Substance P and Alpha-Calcitonin Gene-Related Peptide Differentially Affect Human Osteoarthritic and Healthy Chondrocytes

GND
1045251739
Zugehörigkeit
Department of Orthopaedic Surgery, Experimental Orthopaedics, Center for Medical Biotechnology, University of Regensburg
Stöckl, Sabine;
GND
129357898
Zugehörigkeit
Department of Trauma, Hand and Reconstructive Surgery, Experimental Trauma Surgery, Jena University Hospital, Friedrich-Schiller-University Jena
Eitner, Annett;
GND
170368912
Zugehörigkeit
Department of Oral and Maxillofacial Surgery, Center for Medical Biotechnology, University Hospital Regensburg
Bauer, Richard J.;
Zugehörigkeit
Department of Orthopedics, University Medical Center Regensburg, Asklepios Klinikum Bad Abbach
König, Matthias;
GND
1201579929
Zugehörigkeit
Department of Orthopaedics and Rehabilitation, Oregon Health & Science University
Johnstone, Brian;
GND
143770586
Zugehörigkeit
Department of Orthopaedic Surgery, Experimental Orthopaedics, Center for Medical Biotechnology, University of Regensburg
Grässel, Susanne

Osteoarthritis (OA) is a degenerative joint disease that not only causes cartilage loss but also structural damage in all joint tissues. Joints are innervated by alpha-calcitonin gene-related peptide (αCGRP) and substance P (SP)-positive sensory nerve fibers. Alteration of sensory joint innervation could be partly responsible for degenerative changes in joints that contribute to the development of OA. Therefore, our aim was to analyze and compare the molecular effects of SP and αCGRP on the metabolism of articular chondrocytes from OA patients and non-OA cartilage donors. We treated the cells with SP or αCGRP and analysed the influence of these neuropeptides on chondrocyte metabolism and modulation of signaling pathways. In chondrocytes from healthy cartilage, SP had minimal effects compared with its effects on OA chondrocytes, where it induced inflammatory mediators, inhibited chondrogenic markers and promoted apoptosis and senescence. Treatment with αCGRP also increased apoptosis and senescence and reduced chondrogenic marker expression in OA chondrocytes, but stimulated an anabolic and protective response in healthy chondrocytes. The catabolic influence of SP and αCGRP might be due to activation of ERK signaling that could be counteracted by an increased cAMP response. We suggest that a switch between the G-subunits of the corresponding receptors after binding their ligands SP or αCGRP plays a central role in mediating the observed effects of sensory neuropeptides on chondrocytes.

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Rechteinhaber: Copyright © 2021 Stöckl, Eitner, Bauer, König, Johnstone and Grässel

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