Differential expression of immunity-related genes in larval Manduca sexta tissues in response to gut and systemic infection

Yvette M von Bredow; Petra Prochazkova; Jiri Dvorak; Frantisek Skanta; Tina E Trenczek; Martin Bilej; Christoph-Rüdiger von Bredow

doi:10.3389/fcimb.2023.1258142

Differential expression of immunity-related genes in larval Manduca sexta tissues in response to gut and systemic infection

Front Cell Infect Microbiol. 2023 Oct 11:13:1258142. doi: 10.3389/fcimb.2023.1258142. eCollection 2023.

Authors

Yvette M von Bredow¹, Petra Prochazkova², Jiri Dvorak², Frantisek Skanta², Tina E Trenczek¹, Martin Bilej², Christoph-Rüdiger von Bredow^{1

3}

Affiliations

¹ Institute of Zoology and Developmental Biology, Justus-Liebig-University Gießen, Gießen, Germany.
² Laboratory of Cellular and Molecular Immunology, Institute of Microbiology of the Czech Academy of Sciences, Prague, Czechia.
³ Applied Zoology, Department of Biology, Technische Universität Dresden, Dresden, Germany.

Abstract

Introduction: The midgut epithelium functions as tissue for nutrient uptake as well as physical barrier against pathogens. Additionally, it responds to pathogen contact by production and release of various factors including antimicrobial peptides, similar to the systemic innate immune response. However, if such a response is restricted to a local stimulus or if it appears in response to a systemic infection, too is a rather underexplored topic in insect immunity. We addressed the role of the midgut and the role of systemic immune tissues in the defense against gut-borne and systemic infections, respectively.

Methods: Manduca sexta larvae were challenged with DAP-type peptidoglycan bacteria - Bacillus thuringiensis for local gut infection and Escherichia coli for systemic stimulation. We compared the immune response to both infection models by measuring mRNA levels of four selected immunity-related genes in midgut, fat body, hematopoietic organs (HOs), and hemocytes, and determined hemolymph antimicrobial activity. Hemocytes and HOs were tested for presence and distribution of lysozyme mRNA and protein.

Results: The midgut and circulating hemocytes exhibited a significantly increased level of lysozyme mRNA in response to gut infection but did not significantly alter expression in response to a systemic infection. Conversely, fat body and HOs responded to both infection models by altered mRNA levels of at least one gene monitored. Most, but not all hemocytes and HO cells contain lysozyme mRNA and protein.

Discussion: These data suggest that the gut recruits immune-related tissues in response to gut infection whereas systemic infections do not induce a response in the midgut. The experimental approach implies a skewed cross-talk: An intestinal infection triggers immune activity in systemic immune organs, while a systemic infection does not elicit any or only a restricted immune response in the midgut. The HOs, which form and release hemocytes in larval M. sexta, i) synthesize lysozyme, and ii) respond to immune challenges by increased immune gene expression. These findings strongly suggest that they not only provide phagocytes for the cellular immune response but also synthesize humoral immune components.

Keywords: Bacillus thuringiensis; comparative immune response; gut immunity; hematopoietic organ; insect immunity; insect midgut; lysozyme.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Immunity, Innate
Larva
Manduca* / genetics
Manduca* / metabolism
Muramidase / genetics
Muramidase / metabolism
RNA, Messenger / metabolism

Substances

Muramidase
RNA, Messenger

Grants and funding

The authors declare financial support was received for the research, authorship, and/or publication of this article. A grant was received from the German Academic Exchange Service (DAAD), project No. 54430024, covering travel costs for CvB, YvB, TT, JD, FS, and MB. The Article Processing Charges (APC) were funded by the joint publication funds of the TU Dresden, including Carl Gustav Carus Faculty of Medicine, and the SLUB Dresden as well as the Open Access Publication Funding of the DFG.