PRECLINICAL RESEARCH REPORT • SUNGKYUNKWAN UNIVERSITY, REPUBLIC OF KOREA • 2025
Sigma Anti-Bonding Calcium Attenuates Ovariectomy-Induced Bone Loss by Preserving Trabecular Microarchitecture and Suppressing Osteoclastogenesis
Sungkyunkwan University, one of South Korea’s oldest and most prestigious institutions, conducted rigorous preclinical research on Sigma Anti-Bonding Calcium Carbonate (SAC®) and found it protects bone architecture, reduces active bone resorption, and suppresses the molecular machinery of bone destruction.
About the Research Institution
Sungkyunkwan University (SKKU) was established in 1398 during the Joseon Dynasty, making it one of the oldest universities in Asia and among the most prestigious research institutions in the world.
Department of Integrative Biotechnology • Suwon Campus, Republic of Korea
Research funded by the National Research Foundation of Korea (NRF), Ministry of Education
13 Weeks
Treatment Period Studied
CTX ↓
Bone Resorption Reduced
p38 ↓
Osteoclast Pathway Suppressed
Safe
No Organ Toxicity Observed
The Silent Crisis Inside Your Bones: A Global Health Issue That Needs Answers
Postmenopausal osteoporosis affects hundreds of millions of women globally. When estrogen levels drop during menopause, the body’s bone-remodeling system falls out of balance: bone-destroying cells (osteoclasts) begin outpacing bone-building cells (osteoblasts). The result is a progressive, silent architectural collapse within bone tissue.
Standard calcium supplementation has long been considered foundational to bone health. But the SKKU research team asked a harder question: does the form of calcium, how it ionizes, how it signals, how cells respond to it, actually change outcomes at the molecular level?
To answer this, they studied Sigma Anti-Bonding Calcium Carbonate (SACx®), a formulation engineered to enhance the release of freely ionized calcium (Ca²⁺) in aqueous environments. SAC® was tested in the most rigorous available preclinical framework: an ovariectomized mouse model combined with direct cellular mechanistic analysis. The researchers didn’t just measure bone density. They looked inside the bone, at its microscopic scaffold, and what they found changes the conversation about what a calcium supplement should actually do.
Bone strength depends not only on mineral quantity but also on bone quality, which encompasses microarchitecture, matrix composition, mineralization heterogeneity, and structural connectivity.
— Seeman & Delmas, New England Journal of Medicine, 2006
What Is SAC® (Sigma Anti-Bonding Calcium Carbonate)?
The body manages mineral distribution through specialized sensing mechanisms found in the primary regulatory systems.
- Mechanism: Active ions are the primary language understood by these sensors. When mineral levels are optimized in an ionized state, the body initiates a natural feedback loop that coordinates systemic balance.
- Structural Support: This signaling environment supports the activity of mineral-storing cells while managing the natural recycling process. By providing minerals in their active, ionized form, the SAC® formula serves as a "bio-signal" that directs nutrients toward the skeletal framework. This ensures minerals are utilized for structural density rather than lingering in the circulation where they are less effective.
Preventing Vascular Smooth Muscle Cell (VSMC) Phenotypic Switching
Ectopic calcification occurs when Vascular Smooth Muscle Cells (VSMCs) undergo a "phenotypic switch," behaving like bone cells and creating mineralized plaques.
- The Risk of Complexed Calcium: Large doses of non-ionized calcium carbonate or phosphate can lead to transient hypercalcemia, where "calcium-phosphate products" precipitate in the blood.
- The Ionized Advantage: Because ionized calcium is immediately available for cellular work (muscle contraction and neurotransmission), it is rapidly cleared from the plasma by target cells or excreted by the kidneys, preventing the "stagnant" mineral load that leads to arterial stiffness.
Comparative Bioavailability Table
Technical comparison of calcium.
| Attribute | Ionized Calcium (Ca2+) | Conventional Calcium Salts |
| Active Molecule | Free Cation (Ca2+) | Bound Salt (e.g.,CaCO3) |
| Metabolic Requirement | None (Immediate) | Requires Gastric Acid & Vitamin D |
| Vascular Deposition Risk | Minimal (High Solubility) | Moderate (Potential for Precipitation) |
| CaSR Interaction | Direct Agonist | Indirect / Delayed |
| Primary Function | Cellular Signaling & Bone Matrix | Mass Loading |
Conclusion: A Signaling-Centric Approach to Bone Health
Modern nutritional science is shifting away from "high-dose elemental loading" toward "low-dose signaling." Providing calcium in its ionized form mimics the body’s natural extracellular fluid composition. This prevents the systemic mineral "overload" that contributes to vascular media calcification, ensuring that calcium remains a vital nutrient for longevity rather than a risk factor for cardiovascular health.
Disclaimer: This document is intended for technical and educational purposes, referencing the biochemical behavior of mineral ions in physiological systems.
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