Your search keyword '"Mahak Singhal"' showing total 30 results

1. Caspase‐8 in endothelial cells maintains gut homeostasis and prevents small bowel inflammation in mice

Author

Nathalie Tisch, Carolin Mogler, Ana Stojanovic, Robert Luck, Emilia A Korhonen, Alexander Ellerkmann, Heike Adler, Mahak Singhal, Géza Schermann, Lena Erkert, Jay V Patankar, Andromachi Karakatsani, Anna‐Lena Scherr, Yaron Fuchs, Adelheid Cerwenka, Stefan Wirtz, Bruno Christian Köhler, Hellmut G Augustin, Christoph Becker, Thomas Schmidt, and Carmen Ruiz de Almodóvar

Subjects

caspase‐8, chronic intestinal inflammation, endothelium, necroptosis, vascular homeostasis, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract The gut has a specific vascular barrier that controls trafficking of antigens and microbiota into the bloodstream. However, the molecular mechanisms regulating the maintenance of this vascular barrier remain elusive. Here, we identified Caspase‐8 as a pro‐survival factor in mature intestinal endothelial cells that is required to actively maintain vascular homeostasis in the small intestine in an organ‐specific manner. In particular, we find that deletion of Caspase‐8 in endothelial cells results in small intestinal hemorrhages and bowel inflammation, while all other organs remained unaffected. We also show that Caspase‐8 seems to be particularly needed in lymphatic endothelial cells to maintain gut homeostasis. Our work demonstrates that endothelial cell dysfunction, leading to the breakdown of the gut‐vascular barrier, is an active driver of chronic small intestinal inflammation, highlighting the role of the intestinal vasculature as a safeguard of organ function.

Published

2022

2. Preclinical validation of a novel metastasis‐inhibiting Tie1 function‐blocking antibody

Author

Mahak Singhal, Nicolas Gengenbacher, Silvia La Porta, Stephanie Gehrs, Jingjing Shi, Miki Kamiyama, Diane M Bodenmiller, Anthony Fischl, Benjamin Schieb, Eva Besemfelder, Sudhakar Chintharlapalli, and Hellmut G Augustin

Subjects

angiogenesis, angiopoietin–Tie signaling, cancer, endothelial cells, metastasis, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract The angiopoietin (Ang)–Tie pathway has been intensely pursued as candidate second‐generation anti‐angiogenic target. While much of the translational work has focused on the ligand Ang2, the clinical efficacy of Ang2‐targeting drugs is limited and failed to improve patient survival. In turn, the orphan receptor Tie1 remains therapeutically unexplored, although its endothelial‐specific genetic deletion has previously been shown to result in a strong reduction in metastatic growth. Here, we report a novel Tie1 function‐blocking antibody (AB‐Tie1‐39), which suppressed postnatal retinal angiogenesis. During primary tumor growth, neoadjuvant administration of AB‐Tie1‐39 strongly impeded systemic metastasis. Furthermore, the administration of AB‐Tie1‐39 in a perioperative therapeutic window led to a significant survival advantage as compared to control‐IgG‐treated mice. Additional in vivo experimental metastasis and in vitro transmigration assays concurrently revealed that AB‐Tie1‐39 treatment suppressed tumor cell extravasation at secondary sites. Taken together, the data phenocopy previous genetic work in endothelial Tie1 KO mice and thereby validate AB‐Tie1‐39 as a Tie1 function‐blocking antibody. The study establishes Tie1 as a therapeutic target for metastasis in a perioperative or neoadjuvant setting.

Published

2020

3. KANK4 Promotes Arteriogenesis by Potentiating VEGFR2 Signaling in a TALIN-1–Dependent Manner

Author

Chonghe Zhang, Hao He, Jianing Dai, Yunxia Li, Jing He, Wu Yang, Jialin Dai, Feng Han, Wenyan Kong, Xiaohong Wang, Xiangjian Zheng, Jing Zhou, Weijun Pan, Zhongwen Chen, Mahak Singhal, Yaoyang Zhang, Feng Guo, and Junhao Hu

Subjects

Mice, Knockout, Talin, Vascular Endothelial Growth Factor A, Collateral Circulation, Endothelial Cells, Neovascularization, Physiologic, Arterial Occlusive Diseases, Hindlimb, Disease Models, Animal, Mice, Ischemia, Regional Blood Flow, Animals, Muscle, Skeletal, Cardiology and Cardiovascular Medicine

Abstract

Background: Arteriogenesis plays a critical role in maintaining adequate tissue blood supply and is related to a favorable prognosis in arterial occlusive diseases. Strategies aimed at promoting arteriogenesis have thus far not been successful because the factors involved in arteriogenesis remain incompletely understood. Previous studies suggest that evolutionarily conserved KANK4 (KN motif and ankyrin repeat domain-containing proteins 4) might involve in vertebrate vessel development. However, how the KANK4 regulates vessel function remains unknown. We aim to determine the role of endothelial cell-specifically expressed KANK4 in arteriogenesis. Methods: The role of KANK4 in regulating arteriogenesis was evaluated using Kank4 −/− and KANK4 iECOE mice. Molecular mechanisms underlying KANK4-potentiated arteriogenesis were investigated by employing RNA transcriptomic profiling and mass spectrometry analysis. Results: By analyzing Kank4-EGFP reporter mice, we showed that KANK4 was specifically expressed in endothelial cells. In particular, KANK4 displayed a dynamic expression pattern from being ubiquitously expressed in all endothelial cells of the developing vasculature to being explicitly expressed in the endothelial cells of arterioles and arteries in matured vessels. In vitro microfluidic chip-based vascular morphology analysis and in vivo hindlimb ischemia assays using Kank4 −/− and KANK4 iECOE mice demonstrated that deletion of KANK4 impaired collateral artery growth and the recovery of blood perfusion, whereas KANK4 overexpression leads to increased vessel caliber and blood perfusion. Bulk RNA sequencing and Co-immunoprecipitation/mass spectrometry (Co-IP/MS) analysis identified that KANK4 promoted EC proliferation and collateral artery remodeling through coupling VEGFR2 (vascular endothelial growth factor receptor 2) to TALIN-1, which augmented the activation of the VEGFR2 signaling cascade. Conclusions: This study reveals a novel role for KANK4 in arteriogenesis in response to ischemia. KANK4 links VEGFR2 to TALIN-1, resulting in enhanced VEGFR2 activation and increased EC proliferation, highlighting that KANK4 is a potential therapeutic target for promoting arteriogenesis for arterial occlusive diseases.

Published

2022

4. Supplementary Data from Active Remodeling of Capillary Endothelium via Cancer Cell–Derived MMP9 Promotes Metastatic Brain Colonization

Author

Frank Winkler, Wolfgang Wick, Yannick Schwab, Jacky G. Goetz, Hellmut G. Augustin, Dana Westphal, Stefan W. Schneider, Dirk Schadendorf, Iris Helfrich, Michael Hölzel, Daniel Hinze, Marc C. Schubert, Varun Venkataramani, Mahak Singhal, Luc Mercier, Cedric Tehranian, Nicole L. Schieber, Manuel J. Feinauer, Nils Hebach, Katharina Frey, Chanté D. Mayer, Anna S. Berghoff, Gergely Solecki, Alexander T. Bauer, and Matthia A. Karreman

Abstract

Supplementary Figures and Figure legends, Supplementary Video legends and supplementary materials and methods

Published

2023

5. Data from Active Remodeling of Capillary Endothelium via Cancer Cell–Derived MMP9 Promotes Metastatic Brain Colonization

Author

Frank Winkler, Wolfgang Wick, Yannick Schwab, Jacky G. Goetz, Hellmut G. Augustin, Dana Westphal, Stefan W. Schneider, Dirk Schadendorf, Iris Helfrich, Michael Hölzel, Daniel Hinze, Marc C. Schubert, Varun Venkataramani, Mahak Singhal, Luc Mercier, Cedric Tehranian, Nicole L. Schieber, Manuel J. Feinauer, Nils Hebach, Katharina Frey, Chanté D. Mayer, Anna S. Berghoff, Gergely Solecki, Alexander T. Bauer, and Matthia A. Karreman

Abstract

Crossing the blood–brain barrier is a crucial, rate-limiting step of brain metastasis. Understanding of the mechanisms of cancer cell extravasation from brain microcapillaries is limited as the underlying cellular and molecular processes cannot be adequately investigated using in vitro models and endpoint in vivo experiments. Using ultrastructural and functional imaging, we demonstrate that dynamic changes of activated brain microcapillaries promote the mandatory first steps of brain colonization. Successful extravasation of arrested cancer cells occurred when adjacent capillary endothelial cells (EC) entered into a distinct remodeling process. After extravasation, capillary loops were formed, which was characteristic of aggressive metastatic growth. Upon cancer cell arrest in brain microcapillaries, matrix-metalloprotease 9 (MMP9) was expressed. Inhibition of MMP2/9 and genetic perturbation of MMP9 in cancer cells, but not the host, reduced EC projections, extravasation, and brain metastasis outgrowth. These findings establish an active role of ECs in the process of cancer cell extravasation, facilitated by cross-talk between the two cell types. This extends our understanding of how host cells can contribute to brain metastasis formation and how to prevent it.Significance:Tracking single extravasating cancer cells using multimodal correlative microscopy uncovers a brain seeding mechanism involving endothelial remodeling driven by cancer cell–derived MMP9, which might enable the development of approaches to prevent brain metastasis.See related commentary by McCarty, p. 1167

Published

2023

6. Supplementary Table from Timed Ang2-Targeted Therapy Identifies the Angiopoietin–Tie Pathway as Key Regulator of Fatal Lymphogenous Metastasis

Author

Hellmut G. Augustin, Sudhakar R. Chintharlapalli, Rienk Offringa, Matthias Schlesner, Junhao Hu, Moritz Felcht, Jochen Utikal, Stephanie Gehrs, Daniel Baumann, Claudine Fricke, Eva Besemfelder, Ashik Ahmed Abdul Pari, Laura Milde, Ling Hai, Carolin Mogler, Mahak Singhal, and Nicolas Gengenbacher

Abstract

Table S1

Published

2023

7. Supplementary Figures from Timed Ang2-Targeted Therapy Identifies the Angiopoietin–Tie Pathway as Key Regulator of Fatal Lymphogenous Metastasis

Author

Hellmut G. Augustin, Sudhakar R. Chintharlapalli, Rienk Offringa, Matthias Schlesner, Junhao Hu, Moritz Felcht, Jochen Utikal, Stephanie Gehrs, Daniel Baumann, Claudine Fricke, Eva Besemfelder, Ashik Ahmed Abdul Pari, Laura Milde, Ling Hai, Carolin Mogler, Mahak Singhal, and Nicolas Gengenbacher

Abstract

Supplementary Figures S1 - S28

Published

2023

8. Data from Timed Ang2-Targeted Therapy Identifies the Angiopoietin–Tie Pathway as Key Regulator of Fatal Lymphogenous Metastasis

Author

Hellmut G. Augustin, Sudhakar R. Chintharlapalli, Rienk Offringa, Matthias Schlesner, Junhao Hu, Moritz Felcht, Jochen Utikal, Stephanie Gehrs, Daniel Baumann, Claudine Fricke, Eva Besemfelder, Ashik Ahmed Abdul Pari, Laura Milde, Ling Hai, Carolin Mogler, Mahak Singhal, and Nicolas Gengenbacher

Abstract

Recent clinical and preclinical advances have highlighted the existence of a previously hypothesized lymphogenous route of metastasis. However, due to a lack of suitable preclinical modeling tools, its contribution to long-term disease outcome and relevance for therapy remain controversial. Here, we established a genetically engineered mouse model (GEMM) fragment–based tumor model uniquely sustaining a functional network of intratumoral lymphatics that facilitates seeding of fatal peripheral metastases. Multiregimen survival studies and correlative patient data identified primary tumor–derived Angiopoietin-2 (Ang2) as a potent therapeutic target to restrict lymphogenous tumor cell dissemination. Mechanistically, tumor-associated lymphatic endothelial cells (EC), in contrast to blood vascular EC, were found to be critically addicted to the Angiopoietin–Tie pathway. Genetic manipulation experiments in combination with single-cell mapping revealed agonistically acting Ang2–Tie2 signaling as key regulator of lymphatic maintenance. Correspondingly, acute presurgical Ang2 neutralization was sufficient to prolong survival by regressing established intratumoral lymphatics, hence identifying a therapeutic regimen that warrants further clinical evaluation.Significance:Exploiting multiple mouse tumor models including a unique GEMM-derived allograft system in combination with preclinical therapy designs closely matching the human situation, this study provides fundamental insight into the biology of tumor-associated lymphatic EC and defines an innovative presurgical therapeutic window of migrastatic Ang2 neutralization to restrict lymphogenous metastasis.This article is highlighted in the In This Issue feature, p. 211

Published

2023

9. Data from Tumor Cell–Derived Angiopoietin-2 Promotes Metastasis in Melanoma

Author

Moritz Felcht, Hellmut G. Augustin, Kairbaan M. Hodivala-Dilke, Sergij Goerdt, Markus Thomas, Jochen Utikal, Cyrill Géraud, Dorothee Terhardt, Louise E. Reynolds, Nicolas Gengenbacher, Anja Gampp, Benjamin Schieb, Carolin Mogler, Corinne Hübers, Mahak Singhal, and Ashik Ahmed Abdul Pari

Abstract

The angiopoietin (Angpt)–TIE signaling pathway controls vascular maturation and maintains the quiescent phenotype of resting vasculature. The contextual agonistic and antagonistic Tie2 ligand ANGPT2 is believed to be exclusively produced by endothelial cells, disrupting constitutive ANGPT1–TIE2 signaling to destabilize the microvasculature during pathologic disorders like inflammation and cancer. However, scattered reports have also portrayed tumor cells as a source of ANGPT2. Employing ISH-based detection of ANGPT2, we found strong tumor cell expression of ANGPT2 in a subset of patients with melanoma. Comparative analysis of biopsies revealed a higher fraction of ANGPT2-expressing tumor cells in metastatic versus primary sites. Tumor cell–expressed Angpt2 was dispensable for primary tumor growth, yet in-depth analysis of primary tumors revealed enhanced intratumoral necrosis upon silencing of tumor cell Angpt2 expression in the absence of significant immune and vascular alterations. Global transcriptional profiling of Angpt2-deficient tumor cells identified perturbations in redox homeostasis and an increased response to cellular oxidative stress. Ultrastructural analyses illustrated a significant increase of dysfunctional mitochondria in Angpt2-silenced tumor cells, thereby resulting in enhanced reactive oxygen species (ROS) production and downstream MAPK stress signaling. Functionally, enhanced ROS in Angpt2-silenced tumor cells reduced colonization potential in vitro and in vivo. Taken together, these findings uncover the hitherto unappreciated role of tumor cell–expressed ANGPT2 as an autocrine-positive regulator of metastatic colonization and validate ANGPT2 as a therapeutic target for a well-defined subset of patients with melanoma.Significance:This study reveals that tumor cells can be a source of ANGPT2 in the tumor microenvironment and that tumor cell-derived ANGPT2 augments metastatic colonization by protecting tumor cells from oxidative stress.

Published

2023

10. Supplementary Data from Tumor Cell–Derived Angiopoietin-2 Promotes Metastasis in Melanoma

Author

Moritz Felcht, Hellmut G. Augustin, Kairbaan M. Hodivala-Dilke, Sergij Goerdt, Markus Thomas, Jochen Utikal, Cyrill Géraud, Dorothee Terhardt, Louise E. Reynolds, Nicolas Gengenbacher, Anja Gampp, Benjamin Schieb, Carolin Mogler, Corinne Hübers, Mahak Singhal, and Ashik Ahmed Abdul Pari

Abstract

This file consists of supplementary figures (SF) 1-11 consisting of: SF1: Melanoma cells express ANGPT2 (A-F). SF2: Melanoma cell-expressed Angpt2 does not modulate tumor cell proliferation (A-B). SF3: Tumor cell knockdown of Angpt2 does not impact growth of primary tumors (A-J). SF4: Angpt2-depletion in melanoma cells does not affect primary tumor microenvironment (A-F). SF5: Angpt2-depletion alters pathways governing metastasis and oxidative stress (A-B). SF6: Angpt2 knockdown in tumor cells affects the cellular redox balance (A-G). SF7: Tumor cell-expressed Angpt2 alters mitochondrial dynamics (A-E). SF8: Tumor cell-expressed Angpt2 promotes metastasis (A-G). SF9: Tumor cell-expressed Angpt2 does not affect early stages of metastasis in vitro (A-H). SF10: Silencing of Angpt2 impairs invasion through the basement membrane and transmigration across the endothelial barrier (A-H). SF11: Silencing of Angpt2 reduces in vitro colony formation (A-F).

Published

2023

11. Sphingosine-1-Phosphate Recruits Macrophages and Microglia and Induces a Pro-Tumorigenic Phenotype That Favors Glioma Progression

Author

Lavinia Arseni, Rakesh Sharma, Norman Mack, Deepthi Nagalla, Sibylle Ohl, Thomas Hielscher, Mahak Singhal, Robert Pilz, Hellmut Augustin, Roger Sandhoff, Christel Herold-Mende, Björn Tews, Peter Lichter, and Martina Seiffert

Subjects

Cancer Research, Oncology, S1P, glioblastoma, microenvironment, tumor-associated macrophages/microglia, anti-inflammatory

Abstract

Glioblastoma is the most aggressive brain tumor in adults. Treatment failure is predominantly caused by its high invasiveness and its ability to induce a supportive microenvironment. As part of this, a major role for tumor-associated macrophages/microglia (TAMs) in glioblastoma development was recognized. Phospholipids are important players in various fundamental biological processes, including tumor–stroma crosstalk, and the bioactive lipid sphingosine-1-phosphate (S1P) has been linked to glioblastoma cell proliferation, invasion, and survival. Despite the urgent need for better therapeutic approaches, novel strategies targeting sphingolipids in glioblastoma are still poorly explored. Here, we showed that higher amounts of S1P secreted by glioma cells are responsible for an active recruitment of TAMs, mediated by S1P receptor (S1PR) signaling through the modulation of Rac1/RhoA. This resulted in increased infiltration of TAMs in the tumor, which, in turn, triggered their pro-tumorigenic phenotype through the inhibition of NFkB-mediated inflammation. Gene set enrichment analyses showed that such an anti-inflammatory microenvironment correlated with shorter survival of glioblastoma patients. Inhibition of S1P restored a pro-inflammatory phenotype in TAMs and resulted in increased survival of tumor-bearing mice. Taken together, our results establish a crucial role for S1P in fine-tuning the crosstalk between glioma and infiltrating TAMs, thus pointing to the S1P–S1PR axis as an attractive target for glioma treatment.

Published

2023

12. Primary tumor-derived systemic nANGPTL4 inhibits metastasis

Author

Corinne Hübers, Ashik Ahmed Abdul Pari, Denise Grieshober, Martin Petkov, Alexander Schmidt, Tatjana Messmer, Christian Moritz Heyer, Sebastian Schölch, Stephanie S. Kapel, Nicolas Gengenbacher, Mahak Singhal, Benjamin Schieb, Claudine Fricke, Rainer Will, Kim Remans, Jochen Sven Utikal, Christoph Reissfelder, Matthias Schlesner, Kairbaan M. Hodivala-Dilke, Sander Kersten, Sergij Goerdt, Hellmut G. Augustin, and Moritz Felcht

Subjects

Immunology, Metabolism and Genomics, Peptide Fragments, Voeding, Metabolisme en Genomica, Voeding, Metabolisme en Genomica, Neoplasms, Biomarkers, Tumor, Immunology and Allergy, Humans, Angiopoietin-Like Protein 4, Life Science, Nutrition, Metabolism and Genomics, ddc:004, Angiopoietins, VLAG, Nutrition

Abstract

Primary tumors and distant site metastases form a bidirectionally communicating system. Yet, the molecular mechanisms of this crosstalk are poorly understood. Here, we identified the proteolytically cleaved fragments of angiopoietin-like 4 (ANGPTL4) as contextually active protumorigenic and antitumorigenic contributors in this communication ecosystem. Preclinical studies in multiple tumor models revealed that the C-terminal fragment (cANGPTL4) promoted tumor growth and metastasis. In contrast, the N-terminal fragment of ANGPTL4 (nANGPTL4) inhibited metastasis and enhanced overall survival in a postsurgical metastasis model by inhibiting WNT signaling and reducing vascularity at the metastatic site. Tracing ANGPTL4 and its fragments in tumor patients detected full-length ANGPTL4 primarily in tumor tissues, whereas nANGPTL4 predominated in systemic circulation and correlated inversely with disease progression. The study highlights the spatial context of the proteolytic cleavage-dependent pro- and antitumorigenic functions of ANGPTL4 and identifies and validates nANGPTL4 as a novel biomarker of tumor progression and antimetastatic therapeutic agent.

Published

2023

13. Active Remodeling of Capillary Endothelium via Cancer Cell-Derived MMP9 Promotes Metastatic Brain Colonization

Author

Matthia A. Karreman, Alexander T. Bauer, Gergely Solecki, Anna S. Berghoff, Chanté D. Mayer, Katharina Frey, Nils Hebach, Manuel J. Feinauer, Nicole L. Schieber, Cedric Tehranian, Luc Mercier, Mahak Singhal, Varun Venkataramani, Marc C. Schubert, Daniel Hinze, Michael Hölzel, Iris Helfrich, Dirk Schadendorf, Stefan W. Schneider, Dana Westphal, Hellmut G. Augustin, Jacky G. Goetz, Yannick Schwab, Wolfgang Wick, and Frank Winkler

Subjects

Cancer Research, Oncology, Medizin

Abstract

Crossing the blood–brain barrier is a crucial, rate-limiting step of brain metastasis. Understanding of the mechanisms of cancer cell extravasation from brain microcapillaries is limited as the underlying cellular and molecular processes cannot be adequately investigated using in vitro models and endpoint in vivo experiments. Using ultrastructural and functional imaging, we demonstrate that dynamic changes of activated brain microcapillaries promote the mandatory first steps of brain colonization. Successful extravasation of arrested cancer cells occurred when adjacent capillary endothelial cells (EC) entered into a distinct remodeling process. After extravasation, capillary loops were formed, which was characteristic of aggressive metastatic growth. Upon cancer cell arrest in brain microcapillaries, matrix-metalloprotease 9 (MMP9) was expressed. Inhibition of MMP2/9 and genetic perturbation of MMP9 in cancer cells, but not the host, reduced EC projections, extravasation, and brain metastasis outgrowth. These findings establish an active role of ECs in the process of cancer cell extravasation, facilitated by cross-talk between the two cell types. This extends our understanding of how host cells can contribute to brain metastasis formation and how to prevent it. Significance: Tracking single extravasating cancer cells using multimodal correlative microscopy uncovers a brain seeding mechanism involving endothelial remodeling driven by cancer cell–derived MMP9, which might enable the development of approaches to prevent brain metastasis. See related commentary by McCarty, p. 1167

Published

2023

14. Activating NO–sGC crosstalk in the mouse vascular niche promotes vascular integrity and mitigates acute lung injury

Author

Hao He, Wu Yang, Nan Su, Chuankai Zhang, Jianing Dai, Feng Han, Mahak Singhal, Wenjuan Bai, Xiaolan Zhu, Jing Zhu, Zhen Liu, Wencheng Xia, Xiaoting Liu, Chonghe Zhang, Kai Jiang, Wenhui Huang, Dan Chen, Zhaoyin Wang, Xueyang He, Frank Kirchhoff, Zhenyu Li, Cong Liu, Jingning Huan, Xiaohong Wang, Wu Wei, Jing Wang, Hellmut G. Augustin, and Junhao Hu

Subjects

Lipopolysaccharides, Mice, Soluble Guanylyl Cyclase, Acute Lung Injury, Immunology, Animals, Immunology and Allergy, Pericytes, Nitric Oxide

Abstract

Disruption of endothelial cell (ECs) and pericytes interactions results in vascular leakage in acute lung injury (ALI). However, molecular signals mediating EC–pericyte crosstalk have not been systemically investigated, and whether targeting such crosstalk could be adopted to combat ALI remains elusive. Using comparative genome-wide EC–pericyte crosstalk analysis of healthy and LPS-challenged lungs, we discovered that crosstalk between endothelial nitric oxide and pericyte soluble guanylate cyclase (NO–sGC) is impaired in ALI. Indeed, stimulating the NO–sGC pathway promotes vascular integrity and reduces lung edema and inflammation-induced lung injury, while pericyte-specific sGC knockout abolishes this protective effect. Mechanistically, sGC activation suppresses cytoskeleton rearrangement in pericytes through inhibiting VASP-dependent F-actin formation and MRTFA/SRF-dependent de novo synthesis of genes associated with cytoskeleton rearrangement, thereby leading to the stabilization of EC–pericyte interactions. Collectively, our data demonstrate that impaired NO–sGC crosstalk in the vascular niche results in elevated vascular permeability, and pharmacological activation of this crosstalk represents a promising translational therapy for ALI.

Published

2022

15. Timed Ang2-Targeted Therapy Identifies the Angiopoietin–Tie Pathway as Key Regulator of Fatal Lymphogenous Metastasis

Author

Ling Hai, Matthias Schlesner, Stephanie Gehrs, Nicolas Gengenbacher, Daniel Baumann, Mahak Singhal, Rienk Offringa, Sudhakar Chintharlapalli, Hellmut G. Augustin, Junhao Hu, Claudine Fricke, Ashik Ahmed Abdul Pari, Jochen Utikal, Laura Milde, Moritz Felcht, Eva Besemfelder, and Carolin Mogler

Subjects

0301 basic medicine, Lung Neoplasms, medicine.medical_treatment, government.form_of_government, Regulator, Mice, Transgenic, Mice, SCID, Metastasis, Targeted therapy, Angiopoietin-2, Functional networks, Angiopoietin, Mice, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, ddc:610, business.industry, Endothelial Cells, medicine.disease, Receptor, TIE-2, Mice, Inbred C57BL, Disease Models, Animal, Lymphatic Endothelium, 030104 developmental biology, Lymphatic system, Oncology, Lymphatic Metastasis, 030220 oncology & carcinogenesis, Genetically Engineered Mouse, Cancer research, government, Female, business, Signal Transduction

Abstract

Recent clinical and preclinical advances have highlighted the existence of a previously hypothesized lymphogenous route of metastasis. However, due to a lack of suitable preclinical modeling tools, its contribution to long-term disease outcome and relevance for therapy remain controversial. Here, we established a genetically engineered mouse model (GEMM) fragment–based tumor model uniquely sustaining a functional network of intratumoral lymphatics that facilitates seeding of fatal peripheral metastases. Multiregimen survival studies and correlative patient data identified primary tumor–derived Angiopoietin-2 (Ang2) as a potent therapeutic target to restrict lymphogenous tumor cell dissemination. Mechanistically, tumor-associated lymphatic endothelial cells (EC), in contrast to blood vascular EC, were found to be critically addicted to the Angiopoietin–Tie pathway. Genetic manipulation experiments in combination with single-cell mapping revealed agonistically acting Ang2–Tie2 signaling as key regulator of lymphatic maintenance. Correspondingly, acute presurgical Ang2 neutralization was sufficient to prolong survival by regressing established intratumoral lymphatics, hence identifying a therapeutic regimen that warrants further clinical evaluation. Significance: Exploiting multiple mouse tumor models including a unique GEMM-derived allograft system in combination with preclinical therapy designs closely matching the human situation, this study provides fundamental insight into the biology of tumor-associated lymphatic EC and defines an innovative presurgical therapeutic window of migrastatic Ang2 neutralization to restrict lymphogenous metastasis. This article is highlighted in the In This Issue feature, p. 211

Published

2021

16. Tumor Cell–Derived Angiopoietin-2 Promotes Metastasis in Melanoma

Author

Anja Gampp, Moritz Felcht, Louise E. Reynolds, Jochen Utikal, Carolin Mogler, Hellmut G. Augustin, Dorothee Terhardt, Benjamin Schieb, Mahak Singhal, Corinne Hübers, Cyrill Géraud, Kairbaan Hodivala-Dilke, Markus Thomas, Sergij Goerdt, Nicolas Gengenbacher, and Ashik Ahmed Abdul Pari

Subjects

0301 basic medicine, Cancer Research, Skin Neoplasms, MAP Kinase Signaling System, Biopsy, Inflammation, Kaplan-Meier Estimate, Biology, Article, Metastasis, Angiopoietin-2, Angiopoietin, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, Cell Line, Tumor, Human Umbilical Vein Endothelial Cells, Tumor Microenvironment, medicine, Animals, Humans, Gene silencing, Melanoma, Nevus, Skin, Tumor microenvironment, Gene Expression Profiling, medicine.disease, Primary tumor, 3. Good health, Autocrine Communication, Disease Models, Animal, 030104 developmental biology, Oncology, Tissue Array Analysis, Gene Knockdown Techniques, 030220 oncology & carcinogenesis, Disease Progression, Cancer research, Female, medicine.symptom, Reactive Oxygen Species

Abstract

The angiopoietin (Angpt)–TIE signaling pathway controls vascular maturation and maintains the quiescent phenotype of resting vasculature. The contextual agonistic and antagonistic Tie2 ligand ANGPT2 is believed to be exclusively produced by endothelial cells, disrupting constitutive ANGPT1–TIE2 signaling to destabilize the microvasculature during pathologic disorders like inflammation and cancer. However, scattered reports have also portrayed tumor cells as a source of ANGPT2. Employing ISH-based detection of ANGPT2, we found strong tumor cell expression of ANGPT2 in a subset of patients with melanoma. Comparative analysis of biopsies revealed a higher fraction of ANGPT2-expressing tumor cells in metastatic versus primary sites. Tumor cell–expressed Angpt2 was dispensable for primary tumor growth, yet in-depth analysis of primary tumors revealed enhanced intratumoral necrosis upon silencing of tumor cell Angpt2 expression in the absence of significant immune and vascular alterations. Global transcriptional profiling of Angpt2-deficient tumor cells identified perturbations in redox homeostasis and an increased response to cellular oxidative stress. Ultrastructural analyses illustrated a significant increase of dysfunctional mitochondria in Angpt2-silenced tumor cells, thereby resulting in enhanced reactive oxygen species (ROS) production and downstream MAPK stress signaling. Functionally, enhanced ROS in Angpt2-silenced tumor cells reduced colonization potential in vitro and in vivo. Taken together, these findings uncover the hitherto unappreciated role of tumor cell–expressed ANGPT2 as an autocrine-positive regulator of metastatic colonization and validate ANGPT2 as a therapeutic target for a well-defined subset of patients with melanoma. Significance: This study reveals that tumor cells can be a source of ANGPT2 in the tumor microenvironment and that tumor cell-derived ANGPT2 augments metastatic colonization by protecting tumor cells from oxidative stress.

Published

2020

17. STAT3-YAP/TAZ signaling in endothelial cells promotes tumor angiogenesis

Author

Ying Shen, Xiaohong Wang, Yi Liu, Mahak Singhal, Can Gürkaşlar, Aida Freire Valls, Yi Lei, Wenjie Hu, Géza Schermann, Heike Adler, Fa-Xing Yu, Tamás Fischer, Yi Zhu, Hellmut G. Augustin, Thomas Schmidt, and Carmen Ruiz de Almodóvar

Subjects

STAT3 Transcription Factor, Neoplasms, Endothelial Cells, Humans, YAP-Signaling Proteins, Cell Biology, Phosphoproteins, Molecular Biology, Biochemistry, Adaptor Proteins, Signal Transducing, Signal Transduction

Abstract

The nuclear translocation and activity of the cotranscriptional activators YAP and TAZ (YAP/TAZ) in endothelial cells (ECs) are crucial during developmental angiogenesis. Here, we studied the role of YAP/TAZ signaling in ECs in tumor angiogenesis and found that the expression of

Published

2021

18. Temporal multi-omics identifies LRG1 as a vascular niche instructor of metastasis

Author

Martin R. Sprick, Carolin Mogler, Mathias Heikenwalder, Stephen E. Moss, Jeroen Krijgsveld, Matthias Schlesner, David Kallenberg, Mahak Singhal, Hellmut G. Augustin, Barbara Leuchs, Ling Hai, Shubhada Rajabhau Kulkarni, Junhao Hu, Danijela Heide, Bianca J. Kuhn, Stephanie F. Preuß, John A. Greenwood, Nicolas Gengenbacher, Eva Besemfelder, Andreas Trumpp, Ashik Ahmed Abdul Pari, Elisa Espinet, Miki Kamiyama, and Carlotta Camilli

Subjects

Tumor cells, General Medicine, Biology, medicine.disease, Metastasis, LRG1, Neoplasms, Cancer research, medicine, Humans, Multi omics, Vascular niche, ddc:610, Glycoproteins

Abstract

Metastasis is the primary cause of cancer-related mortality. Tumor cell interactions with cells of the vessel wall are decisive and potentially rate-limiting for metastasis. The molecular nature of this cross-talk is, beyond candidate gene approaches, hitherto poorly understood. Using endothelial cell (EC) bulk and single-cell transcriptomics in combination with serum proteomics, we traced the evolution of the metastatic vascular niche in surgical models of lung metastasis. Temporal multiomics revealed that primary tumors systemically reprogram the body’s vascular endothelium to perturb homeostasis and to precondition the vascular niche for metastatic growth. The vasculature with its enormous surface thereby serves as amplifier of tumor-induced instructive signals. Comparative analysis of lung EC gene expression and secretome identified the transforming growth factor–β (TGFβ) pathway specifier LRG1, leucine-rich alpha-2-glycoprotein 1, as an early instructor of metastasis. In the presence of a primary tumor, ECs systemically up-regulated LRG1 in a signal transducer and activator of transcription 3 (STAT3)–dependent manner. A meta-analysis of retrospective clinical studies revealed a corresponding up-regulation of LRG1 concentrations in the serum of patients with cancer. Functionally, systemic up-regulation of LRG1 promoted metastasis in mice by increasing the number of prometastatic neural/glial antigen 2 (NG2)

Published

2021

19. Emerging paradigms in metastasis research

Author

Hellmut G. Augustin, Ashik Ahmed Abdul Pari, and Mahak Singhal

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Biomedical Research, Cancer Focus, Immunology, Disease, Review, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Neoplasms, Immunology and Allergy, Medicine, Animals, Humans, natural sciences, Solid Tumors, Neoplasm Metastasis, Grand Challenges, Metastatic cascade, business.industry, Mechanism (biology), technology, industry, and agriculture, Patient survival, medicine.disease, Primary tumor, Gene Expression Regulation, Neoplastic, Metastatic colonization, 030104 developmental biology, 030220 oncology & carcinogenesis, Disease Progression, business

Abstract

Building on the status quo of metastasis research, this review highlights key bottlenecks in the spatiotemporal progression of metastasis and provides a framework for propelling bench-to-bedside translation of fundamental preclinical discoveries., Historically, therapy of metastatic disease has essentially been limited to using strategies that were identified and established to shrink primary tumors. The limited efficacy of such treatments on overall patient survival stems from diverging intrinsic and extrinsic characteristics of a primary tumor and metastases originating therefrom. To develop better therapeutic strategies to treat metastatic disease, there is an urgent need to shift the paradigm in preclinical metastasis research by conceptualizing metastatic dissemination, colonization, and growth as spatiotemporally dynamic processes and identifying rate-limiting vulnerabilities of the metastatic cascade. Clinically, while metastatic colonization remains the most attractive therapeutic avenue, comprehensive understanding of earlier steps may unravel novel metastasis-restricting therapies for presurgical neoadjuvant application. Moving beyond a primary tumor-centric view, this review adopts a holistic approach to understanding the spatial and temporal progression of metastasis. After reviewing recent developments in metastasis research, we highlight some of the grand challenges and propose a framework to expedite mechanism-based discovery research feeding the translational pipeline.

Published

2020

20. Endothelial Tie1–mediated angiogenesis and vascular abnormalization promote tumor progression and metastasis

Author

Ralf H. Adams, Carolin Mogler, Soniya Savant, H. Scott Baldwin, Carleen Spegg, Hellmut G. Augustin, Mahak Singhal, Xianghu Qu, Lise Roth, Silvia La Porta, and Benjamin Schieb

Subjects

Male, 0301 basic medicine, Lung Neoplasms, Angiogenesis, Melanoma, Experimental, Mural cell, TIE1, Metastasis, Mice, Necrosis, 03 medical and health sciences, Circulating tumor cell, Cell Line, Tumor, Human Umbilical Vein Endothelial Cells, medicine, Animals, Humans, Neoplasm Metastasis, Mice, Knockout, Neovascularization, Pathologic, business.industry, Endothelial Cells, Receptor, TIE-1, General Medicine, medicine.disease, Primary tumor, Extravasation, 030104 developmental biology, Tumor progression, Disease Progression, Cancer research, Female, business, Gene Deletion, Neoplasm Transplantation, Research Article

Abstract

The endothelial tyrosine kinase receptor Tie1 remains poorly characterized, largely owing to its orphan receptor status. Global Tie1 inactivation causes late embryonic lethality, thereby reflecting its importance during development. Tie1 also plays pivotal roles during pathologies such as atherosclerosis and tumorigenesis. In order to study the contribution of Tie1 to tumor progression and metastasis, we conditionally deleted Tie1 in endothelial cells at different stages of tumor growth and metastatic dissemination. Tie1 deletion during primary tumor growth in mice led to a decrease in microvessel density and an increase in mural cell coverage with improved vessel perfusion. Reduced angiogenesis and enhanced vascular normalization resulted in a progressive increase of intratumoral necrosis that caused a growth delay only at later stages of tumor progression. Concomitantly, surgical removal of the primary tumor decreased the number of circulating tumor cells, reduced metastasis, and prolonged overall survival. Additionally, Tie1 deletion in experimental murine metastasis models prevented extravasation of tumor cells into the lungs and reduced metastatic foci. Taken together, the data support Tie1 as a therapeutic target by defining its regulatory functions during angiogenesis and vascular abnormalization and identifying its role during metastasis.

Published

2018

21. LRG1 destabilizes tumor vessels and restricts immunotherapeutic potency

Author

Owen J. Sansom, Markella Alatsatianos, Marie N. O'Connor, Stephen E. Moss, Rene Jackstadt, Hellmut G. Augustin, Ann Ager, Athina Dritsoula, Mahak Singhal, Chantelle E. Bowers, Julia Ohme, David Kallenberg, Xiaomeng Wang, Jack W.D. Blackburn, Carlotta Camilli, John A. Greenwood, Laura Dowsett, Jestin George, H. Angharad Watson, and Camilla Pilotti

Subjects

Tumor microenvironment, Neovascularization, Pathologic, business.industry, medicine.medical_treatment, Endothelial Cells, General Medicine, Immunotherapy, Functioning tumor, Immune checkpoint, Mice, Immune system, LRG1, Tumor progression, Neoplasms, Knockout mouse, Tumor Microenvironment, Cancer research, Animals, Medicine, business, Glycoproteins

Abstract

Summary Background A poorly functioning tumor vasculature is pro-oncogenic and may impede the delivery of therapeutics. Normalizing the vasculature, therefore, may be beneficial. We previously reported that the secreted glycoprotein leucine-rich α-2-glycoprotein 1 (LRG1) contributes to pathogenic neovascularization. Here, we investigate whether LRG1 in tumors is vasculopathic and whether its inhibition has therapeutic utility. Methods Tumor growth and vascular structure were analyzed in subcutaneous and genetically engineered mouse models in wild-type and Lrg1 knockout mice. The effects of LRG1 antibody blockade as monotherapy, or in combination with co-therapies, on vascular function, tumor growth, and infiltrated lymphocytes were investigated. Findings In mouse models of cancer, Lrg1 expression was induced in tumor endothelial cells, consistent with an increase in protein expression in human cancers. The expression of LRG1 affected tumor progression as Lrg1 gene deletion, or treatment with a LRG1 function-blocking antibody, inhibited tumor growth and improved survival. Inhibition of LRG1 increased endothelial cell pericyte coverage and improved vascular function, resulting in enhanced efficacy of cisplatin chemotherapy, adoptive T cell therapy, and immune checkpoint inhibition (anti-PD1) therapy. With immunotherapy, LRG1 inhibition led to a significant shift in the tumor microenvironment from being predominantly immune silent to immune active. Conclusions LRG1 drives vascular abnormalization, and its inhibition represents a novel and effective means of improving the efficacy of cancer therapeutics. Funding Wellcome Trust (206413/B/17/Z), UKRI/MRC (G1000466, MR/N006410/1, MC/PC/14118, and MR/L008742/1), BHF (PG/16/50/32182), Health and Care Research Wales (CA05), CRUK (C42412/A24416 and A17196), ERC (ColonCan 311301 and AngioMature 787181), and DFG (CRC1366).

Published

2021

22. Beyond Angiogenesis: Exploiting Angiocrine Factors to Restrict Tumor Progression and Metastasis

Author

Hellmut G. Augustin and Mahak Singhal

Subjects

0301 basic medicine, Vascular Endothelial Growth Factor A, Cancer Research, Angiogenesis, Carcinogenesis, medicine.medical_treatment, Drug Evaluation, Preclinical, Angiogenesis Inhibitors, Metastasis, Neovascularization, 03 medical and health sciences, 0302 clinical medicine, Immune system, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, Tumor Microenvironment, Medicine, Animals, Humans, Neoplasm Metastasis, Tumor microenvironment, Neovascularization, Pathologic, business.industry, Endothelial Cells, Immunotherapy, medicine.disease, Neoplastic Cells, Circulating, Disease Models, Animal, 030104 developmental biology, Receptors, Vascular Endothelial Growth Factor, Oncology, Tumor progression, 030220 oncology & carcinogenesis, Cancer research, Disease Progression, Fundamental change, Endothelium, Vascular, medicine.symptom, business, Signal Transduction

Abstract

Looking beyond tumor angiogenesis, the past decade has witnessed a fundamental change of paradigm with the discovery that the vascular endothelium does not just respond to exogenous cytokines, but exerts active “angiocrine” gatekeeper roles, controlling their microenvironment in an instructive manner. While vascular niches host disseminated cancer cells and promote their stemness, endothelial cell–derived angiocrine signals orchestrate a favorable immune milieu to facilitate metastatic growth. Here, we discuss recent advances in the field of tumor microenvironment research and propose angiocrine signals as promising targets of future mechanism-driven antimetastatic therapies, which may prove useful to synergistically combine with chemotherapy and immunotherapy.

Published

2019

23. Abstract 450: Vascular Smooth Muscle Cell-expressed Tie2 Controls Atherosclerosis Progression

Author

Claudia Korn, Hellmut G. Augustin, Thomas Korff, Zulfiyya Hasanov, Junhao Hu, Caroline Arnold, Mahak Singhal, Stella Hertel, Stephanie S. Kapel, Sila Appak-Baskoy, Jessica Wojtarowicz, Marius R. Robciuc, Jingjing Shi, and Damir Krunic

Subjects

Pathology, medicine.medical_specialty, Vascular smooth muscle, biology, business.industry, Cell, Angiopoietin receptor, medicine.anatomical_structure, cardiovascular system, medicine, biology.protein, Cardiology and Cardiovascular Medicine, business, tissues

Abstract

Angiopoietin (Angpt)/Tie signaling in microvascular endothelial cells (EC) controls vascular development, remodeling and maturation. Biomarker studies also imply a role of macrovascular Angpt/Tie signaling. The model of Angpt1/stimulation versus Angpt2/destabilization would imply an anti-atherosclerotic function of Angpt1 and a pro-atherosclerotic function of Angpt2. Yet, experimental studies on the role of the Angpt ligands and the Tie receptors in atherosclerosis have yielded conflicting results suggesting spatiotemporally context-dependent pro- and anti-atherosclerotic functions in different experimental settings. The endotheliocentric view of Angpt/Tie signaling is not sufficient to mechanistically explain the divergent roles of Angpt/Tie signaling during atherosclerosis. We hypothesized that vascular smooth muscle cell (VSMC)-expressed Tie2 may contribute to the pathogenesis of atherosclerosis. Employing genetic models, the present study was aimed at elucidating the role of VSMC-expressed Tie2 during atherosclerosis. Compared to EC, VSMC express lower, but consistently detectable levels of functional Tie2. We therefore generated VSMC-specific Tie2 - deficient mice ( Tie2 SMC-KO ), using a mural cell-specific Sm22α-Cre driver line. These were crossed with atherosclerosis-prone ApoE- deficient mice ( ApoE KO Tie2 SMC-KO ). ApoE KO Tie2 SMC-KO mice, fed a Western-type diet for 14 weeks, showed significantly reduced atherosclerotic lesion progression with less VSMC content. Transcriptionally, Tie2 controlled the phenotypic switch of VSMC with increased contractile and reduced synthetic phenotype-specific gene expression in isolated Tie2-deficient VSMC. Correspondingly, migration and proliferation was significantly reduced in Tie2-deficient cultured VSMC. Serum Angpt2 as well as the Angpt2/Angpt1 ratio were significantly increased in ApoE KO Tie2 SMC-KO mice. Collectively, the data expand and revise the endotheliocentric Tie2 signaling concept to show that mural cell-expressed Tie2 is involved in regulating macrovascular functions related to atherosclerosis. VSMC-expressed Tie2 acts pro-atherosclerotic to control the phenotypic switch towards a proliferative and migratory synthetic VSMC phenotype.

Published

2018

24. Endothelial cell fitness dictates the source of regenerating liver vasculature

Author

Jianing Dai, Xiaoting Liu, Nicolas Gengenbacher, Mahak Singhal, Kai Jiang, Weiping Li, Lijian Hui, Hellmut G. Augustin, Susanne Bartels, Eva Besemfelder, Ashik Ahmed Abdul Pari, Hao He, Junhao Hu, and Donato Inverso

Subjects

0301 basic medicine, Endothelium, medicine.medical_treatment, Immunology, Recombinant Granulocyte Colony-Stimulating Factor, Biology, News, Models, Biological, Insights, 03 medical and health sciences, Mice, 0302 clinical medicine, medicine, Immunology and Allergy, Animals, Hepatectomy, Progenitor cell, Bone Marrow Transplantation, Mice, Knockout, Regeneration (biology), Endothelial Cells, Stem-cell therapy, Liver regeneration, 3. Good health, Liver Regeneration, Endothelial stem cell, 030104 developmental biology, medicine.anatomical_structure, Liver, 030220 oncology & carcinogenesis, Cancer research, Bone marrow

Abstract

In this issue of JEM, Singhal et al. explore the cellular mechanisms involved in endothelial cell regeneration in the liver. Using a combination of myeloablative and nonmyeloablative approaches, the authors found that repair of the endothelium is mediated by endothelial cells themselves, but when injured, endothelial cells enlist myeloid counterparts that aid in vascular repair., In this issue of JEM, Singhal et al. (https://doi.org/10.1084/jem.20180008) explore the cellular mechanisms involved in endothelial cell regeneration in the liver. Using a combination of myeloablative and nonmyeloablative approaches, the authors found that repair of the endothelium is mediated by endothelial cells themselves, but when injured, endothelial cells enlist myeloid counterparts that aid in vascular repair.

Published

2018

25. Preclinical mouse solid tumour models: status quo, challenges and perspectives

Author

Nicolas Gengenbacher, Mahak Singhal, and Hellmut G. Augustin

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Status quo, Systematic survey, General Mathematics, media_common.quotation_subject, Translational Research, Biomedical, 03 medical and health sciences, Mice, 0302 clinical medicine, Neoplasms, Medicine, Animals, Humans, media_common, Solid tumour, Human studies, business.industry, Tumor biology, Experimental model, Applied Mathematics, Clinical trial, Disease Models, Animal, 030104 developmental biology, 030220 oncology & carcinogenesis, Observational study, business, Neuroscience

Abstract

Oncology research in humans is limited to analytical and observational studies for obvious ethical reasons, with therapy-focused clinical trials being the one exception to this rule. Preclinical mouse tumour models therefore serve as an indispensable intermediate experimental model system bridging more reductionist in vitro research with human studies. Based on a systematic survey of preclinical mouse tumour studies published in eight scientific journals in 2016, this Analysis provides an overview of how contemporary preclinical mouse tumour biology research is pursued. It thereby identifies some of the most important challenges in this field and discusses potential ways in which preclinical mouse tumour models could be improved for better relevance, reproducibility and translatability.

Published

2017

26. Acetyl-CoA carboxylase 1-dependent protein acetylation controls breast cancer metastasis and recurrence

Author

Stephan Herzig, Mahak Singhal, Brigitte Steinbauer, Sven Christian, Adriano Maida, Mauricio Berriel Diaz, Frits Mattijssen, Holger Hess-Stumpp, Hellmut G. Augustin, Marcos Rios Garcia, Peter P. Nawroth, Karin Müller-Decker, and Kshitij Srivastava

Subjects

Leptin, 0301 basic medicine, Lung Neoplasms, Physiology, CA 15-3, Breast Neoplasms, Biology, Metastasis, Mice, 03 medical and health sciences, Breast cancer, medicine, Animals, Humans, Neoplasm Metastasis, Metastasis Induction, Lung cancer, Molecular Biology, Mice, Inbred BALB C, Emt, Acetyl-coa, Acetylation, Breast Cancer, Pacc, Cancer, Cell Biology, medicine.disease, Primary tumor, Metastatic breast cancer, Mice, Inbred C57BL, Disease Models, Animal, HEK293 Cells, 030104 developmental biology, Tissue Array Analysis, MCF-7 Cells, Cancer research, Female, Neoplasm Recurrence, Local, Acetyl-CoA Carboxylase

Abstract

Breast tumor recurrence and metastasis represent the main causes of cancer-related death in women, and treatments are still lacking. Here, we define thelipogenic enzyme acetyl-CoA carboxylase (ACC) 1 as a key player in breast cancer metastasis. ACC1 phosphorylation was increased in invading cells both in murine and human breast cancer, serving as a point of convergence for leptin and transforming growth factor (TGF) β signaling. ACC1 phosphorylation was mediated by TGFβ-activated kinase (TAK)1, and ACC1 inhibition was indispensable for the elevation of cellular acetyl-CoA, the subsequent increase in Smad2 transcription factor acetylation and activation, and ultimately epithelial-mesenchymal transition and metastasis induction. ACC1 deficiency worsened tumor recurrence upon primary tumor resection in mice, and ACC1 phosphorylation levels correlated with metastatic potential in breast and lung cancer patients. Given the demonstrated effectiveness of anti-leptin receptor antibody treatment in halting ACC1-dependent tumor invasiveness, our work defines a "metabolocentric" approach in metastatic breast cancer therapy.

Published

2017

27. Molecular Mechanism of Regulation of MTA1 Expression by Granulocyte Colony-stimulating Factor*

Author

R P Surabhi, Suresh K. Rayala, Saravana Babu Chidambaram, Mahak Singhal, Ravi Shankar Pitani, Sathiya Sekar, Sankar Jagadeeshan, Ganesh Venkatraman, Hemadev Bhoopalan, Anirudh Subramanian, Arathy S. Kumar, and Prathiba Duvuru

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Tyrosine 3-Monooxygenase, Dopamine, Blotting, Western, Dopamine Agents, Gene Expression, Substantia nigra, Biology, Motor Activity, Biochemistry, Histone Deacetylases, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Cell Line, Tumor, Granulocyte Colony-Stimulating Factor, medicine, Animals, Humans, Gene Regulation, Molecular Biology, Neurons, Tyrosine hydroxylase, Reverse Transcriptase Polymerase Chain Reaction, Dopaminergic, Parkinson Disease, Cell Biology, Human brain, Immunohistochemistry, Blot, Mice, Inbred C57BL, Repressor Proteins, Substantia Nigra, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, 1-Methyl-4-phenyl-1,2,3,6-tetrahydropyridine, Immunology, Trans-Activators, 030217 neurology & neurosurgery, medicine.drug

Abstract

Parkinson disease (PD) is a neurodegenerative disorder with loss of dopaminergic neurons of the brain, which results in insufficient synthesis and action of dopamine. Metastasis-associated protein 1 (MTA1) is an upstream modulator of tyrosine hydroxylase (TH), the rate-limiting enzyme in dopamine synthesis, and hence MTA1 plays a significant role in PD pathogenesis. To impart functional and clinical significance to MTA1, we analyzed MTA1 and TH levels in the substantia nigra region of a large cohort of human brain tissue samples by Western blotting, quantitative PCR, and immunohistochemistry. Our results showed that MTA1 and TH levels were significantly down-regulated in PD samples as compared with normal brain tissue. Correspondingly, immunohistochemistry analysis for MTA1 in substantia nigra sections revealed that 74.1% of the samples had a staining intensity of

Published

2016

28. Threonine 209 phosphorylation on RUNX3 by Pak1 is a molecular switch for its dualistic functions

Author

Rahul Kanumuri, Shilpa Tentu, Kumaresan Ramanathan, Asha S. Nair, Sandhya Sundaram, R Shankar Pitani, Sankar Jagadeeshan, S Srinivasan, Mahak Singhal, S Abhijit, R P Surabhi, B Muthuswamy, Suresh K. Rayala, Ganesh Venkatraman, C Chopra, and Arathy S. Kumar

Subjects

0301 basic medicine, Threonine, Cancer Research, Cytoplasm, Biology, 03 medical and health sciences, Mice, 0302 clinical medicine, PAK1, Cell Line, Tumor, Neoplasms, Genetics, Biomarkers, Tumor, Animals, Humans, Phosphorylation, Molecular Biology, Regulation of gene expression, Cell Nucleus, Kinase, Intracellular Signaling Peptides and Proteins, Cell cycle, Subcellular localization, Xenograft Model Antitumor Assays, digestive system diseases, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Core Binding Factor Alpha 3 Subunit, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Mutagenesis, Site-Directed, Female

Abstract

P21 Activated Kinase 1 (Pak1), an oncogenic serine/threonine kinase, is known to have a significant role in the regulation of cytoskeleton and cellular morphology. Runx3 was initially known for its role in tumor suppressor function, but recent studies have reported the oncogenic role of Runx3 in various cancers. However, the mechanism that controls the paradoxical functions of Runx3 still remains unclear. In this study, we show that Runx3 is a physiologically interacting substrate of Pak1. We identified the site of phosphorylation in Runx3 as Threonine 209 by mass spectrometry analysis and site-directed mutagenesis, and further confirmed the same with a site-specific antibody. Results from our functional studies showed that Threonine 209 phosphorylation in Runx3 alters its subcellular localization by protein mislocalization from the nucleus to the cytoplasm and subsequently converses its biological functions. This was further supported by in vivo tumor xenograft studies in nude mouse models which clearly demonstrated that PANC-28 cells transfected with the Runx3-T209E clone showed high tumorigenic potential as compared with other clones. Our results from clinical samples also suggest that Threonine 209 phosphorylation by Pak1 could be a potential therapeutic target and of great clinical relevance with implications for Runx3 inactivation in cancer cells where Runx3 is known to be oncogenic. The findings presented in this study provide evidence of Runx3-Threonine 209 phosphorylation as a molecular switch in dictating the tissue-specific dualistic functions of Runx3 for the first time.

Published

2015

29. Transcriptional regulation of fibronectin by p21-activated kinase-1 modulates pancreatic tumorigenesis

Author

A Roshini, Asha S. Nair, Sankar Jagadeeshan, K Sadasivan, Mathangi Ravi, Anand Krishnan, A Lakshmi, Leena Dennis Joseph, Ganesh Venkatraman, J Mavuluri, A. Subramanian, Mahak Singhal, Y R Krishnamoorthy, Suresh K. Rayala, and Ganga Baskar

Subjects

Cancer Research, Transcription, Genetic, transcription factor RelA, cell transformation, Biology, medicine.disease_cause, Mice, PAK1, promoter region, Downregulation and upregulation, fibronectin, Pancreatic cancer, Cell Line, Tumor, medicine, Transcriptional regulation, Animals, Humans, animal, genetics, human, Promoter Regions, Genetic, Molecular Biology, mouse, Kinase, Cell growth, genetic transcription, tumor cell line, gene expression regulation, medicine.disease, Fibronectins, Fibronectin, Pancreatic Neoplasms, Gene Expression Regulation, Neoplastic, Cell Transformation, Neoplastic, p21-Activated Kinases, physiology, biology.protein, Cancer research, p21 activated kinase, Carcinogenesis, metabolism, Carcinoma, Pancreatic Ductal

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is the eighth largest cause of cancer-related mortality across the world, with a median 5-year survival rate of less than 3.5%. This is partly because the molecules and the molecular mechanisms that contribute to PDAC are not well understood. Our goal is to understand the role of p21-activated kinase 1 (Pak1) signaling axis in the progression of PDAC. Pak1, a serine/threonine kinase, is a well-known regulator of cytoskeletal remodeling, cell motility, cell proliferation and cell survival. Recent reports suggest that Pak1 by itself can have an oncogenic role in a wide variety of cancers. In this study, we analyzed the expression of Pak1 in human pancreatic cancer tissues and found that Pak1 levels are significantly upregulated in PDAC samples as compared with adjacent normals. Further, to study the functional role of Pak1 in pancreatic cancer model systems, we developed stable overexpression and lentiviral short hairpin RNA-mediated knockdown (KD) clones of Pak1 and studied the changes in transforming properties of the cells. We also observed that Pak1 KD clones failed to form tumors in nude mice. By adopting a quantitative PCR array-based approach, we identified fibronectin, a component of the extracellular matrix and a mesenchymal marker, as a transcriptional target of Pak1 signaling. The underlying molecular mechanism of Pak1-mediated transformation includes its nuclear import and recruitment to the fibronectin promoter via interaction with nuclear factor-κB (NF-κB)-p65 complex. To our knowledge, this is the first study illustrating Pak1-NF-κB-p65-mediated fibronectin regulation as a potent tumor-promoting mechanism in KRAS intact model.

Published

2015

30. Preclinical validation of a novel metastasis‐inhibiting Tie1 function‐blocking antibody

Author

Silvia La Porta, Anthony S. Fischl, Sudhakar Chintharlapalli, Hellmut G. Augustin, Nicolas Gengenbacher, Jingjing Shi, Benjamin Schieb, Stephanie Gehrs, Diane M. Bodenmiller, Miki Kamiyama, Mahak Singhal, and Eva Besemfelder

Subjects

0301 basic medicine, Medicine (General), Vascular Biology & Angiogenesis, Angiogenesis, Immunology, QH426-470, TIE1, Metastasis, Angiopoietin, Angiopoietin-2, 03 medical and health sciences, angiogenesis, Mice, 0302 clinical medicine, R5-920, Report, Neoplasms, Blocking antibody, medicine, Genetics, Angiopoietin-1, cancer, metastasis, Animals, Humans, Orphan receptor, Neovascularization, Pathologic, business.industry, angiopoietin–Tie signaling, Receptor, TIE-1, medicine.disease, Primary tumor, Receptor, TIE-2, Extravasation, endothelial cells, 3. Good health, 030104 developmental biology, Cancer research, Molecular Medicine, business, 030217 neurology & neurosurgery, Gene Deletion

Abstract

The angiopoietin (Ang)–Tie pathway has been intensely pursued as candidate second‐generation anti‐angiogenic target. While much of the translational work has focused on the ligand Ang2, the clinical efficacy of Ang2‐targeting drugs is limited and failed to improve patient survival. In turn, the orphan receptor Tie1 remains therapeutically unexplored, although its endothelial‐specific genetic deletion has previously been shown to result in a strong reduction in metastatic growth. Here, we report a novel Tie1 function‐blocking antibody (AB‐Tie1‐39), which suppressed postnatal retinal angiogenesis. During primary tumor growth, neoadjuvant administration of AB‐Tie1‐39 strongly impeded systemic metastasis. Furthermore, the administration of AB‐Tie1‐39 in a perioperative therapeutic window led to a significant survival advantage as compared to control‐IgG‐treated mice. Additional in vivo experimental metastasis and in vitro transmigration assays concurrently revealed that AB‐Tie1‐39 treatment suppressed tumor cell extravasation at secondary sites. Taken together, the data phenocopy previous genetic work in endothelial Tie1 KO mice and thereby validate AB‐Tie1‐39 as a Tie1 function‐blocking antibody. The study establishes Tie1 as a therapeutic target for metastasis in a perioperative or neoadjuvant setting., The Angiopoietin‐Tie signaling pathway maintains vascular quiescence and is often dysregulated during tumor progression. A novel Tie1 function‐blocking antibody (AB‐Tie1‐39) shows anti‐metastatic efficacy and prolonged survival of preclinical metastasis models.