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Osteocyte

An osteocyte is a mature, terminally differentiated derived from osteoblasts that becomes embedded within the mineralized of , serving as the most abundant type in mature , comprising approximately 90–95% of all s. These long-lived s, with a lifespan extending up to 25 years or more, are essential for maintenance and remodeling. In terms of structure, osteocytes are flat, almond-shaped cells typically measuring about 7 μm in depth and 15 μm in length, residing within small cavities known as lacunae embedded between layers of bone matrix called lamellae. Each osteocyte extends 40–60 slender, dendritic cytoplasmic processes that protrude through tiny channels called canaliculi, forming an extensive lacuno-canalicular network that connects adjacent osteocytes and facilitates communication with cells on bone surfaces, such as osteoblasts and osteoclasts. This network, supported by gap junctions, enables the rapid transmission of signals across the bone tissue. Unlike their progenitor osteoblasts, mature osteocytes exhibit reduced endoplasmic reticulum and Golgi apparatus, reflecting their shift from matrix production to sensory and regulatory roles. Osteocytes play a central role in bone homeostasis by acting as primary mechanosensors, detecting mechanical loads and fluid within the bone matrix to orchestrate adaptive remodeling responses. They regulate the activity of osteoblasts and osteoclasts through molecules, such as to promote and sclerostin to inhibit bone formation via the Wnt pathway, ensuring a between bone deposition and breakdown. Additionally, osteocytes function as endocrine cells, secreting factors like 23 (FGF23) to control systemic metabolism and activation, influencing mineral ion beyond the . Their , often triggered by microdamage or disuse, signals the initiation of targeted bone repair by attracting osteoclasts to resorb affected areas. Beyond bone-specific functions, osteocytes contribute to broader physiological processes, including the regulation of energy metabolism and immune responses through secreted proteins that affect distant tissues. Dysfunctions in osteocyte signaling are implicated in skeletal disorders such as , where reduced mechanosensitivity leads to imbalanced remodeling, and in conditions like due to disrupted handling. Overall, osteocytes represent a dynamic, interconnected system that integrates mechanical, hormonal, and biochemical cues to maintain skeletal integrity and systemic mineral throughout life.

Anatomy

Morphology

Osteocytes exhibit an oblate, stellate morphology, characterized by a flattened, star-shaped cell body with numerous thin dendritic processes extending from it. The cell body typically measures 5 to 20 micrometers in diameter, while the dendritic processes, numbering 40 to 100 per cell, can extend up to 20 to 30 micrometers in length. These cells reside within small cavities known as lacunae embedded in the mineralized bone matrix, where the dendritic processes extend through narrow channels called canaliculi, allowing between adjacent osteocytes to form a functional . Compared to their precursor osteoblasts, mature osteocytes display reduced cellular organelles, including minimal rough and Golgi apparatus, reflecting their diminished synthetic activity and adaptation to a primarily regulatory role within the bone tissue. Osteocytes possess an exceptionally long lifespan, often enduring for decades in humans—up to 25 years or more—contributing to the stability of bone structure throughout the organism's life. In the adult , estimates indicate approximately 42 billion live osteocytes, representing over 90% of all cells. These dendritic processes facilitate intercellular communication within the bone matrix.

Network and Location

Osteocytes are embedded within the mineralized of , where they reside in individual lacunae and extend slender processes into surrounding canaliculi, collectively forming a three-dimensional lacuno-canalicular (LCN) that pervades the . This extensive ensures that approximately 80% of the matrix volume is within approximately 3 μm of the nearest lacuna or canaliculus, allowing osteocytes to maintain close proximity to the mineralized environment throughout the skeletal structure. The stellate of osteocytes facilitates the extension of these processes, enabling the intricate connectivity observed in the LCN. The dendritic processes of osteocytes connect adjacent cells via gap junctions, primarily composed of connexin 43 (Cx43), which permit direct intercellular communication by allowing the passage of small molecules and ions between osteocytes. Additionally, the canaliculi surrounding these processes provide pathways for interstitial fluid flow within the bone matrix, facilitating exchange and waste removal across the network. In adult human bone, osteocyte density varies by bone type, with higher concentrations in cortical bone compared to trabecular bone, typically ranging from 20,000 to 30,000 osteocytes per mm³ overall. This distribution reflects the structural demands of load-bearing regions, where cortical bone's denser osteocyte population supports greater mechanical integration. Osteocytes first appeared in the fossil record approximately 400 million years ago during the period, coinciding with the evolutionary transition to cellular bone in early vertebrates and the development of processes. This emergence marked a significant advancement in skeletal , enabling more dynamic bone maintenance in terrestrial and aquatic environments.

Development

Origin from Precursors

Osteocytes originate from mesenchymal stem cells (MSCs), which are multipotent progenitors capable of differentiating into various cell types within the skeletal system. These MSCs commit to the lineage through a series of transcriptional and signaling events, ultimately giving rise to mature osteoblasts that function as bone-forming cells. Only 10-20% of these osteoblasts proceed to terminal differentiation into osteocytes, while the majority either undergo or transition into quiescent lining cells on bone surfaces. The primary precursors for osteocytes are mature osteoblasts located on active bone-forming surfaces, where they actively synthesize and mineralize the . As osteoblasts deposit unmineralized , a subset becomes embedded within the matrix, initiating their transformation into osteocytes. This embedding process is influenced by local environmental cues, including high levels of matrix mineralization and specific embedding signals such as stiffness and interactions with crystals. In certain experimental contexts, such as models of cortical bone formation on soft substrates, up to 50% of osteoblasts may exhibit osteocyte-like , higher than the typical 10-20% , highlighting the role of these factors in promoting terminal . Osteocytes were first described in the mid-19th century by anatomists through microscopic examination of bone tissue, revealing their lacunar-embedded . However, the precise cellular from s was not clarified until the , when advances in histological techniques and early lineage-tracing methods confirmed their derivation from the osteoblast population.

and Maturation

Osteocyte differentiation and maturation represent the terminal phase of the osteoblast , during which matrix-producing osteoblasts become embedded within the mineralizing bone . The process initiates as osteoblasts secrete unmineralized and progressively embed themselves into this extracellular . Subsequent mineralization of the traps the cells, transforming them into osteocytes housed in lacunae, while they extend dendritic processes that form an interconnected network via canaliculi. This embedding and mineralization are critical, as inhibition of matrix mineralization impairs the expression of osteocyte-specific genes and dendritic outgrowth. Key regulators orchestrate this transformation, including dentin matrix protein 1 (DMP-1), which is essential for perilacunar mineralization and phosphate homeostasis in early embedding osteocytes, and sclerostin, whose expression emerges in late-stage, deeply embedded cells to modulate Wnt signaling. Transforming growth factor-beta (TGF-β) signaling also plays a pivotal role, promoting early proliferation while influencing the transition to osteocytes by inducing markers such as DMP-1 and sclerostin through Smad2/3 pathways; however, excessive TGF-β can inhibit late-stage mineralization. These regulators ensure the progressive loss of osteoblast characteristics and acquisition of osteocyte-specific traits. The differentiation unfolds in distinct stages, with initial embedding and early changes observed over approximately 3-5 days in models like MLO-Y4 cells, and full maturation taking longer, as observed in labeling studies. In the early stage, cells exhibit high expression of E11 (also known as podoplanin or gp38), marking the onset of embedding with initial dendritic process formation. The intermediate stage features upregulation of DMP-1, coinciding with matrix mineralization and further process extension. By the late stage, mature osteocytes display full dendritic networks, sclerostin expression, and reduced cell body size by up to 70%. Molecular markers reflect these changes: (ALP), a hallmark of osteoblasts, is progressively lost, while podoplanin and are gained as indicators of osteocytic identity.

Functions

Mechanosensation

Osteocytes serve as the primary mechanosensors in bone, detecting mechanical strain predominantly through fluid generated in the lacuno-canalicular system during loading. This arises from interstitial fluid flow within the narrow canaliculi (diameter 210–260 ), which amplifies tissue-level strains by up to two orders of magnitude due to the confined space and hillocks along the walls. The resulting forces deform osteocyte processes and cell bodies, initiating . Key molecular components include and the . , such as β1 on the body and β3 on , form focal adhesions that link the to the , transmitting shear-induced perturbations; for instance, fluid flow perturbs α5β1 , opening hemichannels to release signaling molecules like prostaglandins. The , particularly F-actin bundles in processes tethered to canalicular walls, maintains and propagates mechanical signals intracellularly, with depolymerization leading to process retraction under stress. Additionally, the mechanosensitive serves as a central transducer in osteocytes, detecting mechanical forces to modulate downstream signaling pathways involved in . In response to loading, osteocytes generate rapid intracellular calcium (Ca²⁺) signaling waves that propagate through the interconnected network. These oscillations occur within seconds of load initiation and are driven by fluid shear in the canaliculi, where interstitial fluid flow reaches velocities of 34–58 μm/s, enabling network-wide coordination and activation of downstream pathways within minutes. This mechanosensation drives adaptive responses: increased loading suppresses osteocyte sclerostin expression within 24 hours, relieving inhibition of Wnt signaling in osteoblasts to promote formation, while unloading elevates sclerostin, enhancing resorption via activation. In vivo evidence from osteocyte-specific β-catenin deletions confirms this; heterozygous deletion (one ) abolishes load-induced anabolic bone formation, with no significant cortical thickening observed post-loading, underscoring β-catenin as a critical mediator of mechanotransduction.

Bone Remodeling Regulation

Osteocytes play a central role in regulating by modulating the activity of osteoclasts and osteoblasts, thereby maintaining skeletal integrity and mass. Through their extensive network within the bone matrix, osteocytes coordinate the balance between and formation, responding to physiological demands such as mechanical loading. This regulation primarily occurs via the secretion of signaling molecules that influence the and function of effector cells on bone surfaces. A key mechanism involves osteocytes modulating the RANKL/OPG ratio to control osteoclastogenesis while inhibiting osteoblast activity. Osteocytes produce receptor activator of nuclear factor kappa-B ligand (), which binds to on osteoclast precursors to promote their differentiation and activation, thereby enhancing bone resorption. In contrast, osteoprotegerin (), also secreted by osteocytes, acts as a decoy receptor that neutralizes RANKL, suppressing osteoclast formation. This dynamic ratio allows osteocytes to fine-tune resorption: an increased RANKL/OPG favors osteoclast activity, while elevated OPG inhibits it, ensuring targeted remodeling. Osteocytes further regulate bone formation by secreting sclerostin, a potent of Wnt/β-catenin signaling in . Sclerostin binds to low-density lipoprotein receptor-related protein 5/6 (/6) co-receptors, preventing Wnt binding and thereby suppressing β-catenin stabilization, which reduces osteoblast , , and mineralizing activity. This inhibition limits excessive bone formation during steady-state conditions. Notably, sclerostin expression decreases in response to loading from exercise, allowing enhanced Wnt signaling and osteoblast-driven bone formation to adapt to increased strain. In addition to soluble factors, serves as a signal for initiating remodeling at sites of potential damage. Apoptotic osteocytes lead to empty lacunae, which attract osteoclast precursors by upregulating expression in surrounding viable osteocytes and releasing factors that recruit and differentiate these precursors. This process targets resorption to microdamaged regions, removing necrotic tissue and facilitating repair by subsequent activity. Osteocytes, comprising over 90% of all cells, thus indirectly regulate the majority of bone turnover through these integrated mechanisms.

Mineral Homeostasis

Osteocytes contribute significantly to systemic mineral homeostasis by regulating phosphate and calcium balance through endocrine mechanisms, primarily via the production of fibroblast growth factor 23 (FGF23). As terminally differentiated cells embedded within the bone matrix, osteocytes sense circulating levels of phosphate and other ions, integrating local and systemic signals to maintain mineral ion concentrations essential for bone health and overall physiology. FGF23, secreted predominantly by osteocytes, targets the kidneys to inhibit phosphate reabsorption and suppress the renal production of active vitamin D (1,25-dihydroxyvitamin D), thereby reducing intestinal phosphate absorption and promoting phosphaturia. This action prevents excessive phosphate accumulation, which could otherwise lead to ectopic calcification or disrupted bone mineralization. Parathyroid hormone (PTH) interacts with osteocytes to fine-tune these processes, enhancing mineral mobilization during periods of calcium demand. in osteocytes downregulates sclerostin expression, an inhibitor of Wnt signaling that promotes activity and bone formation, while also stimulating FGF23 production to facilitate renal excretion. This dual regulation supports the release of calcium and from bone stores while preventing , as seen in conditions like where elevated PTH correlates with increased osteocytic FGF23. The interplay ensures coordinated mineral ion handling, with osteocytes acting as a key endocrine hub. Osteocytes are central to the of , as demonstrated in animal models where their dysregulated FGF23 production mimics human genetic disorders. In the Hyp mouse model of (XLH), a leads to osteocyte-specific overexpression of FGF23, resulting in excessive renal wasting, reduced serum , and impaired mineralization. Transgenic models with osteocyte-targeted FGF23 overexpression similarly exhibit , rickets-like skeletal defects, and elevated circulating FGF23, underscoring the osteocyte's dominant role in driving these phenotypes without requiring contributions from other cell types. These findings highlight how osteocyte dysfunction disrupts systemic balance, paralleling disorders like XLH and tumor-induced . Through ongoing endocrine signaling, osteocytes maintain daily serum phosphate within the physiological range of 2.5-4.5 mg/dL, responding to fluctuations from , , and hormonal cues. This fine-tuning involves pulsatile FGF23 release from the osteocyte , which propagates signals across to adjust renal handling and , ensuring stable mineral levels for skeletal integrity and preventing both hypo- and hyperphosphatemic states. Disruptions in this regulation, often osteocyte-driven, contribute to metabolic imbalances in and other systemic disorders.

Molecular Mechanisms

Signaling Pathways

Osteocytes, as the most abundant cells in bone, orchestrate intracellular and intercellular signaling to maintain skeletal , responding to mechanical cues and coordinating with osteoblasts and osteoclasts through specific cascades. These pathways, including the Wnt/β-catenin, calcium-oscillation, and TGF-β/Smad routes, enable osteocytes to transduce environmental signals into regulatory responses that influence bone formation and resorption. Crosstalk between these pathways further integrates mechanotransductive elements, ensuring adaptive . The canonical Wnt/β-catenin pathway plays a central role in osteocyte-mediated bone regulation, where sclerostin, secreted by osteocytes, binds to receptor-related proteins and LRP6, thereby antagonizing interactions and inhibiting downstream β-catenin stabilization and nuclear translocation in target cells such as . This inhibition suppresses osteoblast activity and formation, maintaining a balance in skeletal mass. Mechanical strain, such as that induced by loading, activates the pathway by downregulating sclerostin expression in osteocytes, allowing proteins to bind receptors and /6 co-receptors, which promotes β-catenin accumulation and transcription of anabolic genes. inhibition by sclerostin also contributes to by modulating activity through upregulation. In the calcium-oscillation pathway, oscillatory fluid flow through the lacunar-canalicular network shears osteocyte processes, triggering ATP release from osteocytes via hemichannels or other mechanisms. This extracellular ATP activates P2 purinergic receptors on osteocyte membranes, stimulating to produce 1,4,5-trisphosphate (IP₃), which in turn induces Ca²⁺ release from stores, generating intracellular Ca²⁺ oscillations that propagate as intercellular waves. These oscillations, more pronounced in osteocyte networks than in osteoblasts, amplify mechanosensory signals, leading to downstream activation of kinases and changes that support bone adaptation. The TGF-β/Smad pathway in osteocytes is activated when TGF-β, latent in the bone matrix, is released and bioactivated during osteoclast-mediated resorption in an acidic environment. TGF-β binds to type II and type I receptors (TβRII and TβRI), phosphorylating receptor-regulated Smads (Smad2/3), which complex with Smad4 to translocate to the and regulate target genes. This signaling promotes osteocyte survival by enhancing anti-apoptotic mechanisms, metabolic reprogramming such as via upregulation, and perilacunar remodeling to maintain cellular viability and matrix integrity. Crosstalk involving /TAZ mechanotransduction integrates cytoskeletal dynamics with gene regulation in osteocytes, where mechanical stimuli reorganize filaments via integrin-RhoA signaling, promoting nuclear translocation of YAP and TAZ transcriptional co-activators. YAP/TAZ then interact with TEAD factors to modulate osteogenic genes, including enhancement of activity, which drives differentiation-related transcription. This pathway links to Wnt/β-catenin by stabilizing β-catenin and cooperates with calcium signals through channels, forming a network that fine-tunes osteocyte responses to load and prevents maladaptive remodeling.

Secreted Factors

Osteocytes secrete a variety of biomolecules that facilitate intercellular communication within bone tissue and beyond. Among these, sclerostin stands out as a key regulator, a 190-amino acid encoded by the SOST gene and predominantly expressed in mature osteocytes rather than osteoblasts. This protein has a very short (on the order of minutes) in circulation, enabling rapid adjustments in its levels to respond to physiological cues. Another prominent secreted factor is , a 251-amino acid hormone primarily produced and released by osteocytes. undergoes proteolytic cleavage by , which processes the full-length intact form into inactive fragments, and its biological activity requires co-receptor interaction with klotho to bind fibroblast growth factor receptors effectively. In addition to sclerostin and FGF23, osteocytes release other factors such as , which promotes activation and differentiation; , an inhibitor of Wnt signaling; and insulin-like growth factors (IGFs), particularly IGF-1, which support osteocyte survival and bone formation processes. The secretion of these factors is tightly regulated by external stimuli. Mechanical loading rapidly downregulates sclerostin and FGF23 expression in osteocytes, often within hours, thereby modulating bone responses to physical stress. Conversely, advancing age is associated with increased expression of sclerostin and FGF23 in osteocytes, contributing to age-related alterations in .

Pathophysiology

Cell Death and Dysfunction

Osteocyte is primarily mediated through activation, involving the intrinsic pathway where mitochondrial outer membrane permeabilization by Bax and Bak releases , leading to the activation of effector such as caspase-3, -6, and -7. This process results in characteristic morphological changes, including shrinkage, nuclear condensation, and fragmentation into apoptotic bodies that are often phagocytosed by neighboring or osteoclasts. Key triggers include mechanical unloading, which disrupts the osteocyte lacunocanalicular network (LCN) and induces , leading to elevated in both trabecular and cortical of . Glucocorticoids promote via Fas/CD95 signaling and Pyk2 activation, increasing (ROS) production and downstream cascades. deficiency similarly elevates rates, with ovariectomy models showing up to a 15% increase in apoptotic osteocytes due to ROS overproduction and impaired survival signaling. In contrast to , osteocyte occurs prominently in conditions like osteonecrosis, where ischemic damage leads to uncontrolled and the formation of empty lacunae as a hallmark histological feature. This necrotic process compromises the structural integrity of , often resulting in microcracks that propagate due to disrupted LCN and reduced cellular support around lacunae. Empty lacunae in necrotic regions are associated with micropetrosis and diminished nutrient diffusion, exacerbating local tissue damage. Osteocyte dysfunction in aging involves hyperactivity of sclerostin, a Wnt signaling secreted by osteocytes, which increases with age and impairs LCN integrity by promoting matrix degradation and reducing mechanosensory communication. This sclerostin upregulation, observed in both and cortical osteocytes, contributes to diminished bone formation and network cohesion. Concurrently, aging elevates osteocyte , with osteocyte density decreasing by approximately 15–30% in older human , as evidenced by increased empty lacunae prevalence and reduced viability. Sclerostin levels also rise under mechanical unloading or disuse, further linking dysfunction to environmental cues. Protective mechanisms against osteocyte death include , which counters by enhancing cellular resilience through Beclin-1 and LC3-II activation, particularly in response to low-dose glucocorticoids or deficiency. Anti-apoptotic members of the , such as and , inhibit mitochondrial permeabilization and promote survival during unloading or fatigue, with overexpression preserving bone volume. These pathways intersect, as can bind Beclin-1 to balance and .

Role in Bone Diseases

Osteocytes play a central role in the pathogenesis of , particularly the postmenopausal form, where deficiency triggers increased osteocyte . This leads to the accumulation of empty lacunae, which signal for through the release of factors like , resulting in elevated activity and net loss. Concurrently, reduced levels upregulate sclerostin expression in surviving osteocytes, inhibiting Wnt/β-catenin signaling and suppressing osteoblast-mediated formation, thereby contributing to uncoupled remodeling where resorption outpaces formation. This condition is highly prevalent in postmenopausal women, affecting millions globally and increasing risk due to diminished density. In contrast, loss-of-function mutations in the SOST gene, which encodes sclerostin, underlie sclerosteosis—a high bone mass disorder often presenting with hyperdense bone resembling aspects of . These mutations abolish sclerostin production by osteocytes, removing inhibition of Wnt signaling and leading to excessive activity and progressive overgrowth, particularly in the and long bones, without primary defects in resorption. The resulting skeletal can cause neurological complications due to cranial compression, highlighting the critical regulatory role of osteocyte-derived sclerostin in maintaining mass balance. Van Buchem disease, another sclerostin-related high bone mass syndrome, arises from homozygous deletions in a regulatory enhancer element upstream of the SOST gene, specifically disrupting osteocyte-specific expression of sclerostin. This noncoding mutation reduces sclerostin levels, similarly derepressing Wnt signaling and promoting generalized bone thickening, though typically milder than in sclerosteosis and without the severe . Affected individuals exhibit elevated bone mineral density and increased fracture resistance, but face risks of and from endosteal . In mellitus, osteocytes exhibit localized sclerostin accumulation in the lacuno-canalicular system, contributing to cortical bone microstructural alterations and increased fragility. Recent research has linked osteocyte dysregulation of 23 (FGF23) to chronic kidney disease-mineral bone disorder (CKD-MBD), where elevated FGF23 secretion from osteocytes occurs early in disease progression as a response to . This dysregulation promotes renal wasting and suppresses 1,25-dihydroxyvitamin D synthesis, exacerbating and high-turnover bone disease, with contributions to vascular and fracture susceptibility in CKD patients. Post-2020 studies emphasize that osteocyte-specific FGF23 overproduction, driven by and uremic toxins, perpetuates mineral imbalances even as FGF23 resistance develops in advanced CKD, underscoring osteocytes as key mediators in this multifactorial disorder.

Clinical Implications

Disease Associations

Osteocyte density in human decreases by approximately 0.4% per year with advancing age, contributing to age-related bone fragility and elevated risk. This progressive loss, observed in histomorphometric analyses of cortical from adults aged 30 to 91 years, shows a reduction from about 210 to 150 lacunae per mm², independent of status, and aligns with broader declines in bone quality that heighten susceptibility to fractures. Recent studies from the further associate osteocyte-derived factors, such as fibroblast growth factor 23 (FGF23), with , where elevated FGF23 levels are linked to frailty and negative effects on muscle function in older adults, potentially contributing to the condition. In , promotes osteocyte , which is linked to increased cortical and bone fragility observed in both type 1 and type 2 diabetic patients. Experimental models demonstrate that sustained high glucose levels induce in osteocytes, reducing their and impairing skeletal integrity, thereby contributing to higher rates despite normal or elevated in affected individuals. This association underscores osteocyte vulnerability as a key factor in diabetic skeletal complications. Osteocytes facilitate to by secreting , which activates survival signaling in s via the receptor. This axis enhances tumor cell homing and persistence within the microenvironment. Such interactions highlight osteocytes' role in supporting viability during colonization. Genetic syndromes like autosomal dominant hypophosphatemic arise from gain-of-function in the FGF23 gene, primarily expressed in osteocytes, leading to excessive wasting and impaired mineralization. These stabilize FGF23 protein against proteolytic cleavage, resulting in elevated circulating levels that disrupt renal reabsorption and cause rickets-like skeletal deformities from childhood. Osteocyte-specific overproduction of mutant FGF23 directly drives the hypophosphatemic phenotype in affected families.

Therapeutic Targets

Osteocytes, as key regulators of through the secretion of sclerostin, have emerged as primary targets for anabolic therapies in and related bone disorders. Anti-sclerostin antibodies, such as , directly inhibit this osteocyte-derived protein to enhance Wnt signaling and promote bone formation while reducing resorption. , a humanized , was approved by the FDA in 2019 for the treatment of postmenopausal in women at high risk for fracture. In the phase 3 trial, monthly of (210 mg) for 12 months increased lumbar spine bone mineral density (BMD) by 11.3% compared to , with sustained benefits after transitioning to , and reduced the risk of new vertebral fractures by 73% at 12 months and clinical fractures by 33% at 24 months. Parathyroid hormone (PTH) analogs, including , indirectly target osteocytes by suppressing sclerostin expression during intermittent dosing, thereby amplifying bone formation via enhanced Wnt/β-catenin signaling. , a recombinant fragment of PTH (1-34), is FDA-approved for severe and administered as daily subcutaneous injections (20 μg) for up to 2 years. Clinical studies demonstrate that this regimen reduces serum sclerostin levels in postmenopausal women with , leading to significant BMD gains (e.g., 9-13% at the lumbar spine after 18-24 months) and a 65% reduction in vertebral fracture risk compared to . Emerging therapies in the 2020s further exploit osteocyte functions for targeted interventions. FGF23 inhibitors, such as burosumab (a against FGF23, an osteocyte-secreted phosphaturic ), address in conditions like (XLH) by normalizing serum phosphate levels and improving bone mineralization; phase 3 trials showed sustained phosphate elevation and reduced disease burden with monthly dosing. Gene therapies aimed at SOST , which cause sclerosteosis (a high-bone-mass disorder due to sclerostin deficiency), are under preclinical exploration to silence SOST expression in osteocytes using adeno-associated virus (AAV) vectors, potentially mimicking anabolic effects for without chronic antibody administration. Additionally, like alendronate protect osteocytes from induced by glucocorticoids or deficiency, preserving their regulatory role in ; studies in mice demonstrate that non-resorptive bisphosphonate analogs prevent osteocyte death and maintain strength. Despite these advances, therapeutic targeting of osteocytes presents challenges, particularly with , where 2023 meta-analyses have highlighted potential cardiovascular risks, including increased incidence of (e.g., and ) in patients with preexisting risk factors, prompting a black-box warning from regulatory agencies. As of 2025, real-world studies indicate romosozumab does not significantly increase cardiovascular risk compared to other anti-osteoporotic treatments in postmenopausal women, though contraindications remain for those with recent cardiovascular events. Ongoing real-world studies and network meta-analyses continue to evaluate these safety concerns to refine patient selection and monitoring protocols.

References

  1. [1]
    Histology, Osteocytes - StatPearls - NCBI Bookshelf - NIH
    Osteocytes are one of the four kinds of bone cells. Due to derivation from osteoblasts, these cells are highly specialized in nature and are responsible for ...Structure · Function · Tissue Preparation · Histochemistry and...
  2. [2]
    Biology of Bone Tissue: Structure, Function, and Factors That ...
    Osteocytes, which comprise 90–95% of the total bone cells, are the most abundant and long-lived cells, with a lifespan of up to 25 years [54]. Different from ...2. Bone Cells · 2.1. Osteoblasts · 2.4. Osteoclasts
  3. [3]
    The osteocyte as a signaling cell | Physiological Reviews
    Instead, osteocytes are multifunctional and dynamic cells capable of integrating hormonal and mechanical signals and transmitting them to effector cells in bone ...
  4. [4]
    Osteocyte Shape and Mechanical Loading - PMC - NIH
    Osteocyte lacunae in woven bone have an irregular spherical shape [19, 20] ... spherical or oblate. They suggested that these differences in morphology ...
  5. [5]
    The Osteocyte: An Endocrine Cell … and More - PMC
    Osteocytes reside in lacunae within the mineralized bone matrix and send their dendritic processes (ranging from 40–100 per cell [1]) through tiny tunnels ...
  6. [6]
    Significance of mechanical loading in bone fracture healing, bone ...
    These cuboidal cells (diameter of 9.33–29.91 μm) have abundant rough endoplasmic reticulum, a prominent Golgi apparatus, and various secretory vesicles, ...
  7. [7]
    The osteocyte and its osteoclastogenic potential - PubMed Central
    May 24, 2023 · They estimated the average total number of lacunae to be 44 billion and live osteocytes to be 42 billion, indicating that approximately 1% of ...
  8. [8]
    Osteocytes: Their Lacunocanalicular Structure and ... - NIH
    Apr 15, 2022 · This network is composed of an intracellular network through osteocyte processes and gap junctions, and an extracellular network through lacunae ...
  9. [9]
    Spatial heterogeneity in the canalicular density of the osteocyte ...
    Applied to the OCLN in sheep it was demonstrated that 80% of the bone matrix is within a distance of only 1.4 μm to the closest canaliculus (Kerschnitzki et al.
  10. [10]
    Control of Bone Matrix Properties by Osteocytes - Frontiers
    Osteocytes make up 90–95% of the cellular content of bone and form a rich dendritic network with a vastly greater surface area than either osteoblasts or ...
  11. [11]
    Connexin 43 in the function and homeostasis of osteocytes - NIH
    Connexin 43 (Cx43) is the main gap junction (GJ) protein and hemichannel protein in bone tissue. It is involved in the formation of hemichannels and GJs.
  12. [12]
    Oscillating fluid flow activation of gap junction hemichannels ...
    Gap junctions (GJs) between osteocytes and osteoblasts provides a mechanism whereby flow-induced signals are detected by osteocytes and transduced to ...
  13. [13]
    Differences in osteocyte and lacunar density between Black and ...
    Values in recent human studies range from 20, 000–30, 000/mm3 [31–33]. Since it has been estimated that 5% of osteocyte lacunae are empty [25,28], this suggests ...Missing: per | Show results with:per
  14. [14]
    Bone metabolism and evolutionary origin of osteocytes - Science
    Mar 31, 2021 · Our results demonstrate that the earliest known osteocytes in the fossil record had similar morphology and likely similar physiological ...Bone Metabolism And... · Osteocyte Lacunae · Canaliculi And...
  15. [15]
    Bone metabolism and evolutionary origin of osteocytes - NIH
    Mar 31, 2021 · Our results demonstrate that the earliest known osteocytes in the fossil record had similar morphology and likely similar physiological ...Osteocyte Lacunae · Canaliculi And... · References And Notes
  16. [16]
    Cell signaling and transcriptional regulation of osteoblast lineage ...
    Jul 2, 2024 · The initiation of osteogenesis primarily occurs as mesenchymal stem cells undergo differentiation into osteoblasts. This differentiation ...Missing: percentage | Show results with:percentage
  17. [17]
    The osteocyte as a signaling cell - PMC - PubMed Central
    Approximately 5–20% of osteoblasts undergo terminal differentiation and become osteocytes. The remainder either die by apoptosis or flatten and turn into ...
  18. [18]
    Buried alive: How osteoblasts become osteocytes - Franz‐Odendaal
    Oct 28, 2005 · This review explores the osteoblast-to-osteocyte transformation during intramembranous ossification from both morphological and molecular perspectives.OSTEOBLAST FATES AND... · THE TRANSFORMATION... · CHOOSING A MODEL
  19. [19]
    Osteocyte differentiation is regulated by extracellular matrix stiffness ...
    ECM stiffness and cell seeding density have been shown to regulate osteoblast differentiation, but the precise cues that initiate osteoblast–osteocyte ...
  20. [20]
    The Osteocyte Transcriptome: Discovering messages buried within ...
    Lineage tracing is a method to identify and track cells within transgenic mice generated so that specific cell populations express a reporter gene (e.g. a ...
  21. [21]
    From inside your bones: Osteocytic signaling pathways as ...
    Sep 5, 2018 · Osteocytes are differentiated osteoblasts that become surrounded by matrix during the process of bone formation.
  22. [22]
    Extracellular Matrix Mineralization Promotes E11/gp38 Glycoprotein ...
    This was confirmed by the decreased expression of the osteocyte-marker genes Dmp1, Phex, Sost and Cd44 by MLO-A5 under mineralization-inhibited conditions; ...
  23. [23]
    The role of matrix mineralisation in osteoblast to osteocyte ...
    Aug 6, 2025 · During bone formation, osteoblasts are embedded in a collagen-rich osteoid tissue and differentiate into an extensive 3D osteocyte network ...
  24. [24]
    Advancing Our Understanding of Osteocyte Cell Biology - PMC - NIH
    DMP1 is expressed in early embedding osteocytes. Sclerostin is only expressed in deeply-embedded late osteocytes.Missing: stages | Show results with:stages
  25. [25]
    Osteocyte intrinsic TGFβ signaling regulates bone quality through ...
    Further supporting the osteocyte intrinsic role of TGFβ, TGFβ induced the expression of the osteocyte marker genes Sclerostin (Sost) and dentin matrix protein-1 ...
  26. [26]
    Osteocyte - an overview | ScienceDirect Topics
    The osteocyte is defined as a cell surrounded by mineralized matrix. Osteocyte apoptosis is linked to bone remodeling as a result of what is called the ...
  27. [27]
    Molecular mechanosensors in osteocytes | Bone Research - Nature
    Jun 8, 2020 · Osteocytes, the most abundant and long-lived cells in bone, are the master regulators of bone remodeling. In addition to their functions in ...
  28. [28]
    Mechanosensation and Transduction in Osteocytes - PMC
    Fluid flow shear stress may induce mechanosensation in osteocytes through perturbation of integrins (34). Integrins, comprised of heterodimers of α and β ...
  29. [29]
    In situ intracellular calcium oscillations in osteocytes in intact mouse ...
    This study provides direct evidence that osteocytes respond to in situ mechanical loading by Ca 2+ oscillations, which are dependent on the P 2 R/PLC/inositol ...
  30. [30]
    Sclerostin's role in bone's adaptive response to mechanical loading
    It then led to proposal of the simple model that local, loading-related down-regulation of osteocyte sclerostin increases bone formation by relieving inhibition ...
  31. [31]
    Deletion of a Single β-catenin Allele in Osteocytes Abolishes ... - NIH
    Our loading studies demonstrate that deletion of a single allele of β-catenin in osteocytes abolishes anabolic load-induced new bone formation. Our studies also ...
  32. [32]
    Osteocyte-Driven Bone Remodeling - PMC - NIH
    Whereas empty lacunae and living osteocytes lacking OPG are distributed throughout cortical bone of mice lacking osteocytic C×43, apoptotic osteocytes ...
  33. [33]
    Osteocyte Regulation of Receptor Activator of NF-κB Ligand ...
    Osteocytes are involved in bone remodeling by contributing in RANKL/OPG regulation. ... empty lacunae and higher RANKL/OPG ratio in osteocytes of this ...
  34. [34]
    The Osteocyte: New Insights - PMC - NIH
    The earliest evidence for the existence of osteocytes within bone comes from jawless fish that lived during the Ordovician period (1). The remains of osteocytes ...Missing: 1856 | Show results with:1856
  35. [35]
    The Mechanosensory Role of Osteocytes and Implications for Bone ...
    Osteocytes regulate this dynamic equilibrium by releasing signaling molecules such as osteoprotegerin (OPG), sclerostin, dickkopf-related protein 1 (DKK1), ...
  36. [36]
    OSTEOCYTE APOPTOSIS - PMC - PubMed Central - NIH
    Dec 11, 2012 · Osteocyte apoptosis is induced by weightlessness in mice and precedes osteoclast recruitment and bone loss. J Bone Miner Res. 2006;21:605–15 ...
  37. [37]
    Apoptotic osteocytes and the control of targeted bone resorption - PMC
    Apoptotic osteocytes, in turn, recruit osteoclasts to initiate targeted bone resorption. This results in the removal of “dead” bone and may improve the ...
  38. [38]
    Roles of osteocytes in phosphate metabolism - PubMed
    Jul 15, 2022 · Osteocytes also govern phosphate homeostasis through the production of fibroblast growth factor 23 (FGF23), which lowers serum phosphate levels.
  39. [39]
    Skeletal secretion of FGF-23 regulates phosphate and vitamin D ...
    Jan 17, 2012 · FGF-23 is secreted by osteoblasts and osteocytes in bone and principally targets the kidney to regulate the reabsorption of phosphate.
  40. [40]
    Advances in understanding of phosphate homeostasis and related ...
    Aug 29, 2022 · FGF23, which is mainly produced by osteocytes in bone, plays a central role in Pi homeostasis and exerts its effects by binding to the FGF ...
  41. [41]
    Parathyroid hormone receptor signaling in osteocytes increases the ...
    Jun 25, 2011 · We now report that PTH receptor activation also regulates in vivo and in vitro the expression of fibroblast growth factor 23 (FGF23), an ...
  42. [42]
    Sclerostin Directly Stimulates Osteocyte Synthesis of Fibroblast ...
    Osteocyte produced fibroblast growth factor 23 (FGF23) is the key regulator of serum phosphate (Pi) homeostasis. The interplay between parathyroid hormone (PTH) ...
  43. [43]
    Parathyroid Hormone Regulates Circulating Levels of Sclerostin and ...
    Feb 18, 2022 · These results indicate that the high level of PTH in PHPT mice leads to increased FGF23 and decreased sclerostin expression in serum and calvaria.
  44. [44]
    Distinct roles for intrinsic osteocyte abnormalities and ... - PubMed
    Sep 11, 2007 · We found that increased FGF23 expression in Hyp bone results from a local effect of PHEX deficiency, since FGF23 was increased in Hyp osteocytes ...
  45. [45]
    Osteocyte-specific deletion of Fgfr1 suppresses FGF23 - PubMed - NIH
    Aug 4, 2014 · Increases in fibroblastic growth factor 23 (FGF23 or Fgf23) production by osteocytes result in hypophosphatemia and rickets in the Hyp mouse ...
  46. [46]
    Osteocyte regulation of phosphate homeostasis and bone ... - PubMed
    Osteocyte regulation of phosphate homeostasis and bone mineralization underlies the pathophysiology of the heritable disorders of rickets and osteomalacia.
  47. [47]
    FGF23 production by osteocytes - PubMed - NIH
    Fibroblast growth factor 23 (FGF23), a known regulator of phosphate homeostasis, is produced by cells residing in bone, namely, osteocytes, to target a distant ...
  48. [48]
    Sclerostin and Osteocalcin: Candidate Bone-Produced Hormones
    Mar 9, 2021 · Sclerostin is a secreted glycoprotein expressed predominantly by mature osteocytes that is best known as a negative regulator of bone formation ...
  49. [49]
    Sclerostin: From Molecule to Clinical Biomarker - MDPI
    Apr 26, 2022 · Sclerostin, a glycoprotein encoded by the SOST gene, is mainly produced by mature osteocytes and is a critical regulator of bone formation.
  50. [50]
    Disparate bone anabolic cues activate bone formation by regulating ...
    Notably, in the absence of a stimulus, the half-life of sclerostin protein is about 3 hr (Figure 3—figure supplement 1B).
  51. [51]
    FGF23 Synthesis and Activity - PMC - PubMed Central - NIH
    The phosphaturic hormone FGF23 is produced primarily in osteoblasts/osteocytes and is known to respond to increases in serum phosphate and 1,25(OH) 2 vitamin D ...
  52. [52]
    1,25-Dihydroxyvitamin D 3 regulates furin-mediated FGF23 cleavage
    Sep 8, 2023 · FGF23 comprises an N-terminal FGF homology domain and a C-terminal domain that interacts with the coreceptor Klotho. Full-length iFGF23 is ...
  53. [53]
    FGF23 Actions on Target Tissues—With and Without Klotho - PMC
    By stimulating FGFR/klotho complexes in the kidney and parathyroid gland, FGF23 reduces renal phosphate uptake and secretion of parathyroid hormone, ...
  54. [54]
    Osteocyte-Related Cytokines Regulate Osteoclast Formation ... - MDPI
    Multiple myeloma cells induce osteocyte apoptosis that increases osteocyte-derived sclerostin and the RANKL/OPG ratio, resulting in osteoclast formation and ...Osteocyte-Related Cytokines... · 3. Osteocyte-Related... · 3.1. Rankl And OpgMissing: empty | Show results with:empty
  55. [55]
    The Osteocyte as the New Discovery of Therapeutic Options in Rare ...
    Osteocytes produce a variety of proteins and signaling molecules such as sclerostin, cathepsin K, Wnts, DKK1, DMP1, IGF1, and RANKL/OPG to regulate osteoblast ...
  56. [56]
    Osteocyte-derived insulin-like growth factor I is essential for ...
    This study sought to determine whether deficient Igf1 expression in osteocytes would affect loading-induced osteogenic response. Tibias of osteocyte Igf1 ...
  57. [57]
    Osteocyte control of bone remodeling: is sclerostin a key molecular ...
    Jul 17, 2014 · This review presents a model suggesting that sclerostin is major mediator for integrating mechanical, local, and hormonal signals, sensed by the osteocytes.
  58. [58]
    Mapping the Response of Human Osteocytes in Native Matrix to ...
    SOST gene expression and sclerostin production are decreased by mechanical loading in osteocytes. ... FGF23 messenger RNA (mRNA) is decreased by mechanical ...Materials And Methods · Human Bone Retrieval And... · Results
  59. [59]
    Effects of Age on Bone mRNA Levels of Sclerostin and Other Genes ...
    Several previous clinical studies have shown that circulating sclerostin levels increase with age, raising the possibility that increased production of ...
  60. [60]
    Roles of osteocytes in phosphate metabolism - Frontiers
    The osteocytic expression of DMP1 and PHEX declines from youth to adulthood, which leads to an increase in the production of FGF23 and decrease in serum ...
  61. [61]
    Osteocyte apoptosis: the roles and key molecular mechanisms in ...
    Oct 12, 2020 · All results strongly suggest that estrogen deficiency could give rise to osteocyte apoptosis, followed by resorption-related bone loss. It ...
  62. [62]
    Definition of bone necrosis by the pathologist - PMC - NIH
    It has long been accepted that the histologic sign indicative of osteonecrosis is empty osteocytic lacunae, but it is now clear that artefactual loss of ...
  63. [63]
    The Amazing Osteocyte - PMC - NIH
    Osteocytes compose 90% to 95% of all bone cells in adult bone and are the longest lived bone cell, up to decades within their mineralized environment.Missing: tracing | Show results with:tracing
  64. [64]
    Sclerostin Immunoreactivity Increases in Cortical Bone Osteocytes ...
    Although serum levels of sclerostin markedly increase with age, relatively little is known about whether cells in the skeleton change their expression of ...
  65. [65]
    Localized sclerostin accumulation in osteocyte lacunar-canalicular ...
    Apr 25, 2025 · Elevated SOST likely contributes to LCS dysfunction through two primary mechanisms: upregulation of PLR-related matrix-degrading enzymes and ...
  66. [66]
    Differential Bone Adaptation to Mechanical Unloading and ... - NIH
    Dec 16, 2022 · By 10 weeks of age, approximately 50% of osteocytes are dead and by 16 weeks of age 75% of osteocytes have died [13, 14], establishing these ...
  67. [67]
    Sclerostin, an emerging therapeutic target for treating osteoporosis ...
    The activation of the bone remodelling process is mediated by osteocytes through osteocyte apoptosis, which recruits osteoclasts precursor cells for bone ...
  68. [68]
    The Role of Sclerostin in Bone Diseases - PMC - NIH
    Feb 2, 2022 · Sclerostin's downregulation was attributed to increased osteocyte apoptosis [59]. Low sclerostin expression causes enhanced osteoblast ...
  69. [69]
    Sclerostin Is an Osteocyte-expressed Negative Regulator of Bone ...
    Sclerosteosis, a skeletal disorder characterized by high bone mass due to increased osteoblast activity, is caused by loss of the SOST gene product, sclerostin.
  70. [70]
    Genetics of Sost/SOST in sclerosteosis and van Buchem disease ...
    In bone, SOST is expressed predominantly by osteocytes and sclerostin suppresses bone formation by inhibiting the canonical Wnt signaling pathway. Here we ...2. Sclerosteosis · 3. Van Buchem Disease · 5. Sclerostin
  71. [71]
    Targeted deletion of Sost distal enhancer increases bone ... - PNAS
    Aug 10, 2012 · Unlike sclerosteosis, VB patients lack SOST coding mutations but carry a homozygous 52 kb noncoding deletion that is essential for the ...
  72. [72]
    How FGF23 shapes multiple organs in chronic kidney disease - PMC
    Sep 18, 2021 · This short review summarizes regulators of FGF23 synthesis altered in CKD and the main CKD-mediated organ dysfunctions related to high FGF23 levels.
  73. [73]
    Molecular pathophysiology of chronic kidney disease–mineral and ...
    Feb 27, 2025 · In CKD, elevated FGF23 levels and reduced Klotho expression contribute to mineral homeostasis disturbances and bone abnormalities. The ...
  74. [74]
    Osteocyte density changes in aging and osteoporosis - PubMed
    In healthy adults ranging from 30 to 91 years, lacunar number per bone area decreases with advancing age, from about 210/mm(2) to 150/mm(2). Significantly ...
  75. [75]
    The Role of Osteokines in Sarcopenia: Therapeutic Directions and ...
    We comprehensively summarize the latest research progress on the effects of the osteokines FGF-23, IGF-1, RANKL and osteocalcin on muscle.
  76. [76]
    Hyperglycemia compromises Rat Cortical Bone by Increasing ...
    Jan 9, 2020 · Uncontrolled diabetes is associated with increased risk of bony fractures. However, the mechanisms have yet to be understood.
  77. [77]
    Diabetes Mellitus-induced Bone Fragility - PMC - NIH
    Furthermore, osteocyte apoptosis may be associated with cortical porosity in DM-induced bone fragility. Dysfunction of Osteoblasts and Osteocytes in DM. 1 ...
  78. [78]
    The Emerging Role of Osteocytes in Cancer in Bone
    Feb 13, 2019 · 64-66 Osteocytes produce CXCL12 and therefore could activate the CXCL12-CXCR4 signaling axis in cancer cells, favoring their homing to bone.
  79. [79]
    Pathological Crosstalk between Metastatic Breast Cancer Cells and ...
    Through activation of the CXCL12-CXCR4 signaling cascade in cancer cells, osteocytes could consequently mediate cancer cell homing to bone. Importantly, there ...
  80. [80]
    Coupling fibroblast growth factor 23 production and cleavage
    Recent findings: Autosomal dominant hypophosphatemic rickets (ADHR) is caused by gain-of-function mutations in FGF23 that prevent its proteolytic cleavage ...
  81. [81]
    Physiological Actions of Fibroblast Growth Factor-23 - Frontiers
    Introduction. In the year 2000, gain-of-function mutations in fibroblast growth factor-23 (FGF23) were identified as the genetic cause of autosomal ...
  82. [82]
    Romosozumab Treatment in Postmenopausal Women with ...
    Sep 18, 2016 · Romosozumab was associated with a lower risk of vertebral fracture than placebo at 12 months and, after the transition to denosumab, at 24 months.
  83. [83]
    Sclerostin antibody stimulates periodontal regeneration in large ...
    Oct 1, 2020 · Based on those studies, Evenity was approved in 2019 by the Food and Drug Administration (FDA) and other regulatory agencies as a bone-forming ...
  84. [84]
    Once-weekly teriparatide reduces serum sclerostin levels ... - PubMed
    Dec 17, 2018 · The present study showed that once-weekly teriparatide treatment reduced serum sclerostin levels in postmenopausal women with osteoporosis.
  85. [85]
    Teriparatide - StatPearls - NCBI Bookshelf
    Teriparatide is a medication used in the management and treatment of osteoporosis. The drug is in the anabolic class of osteoporosis medications.
  86. [86]
    Clinical effects of teriparatide, abaloparatide, and romosozumab in ...
    Jul 15, 2024 · Furthermore, PTH decreases sclerostin expression, a bone formation inhibitor primarily produced by osteocytes, further promoting bone formation ...
  87. [87]
    FGF23, Hypophosphatemia, and Emerging Treatments - PMC - NIH
    Anti‐FGF23 neutralizing antibody therapy such as burosumab has emerged as a safe and effective treatment for X‐linked hypophosphatemia and can rapidly stabilize ...Missing: 2020s | Show results with:2020s
  88. [88]
    WNT-modulating gene silencers as a gene therapy for osteoporosis ...
    In contrast, AAV-mediated silencing of Sost in osteocytes primarily affects the osteoblasts residing on the surface of cortical bone in close proximity to ...
  89. [89]
    Prevention of osteocyte and osteoblast apoptosis by ...
    The results of the studies reported herein demonstrate that bisphosphonates inhibit osteocyte and osteoblast apoptosis, regardless of the proapoptotic stimulus ...Missing: protect | Show results with:protect
  90. [90]
    Cardiac Arrhythmia and Heart Failure Shortly After Starting ... - NIH
    Dec 11, 2023 · Similarly, another systematic review and meta-analysis revealed comparable rates of total and severe adverse events between romosozumab and the ...
  91. [91]
    Treatment effects, adverse outcomes and cardiovascular safety of ...
    It is known that there is a warning for romosozumab in which there is potential risk of serious cardiovascular events such as myocardial infarction and stroke.