Your search keyword '"Kropf, Pascale"' showing total 15 results

1. Arginase activity in the blood of patients with visceral leishmaniasis and HIV infection.

Author

Takele Y, Abebe T, Weldegebreal T, Hailu A, Hailu W, Hurissa Z, Ali J, Diro E, Sisay Y, Cloke T, Modolell M, Munder M, Tacchini-Cottier F, Müller I, and Kropf P

Subjects

Adolescent, Adult, Coinfection diagnosis, Coinfection pathology, Cross-Sectional Studies, Ethiopia, HIV Infections diagnosis, Humans, Leishmaniasis, Visceral diagnosis, Male, Severity of Illness Index, Young Adult, Arginase blood, Biomarkers blood, HIV Infections complications, HIV Infections pathology, Leishmaniasis, Visceral complications, Leishmaniasis, Visceral pathology

Abstract

Background: Visceral leishmaniasis is a parasitic disease associated with high mortality. The most important foci of visceral leishmaniasis in Ethiopia are in the Northwest and are predominantly associated with high rates of HIV co-infection. Co-infection of visceral leishmaniasis patients with HIV results in higher mortality, treatment failure and relapse. We have previously shown that arginase, an enzyme associated with immunosuppression, was increased in patients with visceral leishmaniasis and in HIV seropositive patients; further our results showed that high arginase activity is a marker of disease severity. Here, we tested the hypothesis that increased arginase activities associated with visceral leishmaniasis and HIV infections synergize in patients co-infected with both pathogens., Methodology/principal Findings: We recruited a cohort of patients with visceral leishmaniasis and a cohort of patients with visceral leishmaniasis and HIV infection from Gondar, Northwest Ethiopia, and recorded and compared their clinical data. Further, we measured the levels of arginase activity in the blood of these patients and identified the phenotype of arginase-expressing cells. Our results show that CD4(+) T cell counts were significantly lower and the parasite load in the spleen was significantly higher in co-infected patients. Moreover, our results demonstrate that arginase activity was significantly higher in peripheral blood mononuclear cells and plasma of co-infected patients. Finally, we identified the cells-expressing arginase in the PBMCs as low-density granulocytes., Conclusion: Our results suggest that increased arginase might contribute to the poor disease outcome characteristic of patients with visceral leishmaniasis and HIV co-infection.

Published

2013

2. Arginase activity - a marker of disease status in patients with visceral leishmaniasis in ethiopia.

Author

Abebe T, Takele Y, Weldegebreal T, Cloke T, Closs E, Corset C, Hailu A, Hailu W, Sisay Y, Corware K, Corset M, Modolell M, Munder M, Tacchini-Cottier F, Müller I, and Kropf P

Subjects

Adolescent, Adult, Arginine blood, CD3 Complex analysis, Ethiopia, Humans, Male, Neutrophils immunology, T-Lymphocytes chemistry, Young Adult, Arginase blood, Biomarkers analysis, Immune Tolerance, Leishmaniasis, Visceral diagnosis, Leishmaniasis, Visceral immunology

Abstract

The underlying mechanisms resulting in the profound immune suppression characteristic of human visceral leishmaniasis (VL) are not fully understood. Here, we tested the hypothesis that arginase, an enzyme associated with immunosuppression, is higher in patients with VL and contributes to impaired T cell responses. We recruited patients with VL before and after treatment and healthy controls and measured the arginase metabolism in the blood of these individuals. Our results show that arginase activity is significantly higher in the blood of patients with active VL as compared to controls. These high levels of arginase decline considerably once the patients are successfully treated. We identified the phenotype of arginase-expressing cells among PBMCs as neutrophils and show that their frequency was increased in PBMCs of patients before treatment; this coincides with reduced levels of L-arginine in the plasma and decreased expression levels of CD3ζ in T cells.

Published

2013

3. Local increase of arginase activity in lesions of patients with cutaneous leishmaniasis in Ethiopia.

Author

Abebe T, Hailu A, Woldeyes M, Mekonen W, Bilcha K, Cloke T, Fry L, Seich Al Basatena NK, Corware K, Modolell M, Munder M, Tacchini-Cottier F, Müller I, and Kropf P

Subjects

Adolescent, Adult, Biopsy, CD3 Complex analysis, CD4 Antigens analysis, CD8 Antigens analysis, Child, Ethiopia, Female, Humans, Leukocytes, Mononuclear chemistry, Leukocytes, Mononuclear enzymology, Male, Middle Aged, Young Adult, Arginase metabolism, Leishmaniasis, Cutaneous pathology, Skin enzymology, Skin pathology

Abstract

Background: Cutaneous leishmaniasis is a vector-borne disease that is in Ethiopia mainly caused by the parasite Leishmania aethiopica. This neglected tropical disease is common in rural areas and causes serious morbidity. Persistent nonhealing cutaneous leishmaniasis has been associated with poor T cell mediated responses; however, the underlying mechanisms are not well understood., Methodology/principal Findings: We have recently shown in an experimental model of cutaneous leishmaniasis that arginase-induced L-arginine metabolism suppresses antigen-specific T cell responses at the site of pathology, but not in the periphery. To test whether these results translate to human disease, we recruited patients presenting with localized lesions of cutaneous leishmaniasis and assessed the levels of arginase activity in cells isolated from peripheral blood and from skin biopsies. Arginase activity was similar in peripheral blood mononuclear cells (PBMCs) from patients and healthy controls. In sharp contrast, arginase activity was significantly increased in lesion biopsies of patients with localized cutaneous leishmaniasis as compared with controls. Furthermore, we found that the expression levels of CD3ζ, CD4 and CD8 molecules were considerably lower at the site of pathology as compared to those observed in paired PBMCs., Conclusion: Our results suggest that increased arginase in lesions of patients with cutaneous leishmaniasis might play a role in the pathogenesis of the disease by impairing T cell effector functions.

Published

2012

4. Arginine depletion as a mechanism for the immune privilege of corneal allografts.

Author

Fu H, Khan A, Coe D, Zaher S, Chai JG, Kropf P, Müller I, Larkin DF, and George AJ

Subjects

Animals, Arginase metabolism, Arginine administration & dosage, Arginine analogs & derivatives, Arginine pharmacology, CD4-Positive T-Lymphocytes metabolism, Cell Proliferation drug effects, Cells, Cultured, Endothelium, Corneal immunology, Endothelium, Corneal metabolism, Epithelium, Corneal immunology, Epithelium, Corneal metabolism, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Polymerase Chain Reaction, Skin Transplantation, Transplantation, Homologous, Arginase antagonists & inhibitors, Arginine metabolism, Cornea immunology, Corneal Transplantation, Graft Survival

Abstract

The cornea is an immune privileged tissue. Since arginase has been found to modulate T-cell function by depleting arginine, we investigated the expression of arginase in the cornea and its possible role in immune privilege using a murine transplant model. We found that both the endothelium and epithelium of murine corneas express functional arginase I, capable of down-regulating T-cell proliferation in an in vitro culture system. The administration of the specific arginase inhibitor N-hydroxy-nor-L-Arg to recipient mice resulted in an accelerated rejection of allogeneic C57BL/6 (B6) corneal grafts. In contrast, in vivo blockade of arginase activity had no effect in altering the course of rejection of primary skin grafts that express little, if any, arginase. In addition, the inhibition of arginase did not alter systemic T-cell proliferation. These data show that arginase is functional in the cornea and contributes to the immune privilege of the eye, and that modulation of arginase contributes to graft survival., (Copyright © 2011 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2011

5. Human eosinophil granulocytes do not express the enzyme arginase.

Author

Luckner-Minden C, Fischer I, Langhans CD, Schiller M, Kropf P, Müller I, Hohlfeld JM, Ho AD, and Munder M

Subjects

Adult, Allergens pharmacology, Arginine metabolism, Asthma immunology, Asthma pathology, Bronchoalveolar Lavage, Eosinophils drug effects, Humans, Immunosuppression Therapy, Middle Aged, Ornithine metabolism, Young Adult, Arginase metabolism, Asthma enzymology, Eosinophils enzymology

Abstract

Human polymorphonuclear PMN constitutively express the enzyme arginase I, which hydrolyzes arginine to ornithine and urea. This arginine consumption has been recognized as a key pathway of myeloid cell-mediated suppression of the adaptive immune system during inflammation, infection, and tumor growth. Eos granulocytes are crucial immunoregulatory and effector cells of allergic inflammation and infections with parasites and helminths and in a variety of tumors. Here, we analyzed if human Eos also express arginase with its potential immunosuppressive consequences. We show that human peripheral blood Eos do not express arginase I or II protein or arginase enzymatic activity. Correspondingly, no metabolism of arginine to ornithine can be detected in Eos-S. Neither Eos apoptosis nor cytokine-mediated cellular activation induces arginase in human Eos in vitro. Finally, we show that arginase activity and protein are also undetectable in Eos of allergic patients from peripheral blood or from BALF activated in vivo during allergic pulmonary inflammation. This work demonstrates a fundamental difference between neutrophil and Eos granulocytes. As Eos are not equipped with the immunosuppressive enzyme arginase, they cannot participate, via arginine limitation, in the suppression of the evolving adaptive immune response in allergy, infections, or tumor immunity.

Published

2010

6. Local suppression of T cell responses by arginase-induced L-arginine depletion in nonhealing leishmaniasis.

Author

Modolell M, Choi BS, Ryan RO, Hancock M, Titus RG, Abebe T, Hailu A, Müller I, Rogers ME, Bangham CR, Munder M, and Kropf P

Subjects

Animals, Cell Proliferation, Female, Foot pathology, Immune Tolerance, Interferon-gamma metabolism, Lymph Nodes pathology, Mice, Mice, Inbred BALB C, Mice, Inbred CBA, Arginase metabolism, Arginine metabolism, Leishmaniasis immunology, Leishmaniasis metabolism, T-Lymphocytes immunology

Abstract

The balance between T helper (Th) 1 and Th2 cell responses is a major determinant of the outcome of experimental leishmaniasis, but polarized Th1 or Th2 responses are not sufficient to account for healing or nonhealing. Here we show that high arginase activity, a hallmark of nonhealing disease, is primarily expressed locally at the site of pathology. The high arginase activity causes local depletion of L-arginine, which impairs the capacity of T cells in the lesion to proliferate and to produce interferon-gamma, while T cells in the local draining lymph nodes respond normally. Healing, induced by chemotherapy, resulted in control of arginase activity and reversal of local immunosuppression. Moreover, competitive inhibition of arginase as well as supplementation with L-arginine restored T cell effector functions and reduced pathology and parasite growth at the site of lesions. These results demonstrate that in nonhealing leishmaniasis, arginase-induced L-arginine depletion results in impaired T cell responses. Our results identify a novel mechanism in leishmaniasis that contributes to the failure to heal persistent lesions and suggest new approaches to therapy.

Published

2009

7. Regulation of NK cell function by human granulocyte arginase.

Author

Oberlies J, Watzl C, Giese T, Luckner C, Kropf P, Müller I, Ho AD, and Munder M

Subjects

Arginine deficiency, Arginine physiology, Cell Proliferation, Cell Survival immunology, Cells, Cultured, Exocytosis immunology, Growth Inhibitors physiology, Humans, K562 Cells, Killer Cells, Natural cytology, Killer Cells, Natural metabolism, Neutrophils metabolism, Arginase physiology, Cytotoxicity, Immunologic immunology, Immunosuppression Therapy, Killer Cells, Natural enzymology, Killer Cells, Natural immunology, Lymphocyte Activation immunology, Neutrophils enzymology, Neutrophils immunology

Abstract

The arginine-hydrolyzing enzyme arginase is constitutively expressed by human polymorphonuclear granulocytes (PMN). Upon PMN cell death arginase is liberated and depletes arginine in the microenvironment. This amino acid depletion suppresses T cell proliferation and cytokine secretion and emerges as a key mechanism of immunosuppression during chronic inflammation and tumor growth. Here we show that PMN arginase also severely impairs key functions of primary human NK cells as well as IL-2-activated NK cells. In the absence of arginine, NK cell proliferation and IL-12/IL-18-induced secretion of IFN-gamma are severely diminished. In contrast, NK cell viability, granule exocytosis, and cytotoxicity are independent of extracellular arginine. The mechanism of NK cell suppression by arginine depletion is posttranscriptional since mRNA transcript frequency is unaffected upon NK cell activation in the absence of arginine. Finally, we demonstrate that human purulent exudate ex vivo inhibits NK cell functions exclusively due to liberated arginase. Arginase inhibitors are therefore promising pharmacological agents to treat unwanted suppression of the innate (NK cell) as well as the adaptive (T cell) immune system.

Published

2009

8. Age-related alteration of arginase activity impacts on severity of leishmaniasis.

Author

Müller I, Hailu A, Choi BS, Abebe T, Fuentes JM, Munder M, Modolell M, and Kropf P

Subjects

Age Distribution, Age Factors, Animals, Blotting, Western, CD4-Positive T-Lymphocytes cytology, CD4-Positive T-Lymphocytes metabolism, Cell Proliferation, Cells, Cultured, Enzyme-Linked Immunosorbent Assay, Ethiopia epidemiology, Female, Flow Cytometry, Leishmaniasis immunology, Leishmaniasis, Cutaneous enzymology, Leishmaniasis, Cutaneous epidemiology, Leishmaniasis, Cutaneous immunology, Leishmaniasis, Visceral enzymology, Leishmaniasis, Visceral epidemiology, Leishmaniasis, Visceral immunology, Macrophages metabolism, Macrophages parasitology, Mice, Mice, Inbred BALB C, Arginase metabolism, Leishmaniasis enzymology, Leishmaniasis epidemiology

Abstract

Background: The leishmaniases are a group of vector-borne parasitic diseases that represent a major international public health problem; they belong to the most neglected tropical diseases and have one of the highest rates of morbidity and mortality. The clinical outcome of infection with Leishmania parasites depends on a variety of factors such as parasite species, vector-derived products, genetics, behaviour, and nutrition. The age of the infected individuals also appears to be critical, as a significant proportion of clinical cases occur in children; this age-related higher prevalence of disease is most remarkable in visceral leishmaniasis. The mechanisms resulting in this higher incidence of clinical disease in children are poorly understood. We have recently revealed that sustained arginase activity promotes uncontrolled parasite growth and pathology in vivo. Here, we tested the hypothesis that arginase-mediated L-arginine metabolism differs with age., Methodology: The age distribution of patients with visceral or cutaneous leishmaniasis was determined in cohorts of patients in our clinics in endemic areas in Ethiopia. To exclude factors that are difficult to control in patients, we assessed the impact of ageing on the manifestations of experimental leishmaniasis. We determined parasite burden, T cell responses, and macrophage effector functions in young and aged mice during the course of infection., Results: Our results show that younger mice develop exacerbated lesion pathology and higher parasite burdens than aged mice. This aggravated disease development in younger individuals does not correlate with a change in T helper cytokine profile. To address the underlying mechanisms responsible for the more severe infections in younger mice, we investigated macrophage effector functions. Our results show that macrophages from younger mice do not have an impaired capacity to kill parasites; however, they express significantly higher levels of arginase 1 than aged mice and promote parasite growth more efficiently. Thus, our results demonstrate that ageing differentially impacts on L-arginine metabolism and subsequent effector functions of physiologically distinct macrophage subsets., Conclusions: Here, we show that arginase-mediated L-arginine metabolism is modulated with age and affects the capacity of macrophages to express arginase; the increased capacity to upregulate this enzyme in younger individuals results in a more permissive environment for parasite growth, increased disease severity and pathology. These results suggest that the difference in arginase-mediated L-arginine catabolism is likely to be an important factor contributing to the increased incidence of clinical cases in children. Thus, targeting L-arginine metabolism might be a promising therapeutic strategy against leishmaniasis, especially in children and young adults.

Published

2008

9. Arginase activity mediates reversible T cell hyporesponsiveness in human pregnancy.

Author

Kropf P, Baud D, Marshall SE, Munder M, Mosley A, Fuentes JM, Bangham CR, Taylor GP, Herath S, Choi BS, Soler G, Teoh T, Modolell M, and Müller I

Subjects

Adult, Arginase biosynthesis, Arginine metabolism, Cells, Cultured, Enzyme Activation immunology, Female, Humans, Placenta enzymology, Pregnancy, Pregnancy Proteins biosynthesis, T-Lymphocytes metabolism, Arginase physiology, Immune Tolerance, Pregnancy Proteins physiology, T-Lymphocytes enzymology, T-Lymphocytes immunology

Abstract

Complex regulation of T cell functions during pregnancy is required to ensure materno-fetal tolerance. Here we reveal a novel pathway for the temporary suppression of maternal T cell responses in uncomplicated human pregnancies. Our results show that arginase activity is significantly increased in the peripheral blood of pregnant women and remarkably high arginase activities are expressed in term placentae. High enzymatic activity results in high turnover of its substrate L-arginine and concomitant reduction of this amino acid in the microenvironment. Amino acid deprivation is emerging as a regulatory pathway of lymphocyte responses and we assessed the consequences of this enhanced arginase activity on T cell responses. Arginase-mediated L-arginine depletion induces down-regulation of CD3 zeta, the main signalling chain of the TCR, and functional T cell hyporesponsiveness. Importantly, this arginase-mediated T cell suppression was reversible, as inhibition of arginase activity or addition of exogenous L-arginine restored CD3 zeta chain expression and T cell proliferation. Thus, L-arginine metabolism constitutes a novel physiological mechanism contributing to the temporary suppression of the maternal immune response during human pregnancy.

Published

2007

10. Suppression of T-cell functions by human granulocyte arginase.

Author

Munder M, Schneider H, Luckner C, Giese T, Langhans CD, Fuentes JM, Kropf P, Mueller I, Kolb A, Modolell M, and Ho AD

Subjects

Arginase genetics, Arginine metabolism, Humans, Immunosuppression Therapy methods, Lymphocyte Activation drug effects, Neutrophils enzymology, Neutrophils immunology, Reverse Transcriptase Polymerase Chain Reaction, T-Lymphocytes drug effects, Arginase pharmacology, Granulocytes enzymology, Lymphocyte Activation immunology, T-Lymphocytes immunology

Abstract

Chronic inflammation is accompanied by impaired T-cell immunity. In the mouse, myeloid cell-associated arginase accounts for the suppression of immune reactivity in various models of tumor growth and chronic infections. Here we show that arginase I is liberated from human granulocytes, and very high activities accumulate extracellularly during purulent inflammatory reactions. Human granulocyte arginase induces a profound suppression of T-cell proliferation and cytokine synthesis. This T-cell phenotype is due to arginase-mediated depletion of arginine in the T-cell environment, which leads to CD3zeta chain down-regulation but does not alter T-cell viability. Our study therefore demonstrates that human granulocytes possess a previously unanticipated immunosuppressive effector function. Human granulocyte arginase is a promising pharmacologic target to reverse unwanted immunosuppression.

Published

2006

11. Arginase and polyamine synthesis are key factors in the regulation of experimental leishmaniasis in vivo.

Author

Kropf P, Fuentes JM, Fähnrich E, Arpa L, Herath S, Weber V, Soler G, Celada A, Modolell M, and Müller I

Subjects

Animals, Arginase antagonists & inhibitors, Arginase genetics, Arginine metabolism, Bone Marrow Cells, Enzyme Inhibitors pharmacology, Leishmania major enzymology, Leishmaniasis, Cutaneous parasitology, Leishmaniasis, Cutaneous therapy, Macrophage Activation, Macrophages metabolism, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Mice, Inbred CBA, Polymerase Chain Reaction, RNA, Messenger analysis, Th1 Cells immunology, Th2 Cells immunology, Arginase physiology, Leishmania major growth & development, Leishmaniasis, Cutaneous enzymology, Polyamines metabolism

Abstract

Arginase 1, an enzyme induced by Th2 cytokines, is a hallmark of alternatively activated macrophages and is responsible for the hydrolysis of L-arginine into ornithine, the building block for the production of polyamines. Upregulation of arginase 1 has been observed in a variety of diseases, but the mechanisms by which arginase contributes to pathology are not well understood. We reveal here a unique role for arginase 1 in the pathogenesis of nonhealing leishmaniasis, a prototype Th2 disease, and demonstrate that the activity of this enzyme promotes pathology and uncontrolled growth of Leishmania parasites in vivo. Inhibition of arginase activity during the course of infection has a clear therapeutic effect, as evidenced by markedly reduced pathology and efficient control of parasite replication. Despite the clear amelioration of the disease, this treatment does not alter the Th2 response. To address the underlying mechanisms, the arginase-induced L-arginine catabolism was investigated and the results demonstrate that arginase regulates parasite growth directly by affecting the polyamine synthesis in macrophages.

Published

2005

12. Protein energy malnutrition increases arginase activity in monocytes and macrophages

Author

Corware, Karina, Yardley, Vanessa, Mack, Christopher, Schuster, Steffen, Al-Hassi, Hafid, Herath, Shanthi, Bergin, Philip, Modolell, Manuel, Munder, Markus, Müller, Ingrid, and Kropf, Pascale

Subjects

Nutrition and Dietetics, Science & Technology, Nutrition & Dietetics, Arginase, Research, Endocrinology, Diabetes and Metabolism, Macrophages, IMMUNE, Medicine (miscellaneous), Monocytes, Nitric oxide, Leishmaniasis, MALNOURISHED CHILDREN, INFLAMMATION, MURINE MACROPHAGES, INFECTION, ARGININE METABOLISM, VISCERAL LEISHMANIASIS, SUPPRESSOR-CELLS, NUTRITION, Life Sciences & Biomedicine, PLASMA AMINO-ACIDS

Abstract

Background Protein energy malnutrition is commonly associated with immune dysfunctions and is a major factor in susceptibility to infectious diseases. Methods In this study, we evaluated the impact of protein energy malnutrition on the capacity of monocytes and macrophages to upregulate arginase, an enzyme associated with immunosuppression and increased pathogen replication. Results Our results show that monocytes and macrophages are significantly increased in the bone marrow and blood of mice fed on a protein low diet. No alteration in the capacity of bone marrow derived macrophages isolated from malnourished mice to phagocytose particles, to produce the microbicidal molecule nitric oxide and to kill intracellular Leishmania parasites was detected. However, macrophages and monocytes from malnourished mice express significantly more arginase both in vitro and in vivo. Using an experimental model of visceral leishmaniasis, we show that following protein energy malnutrition, the increased parasite burden measured in the spleen of these mice coincided with increased arginase activity and that macrophages provide a more permissive environment for parasite growth. Conclusions Taken together, these results identify a novel mechanism in protein energy malnutrition that might contributes to increased susceptibility to infectious diseases by upregulating arginase activity in myeloid cells. Electronic supplementary material The online version of this article (doi:10.1186/1743-7075-11-51) contains supplementary material, which is available to authorized users.

Published

2014

13. L-arginine deprivation impairs Leishmania major-specific T-cell responses

Author

Munder, Markus, Choi, Beak-San, Rogers, Matthew, and Kropf, Pascale

Subjects

CD4-Positive T-Lymphocytes, Mice, Inbred BALB C, Arginase, Macrophages, T-Lymphocytes, T cells, Leishmaniasis, Cutaneous, Immunity to Infection, Arginine, Flow Cytometry, Host-Parasite Interactions, Interleukin-10, Interferon-gamma, Mice, Mice, Inbred CBA, Animals, Th1/Th2 cells, Female, Interleukin-4, Cell activation, Cell proliferation, Leishmania major

Abstract

The amino acid L-arginine plays a crucial role in the regulation of immune responses. We have recently shown that uncontrolled replication of Leishmania parasites at the site of pathology correlates with high levels of arginase activity in nonhealing leishmaniasis and that this elevated arginase activity causes local depletion of L-arginine. To further our understanding of the impact of L-arginine deprivation in experimental leishmaniasis, here we characterize in detail the effects of L-arginine deprivation on antigen-specific T cells and MPhi. The results of our study show that decrease of L-arginine levels in the extracellular milieu affects the biological activities of Leishmania major-specific T cells, both at the level of the magnitude and the quality of their responses. L. major-specific CD4(+) T cells rendered hyporesponsive by L-arginine deprivation can be partially rescued by addition of exogenous L-arginine to produce IL-4 and IL-10, but not to produce IFN-gamma. Furthermore, our results show that L-arginine deprivation also greatly impacts parasite growth in activated macrophages. In summary, our results suggest that L-arginine levels affect both Th cell responses and parasite replication.

Published

2009

14. Metabolism via arginase or nitric oxide synthase: two competing arginine pathways in macrophages.

Author

Rath, Meera, Müller, Ingrid, Kropf, Pascale, Closs, Ellen I., and Munder, Markus

Subjects

ARGINASE, NITRIC-oxide synthases, MACROPHAGES, ARGININE, CITRULLINE, ORNITHINE, AUTOIMMUNE diseases

Abstract

Macrophages play a major role in the immune system, both as antimicrobial effector cells and as immunoregulatory cells, which induce, suppress or modulate adaptive immune responses. These key aspects of macrophage biology are fundamentally driven by the phenotype of macrophage arginine metabolism that is prevalent in an evolving or ongoing immune response. M1 macrophages express the enzyme nitric oxide synthase, which metabolizes arginine to nitric oxide (NO) and citrulline. NO can be metabolized to further downstream reactive nitrogen species, while citrulline might be reused for efficient NO synthesis via the citrulline-NO cycle. M2 macrophages are characterized by expression of the enzyme arginase, which hydrolyzes arginine to ornithine and urea. The arginase pathway limits arginine availability for NO synthesis and ornithine itself can further feed into the important downstream pathways of polyamine and proline syntheses, which are important for cellular proliferation and tissue repair. M1 versus M2 polarization leads to opposing outcomes of inflammatory reactions, but depending on the context, M1 and M2 macrophages can be both pro- and anti-inflammatory. Notably, M1/M2 macrophage polarization can be driven by microbial infection or innate danger signals without any influence of adaptive immune cells, secondarily driving the T helper (Th)1/Th2 polarization of the evolving adaptive immune response. Since both arginine metabolic pathways cross-inhibit each other on the level of the respective arginine break-down products andTh1 andTh2 lymphocytes can drive or amplify macrophage M1/M2 dichotomy via cytokine activation, this forms the basis of a self-sustaining M1/M2 polarization of the whole immune response. Understanding the arginine metabolism of M1/M2 macrophage phenotypes is therefore central to find new possibilities to manipulate immune responses in infection, autoimmune diseases, chronic inflammatory conditions, and cancer. [ABSTRACT FROM AUTHOR]

Published

2014

15. Characterization of Neutrophil Subsets in Healthy Human Pregnancies.

Author

Ssemaganda, Aloysius, Kindinger, Lindsay, Bergin, Philip, Nielsen, Leslie, Mpendo, Juliet, Ssetaala, Ali, Kiwanuka, Noah, Munder, Markus, Teoh, Tiong Ghee, Kropf, Pascale, and Müller, Ingrid

Subjects

NEUTROPHILS, ARGINASE, ENZYME activation, GRANULOCYTES, MATERNAL health, GENE expression, IMMUNE system, NATURAL immunity

Abstract

We have previously shown that in successful pregnancies increased arginase activity is a mechanism that contributes to the suppression of the maternal immune system. We identified the main type of arginase-expressing cells as a population of activated low-density granulocytes (LDGs) in peripheral blood mononuclear cells and in term placentae. In the present study, we analyzed the phenotype of LDGs and compared it to the phenotype of normal density granulocytes (NDGs) in maternal peripheral blood, placental biopsies and cord blood. Our data reveal that only LDGs but no NDGs could be detected in placental biopsies. Phenotypically, NDGs and LDGs from both maternal and cord blood expressed different levels of maturation, activation and degranulation markers. NDGs from the maternal and cord blood were phenotypically similar, while maternal, cord and placental LDGs showed different expression levels of CD66b. LDGs present in cord blood expressed higher levels of arginase compared to maternal and placental LDGs. In summary, our results show that in maternal and cord blood, two phenotypically different populations of neutrophils can be identified, whereas in term placentae, only activated neutrophils are present. [ABSTRACT FROM AUTHOR]

Published

2014