Organization and morphology of calcitonin gene‐related peptide‐immunoreactive axons in the whole mouse stomach

Author:

Ma Jichao1,Nguyen Duyen1ORCID,Madas Jazune1,Bizanti Ariege1ORCID,Mistareehi Anas1,Kwiat Andrew M.1,Chen Jin1ORCID,Lin Mabelle2ORCID,Christie Richard2ORCID,Hunter Peter2ORCID,Heal Maci3ORCID,Baldwin Shane3,Tappan Susan4ORCID,Furness John B.5ORCID,Powley Terry L.6ORCID,Cheng Zixi (Jack)1ORCID

Affiliation:

1. Burnett School of Biomedical Sciences, College of Medicine University of Central Florida Orlando Florida USA

2. Auckland Bioengineering Institute University of Auckland Auckland New Zealand

3. MBF Bioscience Williston Vermont USA

4. Rock Maple Science Hinesburg Vermont USA

5. Department of Anatomy & Physiology, Florey Institute of Neuroscience and Mental Health University of Melbourne Parkville Victoria Australia

6. Department of Psychological Sciences Purdue University West Lafayette Indiana USA

Abstract

AbstractNociceptive afferent axons innervate the stomach and send signals to the brain and spinal cord. Peripheral nociceptive afferents can be detected with a variety of markers (e.g., substance P [SP] and calcitonin gene‐related peptide [CGRP]). We recently examined the topographical organization and morphology of SP‐immunoreactive (SP‐IR) axons in the whole mouse stomach muscular layer. However, the distribution and morphological structure of CGRP‐IR axons remain unclear. We used immunohistochemistry labeling and applied a combination of imaging techniques, including confocal and Zeiss Imager M2 microscopy, Neurolucida 360 tracing, and integration of axon tracing data into a 3D stomach scaffold to characterize CGRP‐IR axons and terminals in the whole mouse stomach muscular layers. We found that: (1) CGRP‐IR axons formed extensive terminal networks in both ventral and dorsal stomachs. (2) CGRP‐IR axons densely innervated the blood vessels. (3) CGRP‐IR axons ran in parallel with the longitudinal and circular muscles. Some axons ran at angles through the muscular layers. (4) They also formed varicose terminal contacts with individual myenteric ganglion neurons. (5) CGRP‐IR occurred in DiI‐labeled gastric‐projecting neurons in the dorsal root and vagal nodose ganglia, indicating CGRP‐IR axons were visceral afferent axons. (6) CGRP‐IR axons did not colocalize with tyrosine hydroxylase or vesicular acetylcholine transporter axons in the stomach, indicating CGRP‐IR axons were not visceral efferent axons. (7) CGRP‐IR axons were traced and integrated into a 3D stomach scaffold. For the first time, we provided a topographical distribution map of CGRP‐IR axon innervation of the whole stomach muscular layers at the cellular/axonal/varicosity scale.

Funder

National Institutes of Health

Publisher

Wiley

Subject

General Neuroscience

Reference97 articles.

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