2021
DOI: 10.1007/s11033-021-06731-0
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Increase in NO causes osteoarthritis and chondrocyte apoptosis and chondrocyte ERK plays a protective role in the process

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Cited by 5 publications
(6 citation statements)
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“…Fortunately, we observed potent antiapoptotic effect in chondrocytes followed by daphnoretin treatment. Moreover, daphnoretin abated the IL-1β-induced production of PGE2, NO, TNF-α and IL-6, which are all involved in chondrocyte apoptosis and cell viability decline [31][32][33][34]. In vivo experiments showed that daphnoretin alleviated the pathological injury of the knee joint in OA mice.…”
Section: Discussionmentioning
confidence: 92%
“…Fortunately, we observed potent antiapoptotic effect in chondrocytes followed by daphnoretin treatment. Moreover, daphnoretin abated the IL-1β-induced production of PGE2, NO, TNF-α and IL-6, which are all involved in chondrocyte apoptosis and cell viability decline [31][32][33][34]. In vivo experiments showed that daphnoretin alleviated the pathological injury of the knee joint in OA mice.…”
Section: Discussionmentioning
confidence: 92%
“…22 Pre-vious studies have suggested that low concentrations of NO protect cells from apoptosis, whereas excessive NO induces apoptosis. 23,24 The antiapoptotic mechanism can be the regulation of protective genes such as Bcl-2 as well as direct inhibition of the apoptotic caspase family. 25,26 Except for the ability of L-arg to regulate apoptosis, L-arg has also been reported to promote the proliferation of osteoblasts.…”
Section: Discussionmentioning
confidence: 99%
“…As a basic substrate of NO, L‐arg generates NO under the action of nitric oxide synthase (NOS) and subsequently regulates apoptosis 22 . Previous studies have suggested that low concentrations of NO protect cells from apoptosis, whereas excessive NO induces apoptosis 23,24 . The antiapoptotic mechanism can be the regulation of protective genes such as Bcl‐2 as well as direct inhibition of the apoptotic caspase family 25,26 .…”
Section: Discussionmentioning
confidence: 99%
“…The release of proinflammatory factors can contribute to the induction of NO synthesis by NO synthase, inhibit chondrocyte proliferation, and reduce the synthesis of the extracellular matrix. At the same time, NO can also directly damage the vascular wall, increase the permeability of the vascular wall and cause synovial congestion and edema and leukocyte exudation (52). TNF-a, as a common inflammatory mediator, can act alone or synergistically with other cytokines such as IL-1b and IL-6 to stimulate the production of cartilage, and synovial and subchondral bone layer-associated cells to produce matrix metalloproteinases, leading to gradual loss of cartilage collagen and proteoglycan and inhibition of proteoglycan and type II collagen synthesis, indirectly causing chondrocyte death and disrupting the homeostatic balance between cartilage damage and repair, which results in varying degrees of cartilage lysis and damage (53)(54)(55).…”
Section: Discussionmentioning
confidence: 99%