The route of infection with Leptospira interrogans serovar Copenhageni affects the kinetics of bacterial dissemination and kidney colonization.

Tytuł:: The route of infection with Leptospira interrogans serovar Copenhageni affects the kinetics of bacterial dissemination and kidney colonization.
Autorzy:: Nair N; Department of Microbiology, Immunology and Biochemistry, The University of Tennessee Health Science Center, Memphis, Tennessee, United States of America.
Guedes MS; Department of Microbiology, Immunology and Biochemistry, The University of Tennessee Health Science Center, Memphis, Tennessee, United States of America.; Immuno Technologies, Inc, Memphis, Tennessee, United States of America.
Werts C; Institut Pasteur, Biology and Genetics of the Bacterial Cell Wall Unit, Paris, France.
Gomes-Solecki M; Department of Microbiology, Immunology and Biochemistry, The University of Tennessee Health Science Center, Memphis, Tennessee, United States of America.; Immuno Technologies, Inc, Memphis, Tennessee, United States of America.
Źródło:: PLoS neglected tropical diseases [PLoS Negl Trop Dis] 2020 Jan 06; Vol. 14 (1), pp. e0007950. Date of Electronic Publication: 2020 Jan 06 (Print Publication: 2020).
Typ publikacji:: Journal Article; Research Support, N.I.H., Extramural
Język:: English
Imprint Name(s):: Original Publication: San Francisco, CA : Public Library of Science
MeSH Terms:: Leptospira interrogans/*physiology
Leptospirosis/*microbiology
Leptospirosis/*transmission
Animals ; Immunity, Innate ; Immunoglobulins/blood ; Kinetics ; Leptospira interrogans/immunology ; Leptospirosis/immunology ; Mice, Inbred C3H ; Mouth Mucosa ; Nasal Mucosa ; Nephritis/immunology ; Nephritis/microbiology ; Nephritis/pathology ; Skin/injuries ; Skin/microbiology ; Urine/microbiology
References:: PLoS Negl Trop Dis. 2014 Jan 30;8(1):e2664. (PMID: 24498450)
Infect Immun. 2005 Oct;73(10):7014-7. (PMID: 16177383)
PLoS Negl Trop Dis. 2014 Nov 20;8(11):e3307. (PMID: 25411782)
J Med Microbiol. 2010 Sep;59(Pt 9):1101-6. (PMID: 20558584)
J Infect Dis. 1988 Jul;158(1):246-7. (PMID: 3392418)
Nat Rev Microbiol. 2009 Oct;7(10):736-47. (PMID: 19756012)
J Exp Med. 1999 Feb 15;189(4):615-25. (PMID: 9989976)
Infect Immun. 2017 Mar 23;85(4):. (PMID: 28115508)
J Immunol. 1998 Jan 1;160(1):20-3. (PMID: 9551950)
Curr Protoc Microbiol. 2006 Sep;Chapter 12:Unit 12E.2. (PMID: 18770576)
Front Immunol. 2017 Feb 21;8:58. (PMID: 28270811)
Hum Exp Toxicol. 2002 Sep-Oct;21(9-10):493-8. (PMID: 12458906)
J Immunol. 2012 Mar 15;188(6):2805-14. (PMID: 22323544)
J Immunol. 2009 Aug 15;183(4):2669-77. (PMID: 19635914)
Curr Top Microbiol Immunol. 2015;387:65-97. (PMID: 25388133)
Clin Infect Dis. 2002 Jun 15;34(12):1593-9. (PMID: 12032894)
PLoS Negl Trop Dis. 2016 Mar 31;10(3):e0004569. (PMID: 27031867)
Exp Toxicol Pathol. 1998 Jun;50(3):191-8. (PMID: 9681649)
Lancet Infect Dis. 2003 Dec;3(12):757-71. (PMID: 14652202)
J Biol Chem. 2004 Jun 11;279(24):25420-9. (PMID: 15044492)
Postgrad Med J. 1988 Feb;64(748):163-4. (PMID: 3174532)
Infect Immun. 2015 Dec;83(12):4693-700. (PMID: 26416909)
Trends Immunol. 2019 Mar;40(3):197-211. (PMID: 30745265)
Infect Immun. 2011 Jul;79(7):2936-40. (PMID: 21576342)
Clin Diagn Lab Immunol. 2005 Jan;12(1):60-7. (PMID: 15642986)
Infect Immun. 2006 Feb;74(2):887-95. (PMID: 16428731)
PLoS Negl Trop Dis. 2017 Aug 25;11(8):e0005870. (PMID: 28841659)
Can J Microbiol. 2014 Jun;60(6):383-9. (PMID: 24861456)
PLoS Negl Trop Dis. 2014 Dec 04;8(12):e3359. (PMID: 25474719)
J Immunol. 2005 Nov 1;175(9):6022-31. (PMID: 16237097)
Grant Information:: R21 AI142129 United States AI NIAID NIH HHS; R43 AI096551 United States AI NIAID NIH HHS; R43 AI136551 United States AI NIAID NIH HHS; R44 AI096551 United States AI NIAID NIH HHS
Substance Nomenclature:: 0 (Immunoglobulins)
Entry Date(s):: Date Created: 20200107 Date Completed: 20200413 Latest Revision: 20230224
Update Code:: 20240105
PubMed Central ID:: PMC6964914
DOI:: 10.1371/journal.pntd.0007950
PMID:: 31905198
: Czasopismo naukowe

Pełny tekst

The goal of this study was to characterize how natural routes of infection affect the kinetics of pathogenic Leptospira dissemination to blood and kidney. C3H/HeJ mice were sublethally infected with L. interrogans serovar Copenhageni FioCruz L1-130 (Leptospira) through exposure of a dermis wound and through oral and nasal mucosa, in comparison to uninfected mice and to mice infected via standard intraperitoneal inoculation. In striking contrast to oral mucosa inoculation, transdermal and nasal mucosa infections led to weight loss, renal colonization and inflammation, as previously observed for conjunctival and intraperitoneal infections. However, the timing at which Leptospira gained access to blood, as well as Leptospira' colonization of the kidney and shedding in urine, differed from intraperitoneal infection. Furthermore, a comparative analysis of transcription of pro-inflammatory mediators in kidney and total immunoglobulin isotyping in serum from infected mice, showed increased innate immune response markers (KC, MIP-2, TNF-α) and lower Th1 associated IFN-γ in kidney, as well as lower Th1 associated IgG2a in mice infected through the nasal mucosa as compared to intraperitoneal infection. We conclude that the route of infection affects the timing at which Leptospira gains access to blood for dissemination, as well as the dynamics of colonization and inflammation of the kidney.
Competing Interests: I have read the journal's policy and some of the authors of this manuscript have the following competing interests: MSG and MGS are or were employed in part by a commercial company, Immuno Technologies, Inc. MGS holds more than 5% financial interest in Immuno Technologies, Inc. NN and CW declare no conflicts.

Zaloguj się, aby uzyskać dostęp do pełnego tekstu.

Informacja