Proteogenomic and metabolomic characterization of human glioblastoma

Wang, Liang-Bo; Karpova, Alla; Gritsenko, Marina; Kyle, Jennifer; Cao, Song; Li, Yize; Rykunov, Dmitry; Colaprico, Antonio; Rothstein, Joseph H.; Hong, Runyu; Stathias, Vasileios; Cornwell, MacIntosh; Petralia, Francesca; Wu, Yige; Reva, Boris; Krug, Karsten; Pugliese, Pietro; Kawaler, Emily; Olsen, Lindsey K.; Liang, Wen-Wei; Song, Xiaoyu; Dou, Yongchao; Wendl, Michael C.; Caravan, Wagma; Liu, Wenke; Zhou, Daniel Cui; Ji, Jiayi; Tsai, Chia‐Feng; Petyuk, Vladislav; Moon, Jamie; Ma, Wanli; Chu, Rosalie K.; Weitz, Karl K.; Moore, Ronald J.; Monroe, Matthew E.; Zhao, Rui; Yang, Xiaolu; Yoo, Seungyeul; Krek, Azra; Demopoulos, Alexis; Zhu, Houxiang; Wyczalkowski, Matthew A.; McMichael, Joshua F.; Henderson, Brittany; Lindgren, Caleb M.; Boekweg, Hannah; Lu, Shuangjia; Baral, Jessika; Yao, Lijun; Stratton, Kelly G.; Bramer, Lisa; Zink, Erika; Couvillion, Sneha; Bloodsworth, Kent; Satpathy, Shankha; Sieh, Weiva; Boca, Simina M.; Schürer, Stephan C.; Chen, Feng; Wiznerowicz, Maciej; Ketchum, Karen A.; Boja, Emily S.; Kinsinger, Christopher R.; Robles, Ana I.; Hiltke, Tara; Thiagarajan, Mathangi; Nesvizhskii, Alexey I.; Zhang, Bing; Mani, D. R.; Ceccarelli, Michele; Chen, Xi S.; Cottingham, Sandra; Li, Qing Kay; Kim, Albert H.; Fenyö, David; Ruggles, Kelly V.; Rodriguez, Henry; Mesri, Mehdi; Payne, Samuel H.; Wang, Pei; Smith, Richard; Iavarone, Antonio; Chheda, Milan G.; Barnholtz‐Sloan, Jill S.; Rodland, Karin D.; Liu, Tao; Li, Ding; Agarwal, Anupriya; Amin, Mitual; An, Eunkyung; Anderson, Matthew L.; Andrews, David W.; Bauer, Thomas; Birger, Chet; Birrer, Michael J.; Blumenberg, Lili M.; Bocik, William; Borate, Uma; Borucki, Melissa; Burke, Meghan C.; Cai, Shuang; Calinawan, Anna; Carr, Steven A.; Cerda, Sandra; Chan, Daniel W.; Charamut, Alyssa; Chen, Lin S.; Chesla, David; Chinnaiyan, Arul M.; Chowdhury, Shrabanti; Cieślik, Marcin; Clark, David; Culpepper, Houston; Czernicki, Tomasz; D’Angelo, Fulvio; Day, Jacob; Young, Stephanie; Demir, Emek; Dhanasekaran, Saravana M.; Dhir, Rajiv; Domagalski, Marcin J.; Druker, Brian J.; Duffy, Elizabeth; Dyer, Maureen A.; Edwards, Nathan; Edwards, Robert A.; Elburn, Kimberly; Ellis, Matthew J.; Eschbacher, Jennifer; Francis, Alicia; Gabriel, Stacey; Gabrovski, N; Garofano, Luciano; Getz, Gad; Gillette, Michael A.; Godwin, Andrew K.; Gol'bin, D A; Hanhan, Ziad; Hannick, Linda; Hariharan, Pushpa; Hindenach, Barbara; Hoadley, Katherine A.; Hostetter, Galen; Huang, Chen; Jaehnig, Eric J.; Jewell, Scott D.; Nan, Jun; Jones, Corbin D.; Karz, Alcida; Kaspera, Wojciech; Kim, Lyndon; Kothadia, Ramani B.; Kumar-Sinha, Chandan; Lei, Jonathan T.; Leprevost, Felipe da Veiga; Li, Kai; Liao, Yuxing; Lilly, Jena; Liu, Hongwei; Lubiński, Jan; Madan, Rashna; Maggio, William W.; Malc, Ewa; Malovannaya, Anna; Mareedu, Sailaja; Markey, Sanford P.; Marrero-Oliveras, Annette; Martinez, Nina; Maunganidze, Nicollette; McDermott, Jason; McGarvey, Peter B.; McGee, John P.; Mieczkowski, Piotr A.; Migliozzi, Simona; Modugno, Francesmary; Montgomery, Rebecca; Newton, Chelsea J.; Omenn, Gilbert S.; Özbek, Umut; Paklina, Oxana; Paulovich, Amanda G.; Perou, Amy M.; Pico, Alexander; Piehowski, Paul; Placantonakis, Dimitris G.; Polonskaya, Larisa; Potapova, Olga; Pruetz, Barbara L.; Qi, Liqun; Ramkissoon, Shakti; Resnick, Adam; Richey, Shannon; Riggins, Gregory J.; Robinson, Karna; Roche, Nancy; Rohrer, Daniel C.; Rood, Brian R.; Rossell, Larissa L.; Savage, Sara R.; Schadt, Eric E.; Shi, Yan; Shi, Zhiao; Shutack, Yvonne; Singh, Shilpi; Skelly, Tara; Sokoll, Lori J.; Stawicki, Jakub; Stein, Stephen E.; Suh, James; Szopa, Wojciech; Tabor, Dave; Tan, Donghui; Tansil, Darlene; Thangudu, Ratna R.; Tognon, Cristina E.; Traer, Elie; Tsang, Shirley; Tyner, Jeffrey W.; Um, Ki Sung; Valley, Dana R.; Vasaikar, Suhas; Vatanian, Negin; Velvulou, Uma; Vernon, Michael; Wan, Weiqing; Wang, Junmei; Webster, Alex; Wen, Bo; Whiteaker, Jeffrey R.; Wilson, George; Zakhartsev, Yuriy; Zelt, Robert; Zhang, Hui; Zhang, Liwei; Zhang, Zhen; Zhao, Grace; Zhu, Jun

doi:10.1016/j.ccell.2021.01.006

Cited by 347 publications

(269 citation statements)

References 145 publications

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“…Another approach distinguished among three subtypes of GBM based on phenotypes and prognosis referred to as mitotic (or favorable), intermediate, and invasive (or poor prognosis) [23]. These categories were verified by distinct genetic fingerprints showing similar but not identical trends as the TCGA-based classification [22,25]. However, the GBM subtype-specific markers are variable and simultaneously expressed across individual cells even within a single tumor [26,27].…”

Section: Subtypes and Genetics And Of Glioblastomamentioning

confidence: 99%

“…Short-term relapse after radiation therapy is characterized by both increased expression of MES–GBM subtype genes and a gene signature based on TME inference, associated with decreased monocyte invasion, increased macrophages/microglial cells, and CD8 + T cell enrichment. A recent pathogenetic characterization of GBM revealed that four immune GBM subtypes could be identified in IDH -wild-type GBM and IDH -mutant astrocytoma [ 25 ]. Taken together, higher intertumor and intratumor heterogeneity are associated with lower overall patient survival, in spite of modern modalities of standard-of-care GBM therapy [ 32 ], and novel targeted approaches are undoubtedly needed.…”

Section: Glioblastomamentioning

confidence: 99%

“…Since several studies confirmed that GBM therapy results in recurrences with more invasive mesenchymal subtypes, it has been hypothesized that this process involves a proneural (PN) to mesenchymal (MES) GSC subtype reprogramming, or “PMT transition” [ 22 , 24 , 25 ].…”

Section: Glioblastoma Microenvironment (Gme)mentioning

confidence: 99%

See 2 more Smart Citations

An Update on Glioblastoma Biology, Genetics, and Current Therapies: Novel Inhibitors of the G Protein-Coupled Receptor CCR5

Turnšek

Jiao

Novak

et al. 2021

IJMS

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The mechanisms governing therapeutic resistance of the most aggressive and lethal primary brain tumor in adults, glioblastoma, have increasingly focused on tumor stem cells. These cells, protected by the periarteriolar hypoxic GSC niche, contribute to the poor efficacy of standard of care treatment of glioblastoma. Integrated proteogenomic and metabolomic analyses of glioblastoma tissues and single cells have revealed insights into the complex heterogeneity of glioblastoma and stromal cells, comprising its tumor microenvironment (TME). An additional factor, which isdriving poor therapy response is the distinct genetic drivers in each patient’s tumor, providing the rationale for a more individualized or personalized approach to treatment. We recently reported that the G protein-coupled receptor CCR5, which contributes to stem cell expansion in other cancers, is overexpressed in glioblastoma cells. Overexpression of the CCR5 ligand CCL5 (RANTES) in glioblastoma completes a potential autocrine activation loop to promote tumor proliferation and invasion. CCL5 was not expressed in glioblastoma stem cells, suggesting a need for paracrine activation of CCR5 signaling by the stromal cells. TME-associated immune cells, such as resident microglia, infiltrating macrophages, T cells, and mesenchymal stem cells, possibly release CCR5 ligands, providing heterologous signaling between stromal and glioblastoma stem cells. Herein, we review current therapies for glioblastoma, the role of CCR5 in other cancers, and the potential role for CCR5 inhibitors in the treatment of glioblastoma.

show abstract

Section: Subtypes and Genetics And Of Glioblastomamentioning

confidence: 99%

Section: Glioblastomamentioning

confidence: 99%

See 1 more Smart Citation

An Update on Glioblastoma Biology, Genetics, and Current Therapies: Novel Inhibitors of the G Protein-Coupled Receptor CCR5

Turnšek

Jiao

Novak

et al. 2021

IJMS

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show abstract

“…To date, metabolic reprogramming of GBM cells has only been considered a consequence of hard nutrient-restricted conditions within the tumor microenvironment. Recently, new molecular subtypes of GBM were delineated by integrating not only proteomic and genomic but also metabolomic analyses [ 2 ]. Indeed, in an elegant and meticulous new study, the use of single-cell mRNA sequencing enabled us to revise the GBM subclassification into four subtypes based on biological and metabolic characteristics, not just on genetic alterations, allowing the prediction of patient outcome.…”

Section: Introductionmentioning

confidence: 99%

Altered Metabolism in Glioblastoma: Myeloid-Derived Suppressor Cell (MDSC) Fitness and Tumor-Infiltrating Lymphocyte (TIL) Dysfunction

Ianni

Musio

Pellegatta

2021

IJMS

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The metabolism of glioblastoma (GBM), the most aggressive and lethal primary brain tumor, is flexible and adaptable to different adverse conditions, such as nutrient deprivation. Beyond glycolysis, altered lipid metabolism is implicated in GBM progression. Indeed, metabolic subtypes were recently identified based on divergent glucose and lipid metabolism. GBM is also characterized by an immunosuppressive microenvironment in which myeloid-derived suppressor cells (MDSCs) are a powerful ally of tumor cells. Increasing evidence supports the interconnection between GBM and MDSC metabolic pathways. GBM cells exert a crucial contribution to MDSC recruitment and maturation within the tumor microenvironment, where the needs of tumor-infiltrating lymphocytes (TILs) with antitumor function are completely neglected. In this review, we will discuss the unique or alternative source of energy exploited by GBM and MDSCs, exploring how deprivation of specific nutrients and accumulation of toxic byproducts can induce T-cell dysfunction. Understanding the metabolic programs of these cell components and how they impact fitness or dysfunction will be useful to improve treatment modalities, including immunotherapeutic strategies.

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“…An InceptionV3-based model achieves a high level of accuracy in determining melanoma possibility, exhibiting significant diagnostic potential (Louis et al, 2016). Moreover, successful deep learning models have also been built to predict molecular and genomic features in cancer, such as microsatellite instability (MSI), immune subtypes, and somatic mutation status, suggesting that machine learning techniques may be able to assist human experts to further exploit clinically relevant information in pathological images (Coudray et al, 2018; Gillette et al, 2020; Hong et al, 2020; Kather et al, 2019; Kim et al, 2019; Wang et al, 2021). In addition, studies have also demonstrated that deep neural network models have the potentials in capturing features across cancer and tissue types (Fu et al, 2020; Kather et al, 2020).…”

Section: Introductionmentioning

confidence: 99%

Predicting Endometrial Cancer Subtypes and Molecular Features from Histopathology Images Using Multi-resolution Deep Learning Models

Hong

Liu

DeLair

et al. 2020

Preprint

Self Cite

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Determining endometrial carcinoma histological subtype is a critical diagnostic process that directly affects prognosis and treatment options. Recently, molecular subtyping and mutation status are gaining popularity as they offer more relevant information to evaluate the severity and develop individualized therapies. However, compared to the histopathological approach, the availability of molecular subtyping is limited as it can only be obtained by genomic sequencing, which is more expensive. Here, we implemented deep convolutional neural network models that predict not only the histological subtypes, but also molecular subtypes and 18 common gene mutations based on digitized H&E stained pathological images. Taking advantage of the multiresolution nature of the whole slide images, we introduced a customized architecture, Panoptes, to integrate features of different magnification. The model was trained and evaluated with images from The Cancer Genome Atlas and Clinical Proteomic Tumor Analysis Consortium. Our models achieved an area under the receiver operating characteristic curve (AUROC) of 0.969 in predicting histological subtype and 0.934 to 0.958 in predicting CNV-H molecular subtype. The prediction tasks of 4 mutations and MSI-High molecular subtype also achieved high performance with AUROC ranging from 0.781 to 0.873. Panoptes showed significantly better performance than InceptionResnet in most of these top predicted tasks by up to 18%. Feature extraction and visualization revealed that the model relied on human-interpretable patterns. Our results suggest that Panoptes can help pathologists determine molecular subtypes and mutations without sequencing, and is generally applicable to any cancer type.

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Proteogenomic and metabolomic characterization of human glioblastoma

Cited by 347 publications

References 145 publications

An Update on Glioblastoma Biology, Genetics, and Current Therapies: Novel Inhibitors of the G Protein-Coupled Receptor CCR5

An Update on Glioblastoma Biology, Genetics, and Current Therapies: Novel Inhibitors of the G Protein-Coupled Receptor CCR5

Altered Metabolism in Glioblastoma: Myeloid-Derived Suppressor Cell (MDSC) Fitness and Tumor-Infiltrating Lymphocyte (TIL) Dysfunction

Predicting Endometrial Cancer Subtypes and Molecular Features from Histopathology Images Using Multi-resolution Deep Learning Models

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