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1. Unique characteristics of the tumor immune microenvironment in young patients with metastatic colorectal cancer

Author

Brian D. Griffith, Jenny Lazarus, Jake McGue, Santhoshi Krishnan, Michael I. D’Angelica, Jinru Shia, Irina Dobrosotskaya, Jaiqi Shi, Jacob Edwards, Arvind Rao, and Timothy L. Frankel

Subjects
tumor immunology, colorectal cancer, immunotherapy, spatial relation analysis, multiplex immunohistochemistry (IHC), Immunologic diseases. Allergy, RC581-607
Abstract

IntroductionMetastatic colorectal cancer (mCRC) remains a common and highly morbid disease, with a recent increase in incidence in patients younger than 50 years. There is an acute need to better understand differences in tumor biology, molecular characteristics, and other age-related differences in the tumor microenvironment (TME).Methods111 patients undergoing curative-intent resection of colorectal liver metastases were stratified by age into those 65 years old, and tumors were subjected to multiplex fluorescent immunohistochemistry (mfIHC) to characterize immune infiltration and cellular engagement.ResultsThere was no difference in infiltration or proportion of immune cells based upon age, but the younger cohort had a higher proportion of programmed death-ligand 1 (PD-L1)+ expressing antigen presenting cells (APCs) and demonstrated decreased intercellular distance and increased cellular engagement between tumor cells (TCs) and cytotoxic T lymphocytes (CTLs), and between TCs and APCs. These trends were independent of microsatellite instability in tumors.DiscussionAge-related differences in PD-L1 expression and cellular engagement in the tumor microenvironment of patients with mCRC, findings which were unrelated to microsatellite status, suggest a more active immune microenvironment in younger patients that may offer an opportunity for therapeutic intervention with immune based therapy.

Published
2023
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2. A Comparison of Spatial and Phenotypic Immune Profiles of Pancreatic Ductal Adenocarcinoma and Its Precursor Lesions

Author

Thomas Enzler, Jiaqi Shi, Jake McGue, Brian D. Griffith, Lei Sun, Vaibhav Sahai, Hari Nathan, and Timothy L. Frankel

Subjects
pancreatic cancer precursor lesions, pancreatic ductal adenocarcinoma, immune microenvironment, immunotherapy, Biology (General), QH301-705.5, Chemistry, QD1-999
Abstract

Pancreatic ductal adenocarcinoma (PDAC) is a devastating disease with a 5-year survival rate of 12.5%. PDAC predominantly arises from non-cystic pancreatic intraepithelial neoplasia (PanIN) and cystic intraductal papillary mucinous neoplasm (IPMN). We used multiplex immunofluorescence and computational imaging technology to characterize, map, and compare the immune microenvironments (IMEs) of PDAC and its precursor lesions. We demonstrate that the IME of IPMN was abundantly infiltrated with CD8+ T cells and PD-L1-positive antigen-presenting cells (APCs), whereas the IME of PanIN contained fewer CD8+ T cells and fewer PD-L1-positive APCs but elevated numbers of immunosuppressive regulatory T cells (Tregs). Thus, immunosuppression in IPMN and PanIN seems to be mediated by different mechanisms. While immunosuppression in IPMN is facilitated by PD-L1 expression on APCs, Tregs seem to play a key role in PanIN. Our findings suggest potential immunotherapeutic interventions for high-risk precursor lesions, namely, targeting PD-1/PD-L1 in IPMN and CTLA-4-positive Tregs in PanIN to restore immunosurveillance and prevent progression to cancer. Tregs accumulate with malignant transformation, as observed in PDAC, and to a lesser extent in IPMN-associated PDAC (IAPA). High numbers of Tregs in the microenvironment of PDAC went along with a markedly decreased interaction between CD8+ T cells and cancerous epithelial cells (ECs), highlighting the importance of Tregs as key players in immunosuppression in PDAC. We found evidence that a defect in antigen presentation, further aggravated by PD-L1 expression on APC, may contribute to immunosuppression in IAPA, suggesting a role for PD-L1/PD-1 immune checkpoint inhibitors in the treatment of IAPA.

Published
2024
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3. Tomatidine targets ATF4-dependent signaling and induces ferroptosis to limit pancreatic cancer progression

Author

Debasmita Mukherjee, Srija Chakraborty, Lena Bercz, Liliana D’Alesio, Jessica Wedig, Molly A. Torok, Timothy Pfau, Hannah Lathrop, Shrina Jasani, Abigail Guenther, Jake McGue, Daniel Adu-Ampratwum, James R. Fuchs, Timothy L. Frankel, Maciej Pietrzak, Stacey Culp, Anne M. Strohecker, Aleksander Skardal, and Thomas A. Mace

Subjects
Therapeutics, Microenvironment, Cancer, Science
Abstract

Summary: Pancreatic ductal adenocarcinoma (PDAC) is an aggressive cancer with high metastasis and therapeutic resistance. Activating transcription factor 4 (ATF4), a master regulator of cellular stress, is exploited by cancer cells to survive. Prior research and data reported provide evidence that high ATF4 expression correlates with worse overall survival in PDAC. Tomatidine, a natural steroidal alkaloid, is associated with inhibition of ATF4 signaling in multiple diseases. Here, we discovered that in vitro and in vivo tomatidine treatment of PDAC cells inhibits tumor growth. Tomatidine inhibited nuclear translocation of ATF4 and reduced the transcriptional binding of ATF4 with downstream promoters. Tomatidine enhanced gemcitabine chemosensitivity in 3D ECM-hydrogels and in vivo. Tomatidine treatment was associated with induction of ferroptosis signaling validated by increased lipid peroxidation, mitochondrial biogenesis, and decreased GPX4 expression in PDAC cells. This study highlights a possible therapeutic approach utilizing a plant-derived metabolite, tomatidine, to target ATF4 activity in PDAC.

Published
2023
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4. Cellular engagement and interaction in the tumor microenvironment predict non-response to PD-1/PD-L1 inhibitors in metastatic non-small cell lung cancer

Author

Angel Qin, Fatima Lima, Samantha Bell, Gregory P. Kalemkerian, Bryan J. Schneider, Nithya Ramnath, Madelyn Lew, Santhoshi Krishnan, Shariq Mohammed, Arvind Rao, and Timothy L. Frankel

Subjects
Medicine, Science
Abstract

Abstract Immune checkpoint inhibitors (ICI) with anti-PD-1/PD-L1 agents have improved the survival of patients with metastatic non-small cell lung cancer (mNSCLC). Tumor PD-L1 expression is an imperfect biomarker as it does not capture the complex interactions between constituents of the tumor microenvironment (TME). Using multiplex fluorescent immunohistochemistry (mfIHC), we modeled the TME to study the influence of cellular distribution and engagement on response to ICI in mNSCLC. We performed mfIHC on pretreatment tissue from patients with mNSCLC who received ICI. We used primary antibodies against CD3, CD8, CD163, PD-L1, pancytokeratin, and FOXP3; simple and complex phenotyping as well as spatial analyses was performed. We analyzed 68 distinct samples from 52 patients with mNSCLC. Patients were 39–79 years old (median 67); 44% were male and 75% had adenocarcinoma histology. The most used ICI was atezolizumab (48%). The percentage of PD-L1 positive epithelial tumor cells (EC), degree of cytotoxic T lymphocyte (CTL) engagement with EC, and degree of CTL engagement with helper T lymphocytes (HTL) were significantly lower in non-responders versus responders (p = 0.0163, p = 0.0026 and p = 0.0006, respectively). The combination of these 3 characteristics generated the best sensitivity and specificity to predict non-response to ICI and was also associated with shortened overall survival (p = 0.0271). The combination of low CTL engagement with EC and HTL along with low expression of EC PD-L1 represents a state of impaired endogenous immune reactivity. Together, they more precisely identified non-responders to ICI compared to PD-L1 alone and illustrate the importance of cellular interactions in the TME.

Published
2022
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5. GaWRDenMap: a quantitative framework to study the local variation in cell–cell interactions in pancreatic disease subtypes

Author

Santhoshi N. Krishnan, Shariq Mohammed, Timothy L. Frankel, and Arvind Rao

Subjects
Medicine, Science
Abstract

Abstract Spatial pattern modelling concepts are being increasingly used in capturing disease heterogeneity. Quantification of heterogeneity in the tumor microenvironment is extremely important in pancreatic ductal adenocarcinoma (PDAC), which has been shown to co-occur with other pancreatic diseases and neoplasms with certain attributes that make visual discrimination difficult. In this paper, we propose the GaWRDenMap framework, that utilizes the concepts of geographically weighted regression (GWR) and a density function-based classification model, and apply it to a cohort of multiplex immunofluorescence images from patients belonging to six different pancreatic diseases. We used an internal cohort of 228 patients comprised of 34 Chronic Pancreatitis (CP), 71 PDAC, 70 intraductal papillary mucinous neoplasm (IPMN), 16 mucinous cystic neoplasm (MCN), 29 pancreatic intraductal neoplasia (PanIN) and 8 IPMN-associated PDAC patients. We utilized GWR to model the relationship between epithelial cells and immune cells on a spatial grid. The GWR model estimates were used to generate density signatures which were used in subsequent pairwise classification models to distinguish between any two pairs of disease groups. Image-level, as well as subject-level analysis, were performed. When applied to this dataset, our classification model showed significant discrimination ability in multiple pairwise comparisons, in comparison to commonly used abundance-based metrics, like the Morisita-Horn index. The model was able to best discriminate between CP and PDAC at both the subject- and image-levels. It was also able to reasonably discriminate between PDAC and IPMN. These results point to a potential difference in the spatial arrangement of epithelial and immune cells between CP, PDAC and IPMN, that could be of high diagnostic significance. Further validation on a more comprehensive dataset would be warranted.

Published
2022
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6. Extrinsic KRAS Signaling Shapes the Pancreatic Microenvironment Through Fibroblast ReprogrammingSummary

Author

Ashley Velez-Delgado, Katelyn L. Donahue, Kristee L. Brown, Wenting Du, Valerie Irizarry-Negron, Rosa E. Menjivar, Emily L. Lasse Opsahl, Nina G. Steele, Stephanie The, Jenny Lazarus, Veerin R. Sirihorachai, Wei Yan, Samantha B. Kemp, Samuel A. Kerk, Murali Bollampally, Sion Yang, Michael K. Scales, Faith R. Avritt, Fatima Lima, Costas A. Lyssiotis, Arvind Rao, Howard C. Crawford, Filip Bednar, Timothy L. Frankel, Benjamin L. Allen, Yaqing Zhang, and Marina Pasca di Magliano

Subjects
Pancreatic Cancer, Transformation, Fibroblasts, Macrophages, Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Background & Aims: Oncogenic Kirsten Rat Sarcoma virus (KRAS) is the hallmark mutation of human pancreatic cancer and a driver of tumorigenesis in genetically engineered mouse models of the disease. Although the tumor cell–intrinsic effects of oncogenic Kras expression have been widely studied, its role in regulating the extensive pancreatic tumor microenvironment is less understood. Methods: Using a genetically engineered mouse model of inducible and reversible oncogenic Kras expression and a combination of approaches that include mass cytometry and single-cell RNA sequencing we studied the effect of oncogenic KRAS in the tumor microenvironment. Results: We have discovered that non–cell autonomous (ie, extrinsic) oncogenic KRAS signaling reprograms pancreatic fibroblasts, activating an inflammatory gene expression program. As a result, fibroblasts become a hub of extracellular signaling, and the main source of cytokines mediating the polarization of protumorigenic macrophages while also preventing tissue repair. Conclusions: Our study provides fundamental knowledge on the mechanisms underlying the formation of the fibroinflammatory stroma in pancreatic cancer and highlights stromal pathways with the potential to be exploited therapeutically.

Published
2022
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7. Myeloid Cell-Derived HB-EGF Drives Tissue Recovery After PancreatitisSummary

Author

Hui-Ju Wen, Shan Gao, Yin Wang, Michael Ray, Mark A. Magnuson, Christopher V.E. Wright, Marina Pasca Di Magliano, Timothy L. Frankel, and Howard C. Crawford

Subjects
Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Background & Aims: Pancreatitis is a major cause of morbidity and mortality and is a risk factor for pancreatic tumorigenesis. Upon tissue damage, an inflammatory response, made up largely of macrophages, provides multiple growth factors that promote repair. Here, we examine the molecular pathways initiated by macrophages to promote pancreas recovery from pancreatitis. Methods: To induce organ damage, mice were subjected to cerulein-induced experimental pancreatitis and analyzed at various times of recovery. CD11b-DTR mice were used to deplete myeloid cells. Hbegff/f;LysM-Cre mice were used to ablate myeloid cell–derived heparin-binding epidermal growth factor (EGF)-like growth factor (HB-EGF). To ablate EGFR specifically during recovery, pancreatitis was induced in Egfrf/f;Ptf1aFlpO/+;FSF-Rosa26CAG-CreERT2 mice followed by tamoxifen treatment. Results: Macrophages infiltrating the pancreas in experimental pancreatitis make high levels of HB-EGF. Both depletion of myeloid cells and ablation of myeloid cell HB-EGF delayed recovery from experimental pancreatitis, resulting from a decrease in cell proliferation and an increase in apoptosis. Mechanistically, ablation of myeloid cell HB-EGF impaired epithelial cell DNA repair, ultimately leading to cell death. Soluble HB-EGF induced EGFR nuclear translocation and methylation of histone H4, facilitating resolution of DNA damage in pancreatic acinar cells in vitro. Consistent with its role as the primary receptor of HB-EGF, in vivo ablation of EGFR from pancreatic epithelium during recovery from pancreatitis resulted in accumulation of DNA damage. Conclusions: By using novel conditional knockout mouse models, we determined that HB-EGF derived exclusively from myeloid cells induces epithelial cell proliferation and EGFR-dependent DNA repair, facilitating pancreas healing after injury. Keywords: DNA Damage, EGFR, Inflammation, Macrophages

Published
2019
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8. Immune determinants of Barrett’s progression to esophageal adenocarcinoma

Author

Kiran H. Lagisetty, Dyke P. McEwen, Derek J. Nancarrow, Johnathon G. Schiebel, Daysha Ferrer-Torres, Dipankar Ray, Timothy L. Frankel, Jules Lin, Andrew C. Chang, Laura A. Kresty, and David G. Beer

Subjects
Immunology, Oncology, Medicine
Abstract

Esophageal adenocarcinoma (EAC) develops from Barrett’s esophagus (BE), a chronic inflammatory state that can progress through a series of transformative dysplastic states before tumor development. While molecular and genetic changes of EAC tumors have been studied, immune microenvironment changes during Barrett’s progression to EAC remain poorly understood. In this study, we identify potential immunologic changes that can occur during BE-to-EAC progression. RNA sequencing (RNA-Seq) analysis on tissue samples from EAC patients undergoing surgical resection demonstrated that a subset of chemokines and cytokines, most notably IL6 and CXCL8, increased during BE progression to EAC. xCell deconvolution analysis investigating immune cell population changes demonstrated that the largest changes in expression during BE progression occurred in M2 macrophages, pro–B cells, and eosinophils. Multiplex immunohistochemical staining of tissue microarrays showed increased immune cell populations during Barrett’s progression to high-grade dysplasia. In contrast, EAC tumor sections were relatively immune poor, with a rise in PD-L1 expression and loss of CD8+ T cells. These data demonstrate that the EAC microenvironment is characterized by poor cytotoxic effector cell infiltration and increased immune inhibitory signaling. These findings suggest an immunosuppressive microenvironment, highlighting the need for further studies to explore immune modulatory therapy in EAC.

Published
2021
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10. Analysis of Donor Pancreata Defines the Transcriptomic Signature and Microenvironment of Early Neoplastic Lesions

Author

Eileen S. Carpenter, Ahmed M. Elhossiny, Padma Kadiyala, Jay Li, Jake McGue, Brian D. Griffith, Yaqing Zhang, Jacob Edwards, Sarah Nelson, Fatima Lima, Katelyn L. Donahue, Wenting Du, Allison C. Bischoff, Danyah Alomari, Hannah R. Watkoske, Michael Mattea, Stephanie The, Carlos E. Espinoza, Meredith Barrett, Christopher J. Sonnenday, Nicholas Olden, Chin-Tung Chen, Nicole Peterson, Valerie Gunchick, Vaibhav Sahai, Arvind Rao, Filip Bednar, Jiaqi Shi, Timothy L. Frankel, and Marina Pasca di Magliano

Subjects
Oncology
Abstract

The adult healthy human pancreas has been poorly studied given the lack of indication to obtain tissue from the pancreas in the absence of disease and rapid postmortem degradation. We obtained pancreata from brain dead donors, thus avoiding any warm ischemia time. The 30 donors were diverse in age and race and had no known pancreas disease. Histopathologic analysis of the samples revealed pancreatic intraepithelial neoplasia (PanIN) lesions in most individuals irrespective of age. Using a combination of multiplex IHC, single-cell RNA sequencing, and spatial transcriptomics, we provide the first-ever characterization of the unique microenvironment of the adult human pancreas and of sporadic PanIN lesions. We compared healthy pancreata to pancreatic cancer and peritumoral tissue and observed distinct transcriptomic signatures in fibroblasts and, to a lesser extent, macrophages. PanIN epithelial cells from healthy pancreata were remarkably transcriptionally similar to cancer cells, suggesting that neoplastic pathways are initiated early in tumorigenesis. Significance: Precursor lesions to pancreatic cancer are poorly characterized. We analyzed donor pancreata and discovered that precursor lesions are detected at a much higher rate than the incidence of pancreatic cancer, setting the stage for efforts to elucidate the microenvironmental and cell-intrinsic factors that restrain or, conversely, promote malignant progression.

Published
2023

11. Supplementary Figures Part 2 from Analysis of Donor Pancreata Defines the Transcriptomic Signature and Microenvironment of Early Neoplastic Lesions

Author

Marina Pasca di Magliano, Timothy L. Frankel, Jiaqi Shi, Filip Bednar, Arvind Rao, Vaibhav Sahai, Valerie Gunchick, Nicole Peterson, Chin-Tung Chen, Nicholas Olden, Christopher J. Sonnenday, Meredith Barrett, Carlos E. Espinoza, Stephanie The, Michael Mattea, Hannah R. Watkoske, Danyah Alomari, Allison C. Bischoff, Wenting Du, Katelyn L. Donahue, Fatima Lima, Sarah Nelson, Jacob Edwards, Yaqing Zhang, Brian D. Griffith, Jake McGue, Jay Li, Padma Kadiyala, Ahmed M. Elhossiny, and Eileen S. Carpenter

Abstract

Supplementary Figures 11-14 and associated legends.

Published
2023

12. Supplementary Figures Part 1 from Analysis of Donor Pancreata Defines the Transcriptomic Signature and Microenvironment of Early Neoplastic Lesions

Author

Marina Pasca di Magliano, Timothy L. Frankel, Jiaqi Shi, Filip Bednar, Arvind Rao, Vaibhav Sahai, Valerie Gunchick, Nicole Peterson, Chin-Tung Chen, Nicholas Olden, Christopher J. Sonnenday, Meredith Barrett, Carlos E. Espinoza, Stephanie The, Michael Mattea, Hannah R. Watkoske, Danyah Alomari, Allison C. Bischoff, Wenting Du, Katelyn L. Donahue, Fatima Lima, Sarah Nelson, Jacob Edwards, Yaqing Zhang, Brian D. Griffith, Jake McGue, Jay Li, Padma Kadiyala, Ahmed M. Elhossiny, and Eileen S. Carpenter

Abstract

Supplementary Figures 1-10 and associated legends

Published
2023

13. Data from Analysis of Donor Pancreata Defines the Transcriptomic Signature and Microenvironment of Early Neoplastic Lesions

Author

Marina Pasca di Magliano, Timothy L. Frankel, Jiaqi Shi, Filip Bednar, Arvind Rao, Vaibhav Sahai, Valerie Gunchick, Nicole Peterson, Chin-Tung Chen, Nicholas Olden, Christopher J. Sonnenday, Meredith Barrett, Carlos E. Espinoza, Stephanie The, Michael Mattea, Hannah R. Watkoske, Danyah Alomari, Allison C. Bischoff, Wenting Du, Katelyn L. Donahue, Fatima Lima, Sarah Nelson, Jacob Edwards, Yaqing Zhang, Brian D. Griffith, Jake McGue, Jay Li, Padma Kadiyala, Ahmed M. Elhossiny, and Eileen S. Carpenter

Abstract

The adult healthy human pancreas has been poorly studied given the lack of indication to obtain tissue from the pancreas in the absence of disease and rapid postmortem degradation. We obtained pancreata from brain dead donors, thus avoiding any warm ischemia time. The 30 donors were diverse in age and race and had no known pancreas disease. Histopathologic analysis of the samples revealed pancreatic intraepithelial neoplasia (PanIN) lesions in most individuals irrespective of age. Using a combination of multiplex IHC, single-cell RNA sequencing, and spatial transcriptomics, we provide the first-ever characterization of the unique microenvironment of the adult human pancreas and of sporadic PanIN lesions. We compared healthy pancreata to pancreatic cancer and peritumoral tissue and observed distinct transcriptomic signatures in fibroblasts and, to a lesser extent, macrophages. PanIN epithelial cells from healthy pancreata were remarkably transcriptionally similar to cancer cells, suggesting that neoplastic pathways are initiated early in tumorigenesis.Significance:Precursor lesions to pancreatic cancer are poorly characterized. We analyzed donor pancreata and discovered that precursor lesions are detected at a much higher rate than the incidence of pancreatic cancer, setting the stage for efforts to elucidate the microenvironmental and cell-intrinsic factors that restrain or, conversely, promote malignant progression.

Published
2023

14. Supplementary Tables from Analysis of Donor Pancreata Defines the Transcriptomic Signature and Microenvironment of Early Neoplastic Lesions

Author

Marina Pasca di Magliano, Timothy L. Frankel, Jiaqi Shi, Filip Bednar, Arvind Rao, Vaibhav Sahai, Valerie Gunchick, Nicole Peterson, Chin-Tung Chen, Nicholas Olden, Christopher J. Sonnenday, Meredith Barrett, Carlos E. Espinoza, Stephanie The, Michael Mattea, Hannah R. Watkoske, Danyah Alomari, Allison C. Bischoff, Wenting Du, Katelyn L. Donahue, Fatima Lima, Sarah Nelson, Jacob Edwards, Yaqing Zhang, Brian D. Griffith, Jake McGue, Jay Li, Padma Kadiyala, Ahmed M. Elhossiny, and Eileen S. Carpenter

Abstract

Supplemental Table 1: Demographics and clinical data for donor Gife of Life Samples Supplemental Table 2: Putative Ligand-Receptor pairs comparing all cell types from single cell sequencing of tumor samples compared to healthy samples. Supplemental Table 3: Differential gene expression using linear mixed model analysis of cell types from spatial transcriptomic ROIs. Supplemental Table 4: Kras mutational profiling on select donor samples Supplemental Table 5: Antibodies used for multiplex immunofluoresence. Supplemental Table 6: Antibodies and RNAScope probe used for co-IF/ISH.

Published
2023

15. Data from DNA-PK Inhibition and Radiation Promote Antitumoral Immunity through RNA Polymerase III in Pancreatic Cancer

Author

Qiang Zhang, Michael D. Green, Meredith A. Morgan, Timothy L. Frankel, Theodore S. Lawrence, Leslie A. Parsels, Joshua D. Parsels, Fatima Lima, David Karnak, Long Jiang, Zhuwen Wang, Xinyi Zhao, Matthew T. McMillan, and Weiwei Wang

Abstract

Targeting the DNA damage response in combination with radiation enhances type I interferon (T1IFN)-driven innate immune signaling. It is not understood, however, whether DNA-dependent protein kinase (DNA-PK), the kinase critical for repairing the majority of radiation-induced DNA double-strand breaks in cancer cells, is immunomodulatory. We show that combining radiation with DNA-PK inhibition increases cytosolic double-stranded DNA and tumoral T1IFN signaling in a cyclic GMP-AMP synthase (cGAS)- and stimulator of interferon genes (STING)-independent, but an RNA polymerase III (POL III), retinoic acid-inducible gene I (RIG-I), and antiviral-signaling protein (MAVS)-dependent manner. Although DNA-PK inhibition and radiation also promote programmed death-ligand 1 (PD-L1) expression, the use of anti–PD-L1 in combination with radiation and DNA-PK inhibitor potentiates antitumor immunity in pancreatic cancer models. Our findings demonstrate a novel mechanism for the antitumoral immune effects of DNA-PK inhibitor and radiation that leads to increased sensitivity to anti–PD-L1 in poorly immunogenic pancreatic cancers.Implications:Our work nominates a novel therapeutic strategy as well as its cellular mechanisms pertinent for future clinical trials combining M3814, radiation, and anti-PD-L1 antibody in patients with pancreatic cancer.

Published
2023

16. Supplementary Figure from DNA-PK Inhibition and Radiation Promote Antitumoral Immunity through RNA Polymerase III in Pancreatic Cancer

Author

Qiang Zhang, Michael D. Green, Meredith A. Morgan, Timothy L. Frankel, Theodore S. Lawrence, Leslie A. Parsels, Joshua D. Parsels, Fatima Lima, David Karnak, Long Jiang, Zhuwen Wang, Xinyi Zhao, Matthew T. McMillan, and Weiwei Wang

Abstract

Supplementary Figure from DNA-PK Inhibition and Radiation Promote Antitumoral Immunity through RNA Polymerase III in Pancreatic Cancer

Published
2023

17. Supplementary Data from Regulatory T-cell Depletion Alters the Tumor Microenvironment and Accelerates Pancreatic Carcinogenesis

Author

Marina Pasca di Magliano, Filip Bednar, Timothy L. Frankel, Costas A. Lyssiotis, Howard C. Crawford, Michelle A. Anderson, Alekya Vinta, Anna C. Nevison, Valerie Irizarry-Negron, Kristee L. Brown, Eileen S. Carpenter, Katelyn Donahue, Ashley Velez-Delgado, Veerin R. Sirihorachai, Samantha B. Kemp, Rosa E. Menjivar, Christopher J. Halbrook, Zeribe C. Nwosu, Ho-Joon Lee, Wei Yan, Nina G. Steele, Jenny Lazarus, and Yaqing Zhang

Abstract

Supplemental figure 1 with legend

Published
2023

18. Data from Regulatory T-cell Depletion Alters the Tumor Microenvironment and Accelerates Pancreatic Carcinogenesis

Author

Marina Pasca di Magliano, Filip Bednar, Timothy L. Frankel, Costas A. Lyssiotis, Howard C. Crawford, Michelle A. Anderson, Alekya Vinta, Anna C. Nevison, Valerie Irizarry-Negron, Kristee L. Brown, Eileen S. Carpenter, Katelyn Donahue, Ashley Velez-Delgado, Veerin R. Sirihorachai, Samantha B. Kemp, Rosa E. Menjivar, Christopher J. Halbrook, Zeribe C. Nwosu, Ho-Joon Lee, Wei Yan, Nina G. Steele, Jenny Lazarus, and Yaqing Zhang

Abstract

Regulatory T cells (Treg) are abundant in human and mouse pancreatic cancer. To understand the contribution to the immunosuppressive microenvironment, we depleted Tregs in a mouse model of pancreatic cancer. Contrary to our expectations, Treg depletion failed to relieve immunosuppression and led to accelerated tumor progression. We show that Tregs are a key source of TGFβ ligands and, accordingly, their depletion reprogramed the fibroblast population, with loss of tumor-restraining, smooth muscle actin–expressing fibroblasts. Conversely, we observed an increase in chemokines Ccl3, Ccl6, and Ccl8 leading to increased myeloid cell recruitment, restoration of immune suppression, and promotion of carcinogenesis, an effect that was inhibited by blockade of the common CCL3/6/8 receptor CCR1. Further, Treg depletion unleashed pathologic CD4+ T-cell responses. Our data point to new mechanisms regulating fibroblast differentiation in pancreatic cancer and support the notion that fibroblasts are a heterogeneous population with different and opposing functions in pancreatic carcinogenesis.Significance:Here, we describe an unexpected cross-talk between Tregs and fibroblasts in pancreatic cancer. Treg depletion resulted in differentiation of inflammatory fibroblast subsets, in turn driving infiltration of myeloid cells through CCR1, thus uncovering a potentially new therapeutic approach to relieve immunosuppression in pancreatic cancer.See related commentary by Aykut et al., p. 345.This article is highlighted in the In This Issue feature, p. 327

Published
2023

19. SFigure1 from Inhibition of Hedgehog Signaling Alters Fibroblast Composition in Pancreatic Cancer

Author

Marina Pasca di Magliano, Benjamin L. Allen, David A. Tuveson, Jonathan B. Preall, Andrzej A. Dlugosz, Filip Bednar, Arvind Rao, Timothy L. Frankel, Costas A. Lyssiotis, Howard C. Crawford, Youngkyu Park, Michelle A. Anderson, Fatima Lima, Craig Johnson, Zeribe C. Nwosu, Eileen S. Carpenter, Kristee Brown, Megan T. Hoffman, Nicole E. Franks, Christopher J. Halbrook, Valerie Irizarry-Negron, Stephanie The, Ahmed Abbas, Carlos Espinoza, Christa Hansma, Abhishek Doshi, Ela Elyada, Erin Brosnan, Tobiloba E. Oni, Yuan Hao, LiJyun Syu, Donovan Drouillard, Yaqing Zhang, Samantha B. Kemp, Giulia Biffi, and Nina G. Steele

Abstract

SFigure1

Published
2023

20. Supplementary Figure 1-4 from Inhibition of ATM Increases Interferon Signaling and Sensitizes Pancreatic Cancer to Immune Checkpoint Blockade Therapy

Author

Meredith A. Morgan, Weiping Zou, Theodore S. Lawrence, Yu L. Lei, Ilona Kryczek, Timothy L. Frankel, Marina Pasca di Magliano, Daniel R. Wahl, Nithya Ramnath, Jiaqi Shi, Leslie A. Parsels, Shuang Wei, Joshua D. Parsels, Jenny Lazarus, Xueting Lang, Michael D. Green, and Qiang Zhang

Abstract

SF1: ATM regulates type I interferon signaling in pancreatic cancer. SF2: ATM regulation of the type I interferon pathway is cGAS/STING independent but SRC dependent. SF3: ATM inhibition cooperates with radiation to activate type I interferon signaling. SF4: ATM regulates pancreatic tumor immunity and ICB efficacy in vivo.

Published
2023

21. Supplementary Data from Coaltered Ras/B-raf and TP53 Is Associated with Extremes of Survivorship and Distinct Patterns of Metastasis in Patients with Metastatic Colorectal Cancer

Author

Michael I. D'Angelica, Nikolaus Schultz, David B. Solit, Rona Yaeger, Agnes Viale, Barry S. Taylor, Julio Garcia-Aguilar, Andrea Cercek, Nancy E. Kemeny, T. Peter Kingham, Vinod Balachandran, William R. Jarnagin, Michael F. Berger, Leonard B. Saltz, Martin R. Weiser, Philip B. Paty, Garrett M. Nash, Jose Guillem, Marla Lipsyc-Sharf, Isaac Wasserman, Karuna Ganesh, Timothy L. Frankel, Efsevia Vakiani, Cyriac Kandoth, John C. McAuliffe, Walid K. Chatila, J. Joshua Smith, and Jashodeep Datta

Abstract

Supplementary Methods, References, and Figures

Published
2023

22. Supplementary Table S1 from Coaltered Ras/B-raf and TP53 Is Associated with Extremes of Survivorship and Distinct Patterns of Metastasis in Patients with Metastatic Colorectal Cancer

Author

Michael I. D'Angelica, Nikolaus Schultz, David B. Solit, Rona Yaeger, Agnes Viale, Barry S. Taylor, Julio Garcia-Aguilar, Andrea Cercek, Nancy E. Kemeny, T. Peter Kingham, Vinod Balachandran, William R. Jarnagin, Michael F. Berger, Leonard B. Saltz, Martin R. Weiser, Philip B. Paty, Garrett M. Nash, Jose Guillem, Marla Lipsyc-Sharf, Isaac Wasserman, Karuna Ganesh, Timothy L. Frankel, Efsevia Vakiani, Cyriac Kandoth, John C. McAuliffe, Walid K. Chatila, J. Joshua Smith, and Jashodeep Datta

Abstract

Genomic and clinical information of MSKCC validation cohort (n=935) with corresponding data dictionary

Published
2023

23. Data from Inhibition of ATM Increases Interferon Signaling and Sensitizes Pancreatic Cancer to Immune Checkpoint Blockade Therapy

Author

Meredith A. Morgan, Weiping Zou, Theodore S. Lawrence, Yu L. Lei, Ilona Kryczek, Timothy L. Frankel, Marina Pasca di Magliano, Daniel R. Wahl, Nithya Ramnath, Jiaqi Shi, Leslie A. Parsels, Shuang Wei, Joshua D. Parsels, Jenny Lazarus, Xueting Lang, Michael D. Green, and Qiang Zhang

Abstract

Combinatorial strategies are needed to overcome the resistance of pancreatic cancer to immune checkpoint blockade (ICB). DNA damage activates the innate immune response and improves ICB efficacy. Because ATM is an apical kinase in the radiation-induced DNA damage response, we investigated the effects of ATM inhibition and radiation on pancreatic tumor immunogenicity. ATM was inhibited through pharmacologic and genetic strategies in human and murine pancreatic cancer models both in vitro and in vivo. Tumor immunogenicity was evaluated after ATM inhibition alone and in combination with radiation by assessing TBK1 and Type I interferon (T1IFN) signaling as well as tumor growth following PD-L1/PD-1 checkpoint inhibition. Inhibition of ATM increased tumoral T1IFN expression in a cGAS/STING-independent, but TBK1- and SRC-dependent, manner. The combination of ATM inhibition with radiation further enhanced TBK1 activity, T1IFN production, and antigen presentation. Furthermore, ATM silencing increased PD-L1 expression and increased the sensitivity of pancreatic tumors to PD-L1–blocking antibody in association with increased tumoral CD8+ T cells and established immune memory. In patient pancreatic tumors, low ATM expression inversely correlated with PD-L1 expression. Taken together, these results demonstrate that the efficacy of ICB in pancreatic cancer is enhanced by ATM inhibition and further potentiated by radiation as a function of increased tumoral immunogenicity, underscoring the potential of ATM inhibition in combination with ICB and radiation as an efficacious treatment strategy for pancreatic cancer.Significance:This study demonstrates that ATM inhibition induces a T1IFN-mediated innate immune response in pancreatic cancer that is further enhanced by radiation and leads to increased sensitivity to anti–PD-L1 therapy.See related commentary by Gutiontov and Weichselbaum, p. 3815

Published
2023

24. Supplementary Data from Inhibition of Hedgehog Signaling Alters Fibroblast Composition in Pancreatic Cancer

Author

Marina Pasca di Magliano, Benjamin L. Allen, David A. Tuveson, Jonathan B. Preall, Andrzej A. Dlugosz, Filip Bednar, Arvind Rao, Timothy L. Frankel, Costas A. Lyssiotis, Howard C. Crawford, Youngkyu Park, Michelle A. Anderson, Fatima Lima, Craig Johnson, Zeribe C. Nwosu, Eileen S. Carpenter, Kristee Brown, Megan T. Hoffman, Nicole E. Franks, Christopher J. Halbrook, Valerie Irizarry-Negron, Stephanie The, Ahmed Abbas, Carlos Espinoza, Christa Hansma, Abhishek Doshi, Ela Elyada, Erin Brosnan, Tobiloba E. Oni, Yuan Hao, LiJyun Syu, Donovan Drouillard, Yaqing Zhang, Samantha B. Kemp, Giulia Biffi, and Nina G. Steele

Abstract

Supp Figure legends

Published
2023

25. Supplementary Figure Legends from Inhibition of ATM Increases Interferon Signaling and Sensitizes Pancreatic Cancer to Immune Checkpoint Blockade Therapy

Author

Meredith A. Morgan, Weiping Zou, Theodore S. Lawrence, Yu L. Lei, Ilona Kryczek, Timothy L. Frankel, Marina Pasca di Magliano, Daniel R. Wahl, Nithya Ramnath, Jiaqi Shi, Leslie A. Parsels, Shuang Wei, Joshua D. Parsels, Jenny Lazarus, Xueting Lang, Michael D. Green, and Qiang Zhang

Abstract

SF1 Legend: ATM regulates type I interferon signaling in pancreatic cancer. SF2 Legend: ATM regulation of the type I interferon pathway is cGAS/STING independent but SRC dependent. SF3 Legend: ATM inhibition cooperates with radiation to activate type I interferon signaling. SF4 Legend: ATM regulates pancreatic tumor immunity and ICB efficacy in vivo.

Published
2023

26. Data from Coaltered Ras/B-raf and TP53 Is Associated with Extremes of Survivorship and Distinct Patterns of Metastasis in Patients with Metastatic Colorectal Cancer

Author

Michael I. D'Angelica, Nikolaus Schultz, David B. Solit, Rona Yaeger, Agnes Viale, Barry S. Taylor, Julio Garcia-Aguilar, Andrea Cercek, Nancy E. Kemeny, T. Peter Kingham, Vinod Balachandran, William R. Jarnagin, Michael F. Berger, Leonard B. Saltz, Martin R. Weiser, Philip B. Paty, Garrett M. Nash, Jose Guillem, Marla Lipsyc-Sharf, Isaac Wasserman, Karuna Ganesh, Timothy L. Frankel, Efsevia Vakiani, Cyriac Kandoth, John C. McAuliffe, Walid K. Chatila, J. Joshua Smith, and Jashodeep Datta

Abstract

Purpose:We aimed to investigate genomic correlates underlying extremes of survivorship in metastatic colorectal cancer and their applicability in informing survival in distinct subsets of patients with metastatic colorectal cancer.Experimental Design:We examined differences in oncogenic somatic alterations between metastatic colorectal cancer cohorts demonstrating extremes of survivorship following complete metastasectomy: ≤2-year (n = 17) and ≥10-year (n = 18) survivors. Relevant genomic findings, and their association with overall survival (OS), were validated in two independent datasets of 935 stage IV and 443 resected stage I–IV patients.Results:In the extremes-of-survivorship cohort, significant co-occurrence of KRAS hotspot mutations and TP53 alterations was observed in ≤2-year survivors (P < 0.001). When validating these findings in the independent cohort of 935 stage IV patients, incorporation of the cumulative effect of any oncogenic Ras/B-raf (i.e., either KRAS, NRAS, or BRAF) and TP53 alteration generated three prognostic clusters: (i) TP53-altered alone (median OS, 132 months); (ii) Ras/B-raf–altered alone (65 months) or Ras/B-raf- and TP53 pan-wild-type (60 months); and (iii) coaltered Ras/B-raf–TP53 (40 months; P < 0.0001). Coaltered Ras/B-raf–TP53 was independently associated with mortality (HR, 2.47; 95% confidence interval, 1.91–3.21; P < 0.001). This molecular profile predicted survival in the second independent cohort of 443 resected stage I–IV patients. Coaltered Ras/B-raf–TP53 was associated with worse OS in patients with liver (n = 490) and lung (n = 172) but not peritoneal surface (n = 149) metastases. Moreover, coaltered Ras/B-raf–TP53 tumors were significantly more likely to involve extrahepatic metastatic sites with limited salvage options.Conclusions:Genomic analysis of extremes of survivorship following colorectal cancer metastasectomy identifies a prognostic role for coaltered Ras/B-raf–TP53 and its association with distinct patterns of colorectal cancer metastasis.

Published
2023

27. Data from Inhibition of Hedgehog Signaling Alters Fibroblast Composition in Pancreatic Cancer

Author

Marina Pasca di Magliano, Benjamin L. Allen, David A. Tuveson, Jonathan B. Preall, Andrzej A. Dlugosz, Filip Bednar, Arvind Rao, Timothy L. Frankel, Costas A. Lyssiotis, Howard C. Crawford, Youngkyu Park, Michelle A. Anderson, Fatima Lima, Craig Johnson, Zeribe C. Nwosu, Eileen S. Carpenter, Kristee Brown, Megan T. Hoffman, Nicole E. Franks, Christopher J. Halbrook, Valerie Irizarry-Negron, Stephanie The, Ahmed Abbas, Carlos Espinoza, Christa Hansma, Abhishek Doshi, Ela Elyada, Erin Brosnan, Tobiloba E. Oni, Yuan Hao, LiJyun Syu, Donovan Drouillard, Yaqing Zhang, Samantha B. Kemp, Giulia Biffi, and Nina G. Steele

Abstract

Purpose:Pancreatic ductal adenocarcinoma (PDAC) is a deadly disease characterized by an extensive fibroinflammatory stroma, which includes abundant cancer-associated fibroblast (CAF) populations. PDAC CAFs are heterogeneous, but the nature of this heterogeneity is incompletely understood. The Hedgehog pathway functions in PDAC in a paracrine manner, with ligands secreted by cancer cells signaling to stromal cells in the microenvironment. Previous reports investigating the role of Hedgehog signaling in PDAC have been contradictory, with Hedgehog signaling alternately proposed to promote or restrict tumor growth. In light of the newly discovered CAF heterogeneity, we investigated how Hedgehog pathway inhibition reprograms the PDAC microenvironment.Experimental Design:We used a combination of pharmacologic inhibition, gain- and loss-of-function genetic experiments, cytometry by time-of-flight, and single-cell RNA sequencing to study the roles of Hedgehog signaling in PDAC.Results:We found that Hedgehog signaling is uniquely activated in fibroblasts and differentially elevated in myofibroblastic CAFs (myCAF) compared with inflammatory CAFs (iCAF). Sonic Hedgehog overexpression promotes tumor growth, while Hedgehog pathway inhibition with the smoothened antagonist, LDE225, impairs tumor growth. Furthermore, Hedgehog pathway inhibition reduces myCAF numbers and increases iCAF numbers, which correlates with a decrease in cytotoxic T cells and an expansion in regulatory T cells, consistent with increased immunosuppression.Conclusions:Hedgehog pathway inhibition alters fibroblast composition and immune infiltration in the pancreatic cancer microenvironment.

Published
2023

28. Supplementary Figure 1 from A High Molecular Weight Melanoma-Associated Antigen–Specific Chimeric Antigen Receptor Redirects Lymphocytes to Target Human Melanomas

Author

Richard A. Morgan, Steven A. Rosenberg, Soldano Ferrone, Steven A. Feldman, Hui Xu, Zhili Zheng, Christian S. Hinrichs, Timothy L. Frankel, Yangbing Zhao, and William R. Burns

Abstract

Supplementary Figure 1 from A High Molecular Weight Melanoma-Associated Antigen–Specific Chimeric Antigen Receptor Redirects Lymphocytes to Target Human Melanomas

Published
2023

29. Supplementary Figure 3 from A High Molecular Weight Melanoma-Associated Antigen–Specific Chimeric Antigen Receptor Redirects Lymphocytes to Target Human Melanomas

Author

Richard A. Morgan, Steven A. Rosenberg, Soldano Ferrone, Steven A. Feldman, Hui Xu, Zhili Zheng, Christian S. Hinrichs, Timothy L. Frankel, Yangbing Zhao, and William R. Burns

Abstract

Supplementary Figure 3 from A High Molecular Weight Melanoma-Associated Antigen–Specific Chimeric Antigen Receptor Redirects Lymphocytes to Target Human Melanomas

Published
2023

30. Supplementary Figure 5 from A High Molecular Weight Melanoma-Associated Antigen–Specific Chimeric Antigen Receptor Redirects Lymphocytes to Target Human Melanomas

Author

Richard A. Morgan, Steven A. Rosenberg, Soldano Ferrone, Steven A. Feldman, Hui Xu, Zhili Zheng, Christian S. Hinrichs, Timothy L. Frankel, Yangbing Zhao, and William R. Burns

Abstract

Supplementary Figure 5 from A High Molecular Weight Melanoma-Associated Antigen–Specific Chimeric Antigen Receptor Redirects Lymphocytes to Target Human Melanomas

Published
2023

31. Supplementary Figure 4 from A High Molecular Weight Melanoma-Associated Antigen–Specific Chimeric Antigen Receptor Redirects Lymphocytes to Target Human Melanomas

Author

Richard A. Morgan, Steven A. Rosenberg, Soldano Ferrone, Steven A. Feldman, Hui Xu, Zhili Zheng, Christian S. Hinrichs, Timothy L. Frankel, Yangbing Zhao, and William R. Burns

Abstract

Supplementary Figure 4 from A High Molecular Weight Melanoma-Associated Antigen–Specific Chimeric Antigen Receptor Redirects Lymphocytes to Target Human Melanomas

Published
2023

32. Supplementary Figure 6 from A High Molecular Weight Melanoma-Associated Antigen–Specific Chimeric Antigen Receptor Redirects Lymphocytes to Target Human Melanomas

Author

Richard A. Morgan, Steven A. Rosenberg, Soldano Ferrone, Steven A. Feldman, Hui Xu, Zhili Zheng, Christian S. Hinrichs, Timothy L. Frankel, Yangbing Zhao, and William R. Burns

Abstract

Supplementary Figure 6 from A High Molecular Weight Melanoma-Associated Antigen–Specific Chimeric Antigen Receptor Redirects Lymphocytes to Target Human Melanomas

Published
2023

33. Analysis of donor pancreata defines the transcriptomic signature and microenvironment of early pre-neoplastic pancreatic lesions

Author

Eileen S. Carpenter, Ahmed M. Elhossiny, Padma Kadiyala, Jay Li, Jake McGue, Brian Griffith, Yaqing Zhang, Jacob Edwards, Sarah Nelson, Fatima Lima, Katelyn L. Donahue, Wenting Du, Allison C. Bischoff, Danyah Alomari, Hannah Watkoske, Michael Mattea, Stephanie The, Carlos Espinoza, Meredith Barrett, Christopher J. Sonnenday, Nicholas Olden, Nicole Peterson, Valerie Gunchick, Vaibhav Sahai, Arvind Rao, Filip Bednar, Jiaqi Shi, Timothy L. Frankel, and Marina Pasca Di Magliano

Abstract

The adult healthy human pancreas has been poorly studied given lack of indication to obtain tissue from the pancreas in the absence of disease and rapid postmortem degradation. We obtained pancreata from brain dead donors thus avoiding any warm ischemia time. The 30 donors were diverse in age and race and had no known pancreas disease. Histopathological analysis of the samples revealed PanIN lesions in most individuals irrespective of age. Using a combination of multiplex immunohistochemistry, single cell RNA sequencing, and spatial transcriptomics, we provide the first ever characterization of the unique microenvironment of the adult human pancreas and of sporadic PanIN lesions. We compared healthy pancreata to pancreatic cancer and peritumoral tissue and observed distinct transcriptomic signatures in fibroblasts, and, to a lesser extent, macrophages. PanIN epithelial cells from healthy pancreata were remarkably transcriptionally similar to cancer cells, suggesting that neoplastic pathways are initiated early in tumorigenesis.Statement of significanceThe causes underlying the onset of pancreatic cancer remain largely unknown, hampering early detection and prevention strategies. Here, we show that PanIN are abundant in healthy individuals and present at a much higher rate than the incidence of pancreatic cancer, setting the stage for efforts to elucidate the microenvironmental and cell intrinsic factors that restrain, or, conversely, promote, malignant progression.

Published
2023

35. Microenvironmental ammonia enhances T cell exhaustion in colorectal cancer

Author

Hannah N. Bell, Amanda K. Huber, Rashi Singhal, Navyateja Korimerla, Ryan J. Rebernick, Roshan Kumar, Marwa O. El-derany, Peter Sajjakulnukit, Nupur K. Das, Samuel A. Kerk, Sumeet Solanki, Jadyn G. James, Donghwan Kim, Li Zhang, Brandon Chen, Rohit Mehra, Timothy L. Frankel, Balázs Győrffy, Eric R. Fearon, Marina Pasca di Magliano, Frank J. Gonzalez, Ruma Banerjee, Daniel R. Wahl, Costas A. Lyssiotis, Michael Green, and Yatrik M. Shah

Subjects
Physiology, Cell Biology, Molecular Biology
Abstract

Effective therapies are lacking for patients with advanced colorectal cancer (CRC). The CRC tumor microenvironment has elevated metabolic waste products due to altered metabolism and proximity to the microbiota. The role of metabolite waste in tumor development, progression, and treatment resistance is unclear. We generated an autochthonous metastatic mouse model of CRC and used unbiased multi-omic analyses to reveal a robust accumulation of tumoral ammonia. The high ammonia levels induce T cell metabolic reprogramming, increase exhaustion, and decrease proliferation. CRC patients have increased serum ammonia, and the ammonia-related gene signature correlates with altered T cell response, adverse patient outcomes, and lack of response to immune checkpoint blockade. We demonstrate that enhancing ammonia clearance reactivates T cells, decreases tumor growth, and extends survival. Moreover, decreasing tumor-associated ammonia enhances anti-PD-L1 efficacy. These findings indicate that enhancing ammonia detoxification can reactivate T cells, highlighting a new approach to enhance the efficacy of immunotherapies.

Published
2022

36. CSCD

Author

Yan Li, Majid Farhadloo, Santhoshi Krishnan, Yiqun Xie, Timothy L Frankel, Shashi Shekhar, and Arvind Rao

Published
2022

38. IFNγ signaling integrity in colorectal cancer immunity and immunotherapy

Author

Michael D. Green, Timothy L. Frankel, Weiping Zou, and Wan Du

Subjects
IFNGR, PD-L1, Colorectal cancer, medicine.medical_treatment, T cell, Immunology, Apoptosis, Review Article, Interferon-gamma, Immunity, PD-1, Tumor Microenvironment, Humans, Ferroptosis, Immunology and Allergy, Medicine, Interferon gamma, EZH2, biology, business.industry, Immunotherapy, medicine.disease, ARID1A, Immune checkpoint, Protein Transport, Infectious Diseases, medicine.anatomical_structure, Oncology, Cancer research, biology.protein, Interferon, MHC, Signal transduction, Colorectal Neoplasms, business, Palmitoylation, Immunosuppression, Signal Transduction, medicine.drug
Abstract

The majority of colorectal cancer patients are not responsive to immune checkpoint blockade (ICB). The interferon gamma (IFNγ) signaling pathway drives spontaneous and ICB-induced antitumor immunity. In this review, we summarize recent advances in the epigenetic, genetic, and functional integrity of the IFNγ signaling pathway in the colorectal cancer microenvironment and its immunological relevance in the therapeutic efficacy of and resistance to ICB. Moreover, we discuss how to target IFNγ signaling to inform novel clinical trials to treat patients with colorectal cancer.

Published
2021

40. MHC Class II Expression Influences the Composition and Distribution of Immune Cells in the Metastatic Colorectal Cancer Microenvironment

Author

Brian D. Griffith, Simon Turcotte, Jenny Lazarus, Fatima Lima, Samantha Bell, Lawrence Delrosario, Jake McGue, Santhoshi Krishnan, Morgan D. Oneka, Hari Nathan, J. Joshua Smith, Michael I. D’Angelica, Jinru Shia, Marina Pasca Di Magliano, Arvind Rao, and Timothy L. Frankel

Subjects
Cancer Research, Oncology, colon cancer, multiplex immunohistochemistry, immuno-oncology
Abstract

Despite advances in therapy over the past decades, metastatic colorectal cancer (mCRC) remains a highly morbid disease. While the impact of MHC-I on immune infiltration in mCRC has been well studied, data on the consequences of MHC-II loss are lacking. Multiplex fluorescent immunohistochemistry (mfIHC) was performed on 149 patients undergoing curative intent resection for mCRC and stratified into high and low human leukocyte antigen isotype DR (HLA-DR) expressing tumors. Intratumoral HLA-DR expression was found in stromal bands, and its expression level was associated with different infiltrating immune cell makeup and distribution. Low HLA-DR expression was associated with increased intercellular distances and decreased population mixing of T helper cells and antigen-presenting cells (APC), suggestive of decreased interactions. This was associated with less co-localization of tumor cells and cytotoxic T lymphocytes (CTLs), which tended to be in a less activated state as determined by Ki67 and granzyme B expression. These findings suggest that low HLA-DR in the tumor microenvironment of mCRC may reflect a state of poor helper T-cell interactions with APCs and CTL-mediated anti-tumor activity. Efforts to restore/enhance MHC-II presentation may be a useful strategy to enhance checkpoint inhibition therapy in the future.

Published
2022
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41. Immunotherapy for pancreatic ductal adenocarcinoma

Author

Clifford S. Cho, Filip Bednar, Marina Pasca di Magliano, Eileen S. Carpenter, Timothy L. Frankel, Vaibhav Sahai, Sarah Nelson, and Hari Nathan

Subjects
Agonist, Pancreatic ductal adenocarcinoma, endocrine system diseases, medicine.drug_class, medicine.medical_treatment, Cancer Vaccines, 03 medical and health sciences, Clinical Trials, Phase II as Topic, 0302 clinical medicine, Immune system, Pancreatic cancer, medicine, Animals, Humans, Immune Checkpoint Inhibitors, Randomized Controlled Trials as Topic, Clinical Trials, Phase I as Topic, business.industry, Cancer, General Medicine, Immunotherapy, medicine.disease, digestive system diseases, Vaccine therapy, Blockade, Pancreatic Neoplasms, Oncology, 030220 oncology & carcinogenesis, Cancer research, 030211 gastroenterology & hepatology, Surgery, business, Carcinoma, Pancreatic Ductal
Abstract

Pancreatic ductal adenocarcinoma (PDAC) remains a lethal cancer with an urgent need for better medical therapies. Efforts have been made to investigate the efficacy of immunotherapy, particularly given the hallmarks of immune suppression and exhaustion in PDAC tumors. Here, we review the molecular components responsible for the immune-privileged state in PDAC and provide an overview of the immunotherapeutic strategies for PDAC including vaccine therapy, checkpoint blockade, myeloid-targeted therapy, and immune agonist therapy.

Published
2021

42. Multimodal mapping of the tumor and peripheral blood immune landscape in human pancreatic cancer

Author

Nina G. Steele, Eileen S. Carpenter, Samantha B. Kemp, Veerin R. Sirihorachai, Stephanie The, Lawrence Delrosario, Jenny Lazarus, El-ad David Amir, Valerie Gunchick, Carlos Espinoza, Samantha Bell, Lindsey Harris, Fatima Lima, Valerie Irizarry-Negron, Daniel Paglia, Justin Macchia, Angel Ka Yan Chu, Heather Schofield, Erik-Jan Wamsteker, Richard Kwon, Allison Schulman, Anoop Prabhu, Ryan Law, Arjun Sondhi, Jessica Yu, Arpan Patel, Katelyn Donahue, Hari Nathan, Clifford Cho, Michelle A. Anderson, Vaibhav Sahai, Costas A. Lyssiotis, Weiping Zou, Benjamin L. Allen, Arvind Rao, Howard C. Crawford, Filip Bednar, Timothy L. Frankel, and Marina Pasca di Magliano

Subjects
Cancer Research, Tumor microenvironment, medicine.medical_treatment, Receptor expression, Cancer, Immunotherapy, CD8-Positive T-Lymphocytes, biochemical phenomena, metabolism, and nutrition, Biology, medicine.disease, Article, Immune checkpoint, Pancreatic Neoplasms, Immune system, Oncology, TIGIT, Pancreatic cancer, Tumor Microenvironment, medicine, Cancer research, Humans, bacteria
Abstract

Pancreatic ductal adenocarcinoma (PDA) is characterized by an immune-suppressive tumor microenvironment that renders it largely refractory to immunotherapy. We implemented a multimodal analysis approach to elucidate the immune landscape in PDA. Using a combination of CyTOF, single-cell RNA sequencing and multiplex immunohistochemistry on patient tumors, matched blood and non-malignant samples, we uncovered a complex network of immune-suppressive cellular interactions. These experiments revealed heterogeneous expression of immune checkpoint receptors in individual patients’ T cells and increased markers of CD8+ T cell dysfunction in the advanced disease stage. Tumor-infiltrating CD8+ T cells had an increased proportion of cells expressing an exhausted expression profile that included upregulation of the immune checkpoint TIGIT, a finding that we validated at the protein level. Our findings point to a profound alteration of the immune landscape of tumors, and to patient-specific immune changes that should be taken into account as combination immunotherapy becomes available for pancreatic cancer. Using single-cell RNA sequencing, CyTOF and multiplex immunohistochemistry, Steele et al. survey the immune landscape in pancreatic cancers, adjacent tissue and blood, observing heterogeneous immune checkpoint receptor expression within patients.

Published
2020

43. A Pilot Study of Atezolizumab Plus Hypofractionated Image Guided Radiation Therapy for the Treatment of Advanced Non-Small Cell Lung Cancer

Author

Shruti Jolly, Dafydd G. Thomas, Andrea M. H. Towlerton, James A. Hayman, Khaled A. Hassan, Renato G. Martins, Muneesh Tewari, Christina S. Baik, Lili Zhao, Sylvia Lee, Theodore S. Lawrence, Nithya Ramnath, Timothy L. Frankel, Jason W.D. Hearn, Angel Qin, Bernardo H. L. Goulart, Rafael Santana-Davila, Gregory P. Kalemkerian, Ramesh Rengan, Edus H. Warren, Noah A. Brown, and Bryan J. Schneider

Subjects
Adult, Male, Oncology, Cancer Research, medicine.medical_specialty, Lung Neoplasms, Pilot Projects, Antibodies, Monoclonal, Humanized, B7-H1 Antigen, 030218 nuclear medicine & medical imaging, 03 medical and health sciences, 0302 clinical medicine, Atezolizumab, Carcinoma, Non-Small-Cell Lung, Internal medicine, Humans, Medicine, Radiology, Nuclear Medicine and imaging, Prospective cohort study, Lung cancer, Adverse effect, Prior Radiation Therapy, Aged, Pneumonitis, Aged, 80 and over, Radiation, business.industry, Middle Aged, medicine.disease, Combined Modality Therapy, Gene Expression Regulation, Neoplastic, Clinical trial, Regimen, Treatment Outcome, 030220 oncology & carcinogenesis, Female, Radiation Dose Hypofractionation, Safety, business, Radiotherapy, Image-Guided
Abstract

Purpose Preclinical data and subset analyses from immunotherapy clinical trials indicate that prior radiation therapy was associated with better progression-free survival and overall survival when combined with immune checkpoint inhibitors in patients with non-small cell lung cancer. We present a prospective study of hypofractionated image guided radiation therapy (HIGRT) to a single site of metastatic disease concurrently with atezolizumab in patients with metastatic non-small cell lung cancer. Methods and Materials Patients meeting eligibility criteria received 1200 mg of atezolizumab intravenously every 3 weeks with concurrent 3- or 5-fraction HIGRT starting no later than the second cycle. The 3-fraction regimen employed a minimum of 8 Gy per fraction compared with 6 Gy for the 5-fraction regimen. Imaging was obtained every 12 weeks to assess response. Results From October 2015 to February 2017, 12 patients were enrolled in the study (median age 64; range, 55-77 years). The best response by the Response Evaluation in Solid Tumors criteria was partial response in 3 and stable disease in 3, for a disease control rate of 50%. Five patients had a grade 3 immune-related adverse event, including choreoretinitis (n = 1), pneumonitis (n = 1), transaminitis (n = 1), fatigue (n = 1), and peripheral neuropathy (n = 1). The median progression-free survival was 2.3 months, and the median overall survival was 6.9 months (range, 0.4-not reached). There was no clear association between peripheral blood T cell repertoire characteristics at baseline, PD-L1, or tumor mutations and response or outcome. One long-term survivor exhibited oligoclonal T cell populations in a baseline tumor biopsy that were consistently detected in peripheral blood over the entire course of the study. Conclusions HIGRT plus atezolizumab resulted in an overall response rate of 25% and disease control rate of 50% in this pilot study. The incidence of grade 3 adverse events was similar to that of atezolizumab alone. Alhough it was a pilot study with limited sample size, the results generated hypotheses worthy of further investigation.

Published
2020

44. Regulatory T-cell Depletion Alters the Tumor Microenvironment and Accelerates Pancreatic Carcinogenesis

Author

Veerin Sirihorachai, Wei Yan, Nina Steele, Marina Pasca di Magliano, Ashley Velez-Delgado, Costas A. Lyssiotis, Rosa E. Menjivar, Samantha Kemp, Jenny Lazarus, Yaqing Zhang, Michelle A. Anderson, Filip Bednar, Anna C. Nevison, Timothy L. Frankel, Alekya Vinta, Kristee Brown, Katelyn Donahue, Howard C. Crawford, Eileen S. Carpenter, Valerie Irizarry-Negron, Ho-Joon Lee, Christopher J. Halbrook, and Zeribe C. Nwosu

Subjects
0301 basic medicine, Myeloid, Carcinogenesis, T-Lymphocytes, medicine.disease_cause, T-Lymphocytes, Regulatory, Mice, 0302 clinical medicine, Transforming Growth Factor beta, Receptors, Tumor Microenvironment, Chemokine CCL8, 2.1 Biological and endogenous factors, Aetiology, Chemokine CCL3, Cancer, education.field_of_study, hemic and immune systems, Forkhead Transcription Factors, CC, Regulatory, medicine.anatomical_structure, Oncology, Chemokines, CC, 030220 oncology & carcinogenesis, Chemokines, Regulatory T cell, Oncology and Carcinogenesis, Population, Receptors, CCR1, Biology, Article, CCL6, Pancreatic Cancer, 03 medical and health sciences, Rare Diseases, Clinical Research, Pancreatic cancer, medicine, Animals, Humans, education, Pancreas, Tumor microenvironment, Animal, Fibroblasts, medicine.disease, Pancreatic Neoplasms, Disease Models, Animal, 030104 developmental biology, Tumor progression, Disease Models, Cancer research, CCR1, Digestive Diseases
Abstract

Regulatory T cells (Treg) are abundant in human and mouse pancreatic cancer. To understand the contribution to the immunosuppressive microenvironment, we depleted Tregs in a mouse model of pancreatic cancer. Contrary to our expectations, Treg depletion failed to relieve immunosuppression and led to accelerated tumor progression. We show that Tregs are a key source of TGFβ ligands and, accordingly, their depletion reprogramed the fibroblast population, with loss of tumor-restraining, smooth muscle actin–expressing fibroblasts. Conversely, we observed an increase in chemokines Ccl3, Ccl6, and Ccl8 leading to increased myeloid cell recruitment, restoration of immune suppression, and promotion of carcinogenesis, an effect that was inhibited by blockade of the common CCL3/6/8 receptor CCR1. Further, Treg depletion unleashed pathologic CD4+ T-cell responses. Our data point to new mechanisms regulating fibroblast differentiation in pancreatic cancer and support the notion that fibroblasts are a heterogeneous population with different and opposing functions in pancreatic carcinogenesis. Significance: Here, we describe an unexpected cross-talk between Tregs and fibroblasts in pancreatic cancer. Treg depletion resulted in differentiation of inflammatory fibroblast subsets, in turn driving infiltration of myeloid cells through CCR1, thus uncovering a potentially new therapeutic approach to relieve immunosuppression in pancreatic cancer. See related commentary by Aykut et al., p. 345. This article is highlighted in the In This Issue feature, p. 327

Published
2020

45. Coaltered Ras/B-raf and TP53 Is Associated with Extremes of Survivorship and Distinct Patterns of Metastasis in Patients with Metastatic Colorectal Cancer

Author

Michael F. Berger, Andrea Cercek, Nikolaus Schultz, Martin R. Weiser, William R. Jarnagin, Walid K. Chatila, Isaac Wasserman, Michael I. D’Angelica, Leonard B. Saltz, Jose G. Guillem, Julio Garcia-Aguilar, Efsevia Vakiani, Agnes Viale, Nancy E. Kemeny, T. Peter Kingham, John C. McAuliffe, David B. Solit, Garrett M. Nash, Jashodeep Datta, Cyriac Kandoth, Philip B. Paty, Karuna Ganesh, Barry S. Taylor, J. Joshua Smith, Vinod P. Balachandran, Rona Yaeger, Marla Lipsyc-Sharf, and Timothy L. Frankel

Subjects
0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Colorectal cancer, business.industry, medicine.disease, medicine.disease_cause, Metastasis, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Internal medicine, Survivorship curve, Cohort, medicine, Complete Metastasectomy, KRAS, Metastasectomy, business, Survival rate
Abstract

Purpose: We aimed to investigate genomic correlates underlying extremes of survivorship in metastatic colorectal cancer and their applicability in informing survival in distinct subsets of patients with metastatic colorectal cancer. Experimental Design: We examined differences in oncogenic somatic alterations between metastatic colorectal cancer cohorts demonstrating extremes of survivorship following complete metastasectomy: ≤2-year (n = 17) and ≥10-year (n = 18) survivors. Relevant genomic findings, and their association with overall survival (OS), were validated in two independent datasets of 935 stage IV and 443 resected stage I–IV patients. Results: In the extremes-of-survivorship cohort, significant co-occurrence of KRAS hotspot mutations and TP53 alterations was observed in ≤2-year survivors (P < 0.001). When validating these findings in the independent cohort of 935 stage IV patients, incorporation of the cumulative effect of any oncogenic Ras/B-raf (i.e., either KRAS, NRAS, or BRAF) and TP53 alteration generated three prognostic clusters: (i) TP53-altered alone (median OS, 132 months); (ii) Ras/B-raf–altered alone (65 months) or Ras/B-raf- and TP53 pan-wild-type (60 months); and (iii) coaltered Ras/B-raf–TP53 (40 months; P < 0.0001). Coaltered Ras/B-raf–TP53 was independently associated with mortality (HR, 2.47; 95% confidence interval, 1.91–3.21; P < 0.001). This molecular profile predicted survival in the second independent cohort of 443 resected stage I–IV patients. Coaltered Ras/B-raf–TP53 was associated with worse OS in patients with liver (n = 490) and lung (n = 172) but not peritoneal surface (n = 149) metastases. Moreover, coaltered Ras/B-raf–TP53 tumors were significantly more likely to involve extrahepatic metastatic sites with limited salvage options. Conclusions: Genomic analysis of extremes of survivorship following colorectal cancer metastasectomy identifies a prognostic role for coaltered Ras/B-raf–TP53 and its association with distinct patterns of colorectal cancer metastasis.

Published
2020

47. Intersection of immune and oncometabolic pathways drives cancer hyperprogression during immunotherapy

Author

Gaopeng Li, Jae Eun Choi, Ilona Kryczek, Yilun Sun, Peng Liao, Shasha Li, Shuang Wei, Sara Grove, Linda Vatan, Reagan Nelson, Grace Schaefer, Steven G. Allen, Kamya Sankar, Leslie A. Fecher, Mishal Mendiratta-Lala, Timothy L. Frankel, Angel Qin, Jessica J. Waninger, Alangoya Tezel, Ajjai Alva, Christopher D. Lao, Nithya Ramnath, Marcin Cieslik, Paul W. Harms, Michael D. Green, Arul M. Chinnaiyan, and Weiping Zou

Subjects
Cancer Research, Oncology
Published
2023

48. Towards the characterization of the tumor microenvironment through dictionary learning-based interpretable classification of multiplexed immunofluorescence images

Author

Santhoshi N Krishnan, Souptik Barua, Timothy L Frankel, and Arvind Rao

Subjects
Radiological and Ultrasound Technology, Radiology, Nuclear Medicine and imaging
Abstract

Objective. Histology image analysis is a crucial diagnostic step in staging and treatment planning, especially for cancerous lesions. With the increasing adoption of computational methods for image analysis, significant strides are being made to improve the performance metrics of image segmentation and classification frameworks. However, many developed frameworks effectively function as black boxes, granting minimal context to the decision-making process. Thus, there is a need to develop methods that offer reasonable discriminatory power and a biologically-informed intuition to the decision-making process. Approach. In this study, we utilized and modified a discriminative feature-based dictionary learning (DFDL) paradigm to generate a classification framework that allows for discrimination between two distinct clinical histologies. This framework allows us (i) to discriminate between 2 clinically distinct diseases or histologies and (ii) provides interpretable group-specific representative dictionary image patches, or ‘atoms’, generated during classifier training. This implementation is performed on multiplexed immunofluorescence images from two separate patient cohorts- a pancreatic cohort consisting of cancerous and non-cancerous tissues and a metastatic non-small cell lung cancer (mNSCLC) cohort of responders and non-responders to an immunotherapeutic treatment regimen. The analysis was done at both the image-level and subject-level. Five cell types were selected, namely, epithelial cells, cytotoxic lymphocytes, antigen presenting cells, HelperT cells, and T-regulatory cells, as our phenotypes of interest. Results. We showed that DFDL had significant discriminant capabilities for both the pancreatic pathologies cohort (subject-level AUC-0.8878) and the mNSCLC immunotherapy response cohort (subject-level AUC-0.7221). The secondary analysis also showed that more than 50% of the obtained dictionary atoms from the classifier contained biologically relevant information. Significance. Our method shows that the generated dictionary features can help distinguish patients presenting two different histologies with strong sensitivity and specificity metrics. These features allow for an additional layer of model interpretability, a highly desirable element in clinical applications for identifying novel biological phenomena.

Published
2022

49. Extrinsic KRAS signaling shapes the pancreatic microenvironment through fibroblast reprogramming

Author

Ashley Velez-Delgado, Katelyn L. Donahue, Kristee L. Brown, Wenting Du, Valerie Irizarry-Negron, Rosa E. Menjivar, Emily L. Lasse Opsahl, Nina G. Steele, Stephanie The, Jenny Lazarus, Veerin R. Sirihorachai, Wei Yan, Samantha B. Kemp, Samuel A. Kerk, Murali Bollampally, Fatima Lima, Costas A. Lyssiotis, Arvind Rao, Howard C. Crawford, Filip Bednar, Timothy L. Frankel, Yaqing Zhang, and Marina Pasca di Magliano

Subjects
Stromal cell, Cell, Biology, medicine.disease, medicine.disease_cause, medicine.anatomical_structure, Pancreatic tumor, Genetically Engineered Mouse, Pancreatic cancer, medicine, Cancer research, KRAS, Carcinogenesis, Reprogramming
Abstract

Oncogenic KRAS is the hallmark mutation of human pancreatic cancer and a driver of tumorigenesis in genetically engineered mouse models of the disease. While the tumor cell-intrinsic effects of oncogenic Kras expression have been widely studied, its role in regulating the extensive pancreatic tumor microenvironment is less understood. Using a genetically engineered mouse model of inducible and reversible oncogenic Kras expression and a combination of approaches that include mass cytometry and single cell RNA sequencing, we have discovered that non-cell autonomous (i.e., extrinsic) oncogenic KRAS signaling reprograms pancreatic fibroblasts, activating an inflammatory gene expression program. As a result, fibroblasts become a hub of extracellular signaling, mediating the polarization and function of pro-tumorigenic myeloid cells while also preventing tissue repair. Our study provides fundamental new knowledge on the mechanisms underlying the formation of the fibroinflammatory stroma in pancreatic cancer and highlights stromal pathways with the potential to be exploited therapeutically.

Published
2021

50. Metabolism and epigenetics of pancreatic cancer stem cells

Author

Costas A. Lyssiotis, Filip Bednar, Timothy L. Frankel, Joyce K. Thompson, M. Perusina Lanfranca, B. Levi, and Christopher J. Halbrook

Subjects
0301 basic medicine, Cancer Research, Epithelial-Mesenchymal Transition, Cell Plasticity, Biology, medicine.disease_cause, Article, Epigenesis, Genetic, 03 medical and health sciences, 0302 clinical medicine, Cancer stem cell, Pancreatic cancer, medicine, Animals, Humans, Epigenetics, Epithelial–mesenchymal transition, medicine.disease, Phenotype, Gene Expression Regulation, Neoplastic, Pancreatic Neoplasms, 030104 developmental biology, 030220 oncology & carcinogenesis, DNA methylation, Neoplastic Stem Cells, Cancer research, Disease Susceptibility, Stem cell, Energy Metabolism, Carcinogenesis, Carcinoma, Pancreatic Ductal
Abstract

Pancreatic Cancer (PDA) is an aggressive malignancy characterized by early spread and a high mortality. Current studies suggest that a subpopulation of cells exist within tumors, cancer stem cell (CSC), which are capable of self-renewal and give rise to unique progeny which form the major neoplastic cellular component of tumors. While CSCs constitute a small cellular subpopulation within the tumor, their resistance to chemotherapy and radiation make them an important therapeutic target for eradication. Along with distinctive phenotypic properties, CSCs possess a unique metabolic plasticity allowing them to rapidly respond and adapt to environmental changes. These cells and their progeny also display a significantly altered epigenetic state with distinctive patterns of DNA methylation. Several mechanisms of cross-talk between epigenetic and metabolic pathways in PDA exist which ultimately contribute to the observed cellular plasticity and enhanced tumorigenesis. In this review we discuss various examples of this metabolic-epigenetic interplay and how it may constitute a new avenue for therapy specifically targeting CSCs in PDA.

Published
2019

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