Expression of p16<scp><sup>INK</sup></scp><sup>4a</sup> is a biomarker of chondrocyte aging but does not cause osteoarthritis

Diekman, Brian O.; Sessions, Garrett A.; Collins, John A.; Knecht, Anne K.; Strum, Susan L.; Mitin, Natalia K.; Carlson, Cathy S.; Loeser, Richard F.; Sharpless, Norman E.

doi:10.1111/acel.12771

Cited by 118 publications

(99 citation statements)

References 54 publications

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“…Box plot length: 25% and 75% of data; centerline: median; whiskers: 25% -(or 75% +) 1.5 × IQR, dots: outliers. relevant in adult organisms, where retaining arrested yet functional cells may help maintain tissue homeostasis (1,3,63,64). This also raises the possibility that p16 can prevent tumor formation not only by triggering senescence arrest as an early sensor of cellular stress (65), but also by precluding the induction of immune signals that may become detrimental over time if unresolved or unwarranted.…”

Section: Discussionmentioning

confidence: 99%

Targetable mechanisms driving immunoevasion of persistent senescent cells link chemotherapy-resistant cancer to aging

Muñoz¹,

Yannone²,

Daemen³

et al. 2019

JCI Insight

105

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Section: Discussionmentioning

confidence: 99%

Targetable mechanisms driving immunoevasion of persistent senescent cells link chemotherapy-resistant cancer to aging

Muñoz¹,

Yannone²,

Daemen³

et al. 2019

JCI Insight

105

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“…In chondrocytes isolated from cadaveric donors without evidence of OA between 17 to 72 years old, age was found to be responsible for 27% of the variation in p16 levels. However, loss of p16 was not critical enough to prevent the development of age-induced or injury-induced traumatic OA [72]. Collagen type II expression is negatively correlated with p21 expression [73].…”

Section: Hypertrophy and Senescence-related Markers In Oamentioning

confidence: 95%

The Role of Chondrocyte Hypertrophy and Senescence in Osteoarthritis Initiation and Progression

Rim

Nam

2020

IJMS

210

141

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Osteoarthritis (OA) is the most common joint disease that causes pain and disability in the adult population. OA is primarily caused by trauma induced by an external force or by age-related cartilage damage. Chondrocyte hypertrophy or chondrocyte senescence is thought to play a role in the initiation and progression of OA. Although chondrocyte hypertrophy and cell death are both crucial steps during the natural process of endochondral bone formation, the abnormal activation of these two processes after injury or during aging seems to accelerate the progression of OA. However, the exact mechanisms of OA progression and these two processes remain poorly understood. Chondrocyte senescence and hypertrophy during OA share various markers and processes. In this study, we reviewed the changes that occur during chondrocyte hypertrophy or senescence in OA and the attempts that were made to regulate them. Regulation of hypertrophic or senescent chondrocytes might be a potential therapeutic target to slow down or stop OA progression; thus, a better understanding of the processes is required for management.

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“…Reverse transcription was performed using qScript XLT cDNA SuperMix (VWR International) according to the manufacturer's instructions. Quantitative PCR was performed with TaqMan Universal Master Mix on a QuantStudio 6 Flex Machine (Thermo Fisher Scientific) as recently described in Diekman et al (22). SASP gene expression was analyzed using TaqMan primer probes for IL-6 (Mm00446190_m1), IGF binding protein 3 (Mm01187817_m1), matrix metallopeptidase 13 (Mm00439491), and chemokine (C-C motif) ligand 2 (Mm00441242_m1).…”

Section: Rna Isolation and Gene Expression Analysismentioning

confidence: 99%

Controlled induction and targeted elimination of p16^INK4a‐expressing chondrocytes in cartilage explant culture

Sessions¹,

Copp

Liu

et al. 2019

The FASEB Journal

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Cellular senescence is a phenotypic state that contributes to age‐related diseases through the secretion of matrix‐degrading and inflammatory molecules. An emerging therapeutic strategy for osteoarthritis (OA) is to selectively eliminate senescent cells by initiating apoptosis. This study establishes a cartilage explant model of senescence induction and senolytic clearance using p16Ink4a expression as a biomarker of senescence. Growth‐factor stimulation of explants increased the expression of p16Ink4a at both the mRNA and protein levels. Applying this culture system to cartilage from p16tdTom reporter mice (a knockin allele with tdTomato fluorescent protein regulated by the endogenous p16Ink4a promoter) demonstrated the emergence of a p16‐high population that was quantified using flow cytometry for tdTomato. Cell sorting was used to separate chondrocytes based on tdTomato fluorescence and p16‐high cells showed higher senescence‐associated β‐galactosidase activity and increased gene expression of the senescence‐associated secretory phenotype as compared with p16‐low cells. The potential for effective senolysis within the cartilage extracellular matrix was assessed using navitoclax (ABT‐263). Navitoclax treatment reduced the percentage of p16‐high cells from 17.9 to 6.1% (mean of 13 matched pairs; P < 0.001) and increased cleaved caspase‐3 confirmed apoptotic activity. Together, these findings establish a physiologically relevant cartilage explant model for testing the induction and elimination of senescent chondrocytes, which will support investigations of senolytic therapy for OA.—Sessions, G. A., Copp, M. E., Liu, J.‐Y., Sinkler, M. A., D'Costa, S., Diekman, B. O. Controlled induction and targeted elimination of p16INK4a‐expressing chondrocytes in cartilage explant culture. FASEB J. 33, 12364–12373 (2019). http://www.fasebj.org

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Expression of p16^INK^4a is a biomarker of chondrocyte aging but does not cause osteoarthritis

Cited by 118 publications

References 54 publications

Targetable mechanisms driving immunoevasion of persistent senescent cells link chemotherapy-resistant cancer to aging

Targetable mechanisms driving immunoevasion of persistent senescent cells link chemotherapy-resistant cancer to aging

The Role of Chondrocyte Hypertrophy and Senescence in Osteoarthritis Initiation and Progression

Controlled induction and targeted elimination of p16^INK4a‐expressing chondrocytes in cartilage explant culture

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Expression of p16INK4a is a biomarker of chondrocyte aging but does not cause osteoarthritis

Cited by 118 publications

References 54 publications

Targetable mechanisms driving immunoevasion of persistent senescent cells link chemotherapy-resistant cancer to aging

Targetable mechanisms driving immunoevasion of persistent senescent cells link chemotherapy-resistant cancer to aging

The Role of Chondrocyte Hypertrophy and Senescence in Osteoarthritis Initiation and Progression

Controlled induction and targeted elimination of p16INK4a‐expressing chondrocytes in cartilage explant culture

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Expression of p16^INK^4a is a biomarker of chondrocyte aging but does not cause osteoarthritis

Controlled induction and targeted elimination of p16^INK4a‐expressing chondrocytes in cartilage explant culture