Disruption of claudin-18 diminishes ovariectomy-induced bone loss in mice

Kim, Ha-Young; Alarcon, Catrina; Pourteymour, Sheila; Wergedal, Jon E.; Mohan, Subburaman

doi:10.1152/ajpendo.00408.2012

Cited by 9 publications

(13 citation statements)

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“…) or studied after 2 months of ovariectomy (Kim et al. ). This rapid and severe bone loss would be associated with increased fracture risk and is therefore clinically relevant.…”

Section: Discussionmentioning

confidence: 99%

Concurrent muscle and bone deterioration in a murine model of cancer cachexia

Choi

Carruthers

Zhang³

et al. 2013

Physiol Rep

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Cachexia is defined as an excessive, involuntary loss of fat and lean tissue. We tested the validity of the Lewis lung carcinoma (LLC) as a model of cancer cachexia and examined its effect on the two major lean tissue components, skeletal muscle and bone. LLC cells (0.75 × 106) were injected into the left thigh of C57BL/6 mice. Control mice received an equal volume injection of growth media. Tumors were observed in all LLC-injected animals 21 and 25 days post inoculation. LLC-injected animals showed significant reductions in fat and lean mass despite having the same average daily caloric intake as media-treated mice. Global bone mineral density (BMD) had fallen by 5% and 6% in the LLC animals at 21 and 25 days, respectively, compared to a BMD increase of 5% in the 25-day media-treated animals. Extensor digitorum longus (EDL) muscles (isolated from the noninjected hindlimb) showed earlier and quantitatively greater losses in mass, physiological cross-sectional area (pCSA), and tetanic force compared to soleus muscles from the same hindlimb. By the 25th day post-LLC inoculation, EDL force/pCSA was reduced by 19% versus media treatment. This loss in specific force was not trivial as it accounted for about one-third of the reduction in EDL absolute force at this time point. Muscle strips dissected from the diaphragm of LLC mice also exhibited significant reductions in force/pCSA at day 25. We conclude that LLC is a valid model of cachexia that induces rapid losses in global BMD and in limb and respiratory muscle function.

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“…) or studied after 2 months of ovariectomy (Kim et al. ). This rapid and severe bone loss would be associated with increased fracture risk and is therefore clinically relevant.…”

Section: Discussionmentioning

confidence: 99%

Concurrent muscle and bone deterioration in a murine model of cancer cachexia

Choi

Carruthers

Zhang³

et al. 2013

Physiol Rep

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“…By contrast and unexpectedly, evaluation of the skeletal phenotype of ovariectomized or sham operated Cldn-18 KO mice revealed that ovariectomy failed to induce a significant change in BMD and trabecular architecture at different skeletal sites (36). Based on these findings and given that its expression is regulated by estrogen, Cldn-18 may act downstream of estrogen and mediate (at least in part) its effects on osteoclasts (36). It is worth noting that several line of evidence have suggested that the osteoprotective effect of estrogen is in part mediated by modulating osteoblast expression of cytokines that regulate osteoclast activity (55,56).…”

Section: Known Functions Of the Cldnsmentioning

confidence: 93%

“…Recent work by our laboratory on bone cells revealed that Cldn-18 expression is regulated by estrogen (36). In fact, the mRNA levels of Cldn-18 were found to be reduced by 93% in bones of ovariectomized (estrogen deficient) mice compared with sham operated animals, whereas estrogen treatment increased Cldn-18 mRNA levels in bone cells, in vitro (36) (Figure 2A).…”

Section: Regulation Of Cldn Expressionmentioning

confidence: 93%

“…In fact, the mRNA levels of Cldn-18 were found to be reduced by 93% in bones of ovariectomized (estrogen deficient) mice compared with sham operated animals, whereas estrogen treatment increased Cldn-18 mRNA levels in bone cells, in vitro (36) (Figure 2A). Furthermore, Cldn-18 is thought to be a novel estrogen target in the skeleton, as its deletion protects from estrogen deficiency induced bone loss in mice (36). …”

Section: Regulation Of Cldn Expressionmentioning

confidence: 99%

“…These studies revealed that bone resorption parameters were significantly increased by the combined deficiency of calcium and Cldn-18 compared with either calcium or Cldn-18 deficiency alone (32), but the underlying mechanisms that contributed to the interaction between the signaling pathways induced by calcium deficiency and Cldn-18 deficiency remained to be established. By contrast and unexpectedly, evaluation of the skeletal phenotype of ovariectomized or sham operated Cldn-18 KO mice revealed that ovariectomy failed to induce a significant change in BMD and trabecular architecture at different skeletal sites (36). Based on these findings and given that its expression is regulated by estrogen, Cldn-18 may act downstream of estrogen and mediate (at least in part) its effects on osteoclasts (36).…”

Section: Known Functions Of the Cldnsmentioning

confidence: 99%

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Emerging Multifunctional Roles of Claudin Tight Junction Proteins in Bone

Alshbool

Mohan

2014

Endocrinology

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The imbalance between bone formation and resorption during bone remodeling has been documented to be a major factor in the pathogenesis of osteoporosis. Recent evidence suggests a significant role for the tight junction proteins, Claudins (Cldns), in the regulation of bone remodeling processes. In terms of function, whereas Cldns act "canonically" as key determinants of paracellular permeability, there is considerable recent evidence to suggest that Cldns also participate in cell signaling, ie, a "noncanonical function". To this end, Cldns have been shown to regulate cell proliferation, differentiation, and gene expression in a variety of cell types. The present review will discuss Cldns' structure, their expression profile, regulation of expression, and their canonical and non- canonical functions in general with special emphasis on bone cells. In order to shed light on the noncanonical functions of Cldns in bone, we will highlight the role of Cldn-18 in regulating bone resorption and osteoclast differentiation. Collectively, we hope to provide a framework for guiding future research on understanding how Cldns modulate osteoblast and osteoclast function and overall bone homeostasis. Such studies should provide valuable insights into the pathogenesis of osteoporosis, and may highlight Cldns as novel targets for the diagnosis and therapeutic management of osteoporosis.

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Novel Role for Claudin-11 in the Regulation of Osteoblasts via Modulation of ADAM10-Mediated Notch Signaling

Lindsey

Xing

Pourteymoor

et al. 2019

Journal of Bone and Mineral Research

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The claudin (Cldn) family comprises 27 members of 20 to 34 kDa transmembrane tight junction proteins. In addition to Cldns' established canonical role as barriers controlling paracellular flow of molecules, a distinct noncanonical role for them as mediators of cell signaling is now emerging. In our studies evaluating Cldn family expression levels during osteoblast differentiation, Cldn-11 showed the largest increase (60-fold). Immunohistochemistry studies revealed high Cldn-11 expression in trabecular (Tb) bone lining cells. Micro-CT analysis of femurs and vertebrae of Cldn-11 knock-out (KO) mice at 12 weeks of age exhibited a 40% (p < 0.01) reduction in Tb bone volume adjusted for tissue volume compared with control mice, a change caused by significant reductions in Tb number and thickness and increase in Tb separation. Histomorphometry and serum biomarker studies revealed that reduced bone formation, not increased resorption, is the cause for reduced Tb bone volume in the Cldn-11 KO mice. Cldn-11 KO osteoblasts expressed reduced ALP and BSP, whereas Cldn-11 overexpression in MC3T3-E1 cells increased expression of ALP and BSP. Mechanistically, Cldn-11 interacted with tetraspanin (Tspan)3 in osteoblasts, and Tspan3 knockdown reduced osteoblast differentiation. Because members of the Tspan family regulate cell functions via Notch signaling, we evaluated whether Cldn-11/ Tspan3 regulates Notch signaling in osteoblasts. Accordingly, Notch targets Hey1 and Hey2 were significantly upregulated in Cldn-11 overexpressing cultures but downregulated in both Cldn-11 KO and Tspan3 knockdown osteoblasts. Because ADAM10 has been shown to interact with Tspan family members to regulate Notch signaling, we evaluated whether Cldn-11 regulates ADAM10 expression. Cldn-11 overexpressing cells express more mature ADAM10, and an ADAM10 inhibitor blocked the Cldn-11 effect on osteoblast differentiation. Based on these data, we propose Cldn-11 as a novel component of an osteoblast cell surface protein complex, comprising Tspan3 and ADAM10, which regulates Notch signaling and cell differentiation.

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Disruption of claudin-18 diminishes ovariectomy-induced bone loss in mice

Cited by 9 publications

References 50 publications

Concurrent muscle and bone deterioration in a murine model of cancer cachexia

Concurrent muscle and bone deterioration in a murine model of cancer cachexia

Emerging Multifunctional Roles of Claudin Tight Junction Proteins in Bone

Novel Role for Claudin-11 in the Regulation of Osteoblasts via Modulation of ADAM10-Mediated Notch Signaling

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