JOURNAL ARTICLE

Receptor for Advanced Glycation End Product (RAGE) Modulates Inflammation During Feeding of the Hard Tick, Haemaphysalis longicornis in Mice.

  • Published In: Parasite Immunology, 2024, v. 46, n. 6. P. 1 1 of 3

  • Database: Academic Search Ultimate 2 of 3

  • Authored By: Anisuzzaman; Alim, Md. Abdul; Matsubyashi, Makoto; Hossain, Md. Shahadat; Labony, Sharmin Shahid; Shanta, Ireen Sultana; Ali, Md. Haydar; Yamamoto, Yasuhiko; Hatta, Takeshi; Tsuji, Naotoshi 3 of 3

Abstract

Ticks are notorious blood‐sucking ectoparasites that affect both humans and animals. They serve as a unique vector of various deadly diseases. Here, we have shown the roles of the receptor for advanced glycation end products (RAGE) during repeated infestations by the tick Haemaphysalis longicornis using RAGE−/− mice. In primary infestation, a large blood pool developed, which was flooded with numerous RBCs, especially during the rapid feeding phase of the tick both in wild‐type (wt) and RAGE−/− mice. Very few inflammatory cells were detected around the zones of haemorrhage in the primary infestations. However, the number of inflammatory cells gradually increased in the subsequent tick infestations, and during the third infestations, the number of inflammatory cells reached to the highest level (350.3 ± 16.8 cells/focus). The site of attachment was totally occupied by the inflammatory cells in wt mice, whereas very few cells were detected at the ticks' biting sites in RAGE−/− mice. RAGE was highly expressed during the third infestation in wt mice. In the third infestation, infiltration of CD44+ lymphocytes, eosinophils and expression of S100A8 and S100B significantly increased at the biting sites of ticks in wt, but not in RAGE−/− mice. In addition, peripheral eosinophil counts significantly increased in wt but not in RAGE−/− mice. Taken together, our study revealed that RAGE‐mediated inflammation and eosinophils played crucial roles in the tick‐induced inflammatory reactions. [ABSTRACT FROM AUTHOR]

Additional Information

  • Source:Parasite Immunology. 2024/06, Vol. 46, Issue 6, p1
  • Document Type:Article
  • Subject Area:Zoology
  • Publication Date:2024
  • ISSN:0141-9838
  • DOI:10.1111/pim.13039
  • Accession Number:178093631
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