Your search keyword '"Taniyama, Yoshiaki"' showing total 29 results

1. Inhibition of Lp(a)-induced functional impairment of endothelial cells and endothelial progenitor cells by hepatocyte growth factor

Author

Iwabayashi, Masaaki, Taniyama, Yoshiaki, Sanada, Fumihiro, Azuma, Junya, Iekushi, Kazuma, Okayama, Keita, Chatterjee, Amarnath, Rakugi, Hiromi, and Morishita, Ryuichi

Subjects

*HEPATOCYTE growth factor, *ENDOTHELIUM, *PROGENITOR cells, *LIPOPROTEIN A, *ARTERIAL diseases, *GENE therapy, *LABORATORY mice

Abstract

Abstract: Background: Lipoprotein (a) (Lp(a)) is one of the risk factors for peripheral artery disease (PAD). Our previous report demonstrated that hepatocyte growth factor (HGF) gene therapy attenuated the impairment of collateral formation in Lp(a) transgenic mice. Since risk factors for atherosclerosis accelerate endothelial senescence and impair angiogenesis, we examined the role of Lp(a) in dysfunction and senescence of endothelial progenitor cells (EPC) and endothelial cells. Methods: In vitro and in vivo incorporation assays were performed using ex-vivo expanded DiI-labeled human EPC. Senescence of cultured endothelial cells, production of oxidative stress and angiogenesis function were evaluated by SA-β-galactosidase staining, dihydroethidium (DHE) staining and Matrigel assay, respectively. Results: EPC transplantation significantly stimulated recovery of ischemic limb perfusion, while EPC pre-treated with Lp(a) did not increase ischemic limb perfusion. Impairment of angiogenesis by EPC with Lp(a) was associated with a significant decrease in CD31-positive capillaries and DiI-labeled EPC. Importantly, Lp(a) significantly accelerated the onset of senescence and production of reactive oxygen species (ROS) in human aortic endothelial cells, accompanied by a significant increase in the protein expression of p53 and p21. On the other hand, HGF significantly attenuated EPC dysfunction, senescence, ROS production, and p53 and p21 expression induced by Lp(a). Conclusion: Lp(a) might affect atherosclerosis via acceleration of senescence, ROS production, and functional impairment of the endothelial cell lineage. HGF might have inhibitory effects on these atherogenic actions of Lp(a). [Copyright &y& Elsevier]

Published

2012

2. Role of serotonin in angiogenesis: Induction of angiogenesis by sarpogrelate via endothelial 5-HT1B/Akt/eNOS pathway in diabetic mice

Author

Iwabayashi, Masaaki, Taniyama, Yoshiaki, Sanada, Fumihiro, Azuma, Junya, Iekushi, Kazuma, Kusunoki, Hiroshi, Chatterjee, Amarnath, Okayama, Keita, Rakugi, Hiromi, and Morishita, Ryuichi

Subjects

*ATHEROSCLEROSIS treatment, *SEROTONIN, *NEOVASCULARIZATION, *ENDOTHELIUM, *VASCULAR smooth muscle, *GENE expression, *LABORATORY mice

Abstract

Abstract: Serotonin (5-hydroxytryptamine, 5-HT) plays a crucial role in peripheral artery disease (PAD) and diabetes mellitus (DM). In these conditions, the balance between the 5-HT2A receptor in smooth muscle cells and the 5-HT1B receptor in endothelial cells (ECs) regulates vascular tonus. In the present study, we focused on the role of 5-HT in endothelial dysfunction using a selective 5-HT2A receptor blocker, sarpogrelate. In human EC, 5-HT markedly stimulated eNOS expression and the phosphorylation of eNOS, Akt and ERK1/2. In addition, a dose-dependent increase in tubule-formation on Matrigel was observed after 5-HT treatment. In contrast, high glucose significantly inhibited tubule formation and eNOS expression through inactivation of Akt, while 5-HT significantly attenuated these actions of high glucose (P <0.01). These results indicate that 5-HT stimulated angiogenesis through activation of Akt in ECs. However, in clinical situations, 5-HT seems to act as the “devil”. To examine the role of 5-HT in diabetic PAD, a hindlimb ischemia model was created in diabetic mice. The blood flow ratio of the ischemic to non-ischemic limb was significantly lower in DM mice than in normal mice, while sarpogrelate significantly attenuated the decrease in the blood flow ratio compared to control (P <0.01). Consistently, the decrease in eNOS expression and Akt activity in DM mice was significantly attenuated by sarpogrelate. Overall, the present study demonstrated that selective inhibition of 5-HT2A by sarpogrelate significantly restored ischemic limb blood perfusion in a severe diabetic mouse model through stimulation of the eNOS/Akt pathway via the endothelial 5-HT1B receptor. Enhancement of vasodilation and angiogenesis by sarpogrelate might provide a unique treatment for PAD and DM patients. [Copyright &y& Elsevier]

Published

2012

3. HIF-1α Signaling Upstream of NKX2.5 Is Required for Cardiac Development in Xenopus.

Author

Nagao, Kaori, Taniyama, Yoshiaki, Kietzmann, Thomas, Doi, Takefumi, Komuro, Issei, and Morishita, Ryuichi

Subjects

*GENE expression, *GENETIC regulation, *OXYGEN, *ISCHEMIA, *BLOOD circulation disorders

Abstract

HIF-la is originally identified as a transcription factor that activates gene expression in response to hypoxia. In metazoans, HIF-la functions as a master regulator of oxygen homeostasis and regulates adaptive responses to change in oxygen tension during embryogenesis, tissue ischemia, and tumorigenesis. Because H~tL1a~deficient mice exhibit a number of develop- mental defects, the precise role of HIF-la in early cardiac morphogenesis has been uncertain. Therefore, to clarify the role of HIF-la in heart development, we investigated the effect of knockdown of HIF-la in Xenopus embryos using antisense morpholino oligonucleotide microinjection techniques. Knock- down of HIF-la resulted in defects of cardiogenesis. Whole mount in situ hybridization for cardiac troponin I (cTnI) showed the two separated populations of cardiomyocytes, which is indicative of cardia bifida, in HIF-la-depleted embryos. Fur- thermore, the depletion of HIF-la led to the reduction in cTnI expression, suggesting the correlation between HIF-la and car- diac differentiation. We further examined the expression of several heart markers, nkx2.5, gata4, tbx5, bmp4, handi, and hand2 in HIF-la-depleted embryos. Among them, the expression of nkx2.5 was significantly reduced. Luciferase reporter assay using the Nkx2.5 promoter showed that knockdown of HIF-lix decreased its promoter activity. The cardiac abnormality in the HIF-la-depleted embryo was restored with co-injection of nkx2.5 mRNA. Collectively, these findings reveal that HIF-la- regulated nkx2.5 expression is required for heart development in Xenopus. [ABSTRACT FROM AUTHOR]

Published

2008

4. Constitutive over-expression of VEGF results in reduced expression of Hand-1 during cardiac development in Xenopus

Author

Nagao, Kaori, Taniyama, Yoshiaki, Koibuchi, Nobutaka, and Morishita, Ryuichi

Subjects

*VASCULAR endothelial growth factors, *GENE expression, *CELL morphology, *EMBRYOLOGY

Abstract

Abstract: During heart development, various signaling cascades are tightly regulated in a stage- and region-dependent manner. Vascular endothelial growth factor (VEGF) is one of the important molecules required for both vascular development and cardiac morphogenesis. VEGF receptors are present in the embryonic heart, so we focused on heart formation in VEGF-over-expressing Xenopus embryos. Over-expression of VEGF170 caused disorganized vessels, while the expression of an endothelial marker, Tie-2, was increased. The embryo’s heart was distinctly larger than that of control, and showed abnormal morphology. Histological analysis of these embryos showed failure of heart looping. In situ hybridization with Hand-1, which controls intrinsic morphogenetic pathways, revealed that the expression level of Hand-1 was decreased in the heart region. These results suggest that increased VEGF170 levels disturb Hand-1 expression in the region required for normal heart morphogenesis. VEGF expression level may be important in heart morphology during embryonic development. [Copyright &y& Elsevier]

Published

2007

5. The effect of VEGF on blood vessels and blood cells during Xenopus development

Author

Koibuchi, Nobutaka, Taniyama, Yoshiaki, Nagao, Kaori, Ogihara, Toshio, Kaneda, Yasufumi, and Morishita, Ryuichi

Subjects

*GROWTH factors, *EMBRYOLOGY, *BLOOD cells, *BLOOD-vessel physiology, *MEDICAL research

Abstract

Abstract: Vascular endothelial growth factor (VEGF) is known to play an essential role in vascular development. We have overexpressed VEGF122 or VEGF170, which are equivalent to mouse VEGF120 and VEGF164, in developing Xenopus embryos. Overexpression of VEGF170 but not VEGF122 demonstrated an absence of expression of hematopoietic markers α-globin and GATA-1 but only in the posterior portion of the blood island. Interestingly, strong signals of endothelial markers, msr, fli-1, and tie-2, were detectable in those regions, instead of hematopoietic markers. These results suggested both that injection of VEGF170 resulted in disturbance of vasculogenesis in the posterior portion of the blood island, with excessive production of endothelial cells at the expense of blood cells, and that the anterior and posterior portions of the VBI may have distinct characteristics. [Copyright &y& Elsevier]

Published

2006

6. Akt3 overexpression in the heart results in progression from adaptive to maladaptive hypertrophy

Author

Taniyama, Yoshiaki, Ito, Masahiro, Sato, Kaori, Kuester, Christoph, Veit, Kerstin, Tremp, Gunter, Liao, Ronglih, Colucci, Wilson S., Ivashchenko, Yuri, Walsh, Kenneth, and Shiojima, Ichiro

Subjects

*CARDIAC hypertrophy, *HEART diseases, *RODENTS, *MORTALITY

Abstract

Abstract: Akt is a serine/threonine kinase that mediates a variety of cellular responses to external stimuli. Among the three members of mammalian Akt (Akt1, Akt2 and Akt3), Akt3 is unique in that it has an alternatively spliced variant that lacks the carboxy-terminal regulatory phosphorylation site. However, little is known regarding in vivo functions of Akt3 and its spliced variant. In this study we investigated the potential functions of the Akt3 spliced variant by overexpressing its activated form in the heart. Cardiac-specific Akt3 transgenic (TG) mice exhibited marked cardiac hypertrophy. Contractile function of TG hearts was preserved at 4 and 12 weeks, but was impaired at 20 weeks of age. When treated with cardiotoxic drug doxorubicin (Dox), TG mice at 4 weeks of age exhibited improved survival and preserved contractile function. However, these cardioprotective effects were not evident when Dox was injected at 12 weeks of age, and TG mice exhibited even higher mortality rate than wild-type animals when Dox was injected at 20 weeks of age. Endogenous Akt1 and Akt2 protein and phosphorylation levels were downregulated in Akt3 TG hearts, suggesting the existence of negative feedback regulation of Akt signaling at the level of Akt protein amount. Taken together, the Akt3 spliced variant is functional in vivo, promotes cardiac growth and mediates cardioprotective effects. However, continuous overexpression of Akt3 results in contractile dysfunction and increased susceptibility to cardiac injury. Thus, sustained activation of Akt signaling results in progression from adaptive to maladaptive hypertrophy. [Copyright &y& Elsevier]

Published

2005

7. Modification of plasmid DNA-based gene transfer into central nerve system

Author

Taniyama, Yoshiaki, Shimamura, Munehisa, Sato, Naoyuki, Tomita, Naruya, Endho, Masayuki, Azuma, Junya, Iekushi, Kazuma, Kaneda, Yasufumi, Ogihara, Toshio, and Morishita, Ryuichi

Subjects

*NERVOUS system, *CELLS, *GENES, *GENE therapy

Abstract

Although viral vector systems are efficient to transfect foreign genes into a variety of tissues, safety issues remain in relation to human gene therapy. In this study, we examined the feasibility of a novel nonviral vector system by using high-frequency, low-intensity ultrasound irradiation for transfection into vascular cells, kidneys and the central nerve systems of fetal mice. As a result, expression of the reporter gene, Venus, was readily detected in the central nervous system. The transfected cells were mainly detected in meningeal cells with intracisternal injection. Overall, the present study demonstrated the feasibility of efficient plasmid DNA transfer into several organs, especially the central nervous system, providing a new option for treating various diseases. [Copyright &y& Elsevier]

Published

2004

8. Elevated Myocardial Akt Signaling Ameliorates Doxorubicin-induced Congestive Heart Failure and Promotes Heart Growth

Author

Taniyama, Yoshiaki and Walsh, Kenneth

Subjects

*DOXORUBICIN, *CONGESTIVE heart failure, *HEART development

Abstract

Y. T aniyama and K. W alsh. Elevated Myocardial Akt Signaling Ameliorates Doxorubicin-induced Congestive Heart Failure and Promotes Heart Growth. Journal of Molecular and Cellular Cardiology (2002) 34, 1241–1247. Doxorubicin is a chemotherapeutic agent that can induce cardiotoxicity and congestive heart failure (CHF). In this study we tested whether intracoronary Akt1 gene delivery could inhibit doxorubicin-induced CHF. Saline or a replication defective adenoviral vector expressing constitutively-active Akt1 (myrAkt) or β-galactosidase (βgal) was delivered to the myocardium of 8 week old rats one day prior to initiating doxorubicin administration. In animals receiving saline or βgal, doxorubicin resulted in significant decreases in cardiac function and retarded post-natal heart growth at the 5 weeks time point. In contrast, transduction of myrAkt protected hearts against doxorubicin-induced decreases in fractional shortening and cardiac index, and improved left ventricular function at 5 weeks time point. Delivery of myrAkt also reversed the doxorubicin-induced reduction in post-natal heart growth and diminished lung edema. These data show that myocardial Akt can inhibit doxorubicin-induced reductions in cardiac function and growth, suggesting that manipulation of this signaling pathway may have utility for the treatment of congestive heart failure. [Copyright &y& Elsevier]

Published

2002

9. A Role for Periostin Pathological Variants and Their Interaction with HSP70-1a in Promoting Pancreatic Cancer Progression and Chemoresistance.

Author

Tsunetoshi, Yasuo, Sanada, Fumihiro, Kanemoto, Yuko, Shibata, Kana, Masamune, Atsushi, Taniyama, Yoshiaki, Yamamoto, Koichi, and Morishita, Ryuichi

Abstract

Pancreatic ductal adenocarcinoma (PDAC) characterized by an abundant cancer stroma is an aggressive malignancy with a poor prognosis. Periostin (Pn) is a key extracellular matrix (ECM) protein in various tumor progression. Previously, we described the role of Pn alternative splicing variants (ASVs) with specific functional features in breast cancer. Pn is known to associate with a chemoresistance of PDAC, but the functions of the Pn-ASVs remain largely unknown. In this study, we focused on physiological and pathological Pn-ASVs, and examined the characteristics of Pn-expressing cells and the difference in function of each ASV. We found that cancer-associated fibroblasts (CAFs) are a main source of Pn synthesis, which selectively secrete pathological Pn-ASVs with exon 21 both in mouse and human samples. RNA sequencing identified a gene signature of Pn-positive CAFs associated with ECM-related genes and chemokines, factors that shape the chemoresistance tumor microenvironment (TME). Additionally, only pathological Pn-ASVs interacted with heat shock protein 70-1a (HSP70-1a), leading to significant rescue of gemcitabine-induced PDAC apoptosis. In silico analysis revealed that the presence or absence of exon 21 changes the tertiary structure of Pn and the binding sites for HSP70-1a. Altogether, Pn-ASVs with exon 21 secreted from CAFs play a key role in supporting tumor growth by interacting with cancer cell-derived HSP70-1a, indicating that Pn-ASVs with exon 21 might be a potential therapeutic and diagnostic target in PDAC patients with rich stroma. [ABSTRACT FROM AUTHOR]

Published

2024

10. Periostin Short Fragment with Exon 17 via Aberrant Alternative Splicing Is Required for Breast Cancer Growth and Metastasis.

Author

Ikeda-Iwabu, Yuka, Taniyama, Yoshiaki, Katsuragi, Naruto, Sanada, Fumihiro, Koibuchi, Nobutaka, Shibata, Kana, Shimazu, Kenzo, Rakugi, Hiromi, Morishita, Ryuichi, Aqeilan, Rami, and Yun, Chae-OK

Subjects

*METASTATIC breast cancer, *PERIOSTIN, *MOLECULAR interactions, *BREAST cancer, *CANCER prognosis, *EXTRACELLULAR matrix proteins

Abstract

Background: Periostin (POSTN) is a 93 kDa matrix protein that helps to regulate collagen gene expression in the extracellular matrix. POSTN overexpression is a prognostic factor in malignant cancers; however, some researchers have observed it in the stroma, whereas others have reported it on tumors. Objective: This study aimed to investigate the function of POSTN on tumors. Methods and Results: We found that POSTN in cancer cells can be detected by using an antibody against the POSTN C-terminal region exon 17 (Ex17 antibody), but not with an antibody against the POSTN N-terminal region exon 12 (Ex12 antibody) in patients with breast cancer. In a fraction secreted from fibroblasts, LC–MS/MS analysis revealed a short fragment of POSTN of approximately 40 kDa with exon 17. In addition, molecular interaction analysis showed that POSTN with exon 17, but not POSTN without exon 17, bound specifically to wnt3a, and the Ex17 antibody inhibited the binding. Conclusion: A short fragment of POSTN with exon 17, which originates in the fibroblasts, is transported to cancer cells, whereas POSTN fragments without exon 17 are retained in the stroma. The Ex17 antibody inhibits the binding between POSTN exon 17 and wnt3a. [ABSTRACT FROM AUTHOR]

Published

2021

11. Expression of Periostin Alternative Splicing Variants in Normal Tissue and Breast Cancer.

Author

Kanemoto, Yuko, Sanada, Fumihiro, Shibata, Kana, Tsunetoshi, Yasuo, Katsuragi, Naruto, Koibuchi, Nobutaka, Yoshinami, Tetsuhiro, Yamamoto, Koichi, Morishita, Ryuichi, Taniyama, Yoshiaki, and Shimazu, Kenzo

Subjects

*ALTERNATIVE RNA splicing, *EXTRACELLULAR matrix proteins, *PERIOSTIN, *BREAST cancer, *IN situ hybridization

Abstract

(1) Background: Periostin (Pn) is a secreted protein found in the extracellular matrix, and it plays a variety of roles in the human body. Physiologically, Pn has a variety of functions, including bone formation and wound healing. However, it has been implicated in the pathogenesis of various malignant tumors and chronic inflammatory diseases. Pn has alternative splicing variants (ASVs), and our previous research revealed that aberrant ASVs contribute to the pathogenesis of breast cancer and heart failure. However, the difference in expression pattern between physiologically expressed Pn-ASVs and those expressed during pathogenesis is not clear. (2) Methods and results: We examined normal and breast cancer tissues, focusing on the Pn-ASVs expression pattern to assess the significance of pathologically expressed Pn-ASVs as potential diagnostic and therapeutic targets. We found that most physiologically expressed Pn isoforms lacked exon 17 and 21. Next, we used human breast cancer and normal adjacent tissue (NAT) to investigate the expression pattern of Pn-ASVs under pathological conditions. Pn-ASVs with exon 21 were significantly increased in tumor tissues compared with NAT. In situ hybridization identified the synthesis of Pn-ASVs with exon 21 in peri-tumoral stromal cells. Additionally, the in vivo bio-distribution of 89Zr-labeled Pn antibody against exon 21 (Pn-21Ab) in mice bearing breast cancer demonstrated selective and specific accumulation in tumors, while Pn-21Ab significantly suppressed tumor growth in the mouse breast cancer model. (3) Conclusions: Together, these data indicate that Pn-ASVs might have potential for use as diagnostic and therapeutic targets for breast cancer. [ABSTRACT FROM AUTHOR]

Published

2024

12. The Importance of Suppressing Pathological Periostin Splicing Variants with Exon 17 in Both Stroma and Cancer.

Author

Shibata, Kana, Koibuchi, Nobutaka, Sanada, Fumihiro, Katsuragi, Naruto, Kanemoto, Yuko, Tsunetoshi, Yasuo, Ikebe, Shoji, Yamamoto, Koichi, Morishita, Ryuichi, Shimazu, Kenzo, and Taniyama, Yoshiaki

Subjects

*CELL receptors, *EXTRACELLULAR matrix proteins, *PERIOSTIN, *BREAST cancer, *FIBROBLASTS

Abstract

Background: Periostin (POSTN) is a type of matrix protein that functions by binding to other matrix proteins, cell surface receptors, or other molecules, such as cytokines and proteases. POSTN has four major splicing variants (PN1–4), which are primarily expressed in fibroblasts and cancer. We have reported that we should inhibit pathological POSTN (PN1–3), but not physiological POSTN (PN4). In particular, pathological POSTN with exon 17 is present in both stroma and cancer, but it is unclear whether the stroma or cancer pathological POSTN should be suppressed. Methods and Results: We transplanted 4T1 cells (breast cancer) secreting POSTN with exon 17 into 17KO mice lacking POSTN exon 17 to suppress stromal POSTN with exon 17. The results show that 17KO mice had smaller primary tumors and fewer metastases. Furthermore, to suppress cancer POSTN with exon 17, 4T1 cells transfected with POSTN exon 17 skipping oligo or control oligo were transplanted from the tail vein into the lungs. The results show that POSTN exon 17 skipping oligo significantly suppressed lung metastasis. Conclusions: These findings suggest that it is important to suppress POSTN exon 17 in both stroma and cancer. Antibody targeting POSTN exon 17 may be a therapeutic candidate for breast cancer. [ABSTRACT FROM AUTHOR]

Published

2024

13. Experimental Study: The Development of a Novel Treatment for Chemotherapy-Resistant Tongue Cancer with the Inhibition of the Pathological Periostin Splicing Variant 1-2 with Exon 21.

Author

Ikebe, Shoji, Koibuchi, Nobutaka, Shibata, Kana, Sanada, Fumihiro, Shimizu, Hideo, Takenobu, Toshihiko, and Taniyama, Yoshiaki

Subjects

*TONGUE cancer, *SQUAMOUS cell carcinoma, *PERIOSTIN, *TUMOR growth, *GENE expression

Abstract

Tongue squamous cell carcinoma (TSCC) occurs frequently in the oral cavity, and because of its high proliferative and metastatic potential, it is necessary to develop a novel treatment for it. We have reported the importance of the inhibition of the periostin (POSTN) pathological splicing variant, including exon 21 (PN1-2), in various malignancies, but its influence is unclear in tongue cancer. In this study, we investigated the potential of POSTN exon 21-specific neutralizing antibody (PN21-Ab) as a novel treatment for TSCC. Human PN2 was transfected into the human TSCC (HSC-3) and cultured under stress, and PN2 was found to increase cell viability. PN2 induced chemotherapy resistance in HSC-3 via the phosphorylation of the cell survival signal Akt. In tissues from human TSCC and primary tumors of an HSC-3 xenograft model, PN1-2 was expressed in the tumor stroma, mainly from fibroblasts. The intensity of PN1-2 mRNA expression was positively correlated with malignancy. In the HSC-3 xenograft model, CDDP and PN21-Ab promoted CDPP's inhibition of tumor growth. These results suggest that POSTN exon 21 may be a biomarker for tongue cancer and that PN21-Ab may be a novel treatment for chemotherapy-resistant tongue cancer. The treatment points towards important innovations for TSCC, but many more studies are needed to extrapolate the results. [ABSTRACT FROM AUTHOR]

Published

2024

14. Activated Factor X Induces Endothelial Cell Senescence Through IGFBP-5.

Author

Sanada, Fumihiro, Taniyama, Yoshiaki, Muratsu, Jun, Otsu, Rei, Iwabayashi, Masaaki, Carracedo, Miguel, Rakugi, Hiromi, and Morishita, Ryuichi

Published

2016

15. PREVENTION OF END MT AND MYOFIBROBLAST PROLIFERATION AS A THERAPEUTIC TARGET FOR CARDIAC FIBROSIS

Author

Okayama, Keita, Taniyama, Yoshiaki, Dosaka, Norio, Azuma, Junya, Sanada, Fumihiro, Kusunoki, Hiroshi, Iwabayashi, Masaaki, Rakugi, Hiromi, and Morishita, Ryuichi

Published

2011

16. Periostin splice variants affect craniofacial growth by influencing chondrocyte hypertrophy.

Author

Ishihara, Seiko, Usumi-Fujita, Risa, Kasahara, Yuki, Oishi, Shuji, Shibata, Kana, Shimizu, Yasuhiro, Ishida, Yuji, Kaneko, Sawa, Sugiura-Nakazato, Makoto, Tabata, Makoto J., Hosomichi, Jun, Taniyama, Yoshiaki, and Ono, Takashi

Subjects

*PERIOSTIN, *EXTRACELLULAR matrix proteins, *MANDIBULAR condyle, *MANDIBLE, *HYPERTROPHY, *CARTILAGE regeneration

Abstract

Introduction: Periostin, an extracellular matrix protein, plays an important role in osteogenesis and is also known to activate several signals that contribute to chondrogenesis. The absence of periostin in periostin knockout mice leads to several disorders such as craniosynostosis and periostitis. There are several splice variants with different roles in heart disease and myocardial infarction. However, little is known about each variant's role in chondrogenesis, followed by bone formation. Therefore, the aim of this study is to investigate the role of several variants in chondrogenesis differentiation and bone formation in the craniofacial region. Periostin splice variants included a full-length variant (Control), a variant lacking exon 17 (ΔEx17), a variant lacking exon 21 (ΔEx21), and another variant lacking both exon 17 and 21 ***(ΔEx17&21). Materials and Methods: We used C56BL6/N mice (n = 6) for the wild type (Control)*** and the three variant type mice (n = 6 each) to identify the effect of each variant morphologically and histologically. Micro-computed tomography demonstrated a smaller craniofacial skeleton in ΔEx17s, ΔEx21s, and ΔEx17&21s compared to Controls, especially the mandibular bone. We, thus, focused on the mandibular condyle. Results: The most distinctive histological observation was that each defected mouse appeared to have more hypertrophic chondrocytes than Controls. Real-time PCR demonstrated the differences among the group. Moreover, the lack of exon 17 or exon 21 in periostin leads to inadequate chondrocyte differentiation and presents in a diminutive craniofacial skeleton. Discussion: Therefore, these findings suggested that each variant has a significant role in chondrocyte hypertrophy, leading to suppression of bone formation. [ABSTRACT FROM AUTHOR]

Published

2023

17. Blocking Periostin Prevented Development of Inflammation in Rhabdomyolysis-Induced Acute Kidney Injury Mice Model.

Author

Muratsu, Jun, Sanada, Fumihiro, Koibuchi, Nobutaka, Shibata, Kana, Katsuragi, Naruto, Ikebe, Shoji, Tsunetoshi, Yasuo, Rakugi, Hiromi, Morishita, Ryuichi, and Taniyama, Yoshiaki

Subjects

*PERIOSTIN, *ACUTE kidney failure, *EXTRACELLULAR matrix proteins, *ANIMAL disease models, *TUMOR necrosis factors, *INTRAMUSCULAR injections, *MYOGLOBIN

Abstract

Background: Rhabdomyolysis is the collapse of damaged skeletal muscle and the leakage of muscle-cell contents, such as electrolytes, myoglobin, and other sarcoplasmic proteins, into the circulation. The glomeruli filtered these products, leading to acute kidney injury (AKI) through several mechanisms, such as intratubular obstruction secondary to protein precipitation. The prognosis is highly mutable and depends on the underlying complications and etiologies. New therapeutic plans to reduce AKI are now needed. Up to now, several cellular pathways, with the nuclear factor kappa beta (NF-kB), as well as the proinflammatory effects on epithelial and tubular epithelial cells, have been recognized as the major pathway for the initiation of the matrix-producing cells in AKI. Recently, it has been mentioned that periostin (POSTN), an extracellular matrix protein, is involved in the development of inflammation through the modulation of the NF-kB pathway. However, how POSTN develops the inflammation protection in AKI by rhabdomyolysis is uncertain. This study aimed to investigate the role of POSTN in a rhabdomyolysis mice model of AKI induced by an intramuscular injection of 50% glycerol. Methods: In vivo, we performed an intramuscular injection of 50% glycerol (5 mg/kg body weight) to make rhabdomyolysis-induced AKI. We examined the expression level of POSTN through the progression of AKI after glycerol intramuscular injection for C57BL/6J wildtype (WT) mice. We sacrificed mice at 72 h after glycerol injection. We made periostin-null mice to examine the role of POSTN in acute renal failure. The role of periostin was further examined through in vitro methods. The development of renal inflammation is linked with the NF-kB pathway. To examine the POSTN function, we administrated hemin (100 μM) on NIH-3T3 fibroblast cells, and the following signaling pathways were examined. Results: The expression of periostin was highly increased, peaking at about 72 h after glycerol injection. The expression of inflammation-associated mRNAs such as monocyte chemotactic protein-1 (MCP-1), tumor necrosis factor-alpha (TNF-a) and IL-6, and tubular injury score in H-E staining were more reduced in POSTN-null mice than WT mice at 72 h after glycerol injection. Conclusion: POSTN was highly expressed in the kidney through rhabdomyolysis and was a positive regulator of AKI. Targeting POSTN might propose a new therapeutic strategy against the development of acute renal failure. [ABSTRACT FROM AUTHOR]

Published

2022

18. Development of new screening system for Alzheimer disease, in vitro Aβ sink assay, to identify the dissociation of soluble Aβ from fibrils

Author

Sato, Naoyuki, Okochi, Masayasu, Taniyama, Yoshiaki, Kurinami, Hitomi, Shimamura, Munehisa, Takeuchi, Daisuke, Hamada, Hizuki, Fukumori, Akio, Kiyosue, Kazuyuki, Taguchi, Takahisa, Tanaka, Toshiyuki, Miyasaka, Masayuki, Takeda, Masatoshi, Ogihara, Toshio, and Morishita, Ryuichi

Subjects

*ALZHEIMER'S disease, *OLIGOMERS, *VACCINATION, *MONOMERS

Abstract

Abstract: Aβ is one of the primary therapeutic targets for Alzheimer disease (AD). Aβ vaccination induces the disappearance of Aβ deposits. Since few reports have focused on the reverse phase of Aβ aggregation, we established a new screening system, the in vitro Aβ sink assay, to clarify the process of dissociation of soluble forms from fibrils. Aβ42 was more resistant to dissociation from fibrils to monomers and/or low molecular weight (LMW) soluble oligomers than Aβ40. We applied this system to find a potential therapy for AD. Ultrasound irradiation significantly enhanced the dissociation of soluble Aβ from fibrils, while ultrasound experiments also confirmed the difference between Aβ40 and Aβ42. We found that some compounds enhanced the dissociation of Aβ from fibrils. Here, we proposed that Aβ42 was more resistant to dissociation from fibrils to monomers and/or LMW soluble oligomers than Aβ40, and this system might be useful to identify dissociation of soluble Aβ from fibrils. [Copyright &y& Elsevier]

Published

2006

19. Periostin Exon-21 Antibody Neutralization of Triple-Negative Breast Cancer Cell-Derived Periostin Regulates Tumor-Associated Macrophage Polarization and Angiogenesis.

Author

Fujikawa, Tatsuya, Sanada, Fumihiro, Taniyama, Yoshiaki, Shibata, Kana, Katsuragi, Naruto, Koibuchi, Nobutaka, Akazawa, Kaori, Kanemoto, Yuko, Kuroyanagi, Hidehito, Shimazu, Kenzo, Rakugi, Hiromi, and Morishita, Ryuichi

Subjects

*BREAST cancer prognosis, *DISEASE progression, *BIOLOGICAL models, *IMMUNOGLOBULINS, *PERIOSTIN, *XENOGRAFTS, *CANCER chemotherapy, *MACROPHAGES, *GENETIC variation, *CANCER relapse, *METASTASIS, *GENE expression, *EPITHELIAL-mesenchymal transition, *CELL adhesion molecules, *PATHOLOGIC neovascularization, *CELL lines, *TUMOR markers, *DISEASE risk factors

Abstract

Simple Summary: Despite remarkable advances in breast cancer treatment, few strategies other than standard cytotoxic chemotherapy are available for patients with triple-negative breast cancer (TNBC) due to the lack of therapeutic target molecules. TNBC is still the most aggressive subtype, with a high risk of recurrence and metastasis within 2 years after initial treatment. Thus, there is an unmet medical need to develop new treatments for metastatic and recurrent TNBC patients. In this study we tested a new antibody, targeting extracellular periostin protein alternative splicing variants, which are induced by conventional chemotherapy or during the process of endothelial mesenchymal transition. This antibody reduced periostin-secreting TNBC in a mouse xenograft model, accompanied by a decrease in the number of M2 tumor-associated macrophages and tumor vessels. Periostin alternative splicing variants might be a specific and safe therapeutic target in patients with TNBC. Periostin (Pn) is involved in multiple processes of cancer progression. Previously, we reported that Pn expression is correlated with mesenchymal tumor markers and poor prognosis in triple-negative breast cancer (TNBC). In the TNBC xenograft model, chemotherapy increased expression of a Pn alternative splicing variant (ASV) with exon 21, and administration of the neutralizing antibody against Pn with exon 21 (Pn-21 Ab) overcame chemoresistance with a reduction in the mesenchymal cancer cell fraction. In the present study, the role of Pn ASV with exon 21 in TNBC progression has been addressed. We first established a stable cell line carrying a fluorescence-based splicing reporter. Pn-positive TNBC has higher expression of genes related to tumor-associated macrophage (TAM) recruitment and ECM-receptor interaction than Pn-negative cells. In a xenograft model, only Pn-positive cells initiated tumor formation, and the Pn-21 Ab suppressed tumor cell growth, accompanied by decreased M2 TAM polarization and the number of tumor vessels. These data suggest that cancer cell-derived Pn ASV educates TAMs and regulates angiogenesis, which in turn establishes a microenvironmental niche that is supportive of TNBC. [ABSTRACT FROM AUTHOR]

Published

2021

20. Correction to: Periostin splice variants affect craniofacial growth by influencing chondrocyte hypertrophy.

Author

Ishihara, Seiko, Usumi-Fujita, Risa, Kasahara, Yuki, Oishi, Shuji, Shibata, Kana, Shimizu, Yasuhiro, Ishida, Yuji, Kaneko, Sawa, Sugiura-Nakazato, Makoto, Tabata, Makoto J., Hosomichi, Jun, Taniyama, Yoshiaki, and Ono, Takashi

Subjects

*PERIOSTIN, *HYPERTROPHY, *MEDICAL school graduates, *BONE metabolism, *MEDICAL sciences, *PERIODICAL publishing

Abstract

This document is a correction notice for an article titled "Periostin splice variants affect craniofacial growth by influencing chondrocyte hypertrophy" published in the Journal of Bone & Mineral Metabolism. The correction addresses two errors in the original publication. Firstly, the name of the institution in affiliation 3 was published incorrectly and should be corrected to "Section of Molecular Craniofacial Embryology and Oral Histology, Graduate School of Medical and Dental Sciences, Tokyo Medical and Dental University (TMDU), Tokyo, Japan." Secondly, there were errors in the use of the term "C56BL6/N" which should be corrected to "C57BL6/N" throughout the article. The correction notice also includes a statement from the publisher, Springer Nature, emphasizing their neutrality and adherence to ethical standards. [Extracted from the article]

Published

2023

21. Different roles played by periostin splice variants in retinal neovascularization.

Author

Nakama, Takahito, Yoshida, Shigeo, Ishikawa, Keijiro, Kobayashi, Yoshiyuki, Abe, Takaya, Kiyonari, Hiroshi, Shioi, Go, Katsuragi, Naruto, Ishibashi, Tatsuro, Morishita, Ryuichi, and Taniyama, Yoshiaki

Subjects

*NEOVASCULARIZATION, *PERIOSTIN, *RETINAL diseases, *ISCHEMIA, *LABORATORY mice

Abstract

Retinal neovascularization (NV) due to retinal ischemia is one of the major causes of vision reduction in patients with different types of retinal diseases although anti-vascular endothelial growth factor (anti-VEGF) therapy can partially reduce the size of the retinal NV. We recently reported that periostin plays an important role in the development of NV and the formation of preretinal fibrovascular membranes, but the role of the splice variants of periostin on retinal NV has not been determined. We examined the expressions of periostin splice variants in the ischemic retinas of a mouse model of oxygen-induced retinal NV. We also studied the function of periostin splice variants on retinal NV using periostin knock out mice, and the effects of anti-periostin antibodies on retinal NV. Our results showed that the expressions of the periostin splice variants were increased in ischemic retinas. The degree of increase of periostin lacking exon 17 was the highest among the periostin splice variants examined. Both genetic ablation of periostin exons 17 and 21 and antibodies for periostin exons 17 and 21 affected preretinal pathological NV. Inhibition of exon 17 of periostin had the greatest effect in reducing preretinal pathological NV. These findings suggest a causal link between periostin splice variants and retinal NV, and an intravitreal injection of antibody for exon 17 and exon 21 of periostin should be considered to inhibit preretinal pathological NV. [ABSTRACT FROM AUTHOR]

Published

2016

22. Hepatocyte growth factor stimulated angiogenesis without inflammation: Differential actions between hepatocyte growth factor, vascular endothelial growth factor and basic fibroblast growth factor

Author

Kaga, Toshihiro, Kawano, Hirokazu, Sakaguchi, Makoto, Nakazawa, Takahiro, Taniyama, Yoshiaki, and Morishita, Ryuichi

Subjects

*ISCHEMIA treatment, *INFLAMMATION, *HEPATOCYTE growth factor, *NEOVASCULARIZATION, *VASCULAR endothelial growth factors, *FIBROBLAST growth factors, *DRUG synergism, *RANDOMIZED controlled trials

Abstract

Abstract: Based on the potent angiogenic effects of hepatocyte growth factor (HGF), therapeutic angiogenesis using human HGF plasmid DNA increased tissue perfusion and reduced symptoms in patients with critical limb ischemia (CLI) in randomized placebo-controlled clinical trials. To explore further the potent angiogenic activity of HGF, the present study compared the effects of HGF, vascular endothelial growth factor (VEGF) and basic fibroblast growth factor (bFGF) on angiogenesis and vascular inflammation. All of HGF, VEGF and bFGF significantly induced the formation of capillary blood vessel and granulation tissue in the rat paper disc model as an in vivo animal model of angiogenesis. However, although HGF, bFGF and VEGF significantly increased the growth of vascular endothelial cells, bFGF alone, but not HGF or VEGF, significantly increased the growth of vascular smooth muscle cells (VSMCs) in the in vitro proliferation assay. In addition, bFGF, but not HGF or VEGF, significantly activated an essential transcription factor for inflammation, NFκB, and gene expression of its downstream inflammation-related cytokines (IL-8 and MCP-1) in VSMCs, accompanied by an increase in the vascular permeability in the rat paper disc model. Thus, the present results indicated that HGF induced angiogenesis without vascular inflammation, different from bFGF and VEGF. These different properties between HGF, VEGF and bFGF might affect the efficiency of therapeutic angiogenesis. [Copyright &y& Elsevier]

Published

2012

23. Estrogen attenuates vascular remodeling in Lp(a) transgenic mice

Author

Nakagami, Futoshi, Nakagami, Hironori, Osako, Mariana Kiomy, Iwabayashi, Masaaki, Taniyama, Yoshiaki, Doi, Takefumi, Shimizu, Hideo, Shimamura, Munehisa, Rakugi, Hiromi, and Morishita, Ryuichi

Subjects

*ESTROGEN, *LIPOPROTEIN A, *LABORATORY mice, *BLOOD vessels, *TISSUE remodeling, *ATHEROSCLEROSIS, *CAROTID artery, *TRANSGENIC mice, *CARDIOVASCULAR diseases risk factors

Abstract

Abstract: Objective: Although it is well known that Lipoprotein(a) (Lp(a)) is an atherogenic lipoprotein and an independent risk factor for cardiovascular disease, there is no confirmed therapy to decrease Lp(a) or prevent atherosclerosis induced by Lp(a). Thus, it is mandatory to develop novel therapy to prevent atherosclerosis in high Lp(a) concentration. Here, we focused on the effect of estrogen on Lp(a) level and Lp(a)-induced vascular remodeling. Methods: We employed Lp(a) transgenic mice (human apo(a) yeast artificial chromosome (YAC) and human apoB double transgenic mice). Vascular remodeling was induced by ligation of the common carotid artery and the effect of estrogen was evaluated in female mice after ovariectomy with or without estrogen replacement. Results: Estrogen deficiency caused by ovariectomy increased serum Lp(a), and continuous replacement of 17β-estradiol (20μg/kg/day) reversed the change. In the vascular remodeling model induced by carotid artery occlusion, neointima formation was significantly increased in ovariectomized female Lp(a) transgenic mice, but few in male Lp(a) transgenic mice, as compared to wild FVB mice. Importantly, continuous replacement of estrogen in ovariectomized mice significantly attenuated it. In cultured endothelial cells and macrophages, addition of Lp(a) increased mRNA of ICAM-1, VCAM-1, E-selectin and MCP-1 in endothelial cells and TNF-α, IL-1β and MCP-1 in macrophages in a dose-dependent manner. Importantly, pre-treatment with estrogen attenuated these changes in a dose-dependent manner. Conclusion: Estrogen negatively regulates both plasma Lp(a) level and Lp(a)-induced vascular remodeling, suggesting that estrogen might be a strong candidate to reduce serum Lp(a) concentration. [Copyright &y& Elsevier]

Published

2010

24. Ultrasound-microbubble-mediated intercellular adhesion molecule-1 small interfering ribonucleic acid transfection attenuates neointimal formation after arterial injury in mice.

Author

Suzuki J, Ogawa M, Takayama K, Taniyama Y, Morishita R, Hirata Y, Nagai R, Isobe M, Suzuki, Jun-ichi, Ogawa, Masahito, Takayama, Kiyoshi, Taniyama, Yoshiaki, Morishita, Ryuichi, Hirata, Yasunobu, Nagai, Ryozo, and Isobe, Mitsuaki

Abstract

Objectives: The purpose of this study was to investigate the efficiency of small interfering ribonucleic acid (siRNA) in murine arteries. We transfected it using a nonviral ultrasound-microbubble-mediated in vivo gene delivery system. Background: siRNA is an effective methodology to suppress gene function. The siRNA can be synthesized easily; however, a major obstacle in the use of siRNA as therapeutics is the difficulty involved in effective in vivo delivery. Methods: To investigate the efficiency of nonviral ultrasound-microbubble-mediated in vivo siRNA delivery, we used a fluorescein-labeled siRNA, green fluorescent protein (GFP) siRNA, and intercellular adhesion molecule (ICAM)-1 siRNA in murine arteries. Murine femoral arteries were injured using flexible wires to establish arterial injury. Results: The fluorescein-labeled siRNA and GFP siRNA showed that this nonviral approach could deliver siRNA into target arteries effectively without any tissue damage and systemic adverse effects. ICAM-1 siRNA transfection into murine injured arteries significantly suppressed the development of neointimal formation in comparison to those in the control group. Immunohistochemistry revealed that accumulation of T cells and adhesion molecule positive cells was observed in nontreated injured arteries, whereas siRNA suppressed accumulation. Conclusions: The nonviral ultrasound-microbubble delivery of siRNA ensures effective transfection into target arteries. ICAM-1 siRNA has the potential to suppress arterial neointimal formation. Transfection of siRNA can be beneficial for the clinical treatment of cardiovascular and other inflammatory diseases. [ABSTRACT FROM AUTHOR]

Published

2010

25. Ultrasound-Microbubble–Mediated Intercellular Adhesion Molecule-1 Small Interfering Ribonucleic Acid Transfection Attenuates Neointimal Formation After Arterial Injury in Mice

Author

Suzuki, Jun-ichi, Ogawa, Masahito, Takayama, Kiyoshi, Taniyama, Yoshiaki, Morishita, Ryuichi, Hirata, Yasunobu, Nagai, Ryozo, and Isobe, Mitsuaki

Subjects

*ULTRASONIC imaging, *MICROBUBBLE diagnosis, *CELL adhesion molecules, *SMALL interfering RNA, *ARTERIAL injuries, *LABORATORY mice, *IMMUNOHISTOCHEMISTRY

Abstract

Objectives: The purpose of this study was to investigate the efficiency of small interfering ribonucleic acid (siRNA) in murine arteries. We transfected it using a nonviral ultrasound-microbubble–mediated in vivo gene delivery system. Background: siRNA is an effective methodology to suppress gene function. The siRNA can be synthesized easily; however, a major obstacle in the use of siRNA as therapeutics is the difficulty involved in effective in vivo delivery. Methods: To investigate the efficiency of nonviral ultrasound-microbubble–mediated in vivo siRNA delivery, we used a fluorescein-labeled siRNA, green fluorescent protein (GFP) siRNA, and intercellular adhesion molecule (ICAM)-1 siRNA in murine arteries. Murine femoral arteries were injured using flexible wires to establish arterial injury. Results: The fluorescein-labeled siRNA and GFP siRNA showed that this nonviral approach could deliver siRNA into target arteries effectively without any tissue damage and systemic adverse effects. ICAM-1 siRNA transfection into murine injured arteries significantly suppressed the development of neointimal formation in comparison to those in the control group. Immunohistochemistry revealed that accumulation of T cells and adhesion molecule positive cells was observed in nontreated injured arteries, whereas siRNA suppressed accumulation. Conclusions: The nonviral ultrasound-microbubble delivery of siRNA ensures effective transfection into target arteries. ICAM-1 siRNA has the potential to suppress arterial neointimal formation. Transfection of siRNA can be beneficial for the clinical treatment of cardiovascular and other inflammatory diseases. [Copyright &y& Elsevier]

Published

2010

26. Ultrasound-Microbubble-Mediated NF-κB Decoy Transfection Attenuates Neointimal Formation after Arterial Injury in Mice.

Author

Inagaki, Hiroshi, Suzuki, Jun-ichi, Ogawa, Masahito, Taniyama, Yoshiaki, Morishita, Ryuichi, and Isobe, Mitsuaki

Subjects

*GENE transfection, *ARTERIAL injuries, *GENETIC transformation, *FLUORESCEIN, *GENETIC regulation, *LABORATORY mice

Abstract

Objective: Decoy transfection is a significant methodology for suppressing gene activation. The decoy can be synthesized easily; however, the major obstacle is the difficulty involved in effective in vivo delivery. Methods and Results: We used a fluorescein-labeled decoy to investigate the ultrasound-microbubble-mediated in vivo delivery in normal and injured mouse arteries. We showed that this approach could deliver the decoy into target tissues. In addition, we performed in vivo NF-κB decoy transfection into murine injured arteries using the ultrasound-microbubble method. Murine femoral arteries were injured using flexible wires to establish arterial injury. Pathologically, neointima/media areas in the NF-κB decoy transfection using ultrasound-microbubble group showed less than those in the control groups. Immunohistochemistry revealed that enhanced expression of inflammatory factors was observed in nontreated injured arteries, while the NF-κB decoy suppressed the expression. Conclusion: We revealed that ultrasound-microbubble delivery of the decoy is effective for transfection into target organs. We also indicated that NF-κB decoy transfection using this method has potential for the suppression of neointimal formation. Ultrasound-mediated transfection of the decoy can be beneficial for the clinical treatment of restenosis after coronary intervention and other cardiovascular diseases. Copyright © 2006 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2006

27. Local delivery of E2F decoy oligodeoxynucleotides using ultrasound with microbubble agent (Optison) inhibits intimal hyperplasia after balloon injury in rat carotid artery model

Author

Hashiya, Naotaka, Aoki, Motokuni, Tachibana, Katsuro, Taniyama, Yoshiaki, Yamasaki, Keita, Hiraoka, Kazuya, Makino, Hirofumi, Yasufumi, Kaneda, Ogihara, Toshio, and Morishita, Ryuichi

Subjects

*CORONARY restenosis, *ANGIOPLASTY, *TRANSCRIPTION factors, *PROTEINS

Abstract

Since restenosis after angioplasty still remains a major clinical problems, inhibition of neointimal formation is an important subject. In this study, we focused on the transcription factor, E2F, that plays a pivotal role in the transactivation of cell-cycle regulatory genes, and also we developed a newly delivery system of decoy oligodeoxynucleotides (ODN). We transfected E2F decoy ODN mixed with an echo-contrast microbubble agent (Optison) into rat carotid artery balloon-injured model by using therapeutic ultrasound (US) to inhibit neointimal formation. Two weeks after transfection, the intimal to medial area ratio in E2F decoy + Optison + US group was significantly decreased (P<0.01). Inhibition of cell growth was also confirmed by PCNA staining. No apparent toxicity such as inflammation could be detected in blood vessels transfected with E2F decoy ODN with Optison and ultrasound. Overall, the present studies demonstrated a novel non-viral ODN transfer method into blood vessels. A novel therapeutic strategy using E2F decoy ODN with Optison using ultrasound may be useful to inhibit restenosis in clinical practice without a viral vector. [Copyright &y& Elsevier]

Published

2004

28. Hepatocyte growth factor prevents endothelial cell death through inhibition of bax translocation from cytosol to mitochondrial membrane.

Author

Nakagami, Hironori, Morishita, Ryuichi, Yamamoto, Kei, Taniyama, Yoshiaki, Aoki, Motokuni, Yamasaki, Keita, Matsumoto, Kunio, Nakamura, Toshikazu, Kaneda, Yasufumi, and Ogihara, Toshio

Subjects

*HEPATOCYTE growth factor, *MITOCHONDRIAL membranes, *ATHEROSCLEROSIS

Abstract

Injury of endothelial cells has been postulated to be an initial trigger of the progression of atherosclerosis in patients with diabetes. Previously, we demonstrated high D-glucose induced endothelial apoptosis through the bax-caspase pathway and the potential contribution of hepatocyte growth factor (HGF) to the pathogenesis of endothelial dysfunction. In this study, we analyzed the molecular mechanisms of the protective actions of HGF against endothelial cell death under high D-glucose conditions. High concentrations of D-glucose resulted in a significant increase in apoptosis and necrosis. In contrast, HGF attenuated high D-glucose-induced apoptosis and necrosis (P < 0.01). High D-glucose significantly increased bax protein, but not bcl-2, and activated caspase 3-like and 9, whereas HGF significantly increased bcl-2 expression without affecting bax level and attenuated the increase in caspase 3 and 9 activity. Interestingly, high D-glucose resulted in translocation of bax protein from cytosol to the mitochondrial membrane, whereas HGF inhibited the bax translocation. Importantly, this bax translocation was also completely blocked by overexpressed bcl-2. These findings suggest that HGF can activate bcl-2 expression and inhibit translocation of bax protein upstream of the mitochondria, thereby leading to the inhibition of caspase 3 and 9 activation. HGF may be an important factor in the maintenance of endothelial function. [ABSTRACT FROM AUTHOR]

Published

2002

29. Phosphorylation of p38 mitogen-activated protein kinase downstream of bax-caspase-3 pathway leads to cell death induced by high D-glucose in human endothelial cells.

Author

Nakagami, Hironori, Morishita, Ryuichi, Yamamoto, Kei, Yoshimura, Shin-ichi, Taniyama, Yoshiaki, Aoki, Motokuni, Matsubara, Hiroaki, Kim, Shokei, Kaneda, Yasufumi, Ogihara, Toshio, Nakagami, H, Morishita, R, Yamamoto, K, Yoshimura, S I, Taniyama, Y, Aoki, M, Matsubara, H, Kim, S, Kaneda, Y, and Ogihara, T

Subjects

*APOPTOSIS, *PROTEIN kinases, *GLUCOSE

Abstract

Because high D-glucose significantly stimulates endothelial cell death, we examined the molecular mechanisms of high D-glucose-induced endothelial apoptosis. Treatment of human aortic endothelial cells with high D-glucose (25 mmol/l), but not mannitol and L-glucose, resulted in a significant decrease in cell number and a significant increase in apoptotic cells as compared with a physiological concentration (5 mmol/l). Interestingly, high D-glucose treatment significantly increased bax protein, accompanied by translocation of bax protein from cytosol to mitochondria-enriched heavy membrane fraction. In contrast, the expression and distribution of bcl-2 protein were not altered by high D-glucose. In addition, the activity of caspase-3 proteases was increased after exposure to high glucose, whereas caspase inhibitors prevented endothelial cell death induced by high D-glucose. On the other hand, p38 mitogen-activated protein kinase (MAPK) was markedly phosphorylated and showed sustained phosphorylation after stimulation. A specific inhibitor of p38 MAPK, SB 203580, and the overexpression of kinase-inactive p38 MAPK significantly attenuated cell death induced by high D-glucose in human aortic endothelial cells, whereas at 6 h after high D-glucose treatment, SB 203580 and overexpression of kinase-inactive p38 MAPK did not attenuate caspase-3 activation induced by high D-glucose. Importantly, caspase inhibitors significantly attenuated the sustained phosphorylation of p38 MAPK induced by high D-glucose. Thus, we finally focused the MAPK kinase (MEK) kinase 1 (MEKK1) to further examine the cross-talk between p38 MAPK and the bax-caspase proteases pathway. High D-glucose treatment induced MEKK1 cleavage, whereas caspase inhibitors significantly attenuated the cleavage. Importantly, kinase-inactive MEKK1 also blocked the phosphorylation of p38 MAPK induced by high D-glucose. Here, we demonstrated that high D-glucose induced apoptosis in human endothelial cells through activation of the bax-caspase proteases pathway and through phosphorylation of p38 MAPK mediated by MEKK1. Phosphorylation of p38 MAPK downstream of the bax-caspase pathway may play a pivotal role in endothelial apoptosis mediated by high D-glucose. [ABSTRACT FROM AUTHOR]

Published

2001