Your search keyword '"Gang-Qing Yao"' showing total 25 results

1. AgRP Neurons Regulate Bone Mass

Author

Jae Geun Kim, Ben-Hua Sun, Marcelo O. Dietrich, Marco Koch, Gang-Qing Yao, Sabrina Diano, Karl Insogna, and Tamas L. Horvath

Subjects

Biology (General), QH301-705.5

Abstract

The hypothalamus has been implicated in skeletal metabolism. Whether hunger-promoting neurons of the arcuate nucleus impact the bone is not known. We generated multiple lines of mice to affect AgRP neuronal circuit integrity. We found that mice with Ucp2 gene deletion, in which AgRP neuronal function was impaired, were osteopenic. This phenotype was rescued by cell-selective reactivation of Ucp2 in AgRP neurons. When the AgRP circuitry was impaired by early postnatal deletion of AgRP neurons or by cell autonomous deletion of Sirt1 (AgRP-Sirt1−/−), mice also developed reduced bone mass. No impact of leptin receptor deletion in AgRP neurons was found on bone homeostasis. Suppression of sympathetic tone in AgRP-Sirt1−/− mice reversed osteopenia in transgenic animals. Taken together, these observations establish a significant regulatory role for AgRP neurons in skeletal bone metabolism independent of leptin action.

Published

2015

2. An Unusual Case of Rickets and How Whole Exome Sequencing Helped to Correct a Diagnosis

Author

Patricia R. Peter, MD, Catherine A. Brownstein, PhD, Gang-Qing Yao, MD, Elizabeth A. Olear, MS, MA, Christine A. Simpson, MS, MT (ASCP), Pankaj B. Agrawal, MD, MMSC, Thomas O. Carpenter, MD, and Karl L. Insogna, MD

Subjects

Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

ABSTRACT: Objective: Rickets can be caused by a wide variety of underlying nutritional deficiencies or genetic defects. There is significant overlap in the clinical presentations of the various forms of rickets and the risk for misdiagnosis is great. This report describes a diagnostically challenging case of rickets that highlights important differences between two forms of rickets and demonstrates how gene sequencing technology can be instrumental in the identification and further characterization of these diseases.Methods: A patient diagnosed with X-linked hypophosphatemia (XLH) as a toddler did not develop many of the classic clinical features of this disease over time, calling the diagnosis into question. Whole exome sequencing (WES) was performed in this setting to determine the genetic basis of disease.Results: WES revealed that the patient did not have any mutations associated with XLH and instead was a compound heterozygote for 2 frameshift mutations in CYP27B1, leading to a revised diagnosis of 1α-hydroxylase deficiency. One of these two mutations in CYP27B1, an adenosine deletion in exon 7, has not previously been described.Conclusion: Clinical suspicion was aided by modern technology in correcting a decades-old mistaken diagnosis in this patient. This case highlights the potential of next-generation sequencing technology as an aide in establishing the correct diagnosis and management of complex diseases.Abbreviations: 1,25(OH)2D = 1,25-dihydroxyvitamin D3; FGF23 = fibroblast growth factor 23; PTH = parathyroid hormone; WES = whole exome sequencing; XLH = X-linked hypophosphatemia

Published

2016

3. Altered Expression of Several Molecular Mediators of Cerebrospinal Fluid Production inHypMice

Author

Jared Kaplan, Steven Tommasini, Gang-Qing Yao, Meiling Zhu, Sayoko Nishimura, Sevanne Ghazarian, Angeliki Louvi, and Karl Insogna

Subjects

Endocrinology, Diabetes and Metabolism

Abstract

ContextX-linked hypophosphatemia (XLH) is a genetic disease, causing life-long hypophosphatemia due to overproduction of fibroblast growth factor 23 (FGF23). XLH is associated with Chiari malformations, cranial synostosis, and syringomyelia. FGF23 signals through FGFR1c and requires a coreceptor, α-Klotho, which is expressed in the renal distal convoluted tubules and the choroid plexus (ChP). In the ChP, α-Klotho participates in regulating cerebrospinal fluid (CSF) production by shuttling the sodium/potassium adenosine triphosphatase (Na+/K+-ATPase) to the luminal membrane. The sodium/potassium/chloride cotransporter 1 (NKCC1) also makes a substantial contribution to CSF production.ObjectiveSince CSF production has not been studied in XLH, we sought to determine if there are changes in the expression of these molecules in the ChP of Hyp mice, the murine model of XLH, as a first step toward testing the hypothesis that altered CSF production contributes to the cranial and spinal malformations seen this disease.MethodsSemi-quantitative real-time PCR was used to analyze the level of expression of transcripts for Fgfr1c, and thee key regulators of CSF production, Klotho, Atp1a1 and Slc12a2. In situ hybridization was used to provide anatomical localization for the encoded proteins.ResultsReal-time polymerase chain reaction (RT-PCR) demonstrated significant upregulation of Klotho transcripts in the fourth ventricle of Hyp mice compared to controls. Transcript levels for Fgfr1c were unchanged in Hyp mice. Atp1a1 transcripts encoding the alpha-1 subunit of Na+/K+-ATPase were significantly downregulated in the third and lateral ventricles (LV). Expression levels of the Slc12a2 transcript (which encodes NKCC1) were unchanged in Hyp mice compared to controls. In situ hybridization (ISH) confirmed the presence of all 4 transcripts in the LV ChP both of WT and Hyp mice.ConclusionThis is the first study to document a significant change in the level of expression of the molecular machinery required for CSF production in Hyp mice. Whether similar changes occur in patients with XLH, potentially contributing to the cranial and spinal cord abnormalities frequently seen in XLH, remains to be determined.

Published

2023

4. Identification of a 22 bp DNA cis Element that Plays a Critical Role in Colony Stimulating Factor 1-Dependent Transcriptional Activation of the SPHK1 Gene

Author

Gang Qing Yao, Meiling Zhu, Joanne M. Walker, and Karl L. Insogna

Subjects

Transcriptional Activation, 0301 basic medicine, Macrophage colony-stimulating factor, Transcription, Genetic, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Plasma protein binding, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Endocrinology, Animals, Orthopedics and Sports Medicine, Nuclear protein, Transcription factor, Cells, Cultured, Reporter gene, Binding Sites, Chemistry, Macrophage Colony-Stimulating Factor, DNA, Transfection, Fibroblasts, Molecular biology, DNA binding site, Phosphotransferases (Alcohol Group Acceptor), 030101 anatomy & morphology, Transcription Factors

Abstract

Sphingosine-1-phosphate (S1P) is an anabolic clastokine. Colony Stimulating Factor 1 (CSF1) induces expression of the rate limiting enzyme required for S1P synthesis, sphingosine kinase 1 (SPHK1) in bone in vivo, and in osteoclasts in vitro. To study the mechanism of CSF1-induced SPHK1 gene expression, a 2608 bp fragment of the murine SPHK1 gene (− 2497 to + 111 bp relative to the transcription start site) was cloned and transfected into pZen cells (murine fibroblasts engineered to express c-fms). SPHK1 promoter activity was assessed using a dual-luciferase reporter assay system. By analyzing a series of 5′-deletions, a CSF1-responsive region was identified in the region − 1250 to − 1016 bp. To define putative DNA binding site(s) in this fragment, two biotin-labeled fragments that completely overlapped this region were generated, one 163 bp in length (− 1301 to − 1139) and one 169 bp in length (− 1157 to − 989). EMSAs revealed the 163 bp fragment as the target for protein binding. Using EMSAs, the nuclear protein binding region was further narrowed to an 85 bp fragment, (− 1223 to − 1139). Using a series of unlabeled DNA sequences as “cold competitors” in EMSAs, a 22 bp sequence is identified as the smallest fragment that could successfully compete away protein binding. The same 22 bp sequence also competed DNA binding in EMSAs using nuclear protein isolated from primary murine osteoclasts. A full-length wild-type SPHK1 promoter and an SPHK1 promoter in which the ATGGGGG motif was mutated were subsequently expressed in pZen cells. Mutating this ATGGGGG motif nearly completely abrogated the ability of CSF1 to activate the promoter. Although two transcription factors, KLF6 and Sp1 have been reported to bind to this sequence, supershift EMSAs failed to detect either among the proteins bound to the 85 bp DNA fragment.

Published

2020

5. An Unanticipated Role for Sphingosine Kinase-2 in Bone and in the Anabolic Effect of Parathyroid Hormone

Author

Edwin Siu, Ben-hua Sun, Meiling Zhu, Christine A. Simpson, Gang-Qing Yao, Joanne M. Walker, and Karl L. Insogna

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Anabolism, Sphingosine kinase, Parathyroid hormone, Osteoclasts, 030209 endocrinology & metabolism, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Endocrinology, Anabolic Agents, Bone Density, Internal medicine, medicine, Animals, Sphingosine-1-phosphate, Femur, Research Articles, Bone mineral, Mice, Knockout, business.industry, Sphingosine Kinase 2, Spine, SPHK2, Phosphotransferases (Alcohol Group Acceptor), 030104 developmental biology, chemistry, Parathyroid Hormone, Sclerostin, Female, business

Abstract

Sphingosine-1-phosphate (S1P) is an anabolic clastokine. Sphingosine kinase (SPHK) is the rate-limiting enzyme in S1P production and has 2 isoforms. To evaluate the roles of SPHK1 and SPHK2 in bone, we examined the skeletal phenotype of mice with selective deletion of SPHK1 in osteoclasts (SPHK1-Oc−/−) and mice in which the SPHK2 gene was deleted in all tissues (SPHK2−/−). SPHK1-Oc−/− had normal bone mass. By contrast, SPHK2−/− female mice had a 14% lower spinal bone mineral density (BMD; P

Published

2020

6. AgRP Neurons Regulate Bone Mass

Author

Sabrina Diano, Tamas L. Horvath, Marco Koch, Gang-Qing Yao, Ben-hua Sun, Jae Geun Kim, Karl L. Insogna, Marcelo O. Dietrich, Kim, Jae Geun, Sun, Ben-Hua, Dietrich, Marcelo O., Koch, Marco, Yao, Gang-Qing, Diano, Sabrina, Insogna, Karl, and Horvath, Tamas L.

Subjects

Leptin, Male, Ion Channels, Mice, Norepinephrine, 0302 clinical medicine, Sirtuin 1, Bone Density, Ion Channel, Hypothalamu, Homeostasis, Agouti-Related Protein, Uncoupling Protein 2, Femur, Receptor, lcsh:QH301-705.5, Neurons, Mice, Knockout, 0303 health sciences, digestive, oral, and skin physiology, Propranolol, Phenotype, Hypothalamus, Receptors, Leptin, Arcuate Nucleus of Hypothalamu, Signal transduction, hormones, hormone substitutes, and hormone antagonists, Signal Transduction, medicine.medical_specialty, Transgene, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Mitochondrial Proteins, 03 medical and health sciences, Arcuate nucleus, Internal medicine, Homeostasi, Receptors, Adrenergic, beta, medicine, Animals, Mitochondrial Protein, ddc:610, 030304 developmental biology, Leptin receptor, Biochemistry, Genetics and Molecular Biology (all), Tibia, Animal, Arcuate Nucleus of Hypothalamus, Neuron, Bone Diseases, Metabolic, Endocrinology, Gene Expression Regulation, nervous system, lcsh:Biology (General), 030217 neurology & neurosurgery

Abstract

The hypothalamus has been implicated in skeletal metabolism (Ducy et al., 2000; Sato et al., 2007; Yadav et al., 2009). Whether hunger-promoting neurons of the arcuate nucleus impact the bone is not known. We generated multiple lines of mice to affect AgRP neuronal circuit integrity. We found that mice with Ucp2 gene deletion, in which AgRP neuronal function was impaired, were osteopenic. This phenotype was rescued by cell-selective reactivation of Ucp2 in AgRP neurons. When the AgRP circuitry was impaired by early postnatal deletion of AgRP neurons or by cell autonomous deletion of Sirt1 (AgRP-Sirt1−/−), mice also developed reduced bone mass. No impact of leptin receptor deletion in AgRP neurons was found on bone homeostasis. Suppression of sympathetic tone in AgRP-Sirt1−/− mice reversed osteopenia in transgenic animals. Taken together, these observations establish a significant regulatory role for AgRP neurons in skeletal bone metabolism independent of leptin action.

Published

2015

7. The Transcription Factor T-box 3 Regulates Colony-stimulating Factor 1-dependent Jun Dimerization Protein 2 Expression and Plays an Important Role in Osteoclastogenesis

Author

Steven M. Tommasini, Gang-Qing Yao, Karl L. Insogna, Chen Yao, Ben-hua Sun, and Changqing Zhang

Subjects

Transcriptional Activation, Gene isoform, Molecular Sequence Data, Osteoclasts, Repressor, Electrophoretic Mobility Shift Assay, Biochemistry, Bone and Bones, Mice, Bone Density, Osteoclast, Transcriptional regulation, medicine, Animals, Promoter Regions, Genetic, Molecular Biology, Transcription factor, Mice, Knockout, Base Sequence, biology, Macrophage Colony-Stimulating Factor, Promoter, Cell Biology, Molecular biology, Radiography, Repressor Proteins, medicine.anatomical_structure, RANKL, Jun dimerization protein, biology.protein, T-Box Domain Proteins

Abstract

Colony-stimulating factor 1 (CSF1) is known to promote osteoclast progenitor survival, but its roles in osteoclast differentiation and mature osteoclast function are less well understood. In a microarray screen, Jun dimerization protein 2 (JDP2) was identified as significantly induced by CSF1. Recent reports indicate that JDP2 is required for normal osteoclastogenesis and skeletal metabolism. Because there are no reports on the transcriptional regulation of this gene, the DNA sequence from -2612 to +682 bp (relative to the transcription start site) of the JDP2 gene was cloned, and promoter activity was analyzed. The T box-binding element (TBE) between -191 and -141 bp was identified as the cis-element responsible for CSF1-dependent JDP2 expression. Using degenerate PCR, Tbx3 was identified as the major isoform binding the TBE. Overexpression of Tbx3 induced JDP2 promoter activity, whereas suppressing Tbx3 expression substantially attenuated CSF1-induced transcription. Suppressing Tbx3 in osteoclast precursors reduced JDP2 expression and significantly impaired RANKL/CSF1-induced osteoclastogenesis. A MEK1/2-specific inhibitor was found to block CSF1-induced JDP2 expression. Consistent with these data, JDP2(-/-) mice were found to have increased bone mass. In summary, CSF1 up-regulates JDP2 expression by inducing Tbx3 binding to the JDP2 promoter. The downstream signaling cascade from activated c-Fms involves the MEK1/2-ERK1/2 pathway. Tbx3 plays an important role in osteoclastogenesis at least in part by regulating CSF1-dependent expression of JDP2.

Published

2014

8. An Unusual Case of Rickets and How Whole Exome Sequencing Helped to Correct a Diagnosis

Author

Christine A. Simpson, Karl L. Insogna, Thomas O. Carpenter, Elizabeth Olear, Pankaj B. Agrawal, Catherine A. Brownstein, Patricia R Peter, and Gang-Qing Yao

Subjects

Pediatrics, medicine.medical_specialty, Unusual case, business.industry, 030209 endocrinology & metabolism, Rickets, General Medicine, Disease, Compound heterozygosity, medicine.disease, RC648-665, Diseases of the endocrine glands. Clinical endocrinology, Frameshift mutation, Revised diagnosis, 03 medical and health sciences, 0302 clinical medicine, medicine, 030212 general & internal medicine, business, Hypophosphatemia, Exome sequencing

Abstract

Objective: Rickets can be caused by a wide variety of underlying nutritional deficiencies or genetic defects. There is significant overlap in the clinical presentations of the various forms of rickets and the risk for misdiagnosis is great. This report describes a diagnostically challenging case of rickets that highlights important differences between two forms of rickets and demonstrates how gene sequencing technology can be instrumental in the identification and further characterization of these diseases.Methods: A patient diagnosed with X-linked hypophosphatemia (XLH) as a toddler did not develop many of the classic clinical features of this disease over time, calling the diagnosis into question. Whole exome sequencing (WES) was performed in this setting to determine the genetic basis of disease.Results: WES revealed that the patient did not have any mutations associated with XLH and instead was a compound heterozygote for 2 frameshift mutations in CYP27B1, leading to a revised diagnosis of 1α-hydroxylase deficiency. One of these two mutations in CYP27B1, an adenosine deletion in exon 7, has not previously been described.Conclusion: Clinical suspicion was aided by modern technology in correcting a decades-old mistaken diagnosis in this patient. This case highlights the potential of next-generation sequencing technology as an aide in establishing the correct diagnosis and management of complex diseases.Abbreviations: 1,25(OH)2D = 1,25-dihydroxyvitamin D3; FGF23 = fibroblast growth factor 23; PTH = parathyroid hormone; WES = whole exome sequencing; XLH = X-linked hypophosphatemia

Published

2016

9. Selective deletion of the membrane-bound colony stimulating factor 1 isoform leads to high bone mass but does not protect against estrogen-deficiency bone loss

Author

Karl L. Insogna, Jian-Jun Wu, Gang-Qing Yao, Xiao-Yan Xiao, Meiling Zhu, and Nancy Troiano

Subjects

Male, Macrophage colony-stimulating factor, medicine.medical_specialty, Bone density, Endocrinology, Diabetes and Metabolism, Osteoporosis, Osteoclasts, Article, Bone and Bones, Mice, chemistry.chemical_compound, Endocrinology, Colony-Stimulating Factors, Bone Density, Internal medicine, medicine, Animals, Humans, Protein Isoforms, Orthopedics and Sports Medicine, RNA, Messenger, Cells, Cultured, Osteoporosis, Postmenopausal, Hypertriglyceridemia, Mice, Knockout, Sex Characteristics, Osteoblasts, Triglyceride, Chemistry, Cell Differentiation, Osteoblast, General Medicine, medicine.disease, Coculture Techniques, Up-Regulation, Resorption, medicine.anatomical_structure, Solubility, Female, Bone marrow

Abstract

To better define the biologic function of membrane-bound CSF1 (mCSF1) in vivo, we have generated mCSF1 knockout (k/o) mice. Spinal bone density (BMD) was 15.9% higher in k/o mice compared to wild-type (wt) controls (P < 0.01) and total BMD was increased by 6.8% (P < 0.05). A higher mean femur BMD was also observed but did not reach statistical significance (6.9% P = NS). The osteoclastogenic potential of bone marrow isolated from mCSF1 k/o mice was reduced compared to wt marrow. There were no defects in osteoblast number or function suggesting that the basis for the high bone mass phenotype was reduced resorption. In addition to a skeletal phenotype, k/o mice had significantly elevated serum triglyceride levels (123 ± 7 vs. 88 ± 3.2 mg/dl; k/o vs. wt, P < 0.001), while serum cholesterol levels were similar (122 ± 6 vs. 116 ± 6 mg/dl; k/o vs. wt, P = NS). One month after surgery, 5-month-old k/o and wt female mice experienced the same degree of bone loss following ovariectomy (OVX). OVX induced a significant fourfold increase in the expression of the soluble CSF1 isoform (sCSF1) in the bones of wt mice while expression of mCSF1 was unchanged. These findings indicate that mCSF1 is essential for normal bone remodeling since, in its absence, BMD is increased. Membrane-bound CSF1 does not appear to be required for estrogen-deficiency bone loss while in contrast; our data suggest that sCSF1 could play a key role in this pathologic process. The reasons why mCSF1 k/o mice have hypertriglyceridemia are currently under study.

Published

2011

10. Targeted overexpression of Dkk1 in osteoblasts reduces bone mass but does not impair the anabolic response to intermittent PTH treatment in mice

Author

Karl L. Insogna, Gang-Qing Yao, Nancy Troiano, and Jian-Jun Wu

Subjects

musculoskeletal diseases, medicine.medical_specialty, Anabolism, Ratón, Endocrinology, Diabetes and Metabolism, Transgene, Osteoclasts, Parathyroid hormone, Mice, Transgenic, Article, Bone and Bones, Mice, Endocrinology, Osteoclast, In vivo, Internal medicine, medicine, Animals, Humans, Orthopedics and Sports Medicine, Osteoblasts, Reverse Transcriptase Polymerase Chain Reaction, Chemistry, Osteoblast, General Medicine, Rats, medicine.anatomical_structure, DKK1, Parathyroid Hormone, Intercellular Signaling Peptides and Proteins

Abstract

Parathyroid hormone (PTH) is a potent ana- bolic agent, but the cellular mechanisms by which it increases bone mass are not fully understood. Dickkopf 1 (Dkk1) is an endogenous inhibitor of Wnt signaling and suppresses bone formation in vivo. We sought to deter- mine if Dkk1 and anabolic PTH treatment interact in regulating bone mass. PTH treatment of primary murine osteoblasts for 24 h reduced Dkk1 expression by 90% as quantified by real-time PCR, whereas PTH treatment in vivo reduced Dkk1 expression by 30% when given as a single daily subcutaneous dose. To directly determine whether Dkk1 modulates the anabolic response of PTH in vivo, we engineered transgenic (TG) mice expressing murine Dkk1 under the control of the 2.3-kb rat collagen alpha-1 promoter. TG mice had significantly reduced bone mass, which was accompanied by reduced histo- morphometric parameters of bone formation (reduced OV/TV, ObS/OS, and NOb/TAR). Treatment of TG mice and wild-type (WT) littermates with 95 ng/g body weight of human (1-34) PTH daily for 34 days resulted in comparable increases in bone mass at all skeletal sites. Histomorphometric analyses indicated that PTH treat- ment increased the numbers of both osteoblasts and osteoclasts in WT mice but only increased the numbers of osteoblasts in TG mice. We conclude that overex- pression of Dkk1 does not attenuate the anabolic response to PTH in vivo.

Published

2010

11. CSF-1 Induces fos Gene Transcription and Activates the Transcription Factor Elk-1 in Mature Osteoclasts

Author

Indu Paliwal, Gang-Qing Yao, Takashi Itokawa, and Karl L. Insogna

Subjects

Transcriptional Activation, Genetically modified mouse, Transcription, Genetic, Endocrinology, Diabetes and Metabolism, Transgene, Osteoclasts, Mice, Transgenic, Biology, Mice, Endocrinology, Osteoclast, Transcription (biology), Proto-Oncogene Proteins, medicine, Animals, Orthopedics and Sports Medicine, RNA, Messenger, Nuclear protein, Gene, Transcription factor, Cells, Cultured, ets-Domain Protein Elk-1, Cell Nucleus, Macrophage Colony-Stimulating Factor, Genes, fos, Serum Response Element, Molecular biology, DNA-Binding Proteins, medicine.anatomical_structure, Animals, Newborn, Proto-Oncogene Proteins c-fos, Transcription Factors

Abstract

Mice with targeted deletion of the fos gene fail to develop mature osteoclasts, reflecting an absolute requirement for the c-Fos proto-oncogene in osteoclast precursors. C-Fos is also expressed in mature osteoclasts; however, the regulation of fos in these cells has not been studied. By using cultured murine osteoclast-like cells (OCLs) we found that treatment with colony-stimulation factor 1 (CSF-1) induced a 3.9-fold increase in c-Fos rnRNA at 30 minutes and a 2.6-fold increase at 60 minutes. With use of mature osteoclasts isolated from transgenic mice expressing the bacterial Lac-Z gene under the control of the murine fos promoter, we were able to directly demonstrate transcriptional activation of fos by CSF-1 in these cells. Transcriptional activation was 2.6-fold greater at 5 minutes and 2.8-fold greater at 15 minutes in CSF-1-treated cells than in vehicle-treated cells. CSF-1 induced nuclear protein binding to the fos serum response element that was significantly attenuated by antibodies to the transcription factor Elk-1 but not by Sap-1a. Treatment of mature osteoclasts with CSF-1 for 2 hours resulted in a significant increase in the levels of nuclear c-Fos protein. These data demonstrate that CSF-1 upregulates c-fos expression in mature osteoclasts at least in part via transcriptional activation of fos. CSF-1 induced binding of Elk-1 to the fos gene serum response element appears to be part of the molecular mechanism by which this occurs.

Published

2005

12. The Cell Surface Form of Colony-Stimulating Factor-1 Is Biologically Active in Bone in Vivo

Author

Karl L. Insogna, Jain-Jun Wu, Mary Ann Mitnick, Ben-hua Sun, Gang-Qing Yao, and Nancy Troiano

Subjects

Macrophage colony-stimulating factor, Genetically modified mouse, Gene isoform, medicine.medical_specialty, Bone density, Transgene, Cell, Gene Expression, Osteoclasts, Cell Count, Mice, Transgenic, Bone and Bones, Collagen Type I, Mice, Endocrinology, Bone Density, In vivo, Internal medicine, medicine, Animals, Humans, Femur, Promoter Regions, Genetic, Bone Development, Osteoblasts, Chemistry, Macrophage Colony-Stimulating Factor, Osteopetrosis, medicine.disease, Rats, Mice, Inbred C57BL, medicine.anatomical_structure, Tomography, X-Ray Computed

Abstract

The specific biological function of the cell surface or membrane-bound isoform of colony-stimulating factor-1 (mCSF-1) is not well understood. To help define the role of this isoform in bone, we developed a transgenic mouse in which targeted expression of human mCSF-1 in osteoblasts was achieved under the control of the 2.4-kb rat collagen type I α promoter. Bone density, determined by peripheral quantitative computed tomography, was reduced 7% in mCSF-1 transgenic compared with that in wild-type mice. Histomorphometric analyses indicated that the number of osteoclasts in bone (NOc/BPm, NOc/TAR, OcS/BS) was significantly increased in transgenic mice (1.7- to 1.8-fold; P < 0.05 to P < 0.01) compared with that in wild-type animals. Interestingly, the osteoblast-restricted isoform transgene corrected the osteopetrosis seen in CSF-1-deficient op/op mice. Skeletal growth and bone density in op/op mice expressing mCSF-1 in osteoblasts were similar to those in wild-type mice and were dramatically different from those in the unmanipulated op/op animals. The op/op mice expressing mCSF-1 in bone had normal incisor and molar tooth eruption, whereas the op/op mice evidenced the expected failure of tooth eruption. These findings directly support the conclusion that mCSF-1 is functionally active in bone in vivo and is probably an important local source of CSF-1.

Published

2003

13. Selective deletion of the soluble Colony-Stimulating Factor 1 isoform in vivo prevents estrogen-deficiency bone loss in mice

Author

Gang-Qing Yao, Nancy Troiano, Christine A. Simpson, and Karl L. Insogna

Subjects

0301 basic medicine, Bone mineral, Macrophage colony-stimulating factor, Gene isoform, medicine.medical_specialty, Histology, Physiology, medicine.drug_class, Chemistry, Endocrinology, Diabetes and Metabolism, Wild type, Bone tissue, Article, Reverse transcription polymerase chain reaction, 03 medical and health sciences, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Estrogen, In vivo, Internal medicine, medicine, Cancer research, hormones, hormone substitutes, and hormone antagonists

Abstract

Neutralizing CSF1 in vivo completely prevents ovariectomy (OVX)-induced bone loss in mice. There are two isoforms of CSF1, soluble (sCSF1), and membrane-bound (mCSF1), but their individual biological functions are unclear. It had been previously reported that mCSF1 knockout (K/O) and wild type (Wt) female mice experience the same degree of bone loss following OVX. In Wt mice the expression of sCSF1 was elevated fourfold in skeletal tissue following OVX while expression of mCSF1 was unchanged. To examine the role of sCSF1 in OVX-induced bone loss, mice were engineered in which sCSF1 was not expressed but expression of mCSF1 was unaffected (sCSF1 K/O). Isoform-specific reverse transcription PCR confirmed the absence of transcripts for sCSF1 in bone tissue isolated from these animals and no circulating CSF1 was detected by ELISA. Surprisingly, there were no significant differences in bone mineral density (BMD) between sCSF1 K/O mice and Wt controls as assessed by dual-energy X-ray absorptiometry and micro-CT. However, one month after OVX, femoral, spinal and total BMD had declined by 11.2%, 8.9%, and 8.7% respectively in OVX-Wt animals as compared to Sham-OVX. In contrast OVX sCSF1 K/O mice showed changes of +0.1%, −2.4%, and +2.3% at the same 3 sites compared to Sham-OVX sCSF1 K/O mice. These data indicate important non-redundant functions for the two isoforms of CSF1 and suggest that sCSF1, but not mCSF1, plays a key role in estrogen-deficiency bone loss.

Published

2017

14. Increasing dietary protein selectively upregulates the DMT1 isoform that contains an iron responsive element

Author

Carrie Thomas, Gang-Qing Yao, Jane E. Kerstetter, Kimberly O. O'Brien, and Karl L. Insogna

Subjects

Gene isoform, Dietary protein, biology, Chemistry, Genetics, biology.protein, DMT1, Molecular Biology, Biochemistry, Biotechnology, Cell biology

Published

2013

15. Inhibition of Epstein-Barr virus replication by a novel l-nucleoside, 2′-fluoro-5-methyl-β-l-arabinofuranosyluracil

Author

Shwu-Huey Liu, Yung-Chi Cheng, Gang-Qing Yao, Edgar Chou, Marina K. Kukhanova, and Chung K. Chu

Subjects

Herpesvirus 4, Human, Molecular Sequence Data, Virus Replication, medicine.disease_cause, Biochemistry, Virus, chemistry.chemical_compound, hemic and lymphatic diseases, medicine, Humans, Cells, Cultured, Polymerase, Pharmacology, Base Sequence, biology, Nucleoside analogue, Arabinofuranosyluracil, DNA, Epstein–Barr virus, In vitro, Mechanism of action, chemistry, biology.protein, Autoradiography, medicine.symptom, Thymidine, Nucleoside, medicine.drug

Abstract

A novel L-nucleoside analog, 2'-fluoro-5-methyl-beta-L-arabinofuranosyluracil (L-FMAU), was found to be a potent and selective inhibitor of Epstein-Barr virus (EBV) replication. The decrease in the amount of viral production was concentration dependent with a 90% inhibitory concentration of approximately 5 muM. Upon removal of the drug from treated cells, virus production resumed in 21 days. Metabolism studies indicated that L-FMAU could be converted to its mono-,di- and triphosphate metabolites in both EBV producing and non-producing cells than in EBV non-producing cells. The mechanism of selectivity of L-FMAU against EBV producing cells. However, the amount of L-FMAU nucleotides formed was three times larger in EBV producing cells than in EBV non-producing cells. The mechanism of selectivity of L-FMAU against EBV does not appear to be due solely to the preferential phosphorylation of L-FMAU in EBV producing cells. The triphosphate of L-FMAU could not be utilized as a substrate by EBV DNA polymerase or the human DNA polymerases alpha, beta, gamma, or delta. Therefore, the incorporation of L-FMAU residues into viral DNA may not be the mechanism of antiviral activity. This compound appears to have a mechanism of action different from that of any other antiherpes virus nucleoside analogs. In addition, L-FMAU has very low cytotoxicity with 50% inhibition of cell growth occurring at a concentration of 1mM. Given the potent inhibitory activity of this compound against EBV and its inability to be incorporated into cellular DNA, L-FMAU analogs should be explored as a new class of anti-EBV agents.

Published

1996

16. Targeted overexpression of the two colony-stimulating factor-1 isoforms in osteoblasts differentially affects bone loss in ovariectomized mice

Author

Jian-Jun Wu, Shira Ovadia, Gang-Qing Yao, Nancy Troiano, Karl L. Insogna, and Ben-hua Sun

Subjects

Macrophage colony-stimulating factor, Gene isoform, Male, medicine.medical_specialty, Physiology, medicine.drug_class, Ratón, Endocrinology, Diabetes and Metabolism, Ovariectomy, Mice, Transgenic, Biology, Transfection, Mice, Bone Density, Physiology (medical), Internal medicine, medicine, Animals, Protein Isoforms, Bone Resorption, Cells, Cultured, Osteoblasts, Estradiol, Macrophage Colony-Stimulating Factor, Osteoblast, Articles, Colony-stimulating factor, medicine.disease, Up-Regulation, Osteopenia, Mice, Inbred C57BL, Endocrinology, medicine.anatomical_structure, Animals, Newborn, Estrogen, Organ Specificity, Osteopetrosis, Gene Targeting, Ovariectomized rat, Female

Abstract

Colony-stimulating factor-1 (CSF1) is one of two cytokines required for normal osteoclastogenesis. There are two major isoforms of CSF1, the cell-surface or membrane-bound isoform (mCSF1) and soluble CSF1 (sCSF1). Whether these isoforms serve nonredundant functions in bone is unclear. To explore this question, we generated transgenic mice expressing human sCSF1, human mCSF1, or both (s/mCSF1) in osteoblasts using the 2.3-kb rat αI-collagen promoter. Bone density determined by peripheral quantitative computed tomography was significantly reduced in mCSF1, sCSF1, and s/mCSF1 transgenic mice compared with wild-type animals. When analyzed by sex, sCSF1, and s/mCSF1, female animals but not mCSF1 female mice were found to have greater bone loss than their male littermates (−20 vs. −9.2%; P < 0.05 for sCSF1 and −21.6 vs. −11.2% for s/mCSF1; P < 0.01). By breeding CSF1 isoform-selective transgenic mice to an op/op background, mice were generated in which a single CSF1 isoform was the only source of the cytokine (sCSF1op/opand mCSF1op/op). Unlike osteoblast-targeted overexpression of mCSF1, selective transgenic expression of sCSF1 did not completely correct the op/op phenotype in 5-mo-old animals. Interestingly, compared with sham-ovariectomized mice of the same genotype, ovariectomy in sCSF1op/opmice led to a greater loss of spinal bone mineral density (22.1%) than was seen in either mCSF1op/opmice (12.9%) or in wild-type animals (10.9%). Our findings support the conclusion that sCSF1 and mCSF1 serve nonredundant functions in bone and that sCSF1 may play a role in mediating estrogen-deficiency bone loss.

Published

2009

17. The cell-surface isoform of colony stimulating factor 1 (CSF1) restores but does not completely normalize fecundity in CSF1-deficient mice

Author

Shira, Ovadia, Karl, Insogna, and Gang-Qing, Yao

Subjects

Male, Macrophage Colony-Stimulating Factor, Cell Membrane, Uterus, Mice, Transgenic, Spermatozoa, Mice, Fertility, Pregnancy, Animals, Osteoporosis, Protein Isoforms, Female, Lung

Abstract

The complete genetic absence of colony stimulating factor 1 (CSF1) in CSF1-deficient Csf1(op)/Csf1(op) mice leads to reproductive defects in males and females. Although the cell-surface or membrane-bound isoform of CSF1 (mCSF1) is biologically active in bone, little is known about its role in reproduction. Transgenic mice expressing mCSF1 under the control of the 2.4-kb rat collagen type I alpha promoter were developed [Tg(Col1a1-mCSF1)1Gqy] and bred onto a Csf1(op)/Csf1(op) background [Csf1(op)/Csf1(op); Tg(Col1a1-mCSF1)1Gqy] to examine the effects of the mCSF1 isoform in bone in vivo. Surprisingly, when interbred, these mice were fertile. The Csf1(op)/Csf1(op); Tg(Col1a1-mCSF1)1Gqy transgenic male mice have normal libido, sperm number and percent of motile sperm. In Csf1(op)/Csf1(op); Tg(Col1a1-mCSF1)1Gqy females, puberty and estrus cycles are at expected age and duration. Further, females are able to carry pregnancies to term and nurse their offspring. Crosses of Csf1(op)/Csf1(op); Tg(Col1a1-mCSF1)1Gqy males or females with their control littermates showed no significant differences in either number or viability of offspring. However, crossing Csf1(op)/Csf1(op); Tg(Col1a1-mCSF1)1Gqy males with Csf1(op); Tg(Col1a1-mCSF1)1Gqy females resulted in a decline in both the number and viability of offspring, suggesting that a subtle reproductive defect might persist in the transgenic animals that was only manifest when the animals were interbred. Although the gravid murine uterus expresses extremely high levels of CSF1 that are thought to be important for reproduction, uterine tissue levels of CSF1 remained low and unchanged during pregnancy in Csf1(op)/Csf1(op); Tg(Col1a1-mCSF1)1Gqy mice. Low levels of CSF1 protein were detected in serum and in lung and uterine tissue in Csf1(op)/Csf1(op); Tg(Col1a1-mCSF1)1Gqy mouse, which likely result from the known proteolytic shedding of mCSF1 from the cell surface. These data are consistent with the conclusion that mCSF1, when shed from the cell surface, can support reproduction and that high uterine tissue levels of CSF1 may not be required for mouse reproduction.

Published

2005

18. Nuclear factor-kappaB p50 is required for tumor necrosis factor-alpha-induced colony-stimulating factor-1 gene expression in osteoblasts

Author

Ben-hua Sun, Gang-Qing Yao, Karl L. Insogna, and Eleanor C. Weir

Subjects

Macrophage colony-stimulating factor, Mice, Knockout, Messenger RNA, P50, Binding Sites, Osteoblasts, Tumor Necrosis Factor-alpha, Hematopoietic growth factor, Immune Sera, Macrophage Colony-Stimulating Factor, NF-kappa B, RNA, Gene Expression, Biology, Molecular biology, Bone remodeling, Mice, Endocrinology, Gene expression, Animals, Humans, Tumor necrosis factor alpha, RNA, Messenger, Promoter Regions, Genetic

Abstract

Colony-stimulating factor (CSF)-1 is a hematopoietic growth factor that is released by osteoblasts and is recognized to play a critical role in bone remodeling in vivo and in vitro. We have reported that osteoblasts express CSF-1 constitutively and that tumor necrosis factor (TNF)-alpha, a potent bone-resorbing agent, increases CSF-1 gene expression by a transcriptional mechanism. In the present study, we report that an NF-kappaB site in the CSF-1 promoter is required for TNF-alpha-induced CSF-1 expression in osteoblasts. As determined by electrophoretic mobility shift assays, antiserum against the NF-kappaB-binding protein, p50, retarded the mobility of the inducible complex, whereas antisera against p52, p65, c-Rel, Rel B, IkappaB alpha, IkappaB gamma, and Bcl-3 had no effect. To further confirm that p50 is necessary for TNF-alpha-induced CSF-1 expression in osteoblasts, CSF-1 messenger RNA expression from untreated and TNF-alpha-treated osteoblasts, prepared from wild-type and p50 knock-out mice, was examined by Northern analysis. CSF-1 messenger RNA was increased by TNF treatment in wild-type mice but not in NF-kappaB p50 knock-out mice. Our findings support the conclusion that the NF-kappaB subunit p50 is critical for TNF-induced CSF-1 expression in osteoblasts.

Published

2000

19. The cell-surface form of colony-stimulating factor-1 is regulated by osteotropic agents and supports formation of multinucleated osteoclast-like cells

Author

Eleanor C. Weir, Elizabeth Spencer, Ben-hua Sun, Mark C. Horowitz, Karl L. Insogna, Gang-Qing Yao, and Elizabeth E. Hammond

Subjects

Macrophage colony-stimulating factor, medicine.medical_specialty, Hematopoietic growth factor, Cell, Parathyroid hormone, Osteoclasts, Biology, Transfection, Biochemistry, Bone remodeling, Flow cytometry, Mice, Osteoclast, Internal medicine, medicine, Animals, Humans, RNA, Messenger, Molecular Biology, Osteoblasts, medicine.diagnostic_test, Histocytochemistry, Tumor Necrosis Factor-alpha, Macrophage Colony-Stimulating Factor, Gene Expression Regulation, Developmental, Membrane Proteins, Cell Differentiation, Cell Biology, 3T3 Cells, Flow Cytometry, Cell biology, medicine.anatomical_structure, Endocrinology, Parathyroid Hormone, Tumor necrosis factor alpha

Abstract

Colony-stimulating factor-1 (CSF-1) is a hematopoietic growth factor that is released by osteoblasts and is recognized to play a critical role in bone remodeling in vivo and in vitro. CSF-1 is synthesized as a soluble or cell-surface protein. It is unclear, however, whether human osteoblasts express both molecular forms of CSF-1, and whether these isoforms can independently mediate osteoclastogenesis. In the present study, using a combination of quantitative reverse transcriptase polymerase chain reaction, flow cytometry, and Western immunoblot analysis, we have demonstrated that human osteoblast-like cells as well as primary human osteoblasts express the cell-surface form of CSF-1 both constitutively and in response to parathyroid hormone and tumor necrosis factor. Furthermore, using an in vitro co-culture system, we have shown that cell-surface CSF-1 alone is sufficient to support osteoclast formation. These findings may be especially significant in view of evidence that direct cell-to-cell contact is critical for osteoclast formation, and suggest that differential regulation of expression of the CSF-1 isoforms may influence osteoclast function modulated by osteotropic hormones.

Published

1998

20. Identification of two oligodeoxyribonucleotide binding proteins on plasma membranes of human cell lines

Author

Yung-Chi Cheng, Gang-Qing Yao, and Simona Corrias

Subjects

Carcinoma, Hepatocellular, Lymphoma, B-Cell, Molecular Sequence Data, HL-60 Cells, Biochemistry, DNA-binding protein, KB Cells, Cell Line, Substrate Specificity, chemistry.chemical_compound, Humans, Magnesium, Binding site, Pharmacology, Serine protease, biology, Base Sequence, Binding protein, Cell Membrane, Liver Neoplasms, Serine Endopeptidases, Sodium, Biological Transport, Thionucleotides, Molecular Weight, Kinetics, Membrane, Membrane protein, chemistry, Oligodeoxyribonucleotides, Phosphodiester bond, biology.protein, Calcium, Electrophoresis, Polyacrylamide Gel, Carrier Proteins, DNA

Abstract

Two oligodeoxyribonucleotide (oligodN) binding proteins of approximately 100–110 kDa were identified in the plasma membranes of human HL-60, HepG2, H1, and KB cells by a photolabeling technique. Solubilization of cellular membranes with a nonionic detergent did not interfere with the binding of these two proteins to oligodNs, and both proteins were susceptible to serine protease action. The binding affinities of these two proteins to oligodNs were found to be similar; Scatchard plot analysis revealed the K d for phosphodiester (PO) 21-mer oligodeoxycytidine to be 60 nM and binding sites numbered approximately 1.2 × 10 6 /cell for HepG2 cells. Both phosphorothioate (PS) and PO oligodNs could bind to these two proteins with the binding affinity for PS oligodNs being much stronger than that for PO oligodNs. The binding to oligodNs was affected by the ionic strength of the reaction. Dextran sulfate, tRNA, and double-stranded DNA inhibited the binding of oligodNs, whereas ATP, ADP, AMP, and TTP had no effect. Given their high affinity for oligodNs, these membrane proteins may play an important role in the action of oligodNs.

Published

1996

21. Characterization of sublines of Epstein-Barr virus producing HR-1 cells and its implication in virus propagation in culture

Author

Ching-Hwa Tsai, Yung-Chi Cheng, and Gang-Qing Yao

Subjects

clone (Java method), DNA Replication, Gene Expression Regulation, Viral, Herpesvirus 4, Human, Virus Cultivation, Biology, medicine.disease_cause, Virus Replication, Virus, Cell Line, chemistry.chemical_compound, Viral Proteins, hemic and lymphatic diseases, Virology, Virus latency, Genetics, medicine, Tumor Cells, Cultured, Humans, Molecular Biology, DNA replication, General Medicine, medicine.disease, Epstein–Barr virus, Molecular biology, Burkitt Lymphoma, Virus Latency, DNA-Binding Proteins, Restriction enzyme, Butyrates, chemistry, Cell culture, DNA, Viral, Trans-Activators, Butyric Acid, Tetradecanoylphorbol Acetate, DNA

Abstract

To understand the mechanism regulating the EBV replication cycle, several sublines were obtained from HR-1 cells by the limiting dilution method. Based on their biochemical and molecular characteristics, these sublines can be categorized into two classes: the high EBV-DNA containing (H) subline and low EBV-DNA containing (L) subline. The amount of EBV proteins, such as EBV polymerases, EBV DNase, EAD, ZEBRA, MA, and VCA, was much higher in H sublines than in L sublines. Only 20% of cells in the H subline express those proteins. In addition to regular EBV DNA restriction enzyme fragments, additional DNA restriction enzyme fragments, as detected by different EBV DNA fragment probes, were found to be present in H sublines but not in L sublines. No BamH1 W-Z DNA fragment rearrangement, which was the primary reason for ZEBRA expression in a high EBV-DNA containing subline, Clone 5, was found in H sublines. When L sublines were treated with 12-0-tetradecanoylphorbol-13-acetate and sodium butyrate, EBV-specific proteins, including ZEBRA protein, could be induced in cells, but no virus could be detected in the medium. Thus, the lack of EBV production by L sublines is more than the simple lack of expression of ZEBRA protein. L sublines are susceptible to EBV infection and are capable of producing EBV after infection. The importance of the presence of L cells in the H subline for the propagation of EBV in culture is suggested.

Published

1995

22. Potent inhibition of Epstein-Barr virus by phosphorothioate oligodeoxynucleotides without sequence specification

Author

Susan P. Grill, W. Egan, Yung-Chi Cheng, and Gang-Qing Yao

Subjects

Herpesvirus 4, Human, Time Factors, DNA polymerase, Molecular Sequence Data, Acyclovir, Microbial Sensitivity Tests, medicine.disease_cause, Antiviral Agents, Virus, Herpesviridae, Organophosphorus Compounds, hemic and lymphatic diseases, medicine, Pharmacology (medical), Ganciclovir, Polymerase, Pharmacology, biology, Base Sequence, Cell growth, Oligonucleotides, Antisense, Epstein–Barr virus, Virology, Infectious Diseases, Mechanism of action, Oligodeoxyribonucleotides, Cell culture, DNA, Viral, biology.protein, medicine.symptom, Foscarnet, Research Article

Abstract

We found that 28-mer phosphorothioate oligodeoxynucleotides (S-oligos) with and without sequence specificity complementary to Epstein-Barr virus (EBV) genes are potent inhibitors of EBV replication in cell culture. The decrease in the amount of EBV DNA, the activity of intracellular viral DNA polymerase, and virus production were dose dependent, with a 90% inhibitory dose of approximately 0.5 microM. No inhibition of cell growth was observed with the S-oligos at concentrations up to 20 microM. The mechanism of action appears to be the inhibition of EBV DNA synthesis. The reversibility of anti-EBV action is dependent on the dose and duration of drug exposure. S-oligos should be considered a new class of anti-EBV agents.

Published

1993

23. The Transcription Factor T-box 3 Regulates Colony-stimulating Factor 1-dependent Jun Dimerization Protein 2 Expression and Plays an Important Role in Osteoclastogenesis.

Author

Chen Yao, Gang-Qing Yao, Ben-hua Sun, Changqing Zhang, Tommasini, Steven M., and Insogna, Karl

Subjects

*COLONY-stimulating factors (Physiology), *OSTEOCLASTS, *CELL differentiation, *NUCLEOTIDE sequence, *GENETIC transcription

Abstract

Colony-stimulating factor 1 (CSF1) is known to promote osteoclast progenitor survival, but its roles in osteoclast differentiation and mature osteoclast function are less well understood. In a microarray screen, Jun dimerization protein 2 (JDP2) was identified as significantly induced by CSF1. Recent reports indicate that JDP2 is required for normal osteoclastogenesis and skeletal metabolism. Because there are no reports on the tran-scriptional regulation of this gene, the DNA sequence from -- 2612 to +682 bp (relative to the transcription start site) of the JDP2 gene was cloned, and promoter activity was analyzed. The T box-binding element (TBE) between --191 and --141 bp was identified as the cis-element responsible for CSF1-dependent JDP2 expression. Using degenerate PCR, Tbx3 was identified as the major isoform binding the TBE. Overexpression of Tbx3 induced JDP2 promoter activity, whereas suppressing Tbx3 expression substantially attenuated CSF1-induced transcription. Suppressing Tbx3 in osteoclast precursors reduced JDP2 expression and significantly impaired RANKL/CSF1-induced osteoclastogenesis. A MEK1/2-specific inhibitor was found to block CSF1-induced JDP2 expression. Consistent with these data, JDP2-/- mice were found to have increased bone mass. In summary, CSF1 up-regulates JDP2 expression by inducing Tbx3 binding to the JDP2 promoter. The downstream signaling cascade from activated c-Fms involves the MEK1/2-ERK1/2 pathway. Tbx3 plays an important role in osteoclastogenesis at least in part by regulating CSF1-dependent expression of JDP2. [ABSTRACT FROM AUTHOR]

Published

2014

24. Targeted overexpression of Dkk1 in osteoblasts reduces bone mass but does not impair the anabolic response to intermittent PTH treatment in mice.

Author

Gang-Qing Yao, Jian-Jun Wu, Troiano, Nancy, Insogna, Karl, Yao, Gang-Qing, and Wu, Jian-Jun

Subjects

*GENE expression, *PARATHYROID hormone, *CALCIUM regulating hormones, *OSTEOCLASTS, *BONE cells, *BONE metabolism, *OSTEOBLAST metabolism, *ANIMALS, *BONES, *GROWTH factors, *MACROPHAGES, *MICE, *POLYMERASE chain reaction, *RATS, *REVERSE transcriptase polymerase chain reaction, *OSTEOBLASTS

Abstract

Parathyroid hormone (PTH) is a potent anabolic agent, but the cellular mechanisms by which it increases bone mass are not fully understood. Dickkopf 1 (Dkk1) is an endogenous inhibitor of Wnt signaling and suppresses bone formation in vivo. We sought to determine if Dkk1 and anabolic PTH treatment interact in regulating bone mass. PTH treatment of primary murine osteoblasts for 24 h reduced Dkk1 expression by 90% as quantified by real-time PCR, whereas PTH treatment in vivo reduced Dkk1 expression by 30% when given as a single daily subcutaneous dose. To directly determine whether Dkk1 modulates the anabolic response of PTH in vivo, we engineered transgenic (TG) mice expressing murine Dkk1 under the control of the 2.3-kb rat collagen alpha-1 promoter. TG mice had significantly reduced bone mass, which was accompanied by reduced histomorphometric parameters of bone formation (reduced OV/TV, ObS/OS, and NOb/TAR). Treatment of TG mice and wild-type (WT) littermates with 95 ng/g body weight of human (1-34) PTH daily for 34 days resulted in comparable increases in bone mass at all skeletal sites. Histomorphometric analyses indicated that PTH treatment increased the numbers of both osteoblasts and osteoclasts in WT mice but only increased the numbers of osteoblasts in TG mice. We conclude that overexpression of Dkk1 does not attenuate the anabolic response to PTH in vivo. [ABSTRACT FROM AUTHOR]

Published

2011

25. Targeted overexpression of the two colony-stimulating factor-1 isoforms in osteoblasts differentially affects bone loss in ovariectomized mice.

Author

Gang-Qing Yao, Jian-Jun Wu, Ovadia, Shfra, Troiano, Nancy, Ben Hua Sun, and Insogna, Karl

Subjects

*CYTOKINES, *CELLULAR immunity, *CELL membranes, *TRANSGENIC mice, *LABORATORY animals, *COLLAGEN, *EXTRACELLULAR matrix proteins, *TOMOGRAPHY

Abstract

Colony-stimulating factor-i (CSF1) is one of two cytokines required for normal osteoclastogenesis. There are two major isoforms of CSF1, the cell-surface or membrane-bound isoform (mCSF1) and soluble CSF1 (sCSF1). Whether these isoforms serve nonredundant functions in bone is unclear. To explore this question, we generated transgenic mice expressing human sCSF1, human mCSF1, or both (s/mCSF1) in osteoblasts using the 2.3-kb rat αl-collagen promoter. Bone density determined by peripheral quantitative computed tomography was significantly reduced in mCSF1, sCSF1, and sImCSF1 transgenic mice compared with wild-type animals. When analyzed by sex, sCSF1, and s/mCSF1, female animals but not mCSF1 female mice were found to have greater bone loss than their male littermates (-20 vs. -9.2%; P < 0.05 for sCSF1 and -21.6 vs. - 11.2% for s/mCSF1; P < 0.01). By breeding CSF1 isoform-selective transgenic mice to an op/op background, mice were generated in which a single CSF1 isoform was the only source of the cytokine (sCSF1op/opand mCSF1 op/op). Unlike osteoblast-targeted over-expression of mCSF1, selective transgenic expression of sCSF1 did not completely correct the op/op phenotype in 5-mo-old animals. Interestingly, compared with sham-ovariectomized mice of the same genotype, ovariectomy in sCSF1op/op mice led to a greater loss of spinal bone mineral density (22.1%) than was seen in either mCSF1op/op mice (12.9%) or in wild-type animals (10.9%). Our findings support the conclusion that sCSF1 and mCSF1 serve nonredundant functions in bone and that sCSF1 may play a role in mediating estrogen-deficiency bone loss. [ABSTRACT FROM AUTHOR]

Published

2009