Your search keyword '"Matthew R. Chrostek"' showing total 11 results

1. A phenocopy signature of TP53 loss predicts response to chemotherapy

Author

Hamza Bakhtiar, Marina N. Sharifi, Kyle T. Helzer, Yue Shi, Matthew L. Bootsma, Tianfu A. Shang, Matthew R. Chrostek, Tracy J. Berg, S. Carson Callahan, Viridiana Carreno, Grace C. Blitzer, Malinda T. West, Ruth M. O’Regan, Kari B. Wisinski, Martin Sjöström, and Shuang G. Zhao

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract In preclinical studies, p53 loss of function impacts chemotherapy response, but this has not been consistently validated clinically. We trained a TP53-loss phenocopy gene expression signature from pan-cancer clinical samples in the TCGA. In vitro, the TP53-loss phenocopy signature predicted chemotherapy response across cancer types. In a clinical dataset of 3003 breast cancer samples treated with neoadjuvant chemotherapy, the TP53-loss phenocopy samples were 56% more likely to have a pathologic complete response (pCR), with a significant association between TP53-loss phenocopy and pCR in both ER positive and ER negative tumors. In an independent clinical validation in the I-SPY2 trial (N = 987), we confirmed the association with neoadjuvant chemotherapy pCR and found higher rates of chemoimmunotherapy response in TP53-loss phenocopy tumors compared to non-TP53-loss phenocopy tumors (64% vs. 28%). The TP53-loss phenocopy signature predicts chemotherapy response across cancer types in vitro, and in a proof-of-concept clinical validation is associated with neoadjuvant chemotherapy response across multiple clinical breast cancer cohorts.

Published

2024

2. A platform-independent AI tumor lineage and site (ATLAS) classifier

Author

Nicholas R. Rydzewski, Yue Shi, Chenxuan Li, Matthew R. Chrostek, Hamza Bakhtiar, Kyle T. Helzer, Matthew L. Bootsma, Tracy J. Berg, Paul M. Harari, John M. Floberg, Grace C. Blitzer, David Kosoff, Amy K. Taylor, Marina N. Sharifi, Menggang Yu, Joshua M. Lang, Krishnan R. Patel, Deborah E. Citrin, Kaitlin E. Sundling, and Shuang G. Zhao

Subjects

Biology (General), QH301-705.5

Abstract

Abstract Histopathologic diagnosis and classification of cancer plays a critical role in guiding treatment. Advances in next-generation sequencing have ushered in new complementary molecular frameworks. However, existing approaches do not independently assess both site-of-origin (e.g. prostate) and lineage (e.g. adenocarcinoma) and have minimal validation in metastatic disease, where classification is more difficult. Utilizing gradient-boosted machine learning, we developed ATLAS, a pair of separate AI Tumor Lineage and Site-of-origin models from RNA expression data on 8249 tumor samples. We assessed performance independently in 10,376 total tumor samples, including 1490 metastatic samples, achieving an accuracy of 91.4% for cancer site-of-origin and 97.1% for cancer lineage. High confidence predictions (encompassing the majority of cases) were accurate 98–99% of the time in both localized and remarkably even in metastatic samples. We also identified emergent properties of our lineage scores for tumor types on which the model was never trained (zero-shot learning). Adenocarcinoma/sarcoma lineage scores differentiated epithelioid from biphasic/sarcomatoid mesothelioma. Also, predicted lineage de-differentiation identified neuroendocrine/small cell tumors and was associated with poor outcomes across tumor types. Our platform-independent single-sample approach can be easily translated to existing RNA-seq platforms. ATLAS can complement and guide traditional histopathologic assessment in challenging situations and tumors of unknown primary.

Published

2024

3. Zika virus-based immunotherapy enhances long-term survival of rodents with brain tumors through upregulation of memory T-cells

Author

Andrew T. Crane, Matthew R. Chrostek, Venkatramana D. Krishna, Maple Shiao, Nikolas G. Toman, Clairice M. Pearce, Sarah K. Tran, Christopher J. Sipe, Winston Guo, Joseph P. Voth, Shivanshi Vaid, Hui Xie, Wei-Cheng Lu, Will Swanson, Andrew W. Grande, Mark R. Schleiss, Craig J. Bierle, Maxim C-J. Cheeran, Walter C. Low, and Mohammed Alsharifi

Subjects

Medicine, Science

Abstract

Zika virus (ZIKV) exhibits a tropism for brain tumor cells and has been used as an oncolytic virus to target brain tumors in mice with modest effects on extending median survival. Recent studies have highlighted the potential for combining virotherapy and immunotherapy to target cancer. We postulated that ZIKV could be used as an adjuvant to enhance the long-term survival of mice with malignant glioblastoma and generate memory T-cells capable of providing long-term immunity against cancer remission. To test this hypothesis mice bearing malignant intracranial GL261 tumors were subcutaneously vaccinated with irradiated GL261 cells previously infected with the ZIKV. Mice also received intracranial injections of live ZIKV, irradiation attenuated ZIKV, or irradiated GL261 cells previously infected with ZIKV. Long-term survivors were rechallenged with a second intracranial tumor to examine their immune response and look for the establishment of protective memory T-cells. Mice with subcutaneous vaccination plus intracranial irradiation attenuated ZIKV or intracranial irradiated GL261 cells previously infected with ZIKV exhibited the greatest extensions to overall survival. Flow cytometry analysis of immune cells within the brains of long-term surviving mice after tumor rechallenge revealed an increase in the number of T-cells, including CD4+ and tissue-resident effector/ effector memory CD4+ T-cells, in comparison to long-term survivors that were mock-rechallenged, and in comparison to naïve untreated mice challenged with intracranial gliomas. These results suggest that ZIKV can serve as an adjuvant to subcutaneous tumor vaccines that enhance long-term survival and generate protective tissue-resident memory CD4+ T-cells.

Published

2020

4. Efficacy of Cell-Based Therapies for Traumatic Brain Injuries

Author

Matthew R. Chrostek, Emily G. Fellows, Winston L. Guo, William J. Swanson, Andrew T. Crane, Maxim C. Cheeran, Walter C. Low, and Andrew W. Grande

Subjects

traumatic brain injury, stem cells, inflammation, neuroregeneration, mesenchymal stem cells, neural stem cells, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Traumatic brain injuries (TBIs) are a leading cause of death and disability. Additionally, growing evidence suggests a link between TBI-induced neuroinflammation and neurodegenerative disorders. Treatments for TBI patients are limited, largely focused on rehabilitation therapy, and ultimately, fail to provide long-term neuroprotective or neurorestorative benefits. Because of the prevalence of TBI and lack of viable treatments, new therapies are needed which can promote neurological recovery. Cell-based treatments are a promising avenue because of their potential to provide multiple therapeutic benefits. Cell-based therapies can promote neuroprotection via modulation of inflammation and promote neurorestoration via induction of angiogenesis and neurogenesis. Neural stem/progenitor cell transplantations have been investigated in preclinical TBI models for their ability to directly contribute to neuroregeneration, form neural-like cells, and improve recovery. Mesenchymal stem cells (MSCs) have been investigated in clinical trials through multiple different routes of administration. Intravenous administration of MSCs appears most promising, demonstrating a robust safety profile, correlation with neurological improvements, and reductions in systemic inflammation following TBI. While still preliminary, evidence suggests cell-based therapies may become a viable treatment for TBI based on their ability to promote neuroregeneration and reduce inflammation.

Published

2019

5. ssDNA nanotubes for selective targeting of glioblastoma and delivery of doxorubicin for enhanced survival

Author

Maple Shiao, Kevin Liaw, Huihui Kuang, Matthew R. Chrostek, Andrew T. Crane, Michael A. Harris, Efrosini Kokkoli, M. Gerard O'Sullivan, Walter C. Low, Lucy Lin, Beibei Xu, Thomas Pengo, Rangaramanujam M. Kannan, Zachary Schneiderman, Clark C. Chen, and Alexandru-Flaviu Tabaran

Subjects

Multidisciplinary, business.industry, SciAdv r-articles, medicine.disease, medicine, Cancer research, Effective treatment, Doxorubicin, Biomedicine and Life Sciences, Health and Medicine, business, medicine.drug, Glioblastoma, Research Article, Cancer

Abstract

Description, DNA nanotubes can cross blood-brain tumor barrier and enhance survival with no toxicity when used for the local delivery of DOX., Effective treatment of glioblastoma remains a daunting challenge. One of the major hurdles in the development of therapeutics is their inability to cross the blood-brain tumor barrier (BBTB). Local delivery is an alternative approach that can still suffer from toxicity in the absence of target selectivity. Here, we show that nanotubes formed from self-assembly of ssDNA-amphiphiles are stable in serum and nucleases. After bilateral brain injections, nanotubes show preferential retention by tumors compared to normal brain and are taken up by glioblastoma cells through scavenger receptor binding and macropinocytosis. After intravenous injection, they cross the BBTB and internalize in glioblastoma cells. In a minimal residual disease model, local delivery of doxorubicin showed signs of toxicity in the spleen and liver. In contrast, delivery of doxorubicin by the nanotubes resulted in no systemic toxicity and enhanced mouse survival. Our results demonstrate that ssDNA nanotubes are a promising drug delivery vehicle to glioblastoma.

Published

2021

6. Machine Learning-Enabled High-Resolution Dynamic Deuterium MR Spectroscopic Imaging

Author

Tao Wang, Walter C. Low, Xiao Hong Zhu, Matthew R. Chrostek, Yibo Zhao, Zhi-Pei Liang, Rong Guo, Yudu Li, Yi Zhang, and Wei Chen

Subjects

Magnetic Resonance Spectroscopy, Computer science, Quantitative Biology::Tissues and Organs, Noise reduction, Machine learning, computer.software_genre, Regularization (mathematics), Article, Machine Learning, Animals, Sensitivity (control systems), Electrical and Electronic Engineering, Image resolution, Radiological and Ultrasound Technology, business.industry, Noise (signal processing), Deep learning, Magnetic resonance spectroscopic imaging, Deuterium, Magnetic Resonance Imaging, Computer Science Applications, Rats, Artificial intelligence, business, computer, Software, Subspace topology, Algorithms

Abstract

Deuterium magnetic resonance spectroscopic imaging (DMRSI) has recently been recognized as a potentially powerful tool for noninvasive imaging of brain energy metabolism and tumor. However, the low sensitivity of DMRSI has significantly limited its utility for both research and clinical applications. This work presents a novel machine learning-based method to address this limitation. The proposed method synergistically integrates physics-based subspace modeling and data-driven deep learning for effective denoising, making high-resolution dynamic DMRSI possible. Specifically, a novel subspace model was used to represent the dynamic DMRSI signals; deep neural networks were trained to capture the low-dimensional manifolds of the spectral and temporal distributions of practical dynamic DMRSI data. The learned subspace and manifold structures were integrated via a regularization formulation to remove measurement noise. Theoretical analysis, computer simulations, and in vivo experiments have been conducted to demonstrate the denoising efficacy of the proposed method which enabled high-resolution imaging capability. The translational potential was demonstrated in tumor-bearing rats, where the Warburg effect associated with cancer metabolism and tumor heterogeneity were successfully captured. The new method may not only provide an effective tool to enhance the sensitivity of DMRSI for basic research and clinical applications but also provide a framework for denoising other spatiospectral data.

Published

2021

7. Zika virus-based immunotherapy enhances long-term survival of rodents with brain tumors through upregulation of memory T-cells

Author

Craig J. Bierle, Will Swanson, Matthew R. Chrostek, Clairice Pearce, Wei Cheng Lu, Andrew T. Crane, Christopher J. Sipe, Hui Xie, Andrew W. Grande, Nikolas G. Toman, Walter C. Low, Winston L. Guo, Maple Shiao, Venkatramana D. Krishna, Mark R. Schleiss, Sarah K. Tran, Joseph P. Voth, Maxim C.-J. Cheeran, and Shivanshi Vaid

Subjects

0301 basic medicine, RNA viruses, CD4-Positive T-Lymphocytes, medicine.medical_treatment, T-Lymphocytes, Cancer Treatment, Pathology and Laboratory Medicine, White Blood Cells, Mice, 0302 clinical medicine, Medical Conditions, Cancer immunotherapy, Animal Cells, Medicine and Health Sciences, Medicine, Public and Occupational Health, Oncolytic Virotherapy, 0303 health sciences, Vaccines, Multidisciplinary, T Cells, Brain Neoplasms, Vaccination and Immunization, 3. Good health, Infectious Diseases, Oncology, Medical Microbiology, 030220 oncology & carcinogenesis, Viral Pathogens, Viruses, Immunotherapy, Cellular Types, Pathogens, Adjuvant, Research Article, Infectious Disease Control, Science, Immune Cells, Immunology, Brain tumor, Microbiology, Cancer Vaccines, Cancer Immunotherapy, 03 medical and health sciences, Immune system, Malignant Tumors, Adjuvants, Immunologic, Immunity, Animals, Virotherapy, Microbial Pathogens, 030304 developmental biology, Blood Cells, Flaviviruses, business.industry, Organisms, Cancer, Cancers and Neoplasms, Biology and Life Sciences, Cell Biology, Zika Virus, medicine.disease, Oncolytic virus, Mice, Inbred C57BL, 030104 developmental biology, Cancer research, Clinical Immunology, Preventive Medicine, Clinical Medicine, business, Glioblastoma, Immunologic Memory

Abstract

Zika virus (ZIKV) exhibits a tropism for brain tumor cells and has been used as an oncolytic virus to target brain tumors in mice with modest effects on extending median survival. Recent studies have highlighted the potential for combining virotherapy and immunotherapy to target cancer. We postulated that ZIKV could be used as an adjuvant to enhance the long-term survival of mice with malignant glioblastoma and generate memory T-cells capable of providing long-term immunity against cancer remission. To test this hypothesis mice bearing malignant intracranial GL261 tumors were subcutaneously vaccinated with irradiated GL261 cells previously infected with the ZIKV. Mice also received intracranial injections of live ZIKV, irradiated ZIKV, or irradiated GL261 cells previously infected with ZIKV. Long-term survivors were rechallenged with a second intracranial tumor to examine their immune response and look for the establishment of protective memory T-cells. Mice with subcutaneous vaccination plus intracranial irradiated ZIKV or intracranial irradiated GL261 cells previously infected with ZIKV exhibited the greatest extensions to overall survival. Flow cytometry analysis of immune cells within the brains of long-term surviving mice after tumor rechallenge revealed an upregulation in the levels of T-cells, including CD4+ and tissue-resident memory CD4+ T-cells, in comparison to long-term survivors that were mock-rechallenged, and in comparison to naïve untreated mice challenged with intracranial gliomas. These results suggest that ZIKV can serve as an adjuvant to subcutaneous tumor vaccines that enhance long-term survival and generate protective tissue-resident memory CD4+ T-cells.

Published

2020

8. Efficacy of Cell-Based Therapies for Traumatic Brain Injuries

Author

Walter C. Low, William J. Swanson, Emily G. Fellows, Andrew T. Crane, Winston L. Guo, Andrew W. Grande, Matthew R. Chrostek, and Maxim C.-J. Cheeran

Subjects

Traumatic brain injury, Bioinformatics, Neuroprotection, lcsh:RC321-571, 03 medical and health sciences, 0302 clinical medicine, stem cells, Medicine, Progenitor cell, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Neuroinflammation, neuroregeneration, 030304 developmental biology, neural stem cells, 0303 health sciences, mesenchymal stem cells, business.industry, General Neuroscience, traumatic brain injury, Mesenchymal stem cell, medicine.disease, Neuroregeneration, Neural stem cell, inflammation, Perspective, Stem cell, business, 030217 neurology & neurosurgery

Abstract

Traumatic brain injuries (TBIs) are a leading cause of death and disability. Additionally, growing evidence suggests a link between TBI-induced neuroinflammation and neurodegenerative disorders. Treatments for TBI patients are limited, largely focused on rehabilitation therapy, and ultimately, fail to provide long-term neuroprotective or neurorestorative benefits. Because of the prevalence of TBI and lack of viable treatments, new therapies are needed which can promote neurological recovery. Cell-based treatments are a promising avenue because of their potential to provide multiple therapeutic benefits. Cell-based therapies can promote neuroprotection via modulation of inflammation and promote neurorestoration via induction of angiogenesis and neurogenesis. Neural stem/progenitor cell transplantations have been investigated in preclinical TBI models for their ability to directly contribute to neuroregeneration, form neural-like cells, and improve recovery. Mesenchymal stem cells (MSCs) have been investigated in clinical trials through multiple different routes of administration. Intravenous administration of MSCs appears most promising, demonstrating a robust safety profile, correlation with neurological improvements, and reductions in systemic inflammation following TBI. While still preliminary, evidence suggests cell-based therapies may become a viable treatment for TBI based on their ability to promote neuroregeneration and reduce inflammation.

Published

2019

9. Efficacy of stem cell-based therapies for stroke

Author

Emily G. Fellows, Andrew W. Grande, Matthew R. Chrostek, Walter C. Low, and Andrew T. Crane

Subjects

0301 basic medicine, Neurogenesis, Bioinformatics, Mesenchymal Stem Cell Transplantation, Neuroprotection, Article, 03 medical and health sciences, 0302 clinical medicine, Neural Stem Cells, medicine, Animals, Humans, Molecular Biology, Stroke, business.industry, General Neuroscience, Mesenchymal stem cell, Bone Marrow Stem Cell, Brain, Mesenchymal Stem Cells, medicine.disease, Neuroregeneration, Neural stem cell, 030104 developmental biology, Treatment Outcome, Encephalitis, Neurology (clinical), Cord Blood Stem Cell Transplantation, Stem cell, business, 030217 neurology & neurosurgery, Developmental Biology, Stem Cell Transplantation

Abstract

Stroke remains a prevalent disease with limited treatment options. Available treatments offer little in the way of enhancing neurogenesis and recovery. Because of the limitations of available treatments, new therapies for stroke are needed. Stem cell-based therapies for stroke offer promise because of their potential to provide neurorestorative benefits. Stem cell-based therapies aim to promote neurogenesis and replacement of lost neurons or protect surviving neurons in order to improve neurological recovery. The mechanism through which stem cell treatments mediate their therapeutic effect is largely dependent on the type of stem cell and route of administration. Neural stem cells have been shown in pre-clinical and clinical trials to promote functional recovery when used in intracerebral transplantations. The therapeutic effects of neural stem cells have been attributed to their formation of new neurons and promotion of neuroregeneration. Bone marrow stem cells (BMSC) and mesenchymal stem cells (MSC) have been shown to enhance neurogenesis in pre-clinical models in intracerebral transplantations, but lack clinical evidence to support this therapeutic approach in patients and appear to be less effective than neural stem cells. Intravenous and intra-arterial administration of BMSC and MSC have shown more promise, where their effects are largely mediated through neuroprotective mechanisms. The immune system has been implicated in exacerbating initial damage caused by stroke, and BMSC and MSC have demonstrated immunomodulatory properties capable of dampening post-stroke inflammation and potentially improving recovery. While still in development, stem cell therapies may yield new treatments for stroke which can improve neurological recovery.

Published

2019

10. Immunotherapy and checkpoint inhibitors for gliomas

Author

Clairice Pearce, Nikolas G. Toman, Emily G. Fellows, Andrew T. Crane, Walter C. Low, Sarah K. Tran, and Matthew R. Chrostek

Subjects

Neurology, business.industry, Immune checkpoint inhibitors, Glioma, medicine.medical_treatment, Immunology, Cancer research, Medicine, Neurology (clinical), Immunotherapy, business, medicine.disease

Published

2018

11. EXTH-01. ZIKA VIRUS TARGETING OF MALIGNANT HUMAN AND MURINE BRAIN TUMORS

Author

Clairice Pearce, Nikolas G. Toman, Georgette Danczyk, Kyle Schaible, Christopher J. Sipe, Andrew T. Crane, Craig J. Bierle, Joseph P. Voth, Mark R. Schleiss, Shivanshi Vaid, Walter C. Low, Elizabeth Straub, Matthew R. Chrostek, Maple Shiao, and Zach Miller

Subjects

Cancer Research, biology, biology.organism_classification, Neural stem cell, Zika virus, Oncolytic virus, Abstracts, Tissue culture, Oncology, Murine brain, Apoptosis, Cancer research, Nucleic acid, Neurology (clinical), Tropism

Abstract

Previous studies have demonstrated that the tropism of Zika virus (ZIKV) for human neural stem cells (NSCs) leads to severe brain malformations. The proposed mechanisms underlying these brain malformations are thought to include the induction of apoptosis in neural progenitor/stem cells (Zhang et al., Nucleic Acid Res. 44:8610–8620, 2016). Previously, we observed many similarities between NSCs and brain tumor stem cells (BTSCs) (Wu et al., Stem Cells Dev., 17:173–184, 2008) and sought to determine if BTSC could support ZIKV replication. ZIKV infection of skin cells in vitro is mediated by the receptors AXL, DC-SIGN, TIM1, and TYRO3 (Hamel et al., J Virol. 89:8880–8896, 2015). We examined human embryonic brain tissue and have observed that the putative ZIKV receptor TIM1 is expressed by neuronal and astrocytic progenitor cells. Given the similarities between NSCs and BTSCs we examined human and rodent brain tumor cells for putative ZIKV receptor expression. We found TIM1 expression by human GBM6 glioma cells and murine GL261 gliomas. In tissue culture studies, incubation of ZIKV with human GBM6 cells led to high levels of infection. To determine the effects of ZIKV on tumor growth in vivo, we transplanted GL261 cells into the striatal area of the brain in syngeneic C57B/6 mice. Intra-tumoral injections of ZIKV were administered immediately after intra-cranial tumor implantation. Tumor-bearing mice receiving intra-tumoral injections of ZIKV exhibited prolonged survival in comparison to untreated mice. Together these results suggest that ZIKV may have potential as an oncolytic virus for targeting malignant brain tumors. (This work was supported in part by a grant from the Randy Shaver Cancer Research Foundation).

Published

2017