Your search keyword '"Kenn Holmbeck"' showing total 3 results

1. A CCR2 macrophage endocytic pathway mediates extravascular fibrin clearance in vivo

Author

Daniel H. Madsen, Roberto Weigert, Kenn Holmbeck, Matthew J. Flick, David E. Spencer, Michael P. Motley, Daniel A. Lawrence, Thomas H. Bugge, Francis J. Castellino, Roman Szabo, and Henrik J. Jürgensen

Subjects

0301 basic medicine, Receptors, Peptide, Receptors, CCR2, Immunology, Endocytic cycle, Plenary Paper, CX3C Chemokine Receptor 1, Inflammation, Endocytosis, Biochemistry, Fibrin, Collagen receptor, 03 medical and health sciences, Mice, Plasminogen Activators, 0302 clinical medicine, Inside BLOOD Commentary, medicine, Animals, Myeloid Cells, Fibrinolysin, Cell Proliferation, biology, Chemistry, Macrophages, Plasminogen, Cell Biology, Hematology, Molecular biology, Cell biology, 030104 developmental biology, 030220 oncology & carcinogenesis, Proteolysis, biology.protein, Biological Assay, Receptors, Chemokine, medicine.symptom, Plasminogen activator, Mannose receptor, medicine.drug, circulatory and respiratory physiology

Abstract

Extravascular fibrin deposition accompanies many human diseases and causes chronic inflammation and organ damage, unless removed in a timely manner. Here, we used intravital microscopy to investigate how fibrin is removed from extravascular space. Fibrin placed into the dermis of mice underwent cellular endocytosis and lysosomal targeting, revealing a novel intracellular pathway for extravascular fibrin degradation. A C-C chemokine receptor type 2 (CCR2)-positive macrophage subpopulation constituted the majority of fibrin-uptaking cells. Consequently, cellular fibrin uptake was diminished by elimination of CCR2-expressing cells. The CCR2-positive macrophage subtype was different from collagen-internalizing M2-like macrophages. Cellular fibrin uptake was strictly dependent on plasminogen and plasminogen activator. Surprisingly, however, fibrin endocytosis was unimpeded by the absence of the fibrin(ogen) receptors, αMβ2 and ICAM-1, the myeloid cell integrin-binding site on fibrin or the endocytic collagen receptor, the mannose receptor. The study identifies a novel fibrin endocytic pathway engaged in extravascular fibrin clearance and shows that interstitial fibrin and collagen are cleared by different subsets of macrophages employing distinct molecular pathways.

Published

2015

2. Membrane-type MMPs are indispensable for placental labyrinth formation and development

Author

Stacie Kahan, William D. Swaim, Susan S. Yamada, Patricia M. Zerfas, Marek Sramko, Mee-Young Son, Joanne Shi, Ludmila Szabova, and Kenn Holmbeck

Subjects

medicine.medical_specialty, Placenta, Immunology, Blotting, Western, Morphogenesis, Fluorescent Antibody Technique, Biology, Matrix metalloproteinase, Biochemistry, Immunoenzyme Techniques, Mice, Syncytiotrophoblast, Vasculogenesis, Pregnancy, Vascular Biology, Internal medicine, medicine, Matrix Metalloproteinase 14, Animals, Tissue homeostasis, Gene knockdown, Trophoblast, Matrix Metalloproteinase 15, Cell Biology, Hematology, Cell biology, Extracellular Matrix, medicine.anatomical_structure, Endocrinology, Ear, Inner, embryonic structures, Pregnancy, Animal, Female

Abstract

The membrane-type matrix metalloproteinases (MT-MMPs) are essential for pericellular matrix remodeling in late stages of development, as well as in growth and tissue homeostasis in postnatal life. Although early morphogenesis is perceived to involve substantial tissue remodeling, the roles of MT-MMPs in these processes are only partially characterized. Here we explore the functions of 2 prominently expressed MT-MMPs, MT1-MMP and MT2-MMP, and describe their roles in the process of placental morphogenesis. The fetal portion of the placenta, in particular the labyrinth (LA), displays strong overlapping expression of MT1-MMP and MT2-MMP, which is critical for syncytiotrophoblast formation and in turn for fetal vessels. Disruption of trophoblast syncytium formation consequently leads to developmental arrest with only a few poorly branched fetal vessels entering the LA causing embryonic death at embryonic day 11.5. Through knockdown of MMP expression, we demonstrate that either MT1-MMP or MT2-MMP is crucial specifically during development of the LA. In contrast, knockdown of MT-MMP activity after LA formation is compatible with development to term and postnatal life. Taken together these data identify essential but interchangeable roles for MT1-MMP or MT2-MMP in placental vasculogenesis and provide the first example of selective temporal and spatial MMP activity required for development of the mouse embryo.

Published

2010

3. Dlk-1 Regulates B Cell Development Through Altered Bone Marrow Stromal Microenvironment, Not by Affecting Hematopoitic Stem/Progenitor Cells

Author

Steven R. Bauer, Allison L Branchaw, Kenn Holmbeck, Heba Degheidy, and Edyta Pawelczyk

Subjects

Pathology, medicine.medical_specialty, Stromal cell, medicine.diagnostic_test, Immunology, Osteoblast, Cell Biology, Hematology, Biology, Biochemistry, Molecular biology, Flow cytometry, Haematopoiesis, medicine.anatomical_structure, medicine, Bone marrow, Progenitor cell, Stem cell, B cell

Abstract

Abstract 3465 Introduction: DLK-1(delta-like 1) is a member of the EGF-like homeotic protein family whose expression is known to influence cell fate decisions through cell-cell interactions. It is also known to influence the differentiation of bone marrow stromal cells (BMSC) and hematopoietic stem cells (HSC) in bone marrow. Recently, we reported the essential role of DLK-1 in B cell development, which showed that the absence of DLK-1 led to accumulation of the earliest B cell progenitors (pre-pro B cells or Fraction A (Fr A)) in bone marrow, an altered pattern of B cell development in the spleen, and an altered humoral immune response. The objective of this study was to determine whether alterations in the HSC compartment or the BMSC microenvironment contributed to Fr A accumulation in mdlk1−/− mice. Methods: The mdlk1−/− and wild type bone marrow osteoblast and HSC compartments were analyzed by multicolor flow cytometry and in vitro methyl-cellulose colony forming cell assays. Bone marrow harvested from mdlk1−/− and wild type mice was assessed for BMSCs colony forming efficiency (CFU-F) and cultured. Supernatants from cultured BMSCs were analyzed by protein arrays. Since osteoblasts are an important component of the bone marrow microenvironment, OPN+CD45-TER119-ALP+ osteoblasts were identified in the bone marrow and quantified by flow cytometry. Finally, the femurs of mdlk1−/− and wild type mice were analyzed by micro-computed tomography (uCT) scanning. Results: Using flow cytometry, we observed no statistically significant changes in the HSC and progenitor populations in the absence of DLK-1 in mice at 4 and 16 weeks of age. The results of methyl-cellulose assay confirmed the findings of flow cytometry experiments and showed no statistically significant differences in the number of CFU-G, CFU-GM, and CFU-M of 4 and 16 week old mdlk1−/− mice as compared to wild-type control mice. However, significant alterations in the microenvironment of the mdlkl −/− were observed. CFU-F efficiency of mdlk1−/− bone marrow BMSC isolated from 4 week old mice was significantly decreased when compared to age-matched controls. Furthermore, the uCT scans showed the mineral density of the femoral bone significantly decreased in 4 week old mdlk1−/− mice and the number of osteoblast cells analyzed by flow cytometry was decreased by 10%. The analysis of BMSC supernatants revealed a striking down regulation of factors associated with osteoblast function and differentiation such as osteoactivin, PF-4, Follstatin-like 1, Frizzled-6, IGF-1, M-CSF, DKK-1 and others. Conclusions: Our results indicate that accumulation of the earliest B cell progenitors with DLK-1 ablation is the result of multiple defects in the bone marrow microenvironment including decreased CFU-F, decreased number of osteoblasts, decreased bone mineral density or alterations in factors important for osteoblast function but not from increase in numbers of hematopoietic stem or progenitors cells. Our laboratory is investigating this further. Disclosures: Pawelczyk: Baxter Inc.: currently employed by Baxter Inc. Other.

Published

2012