Your search keyword '"Mark J. Solloway"' showing total 10 results

1. The Fibronectin–ILT3 Interaction Functions as a Stromal Checkpoint that Suppresses Myeloid Cells

Author

Jie Tang, Seth Malmersjö, Kevin J. Paavola, Geoffrey Horner, Bernard B. Allan, Lee B. Rivera, Jian Luo, Bin Fan, Vicky Y. Lin, Peirong Chen, Alan Kutach, Raj Haldankar, Julie M. Roda, Martina Molgora, Marco Colonna, Jer-Yuan Hsu, Kyle P. O'Hollaren, Chun Chu, Christina Song, Hung-I H. Chen, Joshua S. Lichtman, Zhen Zhang, Daniel D. Kaplan, Kalyani Mondal, Wenhui Liu, Avantika Kekatpure, Betty Chan Li, Shelley R. Starck, Wei Guo, Suzanne Christine Crawley, Mark J. Solloway, Nikolai A. Sharkov, Richard Ventura, and Yan Wang

Subjects

Cancer Research, Tumor microenvironment, Membrane Glycoproteins, Stromal cell, biology, Chemistry, Immunology, Cell Differentiation, Phenotype, Cell Line, Fibronectins, Cell biology, Fibronectin, Extracellular matrix, biology.protein, Humans, Myeloid Cells, Receptors, Immunologic, Antibody, LILRB4, Ex vivo

Abstract

Suppressive myeloid cells inhibit antitumor immunity by preventing T-cell responses. Immunoglobulin-like transcript 3 (ILT3; also known as LILRB4) is highly expressed on tumor-associated myeloid cells and promotes their suppressive phenotype. However, the ligand that engages ILT3 within the tumor microenvironment and renders tumor-associated myeloid cells suppressive is unknown. Using a screening approach, we identified fibronectin as a functional ligand for ILT3. The interaction of fibronectin with ILT3 polarized myeloid cells toward a suppressive state, and these effects were reversed with an ILT3-specific antibody that blocked the interaction of ILT3 with fibronectin. Furthermore, ex vivo treatment of human tumor explants with anti-ILT3 reprogrammed tumor-associated myeloid cells toward a stimulatory phenotype. Thus, the ILT3–fibronectin interaction represents a “stromal checkpoint” through which the extracellular matrix actively suppresses myeloid cells. By blocking this interaction, tumor-associated myeloid cells may acquire a stimulatory phenotype, potentially resulting in increased antitumor T-cell responses.

Published

2021

2. Antibody-mediated inhibition of GDF15-GFRAL activity reverses cancer cachexia in mice

Author

Van Phung, Higbee Jared Martin, Marilyn Wang, Rowena Suriben, Yan Wang, Dina A. Ayupova, Diana Li, Hung-I Harry Chen, Subhash D. Katewa, André O. White, Zhengyu Gao, Michele McEntee, Andrea Olland, Damodharan Lakshminarasimhan, Richard Ventura, Michael Chen, Julie Oeffinger, Jie Tang, Shelley R. Starck, Jer-Yuan Hsu, Darrin A. Lindhout, Pranali Taskar, Kalyani Mondal, Mark J. Solloway, Raj Haldankar, Avantika Kekatpure, Bernard B. Allan, and Betty Chan Li

Subjects

0301 basic medicine, medicine.medical_specialty, Cachexia, Glial Cell Line-Derived Neurotrophic Factor Receptors, Growth Differentiation Factor 15, Adipose tissue, Crystallography, X-Ray, Proto-Oncogene Mas, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Mice, 0302 clinical medicine, Lipid oxidation, Weight loss, Internal medicine, Cell Line, Tumor, Neoplasms, Weight Loss, medicine, Glial cell line-derived neurotrophic factor, Animals, Humans, Muscle, Skeletal, biology, business.industry, Proto-Oncogene Proteins c-ret, Skeletal muscle, Antibodies, Monoclonal, Lipid metabolism, General Medicine, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Adipose Tissue, 030220 oncology & carcinogenesis, Multiprotein Complexes, Adipose triglyceride lipase, biology.protein, Heterografts, Lipid Peroxidation, medicine.symptom, business, Signal Transduction

Abstract

Cancer cachexia is a highly prevalent condition associated with poor quality of life and reduced survival1. Tumor-induced perturbations in the endocrine, immune and nervous systems drive anorexia and catabolic changes in adipose tissue and skeletal muscle, hallmarks of cancer cachexia2-4. However, the molecular mechanisms driving cachexia remain poorly defined, and there are currently no approved drugs for the condition. Elevation in circulating growth differentiation factor 15 (GDF15) correlates with cachexia and reduced survival in patients with cancer5-8, and a GDNF family receptor alpha like (GFRAL)-Ret proto-oncogene (RET) signaling complex in brainstem neurons that mediates GDF15-induced weight loss in mice has recently been described9-12. Here we report a therapeutic antagonistic monoclonal antibody, 3P10, that targets GFRAL and inhibits RET signaling by preventing the GDF15-driven interaction of RET with GFRAL on the cell surface. Treatment with 3P10 reverses excessive lipid oxidation in tumor-bearing mice and prevents cancer cachexia, even under calorie-restricted conditions. Mechanistically, activation of the GFRAL-RET pathway induces expression of genes involved in lipid metabolism in adipose tissues, and both peripheral chemical sympathectomy and loss of adipose triglyceride lipase protect mice from GDF15-induced weight loss. These data uncover a peripheral sympathetic axis by which GDF15 elicits a lipolytic response in adipose tissue independently of anorexia, leading to reduced adipose and muscle mass and function in tumor-bearing mice.

Published

2020

3. Elevated Serum Amino Acids Induce a Subpopulation of Alpha Cells to Initiate Pancreatic Neuroendocrine Tumor Formation

Author

Derek K. Smith, Nisha Patel, Oded Foreman, Eric Stawiski, Noelyn M. Kljavin, Bernard B. Allan, Andrew S. Peterson, Steffen Durinck, Bence Sipos, Mark J. Solloway, and Lance Kates

Subjects

Blood Glucose, Male, PNET, Population, serum amino-acids, Alpha (ethology), Mice, Transgenic, Tumor initiation, Biology, medicine.disease_cause, pancreatic neuroendocrine tumor, Glucagon-Like Peptide-1 Receptor, General Biochemistry, Genetics and Molecular Biology, Alpha cell, Mice, Glucagon-Like Peptide 1, Report, Insulin-Secreting Cells, Receptors, Glucagon, medicine, Animals, Humans, Insulin, Amino Acids, Progenitor cell, education, PI3K/AKT/mTOR pathway, Mice, Knockout, lcsh:R5-920, education.field_of_study, GCGR, Glucagon, Adenoma, Islet Cell, Pancreatic Neoplasms, tumorigenesis, Neuroendocrine Tumors, Glucose, SLC38A7, Liver, Glucagon-Secreting Cells, SLC38A5, mTOR, Cancer research, Female, lcsh:Medicine (General), Carcinogenesis, Glucagon receptor, Signal Transduction

Abstract

Summary The cellular origin of sporadic pancreatic neuroendocrine tumors (PNETs) is obscure. Hormone expression suggests that these tumors arise from glucagon-producing alpha cells or insulin-producing β cells, but instability in hormone expression prevents linage determination. We utilize loss of hepatic glucagon receptor (GCGR) signaling to drive alpha cell hyperproliferation and tumor formation to identify a cell of origin and dissect mechanisms that drive progression. Using a combination of genetically engineered Gcgr knockout mice and GCGR-inhibiting antibodies, we show that elevated plasma amino acids drive the appearance of a proliferative population of SLC38A5+ embryonic progenitor-like alpha cells in mice. Further, we characterize tumors from patients with rare bi-allelic germline GCGR loss-of-function variants and find prominent tumor-cell-associated expression of the SLC38A5 paralog SLC7A8 as well as markers of active mTOR signaling. Thus, progenitor cells arise from adult alpha cells in response to metabolic signals and, when inductive signals are chronically present, drive tumor initiation., Graphical Abstract, Highlights GCGR inhibition induces an SLC38A5+ alpha cell population in aged mice An SLC38A5+ alpha cell subpopulation initiates pancreatic tumors in aged Gcgr−/− mice Tumors exhibit low mutational burden and response to mTOR inhibition by rapamycin Tumors in GCGR loss-of-function models lack immune cell infiltration, Smith et al. demonstrate that chronic mTOR signaling, driven by elevated serum amino acids, in Gcgr knockout mice promotes tumor initiation from an SLC38A5+ alpha cell subpopulation and supports tumor maintenance. Furthermore, they provide evidence that an SLC7A8+ alpha cell population contains the progenitors for human tumors in GCGR-mutant patients.

Published

2020

4. Congenital Asplenia in Mice and Humans with Mutations in a Pbx/Nkx2-5/p15 Module

Author

Licia Selleri, Ching Pin Chang, Terence D. Capellini, Chisa Hidaka, Nizar Mahlaoui, Matthew Koss, Andrea Brendolan, Matilde Saggese, Richard P. Harvey, Bertrand Boisson, Owen W.J. Prall, Ekaterina D. Bojilova, Mark J. Solloway, David A. Elliott, Elisa Lenti, Alexandre Bolze, and Jean-Laurent Casanova

Subjects

Male, Asplenia, Adolescent, Molecular Sequence Data, Mutation, Missense, Mice, Transgenic, Spleen, Biology, medicine.disease_cause, Article, General Biochemistry, Genetics and Molecular Biology, Mice, Transactivation, Downregulation and upregulation, Proto-Oncogene Proteins, medicine, Animals, Humans, Missense mutation, Exome, Amino Acid Sequence, Molecular Biology, Cells, Cultured, Cyclin-Dependent Kinase Inhibitor p15, Splenic Diseases, Homeodomain Proteins, Mutation, Gene Expression Profiling, Pre-B-Cell Leukemia Transcription Factor 1, fungi, Isolated congenital asplenia, Gene Expression Regulation, Developmental, Infant, Cell Biology, medicine.disease, Molecular biology, Pedigree, DNA-Binding Proteins, medicine.anatomical_structure, Homeobox Protein Nkx-2.5, Cancer research, Female, Splenic disease, Transcription Factors, Developmental Biology

Abstract

SummaryThe molecular determinants of spleen organogenesis and the etiology of isolated congenital asplenia (ICA), a life-threatening human condition, are unknown. We previously reported that Pbx1 deficiency causes organ growth defects including asplenia. Here, we show that mice with splenic mesenchyme-specific Pbx1 inactivation exhibit hyposplenia. Moreover, the loss of Pbx causes downregulation of Nkx2-5 and derepression of p15Ink4b in spleen mesenchymal progenitors, perturbing the cell cycle. Removal of p15Ink4b in Pbx1 spleen-specific mutants partially rescues spleen growth. By whole-exome sequencing of a multiplex kindred with ICA, we identify a heterozygous missense mutation (P236H) in NKX2-5 showing reduced transactivation in vitro. This study establishes that a Pbx/Nkx2-5/p15 regulatory module is essential for spleen development.

Published

2012

5. Chondroitin sulfate synthase 1 (Chsy1) is required for bone development and digit patterning

Author

Flavius Martin, Richard A.D. Carano, Lauri Diehl, Kai H. Barck, Deanna Grant Wilson, Andrew S. Peterson, Khanhky Phamluong, Mark J. Solloway, and Wei Yu Lin

Subjects

Cell, Regulator, Biology, Bone and Bones, Dermatan sulfate, Glycosaminoglycan, Extracellular matrix, Mice, chemistry.chemical_compound, Sulfation, Bone Density, Pregnancy, Chondroitin sulfate synthase 1, medicine, Animals, Humans, Chondroitin, Glucuronosyltransferase, Molecular Biology, Body Patterning, Bone Development, Brachydactyly, Glycosyltransferases, Cell Biology, Multifunctional Enzymes, Cell biology, Disease Models, Animal, medicine.anatomical_structure, chemistry, Biochemistry, N-Acetylgalactosaminyltransferases, Female, Joints, Gene Deletion, Developmental Biology

Abstract

Joint and skeletal development is highly regulated by extracellular matrix (ECM) proteoglycans, of which chondroitin sulfate proteoglycans (CSPGs) are a major class. Despite the requirement of joint CSPGs for skeletal flexibility and structure, relatively little is understood regarding their role in establishing joint positioning or in modulating signaling and cell behavior during joint formation. Chondroitin sulfate synthase 1 (Chsy1) is one of a family of enzymes that catalyze the extension of chondroitin and dermatan sulfate glycosaminoglycans. Recently, human syndromic brachydactylies have been described to have loss-of-function mutations at the CHSY1 locus. In concordance with these observations, we demonstrate that mice lacking Chsy1, though viable, display chondrodysplasia and decreased bone density. Notably, Chsy1−/− mice show a profound limb patterning defect in which orthogonally shifted ectopic joints form in the distal digits. Associated with the digit-patterning defect is a shift in cell orientation and an imbalance in chondroitin sulfation. Our results place Chsy1 as an essential regulator of joint patterning and provide a mouse model of human brachydactylies caused by mutations in CHSY1.

Published

2012

6. BMP/SMAD1 signaling sets a threshold for the left/right pathway in lateral plate mesoderm and limits availability of SMAD4

Author

Orit Wolstein, Christine Biben, Sally L. Dunwoodie, Milena B. Furtado, Jost I. Preis, Yumiko Saga, Mauro W. Costa, Mark J. Solloway, Richard P. Harvey, Vanessa Jones, Patrick P.L. Tam, Elizabeth J. Robertson, and Duncan B. Sparrow

Subjects

Mesoderm, animal structures, Nodal Protein, Nodal signaling, Bone morphogenetic protein, Cell Line, Smad1 Protein, Mice, Gene expression, Genetics, medicine, Animals, Humans, Body Patterning, Smad4 Protein, biology, Lateral plate mesoderm, Forkhead Transcription Factors, Transforming growth factor beta, Anatomy, Cell biology, medicine.anatomical_structure, Bone Morphogenetic Proteins, Mutation, embryonic structures, biology.protein, Signal transduction, NODAL, Signal Transduction, Research Paper, Developmental Biology

Abstract

Bistability in developmental pathways refers to the generation of binary outputs from graded or noisy inputs. Signaling thresholds are critical for bistability. Specification of the left/right (LR) axis in vertebrate embryos involves bistable expression of transforming growth factor β (TGFβ) member NODAL in the left lateral plate mesoderm (LPM) controlled by feed-forward and feedback loops. Here we provide evidence that bone morphogenetic protein (BMP)/SMAD1 signaling sets a repressive threshold in the LPM essential for the integrity of LR signaling. Conditional deletion of Smad1 in the LPM led to precocious and bilateral pathway activation. NODAL expression from both the left and right sides of the node contributed to bilateral activation, indicating sensitivity of mutant LPM to noisy input from the LR system. In vitro, BMP signaling inhibited NODAL pathway activation and formation of its downstream SMAD2/4–FOXH1 transcriptional complex. Activity was restored by overexpression of SMAD4 and in embryos, elevated SMAD4 in the right LPM robustly activated LR gene expression, an effect reversed by superactivated BMP signaling. We conclude that BMP/SMAD1 signaling sets a bilateral, repressive threshold for NODAL-dependent Nodal activation in LPM, limiting availability of SMAD4. This repressive threshold is essential for bistable output of the LR system.

Published

2008

7. Wnt Isoform-Specific Interactions with Coreceptor Specify Inhibition or Potentiation of Signaling by LRP6 Antibodies

Author

Yan Gong, Tim C. Cao, Bonnee Rubinfeld, Richard A.D. Carano, Paul Polakis, Cecilia Chiu, Bob Y. Liu, Eric Bourhis, Mark J. Solloway, James A. Ernst, Scott Stawicki, Rami N. Hannoush, Mike Costa, Khanhky Phamluong, Venita I. DeAlmeida, and Yan Wu

Subjects

Cell signaling, Frizzled, lcsh:Medicine, Down-Regulation, Biology, Receptor tyrosine kinase, Cell Biology/Cell Signaling, Antibodies, Cell Line, Receptors, G-Protein-Coupled, Mice, Species Specificity, Biochemistry/Cell Signaling and Trafficking Structures, Animals, Humans, Protein Isoforms, Autocrine signalling, lcsh:Science, LDL-Receptor Related Proteins, Multidisciplinary, lcsh:R, Wnt signaling pathway, LRP6, LRP5, Cell biology, Up-Regulation, Wnt Proteins, Low Density Lipoprotein Receptor-Related Protein-6, biology.protein, lcsh:Q, WNT3A, Research Article, Biotechnology, Protein Binding, Signal Transduction

Abstract

β-catenin-dependent Wnt signaling is initiated as Wnt binds to both the receptor FZD and coreceptor LRP5/6, which then assembles a multimeric complex at the cytoplasmic membrane face to recruit and inactivate the kinase GSK3. The large number and sequence diversity of Wnt isoforms suggest the possibility of domain-specific ligand-coreceptor interactions, and distinct binding sites on LRP6 for Wnt3a and Wnt9b have recently been identified in vitro. Whether mechanistically different interactions between Wnts and coreceptors might mediate signaling remains to be determined. It is also not clear whether coreceptor homodimerization induced extracellularly can activate Wnt signaling, as is the case for receptor tyrosine kinases. We generated monoclonal antibodies against LRP6 with the unexpected ability to inhibit signaling by some Wnt isoforms and potentiate signaling by other isoforms. In cell culture, two antibodies characterized further show reciprocal activities on most Wnts, with one antibody antagonizing and the other potentiating. We demonstrate that these antibodies bind to different regions of LRP6 protein, and inhibition of signaling results from blocking Wnt binding. Antibody-mediated dimerization of LRP6 can potentiate signaling only when a Wnt isoform is also able to bind the complex, presumably recruiting FZD. Endogenous autocrine Wnt signaling in different tumor cell lines can be either antagonized or enhanced by the LRP6 antibodies, indicating expression of different Wnt isoforms. As anticipated from the roles of Wnt signaling in cancer and bone development, antibody activities can also be observed in mice for inhibition of tumor growth and in organ culture for enhancement of bone mineral density. Collectively, our results indicate that separate binding sites for different subsets of Wnt isoforms determine the inhibition or potentiation of signaling conferred by LRP6 antibodies. This complexity of coreceptor-ligand interactions may allow for differential regulation of signaling by Wnt isoforms during development, and can be exploited with antibodies to differentially manipulate Wnt signaling in specific tissues or disease states.

Published

2010

8. Wnt Signaling Is Regulated by Endoplasmic Reticulum Retention

Author

Youngshik Choe, J. Susie Zoltewicz, Gena Lee, Mark J. Solloway, Amir M. Ashique, Andrew S. Peterson, Stacy Taylor, and Khanhky Phamluong

Subjects

animal structures, Genetics and Genomics/Animal Genetics, lcsh:Medicine, Biology, Bioinformatics, Endoplasmic Reticulum, Polymerase Chain Reaction, Developmental Biology/Pattern Formation, 03 medical and health sciences, Mice, 0302 clinical medicine, Cell Biology/Membranes and Sorting, Developmental Biology/Developmental Molecular Mechanisms, Phospholipase D, Animals, Humans, lcsh:Science, Secretory pathway, Cells, Cultured, 030304 developmental biology, Developmental Biology/Embryology, DNA Primers, 0303 health sciences, Multidisciplinary, Base Sequence, Endoplasmic reticulum, lcsh:R, Wnt signaling pathway, LRP6, ER retention, LRP5, Neuroscience/Neurodevelopment, Cell biology, Developmental Biology/Neurodevelopment, Mice, Inbred C57BL, Wnt Proteins, Gene Knockdown Techniques, embryonic structures, Mutation, lcsh:Q, sense organs, Signal transduction, 030217 neurology & neurosurgery, WNT3A, Research Article, Signal Transduction

Abstract

Precise regulation of Wnt signaling is important in many contexts, as in development of the vertebrate forebrain, where excessive or ectopic Wnt signaling leads to severe brain defects. Mutation of the widely expressed oto gene causes loss of the anterior forebrain during mouse embryogenesis. Here we report that oto is the mouse ortholog of the gpi deacylase gene pgap1, and that the endoplasmic reticulum (ER)-resident Oto protein has a novel and deacylase-independent function during Wnt maturation. Oto increases the hydrophobicities of Wnt3a and Wnt1 by promoting the addition of glycophosphatidylinositol (gpi)-like anchors to these Wnts, which results in their retention in the ER. We also report that oto-deficient embryos exhibit prematurely robust Wnt activity in the Wnt1 domain of the early neural plate. We examine the effect of low oto expression on Wnt1 in vitro by knocking down endogenous oto expression in 293 and M14 melanoma cells using shRNA. Knockdown of oto results in increased Wnt1 secretion which is correlated with greatly enhanced canonical Wnt activity. These data indicate that oto deficiency increases Wnt signaling in vivo and in vitro. Finally, we address the mechanism of Oto-mediated Wnt retention under oto-abundant conditions, by cotransfecting Wnt1 with gpi-specific phospholipase D (GPI-PLD). The presence of GPI-PLD in the secretory pathway results in increased secretion of soluble Wnt1, suggesting that the gpi-like anchor lipids on Wnt1 mediate its retention in the ER. These data now provide a mechanistic framework for understanding the forebrain defects in oto mice, and support a role for Oto-mediated Wnt regulation during early brain development. Our work highlights a critical role for ER retention in regulating Wnt signaling in the mouse embryo, and gives insight into the notoriously inefficient secretion of Wnts.

Published

2009

9. Homeodomain factor Nkx2-5 in heart development and disease

Author

Mauro W. Costa, Christine Biben, C. Hyun, Fiona A. Stennard, D. Lai, T. Yeoh, N. Groves, Mark J. Solloway, Richard P. Harvey, Aaron Schindeler, L. Lavulo, David A. Elliott, Edwin P. Kirk, Owen W.J. Prall, and Milena B. Furtado

Subjects

Heart Defects, Congenital, Homeodomain Proteins, Mice, Knockout, Heart development, business.industry, Genes, Homeobox, Models, Cardiovascular, Gene Expression Regulation, Developmental, Disease, Biology, Xenopus Proteins, Bioinformatics, Biochemistry, Mice, Text mining, Fetal Heart, Genetics, Homeobox Protein Nkx-2.5, Homeobox, Animals, Humans, business, Molecular Biology, Body Patterning, Transcription Factors

Published

2003

10. Molecular pathways in myocardial development: a stem cell perspective

Author

Mark J. Solloway and Richard P. Harvey

Subjects

Pathology, medicine.medical_specialty, Physiology, Cellular differentiation, Heart Ventricles, Biology, Cell therapy, Physiology (medical), Proto-Oncogene Proteins, medicine, Morphogenesis, Animals, Humans, Heart Atria, Embryonic Induction, Heart development, Regeneration (biology), Endogenous regeneration, Heart, Zebrafish Proteins, medicine.disease, Fibroblast Growth Factors, Wnt Proteins, Gene Expression Regulation, Heart failure, Bone Morphogenetic Proteins, Models, Animal, Vertebrates, Stem cell, Cardiology and Cardiovascular Medicine, Neuroscience, Myoblasts, Cardiac, Transcription Factors

Abstract

The heart has long been considered to adapt to increased work or pathology through the cellular growth process of hypertrophy. However, recent evidence for the existence of endogenous stem cells and regenerative capacity in the adult heart has given new impetus to the quest for cell therapies for heart failure, which remains the number one killer in Western cultures. The molecular cues driving cardiac development are now being explored in detail and will come into sharp focus as regimes for stem cell differentiation and efforts to augment endogenous regeneration are trialed. This review briefly outlines the current state of knowledge on the molecular basis of the four modalities of myogenesis that have been identified in the developing vertebrate heart. Stem cell-mediated myogenic repair in the heart represents a fifth modality, and an exciting frontier with basic and practical implications that remain to be explored.

Published

2003