Your search keyword '"Takuya Iyoda"' showing total 50 results

1. Biofunctional Peptide FNIII14: Therapeutic Potential

Author

Motomichi Fujita, Manabu Sasada, Takuya Iyoda, Satoshi Osada, Hiroaki Kodama, and Fumio Fukai

Subjects

extracellular matrix, fibronectin, FNIII14, integrin inactivation, cell adhesion, anti-fibrotic activity, Science

Abstract

Biofunctional peptide FNIII14, which is derived from the 14th fibronectin (FN) type III-like (FN-III) repeat of FN molecule, is capable of inhibiting cell adhesion to the extracellular matrix (ECM). This functional site is usually buried within the molecular structure of FN, but can be exposed by conformational changes and proteolytic cleavage. Peptide FNIII14 can induce a conformational change in β1-integrin from the active to the inactive form, causing functional inactivation. Based on this anti-adhesive activity, peptide FNIII14 exhibits therapeutic potential for several diseases such as metabolic diseases, organ fibrosis, and malignant tumors. Peptide FNIII14 blocks integrin-mediated signaling by a mechanism entirely distinct from that of conventional antagonisitic peptides, including Arg-Gly-Asp peptides that competitively inhibit the ECM binding of integrin.

Published

2021

2. Biologically Active TNIIIA2 Region in Tenascin-C Molecule: A Major Contributor to Elicit Aggressive Malignant Phenotypes From Tumors/Tumor Stroma

Author

Takuya Iyoda, Motomichi Fujita, and Fumio Fukai

Subjects

tenascin-C, TNIIIA2, β1-integrin, macrophage, solid tumor, glioblastoma, Immunologic diseases. Allergy, RC581-607

Abstract

Tenascin (TN)-C is highly expressed specifically in the lesions of inflammation-related diseases, including tumors. The expression level of TN-C in tumors and the tumor stroma is positively correlated with poor prognosis. However, no drugs targeting TN-C are currently clinically available, partly because the role of TN-C in tumor progression remains controversial. TN-C harbors an alternative splicing site in its fibronectin type III repeat domain, and its splicing variants including the type III-A2 domain are frequently detected in malignant tumors. We previously identified a biologically active region termed TNIIIA2 in the fibronectin type III-A2 domain of TN-C molecule and showed that this region is involved in promoting firm and persistent cell adhesion to fibronectin. In the past decade, through the exposure of various cell lines to peptides containing the TNIIIA2 region, we have published reports demonstrating the ability of the TNIIIA2 region to modulate distinct cellular activities, including survival/growth, migration, and invasion. Recently, we reported that the signals derived from TNIIIA2-mediated β1 integrin activation might play a crucial role for inducing malignant behavior of glioblastoma (GBM). GBM cells exposed to the TNIIIA2 region showed not only exacerbation of PDGF-dependent proliferation, but also acceleration of disseminative migration. On the other hand, we also found that the pro-inflammatory phenotypic changes were promoted when macrophages are stimulated with TNIIIA2 region in relatively low concentration and resulting MMP-9 upregulation is needed to release of the TNIIIA2 region from TN-C molecule. With the contribution of TNIIIA2-stimulated macrophages, the positive feedback spiral loop, which consists of the expression of TN-C, PDGF, and β1 integrin, and TNIIIA2 release, seemed to be activated in GBM with aggressive malignancy. Actually, the growth of transplanted GBM grafts in mice was significantly suppressed via the attenuation of β1 integrin activation. In this review, we thus introduce that the TNIIIA2 region has a significant impact on malignant progression of tumors by regulating cell adhesion. Importantly, it has been demonstrated that the TNIIIA2 region exerts unique biological functions through the extremely strong activation of β1-integrins and their long-lasting duration. These findings prompt us to develop new therapeutic agents targeting the TNIIIA2 region.

Published

2020

3. Wound Healing Promotion by Hyaluronic Acid: Effect of Molecular Weight on Gene Expression and In Vivo Wound Closure

Author

Yayoi Kawano, Viorica Patrulea, Emmanuelle Sublet, Gerrit Borchard, Takuya Iyoda, Rihoko Kageyama, Asa Morita, Satoshi Seino, Hideto Yoshida, Olivier Jordan, and Takehisa Hanawa

Subjects

hyaluronic acid, accelerated wound healing, epidermal cells, cytokines, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Hyaluronic acid (HA) has been known to play an important role in wound healing process. However, the effect of molecular weight (MW) of exogenously administered HA on the wound healing process has not been fully understood. In this study, we investigated HA with different MWs on wound healing process using human epidermal keratinocytes and dermal fibroblasts. Cell proliferation and migration ability were assessed by water soluble tetrazolium (WST) assay and wound scratch assay. We examined the effect of HA addition in a full-thickness wound model in mice and the gene expression related to wound healing. Proliferation and migration of HaCaT cells increased with the increase of MW and concentration of HA. Interleukin (IL-1β), IL-8 and vascular endothelial growth factor (VEGF) as well as matrix metalloproteinase (MMP)-9 and MMP-13 were significantly upregulated by high molecular weight (HMW) HA in keratinocytes. Together with VEGF upregulation and the observed promotion of HaCaT migration, HA with the MW of 2290 kDa may hold potential to improve re-epithelialization, a critical obstacle to heal chronic wounds.

Published

2021

4. Involvement of Integrin-Activating Peptides Derived from Tenascin-C in Cancer Aggression and New Anticancer Strategy Using the Fibronectin-Derived Integrin-Inactivating Peptide

Author

Motomichi Fujita, Manabu Sasada, Takuya Iyoda, and Fumio Fukai

Subjects

extracellular matrix, matricellular protein, cell adhesion, β1-integrin, α5-integrin tenascin-C, fibronectin, Organic chemistry, QD241-441

Abstract

Matricellular proteins, which exist in association with the extracellular matrix (ECM) and ECM protein molecules, harbor functional sites within their molecular structures. These functional sites are released through proteolytic cleavage by inflammatory proteinases, such as matrix metalloproteinases (MMPs) and a disintegrin and metalloproteinase with thrombospondin motifs (ADAMTS), and the peptides containing these functional sites have unique biological activities that are often not detected in the parent molecules. We previously showed that tenascin-C (TNC) and plasma fibronectin (pFN), examples of matricellular proteins, have cryptic bioactive sites that have opposite effects on cell adhesion to the ECM. A peptide containing the bioactive site of TNC, termed TNIIIA2, which is highly released at sites of inflammation and in the tumor microenvironment (TME), has the ability to potently and persistently activate β1-integrins. In the opposite manner, the peptide FNIII14 containing the bioactive site of pFN has the ability to inactivate β1-integrins. This review highlights that peptide TNIIIA2 can act as a procancer factor and peptide FNIII14 can act as an anticancer agent, based on the regulation on β1-integrin activation. Notably, the detrimental effects of TNIIIA2 can be inhibited by FNIII14. These findings open the possibility for new therapeutic strategies based on the inactivation of β1-integrin by FNIII14.

Published

2020

5. Coadministration of the FNIII14 Peptide Synergistically Augments the Anti-Cancer Activity of Chemotherapeutic Drugs by Activating Pro-Apoptotic Bim.

Author

Takuya Iyoda, Yumi Nagamine, Yoshitomi Nakane, Yuya Tokita, Shougo Akari, Kazuki Otsuka, Motomichi Fujita, Keisuke Itagaki, You-Ichi Takizawa, Hiroaki Orita, Toshiyuki Owaki, Jyunichi Taira, Ryo Hayashi, Hiroaki Kodama, and Fumio Fukai

Subjects

Medicine, Science

Abstract

The acquisition of drug resistance mediated by the interaction of tumor cells with the extracellular matrix (ECM), commonly referred to as cell adhesion-mediated drug resistance (CAM-DR), has been observed not only in hematopoietic tumor cells but also in solid tumor cells. We have previously demonstrated that a 22-mer peptide derived from fibronectin, FNIII14, can inhibit cell adhesion through the inactivation of β1 integrin; when coadministered with cytarabine, FNIII14 completely eradicates acute myelogenous leukemia by suppressing CAM-DR. In this study, we show that our FNIII14 peptide also enhances chemotherapy efficacy in solid tumors. Coadministration of FNIII14 synergistically enhances the cytotoxicity of doxorubicin and aclarubicin in mammary tumor and melanoma cells, respectively. The solid tumor cell chemosensitization induced by FNIII14 is dependent upon the upregulation and activation of the pro-apoptotic protein, Bim. Furthermore, the metastasis of tumor cells derived from ventrally transplanted mammary tumor grafts is suppressed by the coadministration of FNIII14 and doxorubicin. These results suggest that the coadministration of our FNIII14 peptide with chemotherapy could achieve efficient solid tumor eradication by increasing chemosensitivity and decreasing metastasis. The major causes of tumor recurrence are the existence of chemotherapy-resistant primary tumor cells and the establishment of secondary metastatic lesions. As such, coadministering FNIII14 with anti-cancer drugs could provide a promising new approach to improve the prognosis of patients with solid tumors.

Published

2016

6. New Molecular Mechanisms for Cardiovascular Disease: Cardiac Hypertrophy and Cell-Volume Regulation

Author

Shintaro Yamamoto, Satomi Kita, Takuya Iyoda, Toshiki Yamada, and Takahiro Iwamoto

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

Abstract.: Cardiac hypertrophy is an increase in the muscle volume of the ventricle due to the enlargement of cardiac cells. Physiological cardiac hypertrophy is the normal response to healthy exercise, and pathological hypertrophy is the response to increased stress such as hypertension. Intracellular and extracellular aniosmotic conditions also change cell volume. Since persistent cell swelling or cell shrinkage during aniosmotic conditions results in cell death, the ability to regulate cell volume is important for the maintenance of cellular homeostasis. Cell swelling activates a regulatory volume decrease (RVD) response in which solute leakage pathways are stimulated and solute with water exits cells, reducing the cell volume towards the original value. In cardiac cells, one of the essential factors for cell-volume regulation is the volume-regulated anion channel (VRAC). However, the relationship between cardiac hypertrophy and cell-volume regulation is not clear. In this review, we introduce our recent findings showing that the impairment of VRAC current is exhibited in ventricular cells from mice with cardiac hypertrophy induced by transverse aortic constriction. Similar results were shown in caveolin-3–deficient mice, which develop cardiac hypertrophy without pressure overload. These results suggest that VRAC will be a new target for protection from the development of cardiac hypertrophy. Keywords:: hypertrophy, volume regulation, cardiac cell, anion channel, Cl− current, cardiovascular disease

Published

2011

7. Modulation of Tumor Cell Survival, Proliferation, and Differentiation by the Peptide Derived from Tenascin-C: Implication of β1-Integrin Activation

Author

Takuya Iyoda and Fumio Fukai

Subjects

Cytology, QH573-671

Abstract

Cell adhesion to extracellular matrix (ECM) participates in various biological processes, such as cell survival, proliferation, differentiation, and migration. Since these processes are essential for keeping homeostasis, aberration of these processes leads to a variety of diseases including cancer. Previously, we found that a peptide derived from tenascin- (TN-) C, termed TNIIIA2, stimulates cell adhesion to ECM through activation of β1-integrin. It has been shown that TNIIIA2 can modulate cell proliferation and differentiation. Interestingly, TNIIIA2 could not only enhance cell proliferation but also induce apoptotic cell death, depending on cellular context. In this review, we show the function of the peptide TNIIIA2 in cell survival, proliferation, and differentiation and refer to the possibility of new strategy for tumor suppression by regulating cell adhesion status using the ECM-derived functional peptides.

Published

2012

8. Supplementary table S1 from Aggressive Progression in Glioblastoma Cells through Potentiated Activation of Integrin α5β1 by the Tenascin-C–Derived Peptide TNIIIA2

Author

Fumio Fukai, Hiroaki Kodama, Sadahiro Kamiya, Kazuki Otsuka, Chikako Kudo, Reo Nagai, Manabu Sasada, Tatsuya Fujisawa, Takuya Iyoda, Tetsuya Yamamoto, and Motomichi Fujita

Abstract

Antibody information

Published

2023

9. Data from Aggressive Progression in Glioblastoma Cells through Potentiated Activation of Integrin α5β1 by the Tenascin-C–Derived Peptide TNIIIA2

Author

Fumio Fukai, Hiroaki Kodama, Sadahiro Kamiya, Kazuki Otsuka, Chikako Kudo, Reo Nagai, Manabu Sasada, Tatsuya Fujisawa, Takuya Iyoda, Tetsuya Yamamoto, and Motomichi Fujita

Abstract

Tenascin-C is a member of the matricellular protein family, and its expression level is correlated to poor prognosis in cancer, including glioblastoma, whereas its substantial role in tumor formation and malignant progression remains controversial. We reported previously that peptide TNIIIA2 derived from the cancer-associated alternative splicing domain of tenascin-C molecule has an ability to activate β1-integrin strongly and to maintain it for a long time. Here, we demonstrate that β1-integrin activation by TNIIIA2 causes acquisition of aggressive behavior, dysregulated proliferation, and migration, characteristic of glioblastoma cells. TNIIIA2 hyperstimulated the platelet-derived growth factor–dependent cell survival and proliferation in an anchorage-independent as well as -dependent manner in glioblastoma cells. TNIIIA2 also strongly promoted glioblastoma multiforme cell migration, which was accompanied by an epithelial–mesenchymal transition–like morphologic change on the fibronectin substrate. Notably, acquisition of these aggressive properties by TNIIIA2 in glioblastoma cells was abrogated by peptide FNIII14 that is capable of inducing inactivation in β1-integrin activation. Moreover, FNIII14 significantly inhibited tumor growth in a mouse xenograft glioblastoma model. More importantly, FNIII14 sensitized glioblastoma cells to temozolomide via downregulation of O6-methylguanine-DNA methyltransferase expression. Consequently, FNIII14 augmented the antitumor activity of temozolomide in a mouse xenograft glioblastoma model. Taken altogether, the present study provides not only an interpretation for the critical role of tenascin-C/TNIIIA2 in aggressive behavior of glioblastoma cells, but also an important strategy for glioblastoma chemotherapy. Inhibition of the tenascin-C/β1-integrin axis may be a therapeutic target for glioblastoma, and peptide FNIII14 may represent a new approach for glioblastoma chemotherapy.Significance:These findings provide a proposal of new strategy for glioblastoma chemotherapy based on integrin inactivation.

Published

2023

10. Supplementary Data from Aggressive Progression in Glioblastoma Cells through Potentiated Activation of Integrin α5β1 by the Tenascin-C–Derived Peptide TNIIIA2

Author

Fumio Fukai, Hiroaki Kodama, Sadahiro Kamiya, Kazuki Otsuka, Chikako Kudo, Reo Nagai, Manabu Sasada, Tatsuya Fujisawa, Takuya Iyoda, Tetsuya Yamamoto, and Motomichi Fujita

Abstract

This file shows the supplementary figure (S1-S8).

Published

2023

11. Supplementary Materials and Methods from Aggressive Progression in Glioblastoma Cells through Potentiated Activation of Integrin α5β1 by the Tenascin-C–Derived Peptide TNIIIA2

Author

Fumio Fukai, Hiroaki Kodama, Sadahiro Kamiya, Kazuki Otsuka, Chikako Kudo, Reo Nagai, Manabu Sasada, Tatsuya Fujisawa, Takuya Iyoda, Tetsuya Yamamoto, and Motomichi Fujita

Abstract

This file shows the materials and methods in the results of 'Supplementary Figure'.

Published

2023

12. Supplementary Movie S3 from Aggressive Progression in Glioblastoma Cells through Potentiated Activation of Integrin α5β1 by the Tenascin-C–Derived Peptide TNIIIA2

Author

Fumio Fukai, Hiroaki Kodama, Sadahiro Kamiya, Kazuki Otsuka, Chikako Kudo, Reo Nagai, Manabu Sasada, Tatsuya Fujisawa, Takuya Iyoda, Tetsuya Yamamoto, and Motomichi Fujita

Abstract

Time lapse evaluation of cell scattering (TNIIIA2 + FNIII14)

Published

2023

13. Supplementary Movie legend from Aggressive Progression in Glioblastoma Cells through Potentiated Activation of Integrin α5β1 by the Tenascin-C–Derived Peptide TNIIIA2

Author

Fumio Fukai, Hiroaki Kodama, Sadahiro Kamiya, Kazuki Otsuka, Chikako Kudo, Reo Nagai, Manabu Sasada, Tatsuya Fujisawa, Takuya Iyoda, Tetsuya Yamamoto, and Motomichi Fujita

Abstract

This file shows the legends of Supplementary Movie S1-S3.

Published

2023

14. Heat shock-induced heme oxygenase-1 expression in a mouse hepatoma cell line is dependent on HSF1 and modified by NRF2 and BACH1

Author

Sachiye Inouye, Takanori Kubo, Takafumi Miyamoto, Takuya Iyoda, Naoyuki Okita, and Reiko Akagi

Subjects

Genetics, Cell Biology

Abstract

The induction mechanism of heme oxygenase-1 (HO-1) by heat shock (HS) is still unknown. Here, we discovered that HS activates the HO-1 expression in a mouse hepatoma cell line (Hepa 1-6). Knockdown experiments showed that the HS-induced HO-1 expression was dependent on HS factor 1 (HSF1). A chromatin immunoprecipitation (ChIP) assay demonstrated that the HS-activated HSF1 bound to the HS elements (HSEs) in the upstream enhancer 1 region (E1). Unexpectedly, HS also facilitates the BTB and CNC homology 1 (BACH1) binding to the Maf recognition elements (MAREs) in E1. We examined the effects of a catalytically inactive CRISPR-associated 9 nucleases (dCas9) with short guide RNAs (sgRNAs), and demonstrated that the HSF1 binding to HSEs in E1 was indispensable for the HS-induced HO-1 expression. Heme treatment (HA) dissociates BACH1 from MAREs and facilitated the binding of nuclear factor-erythroid-2-related factor 2 (NRF2) to MAREs. Following treatment with both HS and HA, the HO-1 induction and the HSF1 binding to HSEs in E1 were most notably observed. These results indicate that the HS-induced HO-1 expression is dependent on the HSF1 binding to HSEs in E1, although modulated by the BACH1 and NRF2 binding to MAREs within the same E1.

Published

2022

15. Biofunctional Peptide FNIII14: Therapeutic Potential

Author

Manabu Sasada, Fumio Fukai, Takuya Iyoda, Satoshi Osada, Motomichi Fujita, and Hiroaki Kodama

Subjects

0301 basic medicine, Conformational change, anti-fibrotic activity, extracellular matrix, Science, Integrin, Peptide, Cleavage (embryo), Extracellular matrix, 03 medical and health sciences, 0302 clinical medicine, Fibrosis, fibronectin, medicine, Cell adhesion, FNIII14, chemistry.chemical_classification, biology, cell adhesion, medicine.disease, Cell biology, Fibronectin, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, biology.protein, integrin inactivation

Abstract

Biofunctional peptide FNIII14, which is derived from the 14th fibronectin (FN) type III-like (FN-III) repeat of FN molecule, is capable of inhibiting cell adhesion to the extracellular matrix (ECM). This functional site is usually buried within the molecular structure of FN, but can be exposed by conformational changes and proteolytic cleavage. Peptide FNIII14 can induce a conformational change in β1-integrin from the active to the inactive form, causing functional inactivation. Based on this anti-adhesive activity, peptide FNIII14 exhibits therapeutic potential for several diseases such as metabolic diseases, organ fibrosis, and malignant tumors. Peptide FNIII14 blocks integrin-mediated signaling by a mechanism entirely distinct from that of conventional antagonisitic peptides, including Arg-Gly-Asp peptides that competitively inhibit the ECM binding of integrin.

Published

2021

16. Anoikis resistance conferred by tenascin-C-derived peptide TNIIIA2 and its disruption by integrin inactivation

Author

Chikako Kudo, Fumio Fukai, Motomichi Fujita, Satoshi Osada, Takashi Yamamoto, Manabu Sasada, Reo Nagai, Hiroaki Kodama, and Takuya Iyoda

Subjects

0301 basic medicine, Cell Survival, Integrin, Biophysics, Biochemistry, Extracellular matrix, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Cell Adhesion, Humans, Anoikis, Molecular Biology, Tumor microenvironment, biology, Chemistry, Integrin beta1, Tenascin C, Tenascin, Cell Biology, Fibronectins, 030104 developmental biology, Apoptosis, Cell culture, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, biology.protein, Peptides

Abstract

Glioblastoma multiforme (GBM), the most common brain tumor in adults, has an extremely poor prognosis, which is attributed to the aggressive properties of GBM cells, such as dysregulated proliferation and disseminative migration. We recently found that peptide TNIIIA2, derived from tenascin-C (TNC), which is highly expressed in GBM, contributes to the acquisition of these aggressive properties through β1-integrin activation. In general, cancer cells often acquire an additional malignant property that confers resistance to apoptosis due to loss of adhesion to the extracellular matrix, termed anoikis resistance. Our present results show that regulation of β1-integrin activation also plays a key role in both the development and loss of anoikis resistance in GBM cells. Despite being derived from a GBM with an extremely poor prognosis, the human GBM cell line T98G was susceptible to anoikis but became anoikis resistant via treatment with peptide TNIIIA2, which is able to activate β1-integrin. The TNIIIA2-conferred anoikis resistance of T98G cells was disrupted by further addition of peptide FNIII14, which has the ability to inactivate β1-integrin. Moreover, anchorage-independent survival of GBM cells in suspension culture was abrogated by peptide FNIII14, but not by RGD and CS-1 peptides, which are antagonistic for integrins α5β1, αvβ3, and α4β1. These results suggest that GBM cells develop anoikis resistance through activation of β1-integrin by TNC-derived peptide TNIIIA2, which is abundantly released into the tumor microenvironment of GBM. Inactivation of β1-integrin may provide a promising strategy to overcome the apoptosis resistance of cancer cells, including GBM.

Published

2021

17. Induction of cellular senescence in fibroblasts through β1-integrin activation by tenascin-C-derived peptide and its protumor effect

Author

Motomichi, Fujita, Manabu, Sasada, Mayu, Eguchi, Takuya, Iyoda, Shin, Okuyama, Takuro, Osawa, Kenta, Tsuzuranuki, Mamoru, Sakamoto, Yu, Hagihara, Masaki, Matsumura, Satoshi, Osada, Hiroaki, Kodama, Yoshikazu, Higami, and Fumio, Fukai

Subjects

Original Article

Abstract

Tenascin-C is upregulated during inflammation and tumorigenesis, and its expression level is correlated with a poor prognosis in several malignancies. Nevertheless, the substantial role of tenascin-C in cancer progression is poorly understood. Previously, we found that a peptide derived from tenascin-C, termed TNIIIA2, acts directly on tumor cells to activate β1-integrin and induce malignant progression. Here, we show that β1-integrin activation by TNIIIA2 in human fibroblasts indirectly contributes to cancer progression through the induction of cellular senescence. Prolonged treatment of fibroblasts with TNIIIA2 induced cellular senescence, as characterized by the suppression of cell growth and the induction of senescence-associated-β-galactosidase and p16(INK4a) expression. The production of reactive oxygen species and subsequent DNA damage were responsible for the TNIIIA2-induced senescence of fibroblasts. Interestingly, peptide FNIII14, which inactivates β1-integrin, inhibited fibroblast senescence induced not only by TNIIIA2 but also by H(2)O(2), suggesting that β1-integrin activation plays a critical role in the induction of senescence in fibroblasts. Moreover, TNIIIA2-induced senescent fibroblasts secreted heparin-binding epidermal growth factor-like growth factor (HB-EGF), which caused preneoplastic epithelial HaCaT cells to acquire malignant properties, including colony-forming and focus-forming abilities. Thus, our study demonstrates that tenascin-C-derived peptide TNIIIA2 induces cellular senescence in fibroblasts through β1-integrin activation, causing cancer progression via the secretion of humoral factors such as HB-EGF.

Published

2021

18. Aggressive Progression in Glioblastoma Cells through Potentiated Activation of Integrin α5β1 by the Tenascin-C–Derived Peptide TNIIIA2

Author

Reo Nagai, Sadahiro Kamiya, Tatsuya Fujisawa, Motomichi Fujita, Chikako Kudo, Takashi Yamamoto, Hiroaki Kodama, Manabu Sasada, Takuya Iyoda, Fumio Fukai, and Kazuki Otsuka

Subjects

0301 basic medicine, Cancer Research, Cell Survival, Integrin, Mice, Nude, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Cell Movement, Cell Line, Tumor, Temozolomide, medicine, Animals, Humans, Antineoplastic Agents, Alkylating, neoplasms, Cell Proliferation, Mice, Inbred BALB C, biology, Chemistry, Tenascin C, Matricellular protein, Tenascin, Cell migration, Xenograft Model Antitumor Assays, Fibronectins, Rats, nervous system diseases, Fibronectin, 030104 developmental biology, Oncology, Cell culture, 030220 oncology & carcinogenesis, Disease Progression, biology.protein, Cancer research, Female, Glioblastoma, Peptides, Integrin alpha5beta1, medicine.drug

Abstract

Tenascin-C is a member of the matricellular protein family, and its expression level is correlated to poor prognosis in cancer, including glioblastoma, whereas its substantial role in tumor formation and malignant progression remains controversial. We reported previously that peptide TNIIIA2 derived from the cancer-associated alternative splicing domain of tenascin-C molecule has an ability to activate β1-integrin strongly and to maintain it for a long time. Here, we demonstrate that β1-integrin activation by TNIIIA2 causes acquisition of aggressive behavior, dysregulated proliferation, and migration, characteristic of glioblastoma cells. TNIIIA2 hyperstimulated the platelet-derived growth factor–dependent cell survival and proliferation in an anchorage-independent as well as -dependent manner in glioblastoma cells. TNIIIA2 also strongly promoted glioblastoma multiforme cell migration, which was accompanied by an epithelial–mesenchymal transition–like morphologic change on the fibronectin substrate. Notably, acquisition of these aggressive properties by TNIIIA2 in glioblastoma cells was abrogated by peptide FNIII14 that is capable of inducing inactivation in β1-integrin activation. Moreover, FNIII14 significantly inhibited tumor growth in a mouse xenograft glioblastoma model. More importantly, FNIII14 sensitized glioblastoma cells to temozolomide via downregulation of O6-methylguanine-DNA methyltransferase expression. Consequently, FNIII14 augmented the antitumor activity of temozolomide in a mouse xenograft glioblastoma model. Taken altogether, the present study provides not only an interpretation for the critical role of tenascin-C/TNIIIA2 in aggressive behavior of glioblastoma cells, but also an important strategy for glioblastoma chemotherapy. Inhibition of the tenascin-C/β1-integrin axis may be a therapeutic target for glioblastoma, and peptide FNIII14 may represent a new approach for glioblastoma chemotherapy. Significance: These findings provide a proposal of new strategy for glioblastoma chemotherapy based on integrin inactivation.

Published

2019

19. Inactivation of beta1 integrin induces proteasomal degradation of Myc oncoproteins

Author

Sana Yokoi, Yusuke Suenaga, Tatsufumi Asayama, Shunsuke Sakai, Fumio Fukai, Manabu Sasada, Yoichiro Isohama, Hiroaki Kodama, Takuya Iyoda, and Naoya Kase

Subjects

0301 basic medicine, proteasomal degradation, integrin, Integrin, Peptide, Myc, 03 medical and health sciences, neuroblastoma, 0302 clinical medicine, fibronectin, Neuroblastoma, Pancreatic cancer, medicine, Gene, chemistry.chemical_classification, biology, Beta1 Integrin, medicine.disease, Fibronectin, 030104 developmental biology, Oncology, Targeted drug delivery, chemistry, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Research Paper

Abstract

The MYC family oncogenes (MYC, MYCN, and MYCL) contribute to the genesis of many human cancers. Among them, amplification of the MYCN gene and over-expression of N-Myc protein are the most reliable risk factors in neuroblastoma patients. On the other hand, we previously found that a peptide derived from fibronectin, termed FNIII14, is capable of inducing functional inactivation in β1-integrins. Here, we demonstrate that inactivation of β1-integrin by FNIII14 induced proteasomal degradation in N-Myc of neuroblastoma cells with MYCN amplification. This N-Myc degradation by FNIII14 reduced the malignant properties, including the anchorage-independent proliferation and invasive migration, of neuroblastoma cells. An in vivo experiment using a mouse xenograft model showed that the administration of FNIII14 can inhibit tumor growth, and concomitantly a remarkable decrease in N-Myc levels in tumor tissues. Of note, the activation of proteasomal degradation based on β1-integrin inactivation is applicable to another Myc family oncoprotein, c-myc, which also reverses cancer-associated properties in pancreatic cancer cells. Collectively, β1-integrin inactivation could be a new chemotherapeutic strategy for cancers with highly expressed Myc. FNIII14, which is a unique pharmacological agent able to induce β1-integrin inactivation, may be a promising drug targeting Myc oncoproteins for cancer chemotherapy.

Published

2019

20. Acyclic Retinoid Combined With Tenascin-C-derived Peptide Reduces the Malignant Phenotype of Neuroblastoma Cells Through N-Myc Degradation

Author

Yoshikazu Higami, Hiroaki Kodama, Manabu Sasada, Yusuke Nohara, Takuya Iyoda, Kazuki Otsuka, Fumio Fukai, and Y U Hirano

Subjects

Cancer Research, medicine.medical_treatment, Integrin, Retinoic acid, Mice, Nude, Antineoplastic Agents, Tretinoin, Neuroblastoma, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Western blot, medicine, Animals, neoplasms, Cell Proliferation, Mice, Inbred BALB C, N-Myc Proto-Oncogene Protein, Chemotherapy, biology, medicine.diagnostic_test, Tenascin C, Tenascin, General Medicine, medicine.disease, Tumor Burden, Phenotype, Oncology, Proteasome, chemistry, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Peptides, N-Myc

Abstract

BACKGROUND/AIM Despite intensive chemotherapy, the survival rates for high-risk neuroblastoma, most of which have MYCN amplification, remain low. Overexpression of N-myc oncoprotein promotes expression of cancer-associated properties. We recently found that combination of all-trans retinoic acid (ATRA) with the β1-integrin-activating peptide TNIIIA2 attenuated cancer-associated properties of neuroblastoma cells through N-Myc degradation. However, ATRA has serious side-effects and there are concerns about late adverse effects. The aim of this study was to examine the effects of the combination of acyclic retinoid (ACR) with TNIIIA2 on neuroblastoma. MATERIALS AND METHODS The effects of ACR and TNIIIA2 were examined by neuroblastoma cell proliferation and survival assays as well as by using a neuroblastoma xenograft model. The levels of N-Myc and cancer-associated malignant properties were assayed by western blot and colony formation assay, respectively. RESULTS Combining ACR, which is clinically safe, with TNIIIA2 induced proteasomal degradation of N-Myc and reduction of neuroblastoma cell malignant properties. An in vivo experiment showed therapeutic potential. CONCLUSION ACR-TNIIIA2 combination treatment may be efficacious and clinical safe chemotherapy for high-risk neuroblastoma.

Published

2019

21. Wound Healing Promotion by Hyaluronic Acid: Effect of Molecular Weight on Gene Expression and In Vivo Wound Closure

Author

Satoshi Seino, Hideto Yoshida, Asa Morita, Emmanuelle Sublet, Rihoko Kageyama, Takuya Iyoda, Gerrit Borchard, Olivier Jordan, Takehisa Hanawa, Yayoi Kawano, and Viorica Patrulea

Subjects

Hyaluronic acid, Pharmaceutical Science, lcsh:Medicine, lcsh:RS1-441, 02 engineering and technology, Matrix metalloproteinase, Article, lcsh:Pharmacy and materia medica, 03 medical and health sciences, chemistry.chemical_compound, Downregulation and upregulation, Drug Discovery, hyaluronic acid, 030304 developmental biology, ddc:615, 0303 health sciences, integumentary system, epidermal cells, Cell growth, lcsh:R, Interleukin, Epidermal cells, 021001 nanoscience & nanotechnology, cytokines, accelerated wound healing, Accelerated wound healing, Vascular endothelial growth factor, HaCaT, chemistry, Cancer research, Cytokines, Molecular Medicine, 0210 nano-technology, Wound healing

Abstract

Hyaluronic acid (HA) has been known to play an important role in wound healing process. However, the effect of molecular weight (MW) of exogenously administered HA on the wound healing process has not been fully understood. In this study, we investigated HA with different MWs on wound healing process using human epidermal keratinocytes and dermal fibroblasts. Cell proliferation and migration ability were assessed by water soluble tetrazolium (WST) assay and wound scratch assay. We examined the effect of HA addition in a full-thickness wound model in mice and the gene expression related to wound healing. Proliferation and migration of HaCaT cells increased with the increase of MW and concentration of HA. Interleukin (IL-1β), IL-8 and vascular endothelial growth factor (VEGF) as well as matrix metalloproteinase (MMP)-9 and MMP-13 were significantly upregulated by high molecular weight (HMW) HA in keratinocytes. Together with VEGF upregulation and the observed promotion of HaCaT migration, HA with the MW of 2290 kDa may hold potential to improve re-epithelialization, a critical obstacle to heal chronic wounds.

Published

2021

22. Biologically Active TNIIIA2 Region in Tenascin-C Molecule: A Major Contributor to Elicit Aggressive Malignant Phenotypes From Tumors/Tumor Stroma

Author

Fumio Fukai, Motomichi Fujita, and Takuya Iyoda

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, Immunology, Tenascin, Antineoplastic Agents, TNIIIA2, Review, macrophage, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Cell Movement, Tumor-Associated Macrophages, Cell Adhesion, Tumor Microenvironment, Immunology and Allergy, Animals, Humans, Neoplasm Invasiveness, Protein Interaction Domains and Motifs, Cell adhesion, Cell Proliferation, biology, Brain Neoplasms, Alternative splicing, Tenascin C, glioblastoma, β1-integrin, PDGF, Fibronectins, Fibronectin, 030104 developmental biology, Phenotype, Tumor progression, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, biology.protein, Cancer research, solid tumor, tenascin-C, Stromal Cells, lcsh:RC581-607, Platelet-derived growth factor receptor, Signal Transduction

Abstract

Tenascin (TN)-C is highly expressed specifically in the lesions of inflammation-related diseases, including tumors. The expression level of TN-C in tumors and the tumor stroma is positively correlated with poor prognosis. However, no drugs targeting TN-C are currently clinically available, partly because the role of TN-C in tumor progression remains controversial. TN-C harbors an alternative splicing site in its fibronectin type III repeat domain, and its splicing variants including the type III-A2 domain are frequently detected in malignant tumors. We previously identified a biologically active region termed TNIIIA2 in the fibronectin type III-A2 domain of TN-C molecule and showed that this region is involved in promoting firm and persistent cell adhesion to fibronectin. In the past decade, through the exposure of various cell lines to peptides containing the TNIIIA2 region, we have published reports demonstrating the ability of the TNIIIA2 region to modulate distinct cellular activities, including survival/growth, migration, and invasion. Recently, we reported that the signals derived from TNIIIA2-mediated β1 integrin activation might play a crucial role for inducing malignant behavior of glioblastoma (GBM). GBM cells exposed to the TNIIIA2 region showed not only exacerbation of PDGF-dependent proliferation, but also acceleration of disseminative migration. On the other hand, we also found that the pro-inflammatory phenotypic changes were promoted when macrophages are stimulated with TNIIIA2 region in relatively low concentration and resulting MMP-9 upregulation is needed to release of the TNIIIA2 region from TN-C molecule. With the contribution of TNIIIA2-stimulated macrophages, the positive feedback spiral loop, which consists of the expression of TN-C, PDGF, and β1 integrin, and TNIIIA2 release, seemed to be activated in GBM with aggressive malignancy. Actually, the growth of transplanted GBM grafts in mice was significantly suppressedviathe attenuation of β1 integrin activation. In this review, we thus introduce that the TNIIIA2 region has a significant impact on malignant progression of tumors by regulating cell adhesion. Importantly, it has been demonstrated that the TNIIIA2 region exerts unique biological functions through the extremely strong activation of β1-integrins and their long-lasting duration. These findings prompt us to develop new therapeutic agents targeting the TNIIIA2 region.

Published

2020

23. Exposure of the cryptic de-adhesive site FNIII14 in fibronectin molecule and its binding to membrane-type eEF1A induce migration and invasion of cancer cells via β1-integrin inactivation

Author

Keisuke, Itagaki, Manabu, Sasada, Satoru, Miyazaki, Takuya, Iyoda, Takahiro, Imaizumi, Makoto, Haga, Akira, Kuga, Hiroki, Inomata, Yosuke, Kondo, Satoshi, Osada, Hiroaki, Kodama, Yoshikazu, Higami, and Fumio, Fukai

Subjects

Original Article

Abstract

Cell migration is a highly coordinated process that involves not only integrin-mediated adhesion but also de-adhesion. We previously found that a cryptic de-adhesive site within fibronectin molecule, termed FNIII14, weakens cell adhesion to the extracellular matrix by inactivating β1-integrins. Surprisingly, eukaryotic translation elongation factor-1A (eEF1A), an essential factor during protein biosynthesis, was identified as a membrane receptor that mediates the de-adhesive effect of FNIII14. Here, we demonstrate that FNIII14-mediated de-adhesion causes enhanced migration and invasion in two types of highly invasive/metastatic cancer cells, resulting in the initiation of metastasis. Both in vitro migration and invasion of highly invasive human melanoma cell line, Mum2B, were inhibited by a matrix metalloproteinase (MMP)-2/9 inhibitor or a function-blocking antibody against FNIII14 (anti-FNIII14 Ab), suggesting that MMP-mediated exposure of the cryptic de-adhesive site FNIII14 was responsible for Mum2B cell migration and invasion. The MMP-induced FNIII14 exposure was also shown to be functional in the migration and invasion of highly metastatic mouse breast cancer cell line 4T1. Overexpression and knockdown experiments of eEF1A in Mum2B cells revealed that the migration and invasion were dependent on the membrane levels of eEF1A. In vivo experiments using tumor xenograft mouse models derived from Mum2B and 4T1 cell lines showed that the anti-FNIII14 Ab has a significant anti-metastatic effect. Thus, these results provide novel insights into the regulation of cancer cell migration and invasion and suggest promising targets for anti-metastasis strategies.

Published

2020

24. Development of new formulations for wound-healing

Author

Takeshi, Hanawa, YAYOI, KAWANO, RYOICHI, MORI, HIDETAKE, TORIGOE, and TAKUYA, IYODA

Subjects

ハイドロゲル, nanoparticle, 創傷治癒, Wound healing, hydrogel, ナノ粒子

Published

2019

25. Autocrine Production of PDGF Stimulated by the Tenascin-C-Derived Peptide TNIIIA2 Induces Hyper-Proliferation in Glioblastoma Cells

Author

Tatsuya Fujisawa, Chikako Kudo, Takashi Yamamoto, Motomichi Fujita, Hiroaki Kodama, Takuya Iyoda, Fumio Fukai, Reo Nagai, and Manabu Sasada

Subjects

Male, 0301 basic medicine, medicine.medical_treatment, Matrix (biology), lcsh:Chemistry, Mice, 0302 clinical medicine, Cell Movement, Receptors, Platelet-Derived Growth Factor, lcsh:QH301-705.5, Cells, Cultured, Spectroscopy, Neurons, Platelet-Derived Growth Factor, biology, Brain Neoplasms, Chemistry, Tenascin C, Tenascin, General Medicine, PDGF, musculoskeletal system, Computer Science Applications, Autocrine Communication, 030220 oncology & carcinogenesis, embryonic structures, Matrix Metalloproteinase 2, tenascin-C, Platelet-derived growth factor receptor, endocrine system, animal structures, Article, Catalysis, Inorganic Chemistry, 03 medical and health sciences, Downregulation and upregulation, Cell Line, Tumor, medicine, Animals, Humans, Rats, Wistar, Physical and Theoretical Chemistry, Cell adhesion, Autocrine signalling, Molecular Biology, Cell Proliferation, Growth factor, Organic Chemistry, glioblastoma, β1-integrin, Fibroblasts, Peptide Fragments, In vitro, Rats, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, Cancer research, biology.protein, PDGF receptor

Abstract

Expression level of tenascin-C is closely correlated to poor prognosis in glioblastoma patients, while the substantial role of tenascin-C responsible for aggressive progression in glioblastoma cells has not been clarified. We previously found that peptide TNIIIA2, which is derived from the tumor-associated tenascin-C variants, has the ability to promote cell adhesion by activating &beta, 1-integrins. Our recent study demonstrated that potentiated activation of integrin &alpha, 5&beta, 1 by TNIIIA2 causes not only a dysregulated proliferation in a platelet-derived growth factor (PDGF)-dependent manner, but also disseminative migration in glioblastoma cells. Here, we show that TNIIIA2 enhances the proliferation in glioblastoma cells expressing PDGF-receptor&beta, even without exogenous PDGF. Mechanistically, TNIIIA2 induced upregulated expression of PDGF, which in turn stimulated the expression of tenascin-C, a parental molecule of TNIIIA2. Moreover, in glioblastoma cells and rat brain-derived fibroblasts, tenascin-C upregulated matrix metalloproteinase-2, which has the potential to release TNIIIA2 from tenascin-C. Thus, it was shown that autocrine production of PDGF triggered by TNIIIA2 functions to continuously generate a functional amount of PDGF through a positive spiral loop, which might contribute to hyper-proliferation in glioblastoma cells. TNIIIA2 also enhanced in vitro disseminative migration of glioblastoma cells via the PKC&alpha, signaling. Collectively, the tenascin-C/TNIIIA2 could be a potential therapeutic target for glioblastoma.

Published

2019

26. Combining peptide TNIIIA2 with all

Author

Kazuki, Otsuka, Manabu, Sasada, Takuya, Iyoda, Yusuke, Nohara, Shunsuke, Sakai, Tatsufumi, Asayama, Yusuke, Suenaga, Sana, Yokoi, Yoshikazu, Higami, Hiroaki, Kodama, and Fumio, Fukai

Subjects

Erratum

Abstract

Neuroblastoma is one of the common solid tumors of childhood. Nearly half of neuroblastoma patients are classified into the high-risk group, and their 5-year event-free survival (EFS) rates remain unsatisfactory in the range of 30-40%. High-risk neuroblastoma is characterized by amplification of the MYCN gene and excessive expression of its protein product, N-Myc. Because N-Myc is a transcription factor for various pro-proliferative proteins, the excessive expression causes aberrant or blocked neuronal differentiation during development of sympathetic nervous system, which is a central aspect of neuroblastoma genesis. The current main treatment for high-risk neuroblastoma is intensive chemotherapy using anti-cancer drugs that induce apoptosis in tumor cells, but intensive chemotherapy has another serious risk of long-lasting side effects, so-called "late effects", that occur many years after chemotherapy has ended. As a solution for such situation, differentiation therapy has been expected as a mild chemotherapy with a low risk of late effects, and an application of retinoic acid (RA) and its derivatives as treatment for high-risk neuroblastoma has long been attempted. However, the clinical outcome has not been sufficient with the use of retinoids, including all

Published

2018

27. Control of cell adhesion and proliferation utilizing polysaccharide composite film scaffolds

Author

Atsushi Kakimoto, Mineo Hashizume, Yuna Tsuji, Yuichi Nikaido, Kazutoshi Iijima, Izumi Kuriki, Rie Ninomiya, Fumio Fukai, and Takuya Iyoda

Subjects

0301 basic medicine, Integrins, Alginates, Becaplermin, Biocompatible Materials, Cell Count, 02 engineering and technology, Polysaccharide, Chitosan, 03 medical and health sciences, chemistry.chemical_compound, Mice, Colloid and Surface Chemistry, Glucuronic Acid, Polymer chemistry, Hyaluronic acid, Cell Adhesion, Animals, Physical and Theoretical Chemistry, Hyaluronic Acid, Cell adhesion, Alginic acid, Cell Proliferation, chemistry.chemical_classification, biology, Tissue Scaffolds, Hexuronic Acids, Chondroitin Sulfates, Surfaces and Interfaces, General Medicine, Adhesion, Proto-Oncogene Proteins c-sis, 021001 nanoscience & nanotechnology, Fibronectins, Fibronectin, 030104 developmental biology, chemistry, biology.protein, Biophysics, NIH 3T3 Cells, Surface modification, 0210 nano-technology, Peptides, Biotechnology

Abstract

We have developed polysaccharide composite films made of anionic polysaccharides and chitosan (CHI) by utilizing hot press techniques. In order to demonstrate the versatility of these films as cell scaffolds, the present study investigated the adhesion and proliferation of fibroblasts on composite films prepared by using various kinds of anionic polysaccharides and that were modified with proteins. Cells were spread on heparin/CHI and alginic acid/CHI films and grew well, whereas those on chondroitin sulfate C (CS)/CHI and hyaluronic acid/CHI films were round in shape. The differences in adhesion and proliferation behaviors of cells could be explained by the differences in the biochemical function of the anionic polysaccharides and the physical properties of the films such as morphology, storage modulus, ζ-potentials, and swelling ratios. Among them, the number of cells on CS/CHI films remained almost unchanged. The mechanisms underlying growth suppression on CS/CHI films were investigated by using an integrin stimulator, the TNIIIA2 peptide, and platelet-derived growth factor-B. It was indicated that the growth suppression was due to the lack of fibronectin-integrin growth signaling. The surface modification of CS/CHI films with fibronectin promoted the adhesion and proliferation of cells. These results show that the chemical and physical properties of the polysaccharide composite films, which resulted from the chemical species of anionic polysaccharides or surface modifications of the films, can modulate cell adhesion and proliferation properties thereon.

Published

2017

28. The Promoting Effect of the Extracellular Matrix Peptide TNIIIA2 Derived from Tenascin-C in Colon Cancer Cell Infiltration

Author

Sadahiro Kamiya, Yuka Ito, Hideo Suzuki, Takuya Iyoda, Kazuma Ishibashi, Hikaru Watanabe, Akinori Yanaka, Fumio Fukai, Manabu Sasada, and Yuko Okada

Subjects

0301 basic medicine, Pathology, Lung Neoplasms, Colorectal cancer, TNIIIA2, Matrix metalloproteinase, Metastasis, Extracellular matrix, lcsh:Chemistry, Cell Movement, lcsh:QH301-705.5, Spectroscopy, Extracellular Matrix Proteins, Mice, Inbred BALB C, biology, Reverse Transcriptase Polymerase Chain Reaction, Chemistry, Tenascin C, tenascin C, Tenascin, General Medicine, musculoskeletal system, Computer Science Applications, Gene Expression Regulation, Neoplastic, colon cancer, Colonic Neoplasms, Female, medicine.symptom, medicine.medical_specialty, matrix metalloproteinase, extracellular matrix, Inflammation, Matrix Metalloproteinase Inhibitors, Gene Expression Regulation, Enzymologic, Article, Catalysis, Inorganic Chemistry, 03 medical and health sciences, In vivo, Cell Line, Tumor, medicine, Animals, Humans, Amino Acid Sequence, Physical and Theoretical Chemistry, Molecular Biology, Dose-Response Relationship, Drug, Organic Chemistry, Neoplasms, Experimental, medicine.disease, Matrix Metalloproteinases, In vitro, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, biology.protein, Cancer research, Peptides

Abstract

The extracellular matrix (ECM) molecule tenascin C (TNC) is known to be highly expressed under various pathological conditions such as inflammation and cancer. It has been reported that the expression of TNC is correlated with the malignant potential of cancer. In our laboratory, it was found that the peptide derived from the alternative splicing domain A2 in TNC, termed TNIIIA2, has been shown to influence a variety of cellular processes, such as survival, proliferation, migration, and differentiation. In this study, we investigated the effect of TNC/TNIIIA2 on the invasion and metastasis of colon cancer cells, Colon26-M3.1, or PMF-Ko14, using an in vitro and in vivo experimental system. The degree of cell invasion was increased by the addition of TNC and TNIIIA2 in a dose-dependent manner. The invasion by TNC and TNIIIA2 were suppressed by an MMP inhibitor or TNIIIA2-blocking antibody. In an in vivo experiment, pulmonary metastasis was promoted conspicuously by the addition of TNIIIA2. In this study, we found that colon cancer cell invasion and metastasis was accelerated by TNC/TNIIIA2 via MMP induction. This result suggests the possibility of a new strategy targeting TNC/TNIIIA2 for colon cancer. View Full-Text

Published

2017

29. Tenascin-C-derived Peptide TNIIIA2 Highly Enhances Cell Survival and Platelet-derived Growth Factor (PDGF)-dependent Cell Proliferation through Potentiated and Sustained Activation of Integrin α5β1

Author

Tatsuya Takai, Hirofumi Yajima, Ryo Hayashi, Motomichi Fujita, Sadahiro Kamiya, Yutaka Seki, Fumio Fukai, Takuya Matsunaga, Hiroaki Okutsu, Hiroaki Kodama, Rika Tanaka, Toshiyuki Owaki, Junichi Taira, Yohei Saito, and Takuya Iyoda

Subjects

endocrine system, animal structures, Cell Survival, Integrin, Glycobiology and Extracellular Matrices, Biology, Biochemistry, Collagen receptor, Receptor, Platelet-Derived Growth Factor beta, Mice, Membrane Microdomains, Animals, Humans, Receptors, Vitronectin, Anoikis, Protein kinase A, Molecular Biology, Protein kinase B, Cell Proliferation, Platelet-Derived Growth Factor, Tenascin, Cell Biology, musculoskeletal system, Cell biology, Integrin alpha M, embryonic structures, NIH 3T3 Cells, Cancer research, biology.protein, Syndecan-4, Integrin, beta 6, K562 Cells, Peptides, Platelet-derived growth factor receptor

Abstract

Tenascin-C is an adhesion modulatory matrix protein that is highly expressed in tumors; however, its biochemical activity involved in tumorigenesis is not fully understood. On the other hand, increasing evidence indicates the importance of integrin α5β1 in cancer development. We previously demonstrated that tenascin-C harbors a functional site that can be released as a proadhesive peptide such as TNIIIA2. Peptide TNIIIA2 is capable of inducing activation of β1-integrins including α5β1 via syndecan-4. In this study the proadhesive effect of TNIIIA2 was characterized by potentiated and sustained activation of integrin α5β1. Based on this effect, TNIIIA2 rendered nontransformed fibroblasts (NIH3T3) resistant to serum deprivation-elicited anoikis through activation of the Akt/Bcl-2 pathway. Moreover, TNIIIA2 hyperstimulated PDGF-dependent proliferation of NIH3T3 by activating integrin α5β1. Tenascin-C, a parental protein of TNIIIA2, also stimulated PDGF-dependent proliferation, which was blocked by a matrix metalloproteinase-2/9 inhibitor and an anti-TNIIIA2 function-blocking antibody, suggesting proteolytic exposure of the proadhesive effect of TNIIIA2. Mechanistic analyses revealed that TNIIIA2 induced a lateral association of PDGF receptor β with the molecular complex of activated integrin α5β1 and syndecan-4 in the membrane microdomains enriched with cholesterol/caveolin-1, resulting in prolonged activation of PDGF receptor β and the subsequent Ras/mitogen-activated protein kinase pathway in a PDGF-dependent manner. Of note, TNIIIA2 induced continuous proliferation in NIH3T3 in an integrin α5β1-dependent manner even after they formed a confluent monolayer. Thus, it was proposed that tenascin-C might be involved in deregulated cell growth through potentiated and sustained activation of integrin α5β1 after exposure of the proadhesive effect of TNIIIA2.

Published

2014

30. Peptide TNIIIA2 Derived from Tenascin-C Contributes to Malignant Progression in Colitis-Associated Colorectal Cancer via β1-Integrin Activation in Fibroblasts

Author

Manabu Sasada, Yuka Ito-Fujita, Yuko Okada, Hideo Suzuki, Hiroaki Kodama, Kazuma Ishibashi, Fumio Fukai, Takuro Osawa, Takuya Iyoda, and Motomichi Fujita

Subjects

Male, 0301 basic medicine, Colorectal cancer, cancer-associated fibroblast, Peptide, Metastasis, Malignant transformation, lcsh:Chemistry, chemistry.chemical_compound, 0302 clinical medicine, colitis-associated colorectal cancer, lcsh:QH301-705.5, Spectroscopy, chemistry.chemical_classification, Mice, Inbred ICR, biology, Integrin beta1, Dextran Sulfate, Matricellular protein, Tenascin C, Tenascin, General Medicine, Colitis, musculoskeletal system, Computer Science Applications, 030220 oncology & carcinogenesis, embryonic structures, Disease Progression, tenascin-C, Colorectal Neoplasms, endocrine system, animal structures, Azoxymethane, Colonic Polyps, Article, Catalysis, Inorganic Chemistry, 03 medical and health sciences, Paracrine Communication, medicine, Animals, Humans, Physical and Theoretical Chemistry, Molecular Biology, Cell Proliferation, Organic Chemistry, β1-integrin, Epithelial Cells, AOM/DSS model, Fibroblasts, medicine.disease, Disease Models, Animal, HaCaT, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, chemistry, Culture Media, Conditioned, biology.protein, Cancer research, Caco-2 Cells, Peptides

Abstract

Inflammatory bowel diseases increase the risk of colorectal cancer and colitis-associated colorectal cancer (CAC). Tenascin-C, a matricellular protein, is highly expressed in inflammatory bowel diseases, especially colorectal cancer. However, the role of tenascin-C in the development of CAC is not yet fully understood. We previously showed that a peptide derived from tenascin-C, peptide TNIIIA2, induces potent and sustained activation of &beta, 1-integrin. Moreover, we recently reported that peptide TNIIIA2 promotes invasion and metastasis in colon cancer cells. Here, we show the pathological relevance of TNIIIA2-related functional site for the development of CAC. First, expression of the TNIIIA2-containing TNC peptides/fragments was detected in dysplastic lesions of an azoxymethane/dextran sodium sulfate (AOM/DSS) mouse model. In vitro experiments demonstrated that conditioned medium from peptide TNIIIA2-stimulated human WI-38 fibroblasts induced malignant transformation in preneoplastic epithelial HaCaT cells. Indeed, these pro-proliferative effects stimulated by peptide TNIIIA2 were abrogated by peptide FNIII14, which has the ability to inactivate &beta, 1-integrin. Importantly, peptide FNIII14 was capable of suppressing polyp formation in the AOM/DSS model. Therefore, tenascin-C-derived peptide TNIIIA2 may contribute to the formation of CAC via activation of stromal fibroblasts based on &beta, 1-integrin activation. Peptide FNIII14 could represent a potential prophylactic treatment for CAC.

Published

2019

31. Integrin-Dependent Cell Regulation and its Clinical Application

Author

Takuya Iyoda, Takuya Matsunaga, and Fumio Fukai

Published

2016

32. Coadministration of the FNIII14 Peptide Synergistically Augments the Anti-Cancer Activity of Chemotherapeutic Drugs by Activating Pro-Apoptotic Bim

Author

You-ichi Takizawa, Keisuke Itagaki, Toshiyuki Owaki, Shougo Akari, Ryo Hayashi, Hiroaki Kodama, Takuya Iyoda, Fumio Fukai, Hiroaki Orita, Jyunichi Taira, Yuya Tokita, Yumi Nagamine, Yoshitomi Nakane, Motomichi Fujita, and Kazuki Otsuka

Subjects

0301 basic medicine, Integrins, medicine.medical_treatment, Cytotoxicity, Cell, Cancer Treatment, Melanoma, Experimental, lcsh:Medicine, Apoptosis, Pharmacology, Toxicology, Pathology and Laboratory Medicine, Biochemistry, Metastasis, Mice, 0302 clinical medicine, Basic Cancer Research, Medicine and Health Sciences, Medicine, Post-Translational Modification, Neoplasm Metastasis, lcsh:Science, Mammary tumor, Mice, Inbred BALB C, Multidisciplinary, Bcl-2-Like Protein 11, Pharmaceutics, Melanoma, Drug Synergism, Primary tumor, Extracellular Matrix, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Female, Cellular Structures and Organelles, Signal Peptides, medicine.drug, Aclarubicin, Research Article, Drug Administration, Antineoplastic Agents, 03 medical and health sciences, Drug Therapy, Cell Line, Tumor, Cell Adhesion, Animals, Humans, Doxorubicin, Chemotherapy, business.industry, lcsh:R, Biology and Life Sciences, Cancers and Neoplasms, Proteins, Mammary Neoplasms, Experimental, Cell Biology, medicine.disease, Peptide Fragments, Fibronectins, 030104 developmental biology, Metastatic Tumors, Drug Resistance, Neoplasm, lcsh:Q, business

Abstract

The acquisition of drug resistance mediated by the interaction of tumor cells with the extracellular matrix (ECM), commonly referred to as cell adhesion-mediated drug resistance (CAM-DR), has been observed not only in hematopoietic tumor cells but also in solid tumor cells. We have previously demonstrated that a 22-mer peptide derived from fibronectin, FNIII14, can inhibit cell adhesion through the inactivation of β1 integrin; when coadministered with cytarabine, FNIII14 completely eradicates acute myelogenous leukemia by suppressing CAM-DR. In this study, we show that our FNIII14 peptide also enhances chemotherapy efficacy in solid tumors. Coadministration of FNIII14 synergistically enhances the cytotoxicity of doxorubicin and aclarubicin in mammary tumor and melanoma cells, respectively. The solid tumor cell chemosensitization induced by FNIII14 is dependent upon the upregulation and activation of the pro-apoptotic protein, Bim. Furthermore, the metastasis of tumor cells derived from ventrally transplanted mammary tumor grafts is suppressed by the coadministration of FNIII14 and doxorubicin. These results suggest that the coadministration of our FNIII14 peptide with chemotherapy could achieve efficient solid tumor eradication by increasing chemosensitivity and decreasing metastasis. The major causes of tumor recurrence are the existence of chemotherapy-resistant primary tumor cells and the establishment of secondary metastatic lesions. As such, coadministering FNIII14 with anti-cancer drugs could provide a promising new approach to improve the prognosis of patients with solid tumors.

Published

2016

33. Preferential involvement of Na+/Ca2+ exchanger type-1 in the brain damage caused by transient focal cerebral ischemia in mice

Author

Yusuke Gotoh, Ichiro Horie, Nobuaki Egashira, Toshio Matsuda, Kazuhide Hayakawa, Masamitsu Shimazawa, Kazuhiro Tsuruma, Hideaki Hara, Kenichi Mishima, Kyoji Horie, Michihiro Fujiwara, Takahiro Iwamoto, Issei Komuro, Takuya Iyoda, Hiroko Namimatsu, Satomi Kita, Katsunori Iwasaki, Junji Takeda, Nobutaka Morimoto, and Akemichi Baba

Subjects

Gene isoform, medicine.medical_specialty, Chemistry, Biophysics, Ischemia, Cell Biology, Brain damage, medicine.disease, Biochemistry, Endocrinology, Internal medicine, cardiovascular system, medicine, Middle cerebral artery occlusion, Cerebral infarcts, medicine.symptom, Molecular Biology, Stroke, Intracellular, Homeostasis

Abstract

The Na+/Ca2+ exchanger (NCX), an ion-transporter located in the plasma membrane of neuronal cells, contributes to intracellular Ca2+ homeostasis. Within the brain, three isoforms (NCX1, NCX2, and NCX3) are widely distributed. However, it is not clear to what extent these isoforms are involved in ischemic brain damage in mammals. We therefore used genetically altered mice and isoform-selective NCX inhibitors in a model of transient focal ischemia to investigate the role of each NCX isoform in ischemic brain damage. NCX isoform-mutant mice (NCX1+/−, NCX2+/−, and NCX3+/−) and wild-type mice were subjected to 90 min of middle cerebral artery occlusion (MCAO) followed by 24 h of reperfusion. One of three NCX inhibitors [SN-6, KB-R7943, or SEA0400 (3 or 10 mg kg−1, i.p.)] was administered to ddY mice at 30 min before more prolonged (4-h) MCAO followed by 24 h of reperfusion. After transient MCAO reperfusion, the cerebral infarcts in NCX1+/− mice, but not those in NCX2+/− or NCX3+/− mice, were significantly smaller than those in wild-type mice. SN-6 and SEA0400, which are more selective for the NCX1 isoform, significantly reduced the infarct volume at 10 mg/kg. In contrast, KB-R7943, which is more selective for NCX3, did not. These results suggest that the NCX1 isoform may act preferentially (vs. the NCX2 and NCX3 isoforms) to exacerbate the cerebral damage caused by ischemic insult in mice, and that NCX1-selective inhibitors warrant investigation as a potential therapeutic agents for stroke.

Published

2012

34. OSU-03012, a novel celecoxib derivative, induces cell swelling and shortens action potential duration in mouse ventricular cells

Author

Satomi Kita, Shintaro Yamamoto, Toshiki Yamada, Takuya Iyoda, and Takahiro Iwamoto

Subjects

Male, Cardiac function curve, Patch-Clamp Techniques, Heart Ventricles, Action Potentials, OSU-03012, Pharmacology, Biology, General Biochemistry, Genetics and Molecular Biology, Membrane Potentials, Glibenclamide, Mice, chemistry.chemical_compound, Adenosine Triphosphate, KATP Channels, Glyburide, medicine, Animals, Repolarization, Cell Size, Membrane potential, Sulfonamides, General Medicine, Hypoxia (medical), Mice, Inbred C57BL, chemistry, Celecoxib, Apoptosis, Anesthesia, Pyrazoles, medicine.symptom, medicine.drug

Abstract

OSU03012, a novel celecoxib derivative, has been shown to inhibit proliferation and induce apoptosis in numerous cancer cell lines. However, not much is known about its influence on cell volume regulation and cardiac function in the mammalian heart. We examined the effects of OSU-03012 on cell volume and action potentials in mouse ventricular cells. Video image analysis showed that cell volume increased on application of OSU-03012 in a dose-dependent manner. The action potential duration (APD) at 50% and 90% repolarization (APD(50) and APD(90) respectively) as well as the resting membrane potential (RMP) were measured in current-clamp experiments. OSU-03012 had little effect on APD(50) and RMP but induced approximately 30% shortening of APD(90). These results for cell volume and AP are similar to those in cells under ischaemia/hypoxia, and we confirmed that the shortening of APD(90) was almost completely recovered by glibenclamide, a potent inhibitor of ATP-sensitive potassium channels.We concluded that OSU-03012 may lead to cell swelling and shortening of AP via reduced ATP production in mouse ventricular cells.

Published

2010

35. Infiltrating neutrophils induce allospecific CTL in response to immunization with apoptotic cells via MCP-1 production

Author

Takuya Iyoda, Naoko Tanimoto, Yoshiko Shiratsuchi, Daisuke Kegai, Yoshiro Kobayashi, and Kisaburo Nagata

Subjects

Cytotoxicity, Immunologic, Male, Chemokine, Neutrophils, Recombinant Fusion Proteins, Phagocytosis, Immunology, Apoptosis, Inflammation, CD8-Positive T-Lymphocytes, Antibodies, Mice, Peritoneal cavity, Immune system, Cell Line, Tumor, medicine, Animals, Immunology and Allergy, Cytotoxic T cell, Chemokine CCL4, Peritoneal Cavity, Chemokine CCL2, Chemokine CCL3, biology, Cell Biology, Macrophage Inflammatory Proteins, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, CTL, medicine.anatomical_structure, Neutrophil Infiltration, biology.protein, Cancer research, Immunization, medicine.symptom, Infiltration (medical), Injections, Intraperitoneal

Abstract

Our previous studies demonstrated that i.p. injection of late apoptotic P388 cells caused phagocytosis by macrophages and transient infil- tration of neutrophils into the peritoneal cavity. As neutrophils are known to function as effectors as well as regulators in the immune response, we ex- amined the roles of infiltrating neutrophils in al- loantigen-specific CTL induction after immuniza- tion with late apoptotic P388 cells. The CTL in- duction and infiltration of CD8 T cells into the peritoneal cavity were inhibited by depletion of neutrophils by anti-Gr-1 mAb or inhibition of neu- trophil infiltration by anti-MIP-2 antibody, suggest- ing that neutrophils are involved in CD8 T cell infiltration into the peritoneal cavity. It is known that MIP-1, MIP-1, and MCP-1 are capable of attracting CD8 T cells and that they are produced by neutrophils. These chemokines were detected in the peritoneal cavity, and among them, MCP-1 production was reduced remarkably by suppres- sion of neutrophil infiltration. Moreover, infiltra- tion of CD8 T cells into the peritoneal cavity as well as CTL activity was clearly reduced by admin- istering anti-MCP-1 antibody i.p. Furthermore, the CTL induction and infiltration of CD8 T cells in neutrophil-depleted mice were restored signifi- cantly by administering recombinant murine MCP-1 into the peritoneal cavity. These results indicate that MCP-1 appears to link infiltration of neutrophils with CTL induction. J. Leukoc. Biol. 81: 000-000; 2007.

Published

2006

36. Neutrophils accelerate macrophage-mediated digestion of apoptotic cells in vivo as well as in vitro

Author

Kisaburo Nagata, Yoshiro Kobayashi, Makoto Akashi, and Takuya Iyoda

Subjects

Male, Chemokine, Pathology, medicine.medical_specialty, Neutrophils, Chemokine CXCL2, Immunology, Apoptosis, Mice, Inbred Strains, Inflammation, Thymus Gland, Biology, Neutrophil Activation, Apoptotic cell clearance, Mice, Peritoneal cavity, Phagocytosis, medicine, Animals, Immunology and Allergy, Macrophages, Chemotaxis, medicine.disease, Molecular biology, Coculture Techniques, In vitro, Chemotaxis, Leukocyte, medicine.anatomical_structure, Macrophages, Peritoneal, biology.protein, Chemokines, medicine.symptom, Infiltration (medical), Whole-Body Irradiation

Abstract

It is generally believed that the clearance of apoptotic cells does not lead to inflammation. In contrast, we previously found that injection of apoptotic cells into the peritoneal cavity induced the expression of an inflammatory chemokine, MIP-2, and infiltration of neutrophils, and that anti-MIP-2 Abs suppressed the infiltration significantly. Because our previous study showed that whole-body x-irradiation caused neutrophil infiltration into the thymus along with T cell apoptosis, we examined the role of neutrophils in apoptotic cell clearance. Neutrophil infiltration reached a peak 12 h after irradiation with 1 Gy of x-rays. Immunohistological analysis revealed that apoptotic cells disappeared dramatically from 10.5 to 12 h after x-irradiation. As neutrophils moved from an inner area of the cortex to the periphery, apoptotic cells disappeared concomitantly. Either anti-MIP-2 or anti-CXCR2 Abs suppressed neutrophil infiltration significantly, and the suppression of neutrophil infiltration by anti-MIP-2 Abs delayed the disappearance of apoptotic cells. Moreover, macrophage-mediated digestion of apoptotic thymocytes was accelerated in vitro on coculturing with neutrophils, even if neutrophils were separated from macrophages. These results suggest that neutrophils are recruited to the thymus mainly by MIP-2 after whole-body x-irradiation and that such neutrophils may not induce inflammation but rather accelerate complete digestion of apoptotic cells by macrophages.

Published

2005

37. Involvement of MIP-2 and CXCR2 in neutrophil infiltration following injection of late apoptotic cells into the peritoneal cavity

Author

Takuya Iyoda and Yoshiro Kobayashi

Subjects

Male, Cancer Research, Cell Transplantation, Neutrophils, T-Lymphocytes, Chemokine CXCL2, Clinical Biochemistry, Pharmaceutical Science, Apoptosis, Receptors, Interleukin-8B, Leukocyte Count, Mice, Antibody Specificity, CXC chemokine receptors, Peritoneal Cavity, Etoposide, medicine.diagnostic_test, biology, Flow Cytometry, Blot, medicine.anatomical_structure, Neutrophil Infiltration, Thioglycolates, Female, Rabbits, Chemokines, Antibody, Infiltration (medical), Injections, Intraperitoneal, Recombinant Fusion Proteins, Phagocytosis, Blotting, Western, Peritonitis, Antibodies, Cell Line, Flow cytometry, Peritoneal cavity, Cell Line, Tumor, medicine, Animals, Humans, Pharmacology, Macrophages, Biochemistry (medical), Cell Biology, medicine.disease, Molecular biology, Mice, Inbred C57BL, biology.protein, Interleukin-2, Immunization

Abstract

Apoptotic cells are cleared by phagocytes, such as macrophages, as soon as they appear in vivo. If apoptosis occurs acutely, however, macrophages may be outnumbered by apoptotic cells, which causes late apoptosis. We previously showed that injection of late apoptotic cells into the peritoneal cavity led to transient infiltration of neutrophils. In this study, we examined the involvement of MIP-2 and CXCR2 in the neutrophil infiltration. We first produced a recombinant MIP-2 protein, and a fusion protein between CXCR2 and GST in E. coli, and then generated anti-MIP-2 antibodies and anti-CXCR2 antibodies in rabbits. We then confirmed their specificity by Western blotting analysis and flow cytometry. Injection of late apoptotic cells, such as P388 cells treated with etoposide for 24 hours and CTLL-2 cells cultured in IL-2-free medium for 28 hours, induced neutrophil infiltration into the peritoneal cavity, as expected. The antibodies, but not control antibodies against GST, suppressed the neutrophil infiltration to the level caused by injection of normal (viable) cells, suggesting that MIP-2 and CXCR2 are mainly involved in the neutrophil infiltration caused by late apoptotic cells.

Published

2004

38. A novel mechanism underlying the basic defensive response of macrophages against Mycobacterium infection

Author

Yoshinobu Fukatsu, Takuya Matsunaga, Noriko Shimokawa, Tomokazu Shimada, Tatsuya Fujisawa, Takuya Iyoda, Muneaki Takada, Norio Doi, Fumio Fukai, Shunsuke Kumokoshi, Kimiko Makino, and Hiroshi Terada

Subjects

MAPK/ERK pathway, Programmed cell death, Immunology, Apoptosis, Biology, Mice, Cell surface receptor, In Situ Nick-End Labeling, Immunology and Allergy, Macrophage, Animals, Immunoprecipitation, RNA, Small Interfering, Mycobacterium Infections, Microscopy, Confocal, Macrophages, Mycobacterium tuberculosis, Flow Cytometry, Toll-Like Receptor 2, Cell biology, TLR2, CD18 Antigens, Phosphorylation, Intracellular, Signal Transduction

Abstract

Following inhalation of Mycobacterium tuberculosis, including bacillus Calmette–Guérin (BCG), pathogens enter and grow inside macrophages by taking advantage of their phagocytic mechanisms. Macrophages often fail to eliminate intracellular M. tuberculosis, leading to the induction of host macrophage death. Despite accumulating evidence, the molecular mechanisms underlying M. tuberculosis infection–induced cell death remain controversial. In this study, we show the involvement of two distinct pathways triggered by TLR2 and β2 integrin in BCG infection–induced macrophage apoptosis. First, BCG infection induced activation of ERK1/2, which in turn caused phosphorylation/activation of the proapoptotic protein Bim in mouse macrophage-like Raw 264.7 cells. BCG-infected Raw cells treated with U0126, an MEK/ERK inhibitor, led to the suppression of Bim phosphorylation alongside a remarkable increase in the number of viable macrophages. Small interfering RNA–mediated knockdown of Bim rescued the macrophages from the apoptotic cell death induced by BCG infection. Stimulation with Pam3CSK, a TLR2 agonist, induced macrophage apoptosis with a concomitant increase in the phosphorylation/activation of MEK/ERK and Bim. These observations indicate the important role of the TLR2/MEK/ERK/Bim pathway in BCG infection–induced macrophage apoptosis. Second, we used the β2 integrin agonists C3bi and fibronectin to show that the β2 integrin–derived signal was involved in BCG infection–induced apoptosis, independent of MEK/ERK activation. Interestingly, latex beads coated with Pam3CSK and C3bi were able to induce apoptosis in macrophages to the same extent and specificity as that induced by BCG. Taken together, two distinct pattern-recognition membrane receptors, TLR2 and β2 integrin, acted as triggers in BCG infection–induced macrophage apoptosis, in which MEK/ERK activation played a crucial role following the engagement of TLR2.

Published

2014

39. Pretreatment of donor islets with the Na(+) /Ca(2+) exchanger inhibitor improves the efficiency of islet transplantation

Author

Hiroshi Watarai, Keiko Omori, A. Baba, Masamichi Ohkura, Masaru Taniguchi, Yohichi Yasunami, Takahiro Iwamoto, Satomi Kita, Hitomi Nishinakamura, Junichi Nakai, Shohta Kodama, K. Okamoto, Toshio Matsuda, D. Kojima, J. Ono, Takuya Iyoda, Takeshi Itoh, and Toshiyuki Mera

Subjects

Graft Rejection, Male, endocrine system, endocrine system diseases, Islets of Langerhans Transplantation, Mice, SCID, HMGB1, Sodium-Calcium Exchanger, Diabetes Mellitus, Experimental, Islets of Langerhans, Mice, Mice, Inbred NOD, Immunology and Allergy, Medicine, Animals, Humans, Pharmacology (medical), HMGB1 Protein, Hypoxia, Cell damage, Transplantation, geography, Innate immune system, geography.geographical_feature_category, Aniline Compounds, biology, Sodium-calcium exchanger, business.industry, Phenyl Ethers, Natural killer T cell, Islet, medicine.disease, Flow Cytometry, Mice, Inbred C57BL, surgical procedures, operative, Diabetes Mellitus, Type 1, Immunology, Cancer research, biology.protein, Pancreatic islet transplantation, business

Abstract

Pancreatic islet transplantation is an attractive therapy for the treatment of insulin-dependent diabetes mellitus. However, the low efficiency of this procedure necessitating sequential transplantations of islets with the use of 2-3 donors for a single recipient, mainly due to the early loss of transplanted islets, hampers its clinical application. Previously, we have shown in mice that a large amount of HMGB1 is released from islets soon after their transplantation and that this triggers innate immune rejection with activation of DC, NKT cells and neutrophils to produce IFN-γ, ultimately leading to the early loss of transplanted islets. Thus, HMGB1 release plays an initial pivotal role in this process; however, its mechanism remains unclear. Here we demonstrate that release of HMGB1 from transplanted islets is due to hypoxic damage resulting from Ca(2+) influx into β cells through the Na(+) /Ca(2+) exchanger (NCX). Moreover, the hypoxia-induced β cell damage was prevented by pretreatment with an NCX-specific inhibitor prior to transplantation, resulting in protection and long-term survival of transplanted mouse and human islets when grafted into mice. These findings suggest a novel strategy with potentially great impact to improve the efficiency of islet transplantation in clinical settings by targeting donor islets rather than recipients.

Published

2013

40. Preferential involvement of Na⁺/Ca²⁺ exchanger type-1 in the brain damage caused by transient focal cerebral ischemia in mice

Author

Nobutaka, Morimoto, Satomi, Kita, Masamitsu, Shimazawa, Hiroko, Namimatsu, Kazuhiro, Tsuruma, Kazuhide, Hayakawa, Kenichi, Mishima, Nobuaki, Egashira, Takuya, Iyoda, Ichiro, Horie, Yusuke, Gotoh, Katsunori, Iwasaki, Michihiro, Fujiwara, Toshio, Matsuda, Akemichi, Baba, Issei, Komuro, Kyoji, Horie, Junji, Takeda, Takahiro, Iwamoto, and Hideaki, Hara

Subjects

Brain Infarction, Aniline Compounds, Phenyl Ethers, Thiourea, Apoptosis, Infarction, Middle Cerebral Artery, Mice, Mutant Strains, Sodium-Calcium Exchanger, Brain Ischemia, Mice, Inbred C57BL, Mice, Benzyl Compounds, Animals, Thiazolidines

Abstract

The Na(+)/Ca(2+) exchanger (NCX), an ion-transporter located in the plasma membrane of neuronal cells, contributes to intracellular Ca(2+) homeostasis. Within the brain, three isoforms (NCX1, NCX2, and NCX3) are widely distributed. However, it is not clear to what extent these isoforms are involved in ischemic brain damage in mammals. We therefore used genetically altered mice and isoform-selective NCX inhibitors in a model of transient focal ischemia to investigate the role of each NCX isoform in ischemic brain damage. NCX isoform-mutant mice (NCX1(+/-), NCX2(+/-), and NCX3(+/-)) and wild-type mice were subjected to 90min of middle cerebral artery occlusion (MCAO) followed by 24h of reperfusion. One of three NCX inhibitors [SN-6, KB-R7943, or SEA0400 (3 or 10mgkg(-1), i.p.)] was administered to ddY mice at 30min before more prolonged (4-h) MCAO followed by 24h of reperfusion. After transient MCAO reperfusion, the cerebral infarcts in NCX1(+/-) mice, but not those in NCX2(+/-) or NCX3(+/-) mice, were significantly smaller than those in wild-type mice. SN-6 and SEA0400, which are more selective for the NCX1 isoform, significantly reduced the infarct volume at 10mg/kg. In contrast, KB-R7943, which is more selective for NCX3, did not. These results suggest that the NCX1 isoform may act preferentially (vs. the NCX2 and NCX3 isoforms) to exacerbate the cerebral damage caused by ischemic insult in mice, and that NCX1-selective inhibitors warrant investigation as a potential therapeutic agents for stroke.

Published

2012

41. The cell adhesion and proliferation activities of a peptide derived from human tenascin-C are dependent on two Ile residues

Author

Ryo Hayashi, Yohei Saito, Hiroaki Kodama, Satoshi Osada, Takuya Iyoda, Fumio Fukai, and Shogo Miura

Subjects

Clinical Biochemistry, Pharmaceutical Science, Peptide, Biochemistry, Extracellular matrix, Structure-Activity Relationship, Drug Discovery, Cell Adhesion, Structure–activity relationship, Humans, Isoleucine, Cell adhesion, Molecular Biology, Basic amino acids, Cell Proliferation, chemistry.chemical_classification, biology, Chemistry, Organic Chemistry, Tenascin C, Tenascin, Molecular biology, biology.protein, Molecular Medicine, Peptides

Abstract

A tenascin-C derived peptide (TNIIIA2 peptide, 1) stimulated β1 integrin-mediated cell adhesion via binding to syndecan-4. Ala-substituted peptides were synthesized to understand the structure-activity relationship. Peptides in which basic amino acids were substituted showed reduced cell adhesion activity, but their proliferation activities were similar to or higher than those mediated by peptide 1. In contrast, peptides in which the Ile residues of peptide 1 were replaced were inactive, indicating that the Ile residues are critical for the peptide's activity. CD analysis suggested that the Ile residues are necessary for the formation of a specific conformation required for binding to syndecan-4.

Published

2012

42. Lysophosphatidic Acid Induces Early Growth Response-1 (Egr-1) Protein Expression via Protein Kinase Cδ-regulated Extracellular Signal-regulated Kinase (ERK) and c-Jun N-terminal Kinase (JNK) Activation in Vascular Smooth Muscle Cells*

Author

Mei-Zhen Cui, Xuemin Xu, Takuya Iyoda, Fuqiang Zhang, Carsten Schmitz-Peiffer, Longsheng Sun, and Feng Hao

Subjects

MAPK/ERK pathway, Vascular smooth muscle, MAP Kinase Signaling System, p38 mitogen-activated protein kinases, Myocytes, Smooth Muscle, Gene Expression, Biochemistry, p38 Mitogen-Activated Protein Kinases, Muscle, Smooth, Vascular, chemistry.chemical_compound, Lysophosphatidic acid, Animals, Mitogen-Activated Protein Kinase 9, Mitogen-Activated Protein Kinase 8, RNA, Small Interfering, Receptors, Lysophosphatidic Acid, Protein kinase A, Molecular Biology, Aorta, Cells, Cultured, Early Growth Response Protein 1, Regulation of gene expression, c-jun, Cell Biology, Molecular biology, Cell biology, Rats, body regions, Isoenzymes, Protein Kinase C-delta, chemistry, lipids (amino acids, peptides, and proteins), Signal transduction, biological phenomena, cell phenomena, and immunity, Lysophospholipids, hormones, hormone substitutes, and hormone antagonists, Signal Transduction

Abstract

Lysophosphatidic acid (LPA) modulates vascular cell function in vitro and in vivo via regulating the expression of specific genes. Previously, we reported that a transcriptional mechanism controls LPA-induced expression of Egr-1 in vascular smooth muscle cells. Egr-1 is a master transcription factor mediating the expression of various genes that have been implied to modulate a broad spectrum of vascular pathologies. In this study, we determined the essential intracellular signaling pathway leading to LPA-induced Egr-1 expression. Our data demonstrate that activation of ERK1/2 and JNK, but not p38 MAPK, is required for LPA-induced Egr-1 expression in smooth muscle cells. We provide the first evidence that MEK-mediated JNK activation leads to LPA-induced gene expression. JNK2 is required for Egr-1 induction. Examining the upstream kinases that mediate ERK and JNK activation, leading to Egr-1 expression, we found that LPA-induced activation of MAPKs and expression of Egr-1 are dependent on PKC activation. We observed that LPA rapidly activates PKCδ and PKCθ. Overexpression of dominant-negative PKCδ, but not dominant-negative PKCθ, diminished activation of ERK and JNK and blocked LPA-induced expression of Egr-1 mRNA and protein. We also evaluated LPA receptor involvement. Our data reveal an intracellular regulatory mechanism: LPA induction of Egr-1 expression is via LPA cognate receptor (LPA receptor 1)-dependent and PKCδ-mediated ERK and JNK activation. This study provides the first evidence that PKCδ mediates ERK and JNK activation in the LPA signaling pathway and that this pathway is required for LPA-induced gene regulation as evidenced by Egr-1 expression.

Published

2012

43. Eukaryotic translation elongation factor 1A induces anoikis by triggering cell detachment

Author

Takuya Iyoda, Ryota Iwakiri, Toshiyuki Owaki, Toshihiko Naito, Shintaro Iwashita, Sadahiro Kamiya, Hirofumi Yajima, Yohei Saito, Shougo Miura, Shin-Ichiro Ejiri, Fumio Fukai, Keisuke Itagaki, and Makoto Haga

Subjects

Cell Survival, Cell, Molecular Sequence Data, Eukaryotic Initiation Factor-1, Glycobiology and Extracellular Matrices, Matrix metalloproteinase, Biochemistry, Culture Media, Serum-Free, Cell Line, Mice, Eukaryotic translation, Peptide Elongation Factor 1, Cell surface receptor, hemic and lymphatic diseases, Cell Line, Tumor, medicine, Cell Adhesion, Animals, Humans, Anoikis, Amino Acid Sequence, Molecular Biology, neoplasms, Tissue homeostasis, Binding Sites, Microscopy, Confocal, biology, Cell Membrane, Cell Biology, Cell biology, Extracellular Matrix, Fibronectins, Fibronectin, medicine.anatomical_structure, Apoptosis, biology.protein, NIH 3T3 Cells, Electrophoresis, Polyacrylamide Gel, RNA Interference, K562 Cells

Abstract

Anoikis, apoptosis because of loss of cell anchorage, is crucial for tissue homeostasis. Fibronectin not only provides a scaffold for cell anchorage but also harbors a cryptic antiadhesive site capable of inducing β1-integrin inactivation. In this study, this cryptic antiadhesive site is implicated in spontaneous induction of anoikis. Nontransformed fibroblasts (NIH3T3) adhering to a fibronectin substratum underwent anoikis during serum starvation culture. This anoikis was caused by proteolytic exposure of the cryptic antiadhesive site in fibronectin by matrix metalloproteinase. Eukaryotic elongation factor 1A (eEF1A) was identified as a membrane receptor for the exposed antiadhesive site. Serum starvation raised the membrane residence of eEF1A, and siRNA-based disruption of this increase rendered cells anoikis-resistant. By contrast, cells became more susceptible to anoikis in parallel with increased membrane residence of eEF1A by enforced expression. These results demonstrate that eEF1A acts as a membrane receptor for the cryptic antiadhesive site of fibronectin, which contributes to cell regulation, including anoikis, through negative regulation of cell anchorage.

Published

2012

44. Modulation of Tumor Cell Survival, Proliferation, and Differentiation by the Peptide Derived from Tenascin-C: Implication of β1-Integrin Activation

Author

Fumio Fukai and Takuya Iyoda

Subjects

biology, Cell growth, business.industry, lcsh:Cytology, Tenascin C, Tenascin, Context (language use), Review Article, Cell Biology, Cell biology, Extracellular matrix, Immunology, biology.protein, Medicine, lcsh:QH573-671, Cell adhesion, business, Homeostasis, Function (biology)

Abstract

Cell adhesion to extracellular matrix (ECM) participates in various biological processes, such as cell survival, proliferation, differentiation, and migration. Since these processes are essential for keeping homeostasis, aberration of these processes leads to a variety of diseases including cancer. Previously, we found that a peptide derived from tenascin- (TN-) C, termed TNIIIA2, stimulates cell adhesion to ECM through activation ofβ1-integrin. It has been shown that TNIIIA2 can modulate cell proliferation and differentiation. Interestingly, TNIIIA2 could not only enhance cell proliferation but also induce apoptotic cell death, depending on cellular context. In this review, we show the function of the peptide TNIIIA2 in cell survival, proliferation, and differentiation and refer to the possibility of new strategy for tumor suppression by regulating cell adhesion status using the ECM-derived functional peptides.

Published

2012

45. Caveolin-3 regulates the Volume-Regulated Anion Channel in Mouse Ventricular Cells

Author

Toshiki Yamada, Takahiro Iwamoto, Satomi Kita, Takuya Iyoda, and Shintaro Yamamoto

Subjects

Chemistry, Biophysics, Cell biology, Caveolin 3, chemistry.chemical_compound, Biochemistry, Caveolae, Knockout mouse, cardiovascular system, Extracellular, Tonicity, Phosphatidylinositol, Signal transduction, Intracellular

Abstract

Caveolae are small invaginated microdomains located with a variety of signal transduction molecules on the plasma membrane. Recent reports showed that the knockout mice of a muscle-specific protein caveolin-3 (Cav-3 KO), a principal component of the caveolae in heart, displayed an enlargement of ventricular cells. Volume-regulated outwardly rectifying anion channel (VRAC) is activated by membrane stretch, and play a significant role in cell volume regulation in cardiac cells. However, it is unknown the properties of VRAC in the enlarged cardiac cells from Cav-3 KO mice. In this study, we examined that VRAC current and the cell volume regulation in freshly isolated single ventricular cells from Cav-3 KO mice (Hagiwara et al. 2000). Whole-cell current recording showed that the density of VRAC current induced by extracellular hypotonic solution (HYPO) is markedly reduced in the cells from Cav-3 KO mice, compared to that from wild-type (WT) mice. Video-image analysis revealed that the degree of HYPO-induced cell swelling in Cav-3 KO mice is significantly bigger than that in WT mice, and the regulatory volume decrease, which was seen in WT cells after osmotic swelling, is almost lost in cells from Cav-3 KO mice. This result is in parallel with the VRAC inhibition. In contrast, acidic extracellular pH-activated chloride current and extracellular UTP-activated CFTR current were affected less by the deficiency of caveoline-3. The attenuated VRAC current was restored by intracellular application of a VRAC modulator, phosphatidylinositol 3,4,5-trisphosphate (PIP3). These findings suggested that the attenuation of cardiac VRAC current is due to the PIP3 depletion in Cav-3 KO mice.

Published

2011

46. Cardiac-Specific Overexpression of NCX1.1-Xip Mutant Causes Dilated Cardiomyopathy in Mice

Author

Yuji Arai, Satomi Kita, Satomi Adachi-Akahane, Haruaki Nakaya, Sachio Morimoto, Takuya Iyoda, and Takahiro Iwamoto

Subjects

Genetically modified mouse, Cardiac function curve, Pathology, medicine.medical_specialty, Heart disease, Diastole, Hypertrophic cardiomyopathy, Biophysics, Dilated cardiomyopathy, Biology, medicine.disease, Cell biology, Heart failure, cardiovascular system, medicine, Myocyte

Abstract

The Na+/Ca2+ exchanger (NCX1.1) plays the primary role in Ca2+ extrusion from cardiac myocytes during diastole. There have been many reports showing that NCX1.1 expression levels are elevated in heart failure; however, the importance of NCX1.1 in the pathophysiology of cardiac disease is not well understood. To determine the in vivo cardiac function of NCX1.1, we generated transgenic mouse lines with cardiac-specific overexpression of wild-type or mutated NCX1.1, with Na+-dependent inactivation eliminated. Here we show that NCX1.1 mutant transgenic mice develop dilated cardiomyopathy, whereas wild-type NCX1.1 transgenic mice produce hypertrophic cardiomyopathy. Six-month-old mutant transgenic mice showed contractile dysfunction, ventricular arrhythmias, interstitial fibrosis, and mitochondrial defects. Cardiac myocytes isolated from these mice showed reduced Ca2+ transients, suggesting greater Ca2+ extrusion via overexpressed mutant exchangers. Microarray analysis of their ventricles clearly indicated molecular changes generally associated with the heart disease phenotype. Thus, these mouse models will be useful for understanding the role of NCX1.1 in cardiac diseases.

Published

2010

47. The Promoting Effect of the Extracellular Matrix Peptide TNIIIA2 Derived from Tenascin-C in Colon Cancer Cell Infiltration.

Author

Hideo Suzuki, Manabu Sasada, Sadahiro Kamiya, Yuka Ito, Hikaru Watanabe, Yuko Okada, Kazuma Ishibashi, Takuya Iyoda, Akinori Yanaka, and Fumio Fukai

Subjects

EXTRACELLULAR matrix, MOLECULES, GENE expression, PEPTIDES, COLON cancer

Abstract

The extracellular matrix (ECM) molecule tenascin C (TNC) is known to be highly expressed under various pathological conditions such as inflammation and cancer. It has been reported that the expression of TNC is correlated with the malignant potential of cancer. In our laboratory, it was found that the peptide derived from the alternative splicing domain A2 in TNC, termed TNIIIA2, has been shown to influence a variety of cellular processes, such as survival, proliferation, migration, and differentiation. In this study, we investigated the effect of TNC/TNIIIA2 on the invasion and metastasis of colon cancer cells, Colon26-M3.1, or PMF-Ko14, using an in vitro and in vivo experimental system. The degree of cell invasion was increased by the addition of TNC and TNIIIA2 in a dose-dependent manner. The invasion by TNC and TNIIIA2 were suppressed by an MMP inhibitor or TNIIIA2-blocking antibody. In an in vivo experiment, pulmonary metastasis was promoted conspicuously by the addition of TNIIIA2. In this study, we found that colon cancer cell invasion and metastasis was accelerated by TNC/TNIIIA2 via MMP induction. This result suggests the possibility of a new strategy targeting TNC/TNIIIA2 for colon cancer. [ABSTRACT FROM AUTHOR]

Published

2017

48. Role of Na+/Ca2+ Exchanger (NCX1) in Aldosterone-Induced Cardiac Remodeling

Author

Issei Komuro, Akira Nishiyama, Takahiro Iwamoto, Shintaro Yamamoto, Takuya Iyoda, and Satomi Kita

Subjects

Genetically modified mouse, Cardiac function curve, medicine.medical_specialty, Aldosterone, MILD DYSFUNCTION, business.industry, Biophysics, Eplerenone, chemistry.chemical_compound, Endocrinology, Mineralocorticoid receptor, chemistry, Internal medicine, Cardiac hypertrophy, cardiovascular system, medicine, business, Prolonged treatment, medicine.drug

Abstract

Recent clinical and experimental studies have indicated the utility of eplerenone, a selective mineralocorticoid receptor antagonist, in cardiovascular and renal injuries. Actually, chronic treatment with aldosterone and salt can induce cardiac hypertrophy and renal injuries in experimental animals. However, its underlying mechanism is still unknown. To investigate whether the Na+/Ca2+ exchanger type 1 (NCX1) would be implicated in aldosterone-induced cardiac remodeling, we administered aldosterone (0.3 μg/h) and NaCl (1%) in NCX1 heterozygous mice (N1-KO), heart-specific transgenic mice overexpressing NCX1 (N1-Tg), and wild-type mice (WT). After 4 weeks of treatment, WT and N1-Tg showed a significant increase in heart weight/body weight (HW/BW) ratio with evidence of mild contractile dysfunction, whereas N1-KO maintained average HW/BW ratio and normal cardiac function. More importantly, NCX1 inhibitors (SEA0400, KB-R7943) attenuated aldosterone-induced cardiac hypertrophy and mild dysfunction when administrated to WT for 4 weeks. On the other hand, prolonged treatment with eplerenone (200mg/kg/day) prevented cardiac hypertrophy that was spontaneously induced in N1-Tg. These results suggest that NCX1 participates in aldosterone-induced cardiac remodeling.

Published

2010

49. A Novel Mechanism Underlying the Basic Defensive Response of Macrophages against Mycobacterium Infection.

Author

Takuya Iyoda, Muneaki Takada, Yoshinobu Fukatsu, Shunsuke Kumokoshi, Tatsuya Fujisawa, Tomokazu Shimada, Noriko Shimokawa, Takuya Matsunaga, Kimiko Makino, Norio Doi, Hiroshi Terada, and Fumio Fukai

Subjects

*MYCOBACTERIUM tuberculosis, *TUMOR necrosis factors, *BACILLUS (Bacteria), *BCG vaccines, *CELL death, *PHOSPHORYLATION, *LABORATORY rats

Abstract

Following inhalation of Mycobacterium tuberculosis, including bacillus Calmette-Guérin (BCG), pathogens enter and grow inside macrophages by taking advantage of their phagocytic mechanisms. Macrophages often fail to eliminate intracellular M. tuberculosis, leading to the induction of host macrophage death. Despite accumulating evidence, the molecular mechanisms underlying M. tuberculosis infection-induced cell death remain controversial. In this study, we show the involvement of two distinct pathways triggered by TLR2 and β2 integrin in BCG infection-induced macrophage apoptosis. First, BCG infection induced activation of ERK1/2, which in turn caused phosphorylation/activation of the proapoptotic protein Bim in mouse macrophage-like Raw 264.7 cells. BCG-infected Raw cells treated with U0126, an MEK/ERK inhibitor, led to the suppression of Bim phosphorylation alongside a remarkable increase in the number of viable macrophages. Small interfering RNA-mediated knockdown of Bim rescued the macrophages from the apoptotic cell death induced by BCG infection. Stimulation with Pam3CSK, a TLR2 agonist, induced macrophage apoptosis with a concomitant increase in the phosphorylation/activation of MEK/ERK and Bim. These observations indicate the important role of the TLR2/MEK/ERK/Bim pathway in BCG infection-induced macrophage apoptosis. Second, we used the β2 integrin agonists C3bi and fibronectin to show that the β2 integrin-derived signal was involved in BCG infection-induced apoptosis, independent of MEK/ERK activation. Interestingly, latex beads coated with Pam3CSK and C3bi were able to induce apoptosis in macrophages to the same extent and specificity as that induced by BCG. Taken together, two distinct pattern-recognition membrane receptors, TLR2 and β2 integrin, acted as triggers in BCG infection-induced macrophage apoptosis, in which MEK/ERK activation played a crucial role following the engagement of TLR2. [ABSTRACT FROM AUTHOR]

Published

2014

50. Tenascin-C-derived Peptide TNIIIA2 Highly Enhances Cell Survival and Platelet-derived Growth Factor (PDGF)-dependent Cell Proliferation through Potentiated and Sustained Activation of Integrin α5β1.

Author

Rika Tanaka, Yutaka Seki, Yohei Saito, Sadahiro Kamiya, Motomichi Fujita, Hiroaki Okutsu, Takuya Iyoda, Tatsuya Takai, Toshiyuki Owaki, Hirofumi Yajima, Junichi Taira, Ryo Hayashi, Hiroaki Kodama, Takuya Matsunaga, and Fumio Fukai

Subjects

*TENASCIN, *EXTRACELLULAR matrix proteins, *TUMORS, *NEOPLASTIC cell transformation, *PEPTIDES

Abstract

Tenascin-C is an adhesion modulatory matrix protein that is highly expressed in tumors; however, its biochemical activity involved in tumorigenesis is not fully understood. On the other hand, increasing evidence indicates the importance of integrin α5β1 in cancer development. We previously demonstrated that tenascin-C harbors a functional site that can be released as a proadhesive peptide such as TNIIIA2. Peptide TNIIIA2 is capable of inducing activation of β1-integrins including α5β1 via syndecan-4. In this study the proadhesive effect of TNIIIA2 was characterized by potentiated and sustained activation of integrin α5β1. Based on this effect, TNIIIA2 rendered nontransformed fibroblasts (NIH3T3) resistant to serum deprivation-elicited anoikis through activation of the Akt/Bcl-2 pathway. Moreover, TNIIIA2 hyperstimulated PDGF-dependent proliferation of NIH3T3 by activating integrin α5β1. Tenascin-C, a parental protein of TNIIIA2, also stimulated PDGF-dependent proliferation, which was blocked by a matrix metalloproteinase-2/9 inhibitor and an anti-TNIIIA2 function-blocking antibody, suggesting proteolytic exposure of the proadhesive effect of TNIIIA2. Mechanistic analyses revealed that TNIIIA2 induced a lateral association of PDGF receptor β with the molecular complex of activated integrin α5β1 and syndecan-4 in the membrane microdomains enriched with cholesterol/caveolin-1, resulting in prolonged activation of PDGF receptor β and the subsequent Ras/mitogen-activated protein kinase pathway in a PDGF-dependent manner. Of note, TNIIIA2 induced continuous proliferation in NIH3T3 in an integrin α5β1-dependent manner even after they formed a confluent monolayer. Thus, it was proposed that tenascin-C might be involved in deregulated cell growth through potentiated and sustained activation of integrin α5β1 after exposure of the proadhesive effect of TNIIIA2. [ABSTRACT FROM AUTHOR]

Published

2014