Academic Thesis

Basic information

Name Omori Naoya
Belonging department
Occupation name
researchmap researcher code
researchmap agency

Title

Impact of Histone H1 on the Progression of Allergic Rhinitis and Its Suppression by Neutralizing Antibody in Mice. 

Bibliography Type

Joint Author

Author

 

OwnerRoles

 

Summary

Nuclear antigens are known to trigger off innate and adaptive immune responses. Recent studies have found that the complex of nucleic acids and core histones that are derived from damaged cells may regulate allergic responses. However, no fundamental study has been performed concerning the role of linker histone H1 in mast cell-mediated type I hyperreactivity. In this study, we explored the impact of histone H1 on mast cell-mediated allergic responses both in vitro and in vivo. In the course of a bona-fide experimental allergen sensitization model upon co-injection with alum adjuvant, ovalbumin (OVA), but not PBS, induced elevated levels of circulating histone H1. Intranasal challenge with histone H1 to OVA/alum- (but not PBS/alum)-sensitized mice induced significantly severer symptoms of allergic rhinitis than those in mice sensitized and challenged with OVA. A monoclonal antibody against histone H1 not only suppressed mast cell degranulation, but also ameliorated OVA-induced nasal hyperreactivity and IgE-mediated passive cutaneous anaphylaxis. Our present data suggest that nuclear histone H1 represents an alarmin-like endogenous mediator acting on mast cells, and that its blockage has a therapeutic potential for mast cell-mediated type I hyperreactivity.
データの解析、考察部分

Magazine(name)

PLoS One(in press)

Publisher

 

Volume

 

Number Of Pages

 

StartingPage

 

EndingPage

 

Date of Issue

2016/08

Referee

 

Invited

 

Language

 

Thesis Type

 

International Journal

 

International Collaboration

 

ISSN

 

eISSN

 

DOI

 

NAID

 

Cinii Books Id

 

PMID

 

PMCID

 

URL

Format

 

Download

 

J-GLOBAL ID

 

arXiv ID

 

ORCID Put Code

 

DBLP ID

 

Subject1

 

Subject2

 

Subject3

 

Major Achivement