Sex dimorphic regulation of osteoprogenitor progesterone in bone stromal cells

Kot, Alexander; Zhong, Zhendong; Zhang, Hong‐Liang; Lay, Yu An E.; Lane, Nancy E.; Yao, Wei

doi:10.1530/jme-17-0076

Cited by 10 publications

(23 citation statements)

References 68 publications

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“…We and others have found PR expressed in growth plate chondrocytes, osteoclasts, and osteoblasts, and PR plays a critical role in peak bone mass determination [37, 71,72]. We also have reported that the loss of PR signaling in osteoprogenitor cells regulates key signaling pathways for immune response, especially in males [34].…”

Section: Discussionmentioning

confidence: 88%

“…Additionally, conditional PR deletion in the Prx1 + osteoprogenitor cells significantly suppressed immunomodulatory pathways, especially in the males. The disease pathway analyses from our previous RNA-Seq study suggested that rheumatoid arthritis is a most-likely targeted disease for PR [34]. which prompted further evaluation of the role of PR in the pathogenesis of RA in this current study.…”

Section: Introductionmentioning

confidence: 83%

“…The right knee joints including both the distal femurs (DFM) and the proximal tibiae were scanned and analyzed using VivaCT 40 (Scanco Medical, Bassersdorf Switzerland) with a voxel resolution of 10 µm in all three spatial dimensions and a mono-energetic (70 Kev) X-ray source. We evaluated the entire knee covering a total of 645 mm in length centered around the knee joint to obtain total knee bone volume/tissue volume (BV/TV) ratio [34,51,52] using 3D image-registration schemes Gaussian filters of sigma = 0.8, support = 1 and threshold = 180 for total knee and DFM. Gaussian filters of sigma = 1, support = 2, and threshold = 280 were applied to register the paw.…”

Section: Bone Mass Measurements By Microctmentioning

confidence: 99%

“…The presence or absence or relative proportion of PR in different tissues may explain the PR's sex dimorphic roles in these tissues [29][30][31]. In contrast to the estrogen receptor, PR's role may be more important in immunomodulation in female-dominant diseases such as systemic lupus erythematosus, rheumatoid arthritis, and osteoarthritis [32][33][34]. However, PR as an immunomodulatory regulator in musculoskeletal tissue is not well understood.…”

Section: Introductionmentioning

confidence: 99%

“…which prompted further evaluation of the role of PR in the pathogenesis of RA in this current study. Since we observed the lack of PR signaling in OPC significantly regulated pathways involved in immunomodulation pathways previously [34], we set to perform this follow-up study in the PR ΔPrx1 mice using a CIA model. Total mononuclear cells were collected from peripheral blood using the Ficoll-Paque density gradient method.…”

Section: Introductionmentioning

confidence: 99%

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High susceptibility to collagen-induced arthritis in mice with progesterone receptors selectively inhibited in osteoprogenitor cells

Liu¹,

Jia²,

Jiang

et al. 2020

Preprint

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Abstract Background. Progesterone receptor (PR) affects immunomodulation, and lack of PR in osteoprogenitor cells primarily affects pathways associated with immunomodulation, especially in the males. In this study, we selectively deleted PR from osteoprogenitor cells using Prx1-Cre to evaluate the tissue-specific effects of PR on inflammatory arthritis (IA). Methods. Collagen-induced arthritis (CIA) was used as an IA animal model, which we induced in PR D Prx1 mice and their wild type (WT) littermates were immunized with collagen II (CII) emulsified incomplete Freund's adjuvant ( CFA ) in both sexes. Joint erosion, inflammation, and cartilage damages were assessed using a semiquantitative histologic scoring system. Bone volume and erosions in knee and ankle joints were quantitated using microCT. We found that knee and paw joint erosions developed in 37.5% and 41.7% of the WT and PR D Prx1 female mice, respectively, and in 45.4 and 100%, respectively, of the male mice. Also, both knee and ankle joint inflammation scores, joint damage scores, and subchondral bone erosions were significantly more severe in male PRcKO mice than in male WT mice. Although of lower severity than in male mice, female PR D Prx1 mice also developed higher inflammation scores and bone erosions than the KO-normal or WT-CIA females. Immunohistochemistry staining of the NLRP3 inflammasome revealed the male PR D Prx1 mice had significantly higher expression of NLRP3 inflammasome in the knee joints. Conclusion. Our observations indicate that the presence of PR in osteoprogenitor cells counteracts the development of collagen-induced arthritis and might help to explain the sex differences observed in human inflammatory arthritis.

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Section: Discussionmentioning

confidence: 88%

Section: Introductionmentioning

confidence: 83%

Section: Bone Mass Measurements By Microctmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

High susceptibility to collagen-induced arthritis in mice with progesterone receptors selectively inhibited in osteoprogenitor cells

Liu¹,

Jia²,

Jiang

et al. 2020

Preprint

Self Cite

View full text Add to dashboard Cite

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Bone metabolism regulation: Implications for the treatment of bone diseases

Yao¹,

Huang²,

et al. 2020

Biomedicine & Pharmacotherapy

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Selective inhibition of progesterone receptor in osteochondral progenitor cells, but not in mature chondrocytes, modulated subchondral bone structures

Dai

Jia

Kot

et al. 2020

Bone

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The presence or relative proportion of progesterone nuclear receptors (PR) in different tissues may contribute to sexual dimorphism in these tissues. PR is expressed in chondrocytes, but its function is mostly unknown. We hypothesized that the PR may regulate chondrocyte metabolism and affect subchondral bone structure. Methods: We utilized genetic fate mapping and immunohistochemistry to elucidate PR expression in and effect on cartilage. To define sex-dependent and chondrocyte-specific effects of the PR on subchondral bone, we selectively deleted PR in osteochondrogenic progenitor cells marked by Prx1 (Prx1; PRcKO) and Collagen 2 (Col2; PRcKO), or in matured chondrocytes marked by aggrecan (Acan; PRcKO) and evaluated subchondral bone structure at 4 months of age. Chondrocyte aging was monitored by anti-senescence marker p16INK4a, and MMP13, one of the Senescence-Associated Secretary Phenotype (SASP) components. Results: Compared to wild-type (WT) mice, the female Prx1; PRcKO and the Col2; PRcKO mice had greater total subchondral bone volume and greater subchondral cortical bone thickness, with increased estimated subchondral bone stiffness and failure load in both female and male Col2; PRcKO mice. Moreover, Col2; PRcKO mice from both sexes had greater bone formation and bone strength at the femurs. In contrast, we did not observe any subchondral bone changes in Acan; PRcKO mice other than higher work-to-failure observed in the male Acan; PRcKO mice. Despite no detected difference in articular cartilage between the WT and the PR; chondrocyte conditional deletion mice, there were greater numbers of senescent chondrocytes and increased MMP13 expression, especially in the male mutant mice. Conclusion: These findings suggest that selective inhibition of PR in osteoprogenitor cells, but not in terminally differentiated chondrocytes, induced an increased subchondral bone phenotype and high estimated subchondral bone strength, which might be associated with the development of osteoarthritis in older age.

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Sex dimorphic regulation of osteoprogenitor progesterone in bone stromal cells

Cited by 10 publications

References 68 publications

High susceptibility to collagen-induced arthritis in mice with progesterone receptors selectively inhibited in osteoprogenitor cells

High susceptibility to collagen-induced arthritis in mice with progesterone receptors selectively inhibited in osteoprogenitor cells

Bone metabolism regulation: Implications for the treatment of bone diseases

Selective inhibition of progesterone receptor in osteochondral progenitor cells, but not in mature chondrocytes, modulated subchondral bone structures

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