# Role of Cyr61/CCN1 in Mesenchymal Stem Cell Niche and Aging Bone

> **NIH VA IK2** · SOUTH TEXAS VETERANS HEALTH CARE SYSTEM · 2022 · —

## Abstract

Aging-related skeletal degeneration is associated with changes in bone microarchitecture, loss of
bone mineral density (BMD), increased susceptibility to fracture, and delayed bone healing. A key
factor in these degenerative changes is the formation of osteoprogenitors (i.e. mesenchymal stem
cells [MSCs]), which decreases with aging and are regulated by cues in the local bone marrow
(BM) microenvironment (niche). To date, the specific changes that occur in the BM niche during
aging are unknown. To address this knowledge gap, Dr. Xiao-Dong Chen's lab developed a
culture system that reproduces the BM-MSC niche ex vivo, used in this project to compare the
growth factor responsiveness of MSCs cultured on ECMs produced by BM stromal cells from
“young” (≤25 y/o) and “old” (≥60 y/o) donors. MSCs on “old” ECM displayed less BMP-2
responsiveness compared to cells on “young” ECM. Recent preliminary data showed that
Cyr61/CCN1, a matricellular protein involved in regulating osteogenesis, was deficient in “old”
compared to “young” ECM and knock-down of Cyr61 in young ECM abrogated BMP-2
responsiveness, confirming the importance of this protein in osteogenesis. Further, treating old
BM stromal cells with adenovirus containing the Cyr61 gene prior to ECM synthesis restored MSC
responsiveness to BMP-2 and studies by Zhao et al (2018) using Cyr61 KO mice (i.e. Cyr61 KO
[yKO]) driven by osterix (Osx) showed that KO mice had reduced BMD relative to wild type (WT).
These findings lead to the hypothesis that aging-related bone degeneration is at least partially
related to depletion of Cyr61 in bone ECM, which negatively impacts the BM niche and reduces
MSC osteogenesis. In the proposed studies, Aim 1 will assess the impact of Cyr61 depletion on
bone phenotype and BM matrix proteome in 3 mo. old (WT-y), 18 mo. old (WT-o) and 3 mo. old
KO (yKO) mice. The bone matrix of WT-o and yKO mice is expected to contain less Cyr61, exhibit
similar aging proteomes, and reduced BMD as compared to WT-y mice. Aim 2 will assess the
ability of ECMs, produced by BM stromal cells from WT-y, WT-o and yKO mice, to support MSC
growth factor responsiveness to BMP-2 and IGF-1 and osteoblast differentiation. These studies
are expected to show that matrix bound Cyr61 determines the ability of an ECM to support MSC
responsiveness to growth factors and osteoblast differentiation. Studies to probe the mechanism
of aging-related changes in Cyr61 are expected to show that higher levels of active YAP [i.e. de-
phosphorylated] in young MSCs promote the expression of Cyr61 and its increased incorporation
into young BM-ECM. In contrast, old MSCs are expected to show lower levels of YAP and reduced
Cyr61 in the ECM. Aim 3 will determine if exogenous rhCyr61 promotes lumbar fusion in WT-o
and yKO mice, either alone or in combination with rhBMP-2. The results are expected to show that
co-administration of rhCyr61 and rhBMP-2 will dramatically improve bone healing, better than
either one alone, especially ...

## Key facts

- **NIH application ID:** 10369575
- **Project number:** 1IK2BX005694-01A1
- **Recipient organization:** SOUTH TEXAS VETERANS HEALTH CARE SYSTEM
- **Principal Investigator:** Milos Marinkovic
- **Activity code:** IK2 (R01, R21, SBIR, etc.)
- **Funding institute:** VA
- **Fiscal year:** 2022
- **Award amount:** —
- **Award type:** 1
- **Project period:** 2022-01-01 → 2026-12-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10369575

## Citation

> US National Institutes of Health, RePORTER application 10369575, Role of Cyr61/CCN1 in Mesenchymal Stem Cell Niche and Aging Bone (1IK2BX005694-01A1). Retrieved via AI Analytics 2026-05-25 from https://api.ai-analytics.org/grant/nih/10369575. Licensed CC0.

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