. We modeled the frequent co-occurrence of miR-125boverexpression and MLLtranslocations by examining functional cooperation between miR-125band MLL-AF9. By generating a knock-in mouse model in which miR-125boverexpression is controlled by doxycycline induction, we demonstrated that miR-125bsignificantly enhances MLL-AF9–driven AML in vivo, and the resultant leukemia is partially dependent on continued overexpression of miR-125b. Surprisingly, miR-125bpromotes AML cell expansion and suppresses apoptosis involving a non–cell-intrinsic mechanism. MiR-125bexpression enhances VEGFAexpression and production from leukemia cells, in part by suppressing TET2. Recombinant VEGFA recapitulates the leukemia-promoting effects of miR-125b, whereas knockdown of VEGFAor inhibition of VEGF receptor 2 abolishes the effects of miR-125b. In addition, significant correlation between miR-125band VEGFAexpression is observed in human AMLs. Our data reveal cooperative and dependent relationships between miR-125band the MLLoncogene in AML leukemogenesis, and demonstrate a miR-125b-TET2-VEGFApathway in mediating non–cell-intrinsic leukemia-promoting effects by an oncogenic miRNA.

Published
2017
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43. Isothiazoloquinolones with Enhanced Antistaphylococcal Activities against Multidrug-Resistant Strains: Effects of Structural Modifications at the 6-, 7-, and 8-Positions

Author

Wang, Qiuping, primary, Lucien, Edlaine, additional, Hashimoto, Akihiro, additional, Pais, Godwin C. G., additional, Nelson, David M., additional, Song, Yongsheng, additional, Thanassi, Jane A., additional, Marlor, Christopher W., additional, Thoma, Christy L., additional, Cheng, Jijun, additional, Podos, Steven D., additional, Ou, Yangsi, additional, Deshpande, Milind, additional, Pucci, Michael J., additional, Buechter, Douglas D., additional, Bradbury, Barton J., additional, and Wiles, Jason A., additional

Published
2006
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44. Isothiazoloquinolones containing functionalized aromatic hydrocarbons at the 7-position: Synthesis and in vitro activity of a series of potent antibacterial agents with diminished cytotoxicity in human cells

Author

Wiles, Jason A., primary, Wang, Qiuping, additional, Lucien, Edlaine, additional, Hashimoto, Akihiro, additional, Song, Yongsheng, additional, Cheng, Jijun, additional, Marlor, Christopher W., additional, Ou, Yangsi, additional, Podos, Steven D., additional, Thanassi, Jane A., additional, Thoma, Christy L., additional, Deshpande, Milind, additional, Pucci, Michael J., additional, and Bradbury, Barton J., additional

Published
2006
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45. Biological evaluation of isothiazoloquinolones containing aromatic heterocycles at the 7-position: In vitro activity of a series of potent antibacterial agents that are effective against methicillin-resistant Staphylococcus aureus

Author

Wiles, Jason A., primary, Song, Yongsheng, additional, Wang, Qiuping, additional, Lucien, Edlaine, additional, Hashimoto, Akihiro, additional, Cheng, Jijun, additional, Marlor, Christopher W., additional, Ou, Yangsi, additional, Podos, Steven D., additional, Thanassi, Jane A., additional, Thoma, Christy L., additional, Deshpande, Milind, additional, Pucci, Michael J., additional, and Bradbury, Barton J., additional

Published
2006
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49. Isothiazolopyridones:  Synthesis, Structure, and Biological Activity of a New Class of Antibacterial Agents

Author

A. Wiles, Jason, Hashimoto, Akihiro, A. Thanassi, Jane, Cheng, Jijun, D. Incarvito, Christopher, Deshpande, Milind, J. Pucci, Michael, and J. Bradbury, Barton

Abstract

We report the syntheses of first-generation derivatives of isothiazolopyridones and their in vitro evaluation as antibacterial agents. These compounds, containing a novel heterocyclic nucleus composed of an isothiazolone fused to a quinolizin-4-one (at C-2 and C-3 of the quinolizin-4-one), were prepared using a sequence of seven synthetic transformations. The solid-state structure of 7-chloro-9-ethyl-1-thia-2,4a-diazacyclopenta[b]naphthalene-3,4-dione was determined by X-ray diffraction. The prepared derivatives of desfluoroisothiazolopyridones exhibited (a) antibacterial activity against Gram-negative and Gram-positive organisms, (b) inhibitory activities against DNA gyrase and topoisomerase IV, and (c) no inhibitory activity against human topoisomerase II.

Published
2006
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50. BIMAAPC3, a component of the Aspergillus anaphase promoting complex/cyclosome, is required for a G2 checkpoint blocking entry into mitosis in the absence of NIMA function

Author

Lies, C. Mark, Cheng, Jijun, James, Steven W., Morris, N. Ronald, O’Connell, Matthew J., and Mirabito, P. M.

Abstract

Temperature sensitive (ts) nimA mutants of Aspergillus nidulans arrest at a unique point in G2 which is post activation of CDC2. Here we show that this G2 arrest is due to loss of nimA function and that it is dependent on BIMAAPC3, a component of the anaphase promoting complex/cyclosome (APC/C). Whereas nimA single mutants arrested in G2 with decondensed chromatin and interphase microtubule arrays, nimA, bimAAPC3 double mutants arrested growth with condensed chromatin and aster-like microtubule arrays. nimA, bimAAPC3 double mutants entered mitosis with kinetics similar to bimAAPC3 single mutants and wild-type cells, indicating a checkpoint-like role for BIMAAPC3 in G2. Even cells which had been depleted for NIMA protein and which contained insignificant levels of NIMA kinase activity entered mitosis on inactivation of bimAAPC3. BIMAAPC3 was present in a >25S complex containing BIMEAPC1, and bimAAPC3 mutants were sensitive to elevated CYCLIN B expression, consistent with BIMAAPC3 being a component of the APC/C. Inactivation of bimAAPC3 had little affect on the steady state levels of the B-type cyclin, NIMECydin B. Our results indicate that B?MAAPC?, and most likely the APC/C itself, is activated in G2 in nimA mutants. We propose that APC/C activation is part of a novel, late G2 checkpoint, which responds to a defective process or structure in nimA mutants, and which prevents inappropriate entry into mitosis.

Published
1998
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