Your search keyword '"Sudo, Katsuko"' showing total 31 results

1. miR-27a ameliorates chemoresistance of breast cancer cells by disruption of reactive oxygen species homeostasis and impairment of autophagy

Author

Ueda, Shinobu, Takanashi, Masakatsu, Sudo, Katsuko, Kanekura, Kohsuke, and Kuroda, Masahiko

Abstract

In patients with breast cancer, primary chemotherapy often fails due to survival of chemoresistant breast cancer stem cells (BCSCs) which results in recurrence and metastasis of the tumor. However, the factors determining the chemoresistance of BCSCs have remained to be investigated. Here, we profiled a series of differentially expressed microRNAs (miRNAs) between parental adherent breast cancer cells and BCSC-mimicking mammosphere-derived cancer cells, and identified hsa-miR-27a as a negative regulator for survival and chemoresistance of BCSCs. In the mammosphere, we found that the expression of hsa-miR-27a was downregulated, and ectopic overexpression of hsa-miR-27a reduced both number and size of mammospheres. In addition, overexpression of hsa-miR-27a sensitized breast cancer cells to anticancer drugs by downregulation of genes essential for detoxification of reactive oxygen species (ROS) and impairment of autophagy. Therefore, enhancing the hsa-miR-27a signaling pathway can be a potential therapeutic modality for breast cancer.

Published

2024

2. WAPL induces cervical intraepithelial neoplasia modulated with estrogen signaling without HPV E6/E7

Author

Kumagai, Katsuyoshi, Takanashi, Masakatsu, Ohno, Shin-ichiro, Harada, Yuichirou, Fujita, Koji, Oikawa, Keiki, Sudo, Katsuko, Ikeda, Shun-ichi, Nishi, Hirotaka, Oikawa, Kosuke, and Kuroda, Masahiko

Abstract

Since cervical cancer still afflicts women around the world, it is necessary to understand the underlying mechanism of cervical cancer development. Infection with HPV is essential for the development of cervical intraepithelial neoplasia (CIN). In addition, estrogen receptor signaling is implicated in the development of cervical cancer. Previously, we have isolated human wings apart-like (WAPL), which is expected to cause chromosomal instability in the process of HPV-infected precancerous lesions to cervical cancer. However, the role of WAPL in the development of CIN is still unknown. In this study, in order to elucidate the role of WAPL in the early lesion, we established WAPL overexpressing mice (WAPL Tg mice) and HPV E6/E7 knock-in (KI) mice. WAPL Tg mice developed CIN lesion without HPV E6/E7. Interestingly, in WAPL Tg mice estrogen receptor 1 (ESR1) showed reduction as compared with the wild type, but cell growth factors MYC and Cyclin D1 controlled by ESR1 expressed at high levels. These results suggested that WAPL facilitates sensitivity of ESR1 mediated by some kind of molecule, and as a result, affects the expression of MYC and Cyclin D1 in cervical cancer cells. To detect such molecules, we performed microarray analysis of the uterine cervix in WAPL Tg mice, and focused MACROD1, a co-activator of ESR1. MACROD1 expression was increased in WAPL Tg mice compared with the wild type. In addition, knockdown of WAPL induced the downregulation of MACROD1, MYC, and Cyclin D1 but not ESR1 expression. Furthermore, ESR1 sensitivity assay showed lower activity in WAPL or MACROD1 downregulated cells than control cells. These data suggested that WAPL increases ESR1 sensitivity by activating MACROD1, and induces the expression of MYC and Cyclin D1. Therefore, we concluded that WAPL not only induces chromosomal instability in cervical cancer tumorigenesis, but also plays a key role in activating estrogen receptor signaling in early tumorigenesis.

Published

2021

3. miR-27a ameliorates chemoresistance of breast cancer cells by disruption of reactive oxygen species homeostasis and impairment of autophagy

Author

Ueda, Shinobu, Takanashi, Masakatsu, Sudo, Katsuko, Kanekura, Kohsuke, and Kuroda, Masahiko

Abstract

In patients with breast cancer, primary chemotherapy often fails due to survival of chemoresistant breast cancer stem cells (BCSCs) which results in recurrence and metastasis of the tumor. However, the factors determining the chemoresistance of BCSCs have remained to be investigated. Here, we profiled a series of differentially expressed microRNAs (miRNAs) between parental adherent breast cancer cells and BCSC-mimicking mammosphere-derived cancer cells, and identified hsa-miR-27a as a negative regulator for survival and chemoresistance of BCSCs. In the mammosphere, we found that the expression of hsa-miR-27a was downregulated, and ectopic overexpression of hsa-miR-27a reduced both number and size of mammospheres. In addition, overexpression of hsa-miR-27a sensitized breast cancer cells to anticancer drugs by downregulation of genes essential for detoxification of reactive oxygen species (ROS) and impairment of autophagy. Therefore, enhancing the hsa-miR-27a signaling pathway can be a potential therapeutic modality for breast cancer.

Published

2020

4. Role of interleukin-25 in development of spontaneous arthritis in interleukin-1 receptor antagonist-deficient mice

Author

Abe, Yasuharu, Nambu, Aya, Yamaguchi, Sachiko, Takamori, Ayako, Suto, Hajime, Hirose, Sachiko, Yokosuka, Tadashi, Nakae, Susumu, and Sudo, Katsuko

Abstract

Interleukin (IL)-25, which is a member of the IL-17 family of cytokines, induces production of such Th2 cytokines as IL-4, IL-5, IL-9 and/or IL-13 by various types of cells, including Th2 cells, Th9 cells and group 2 innate lymphoid cells (ILC2). On the other hand, IL-25 can suppress Th1- and Th17-associated immune responses by enhancing Th2-type immune responses. Supporting this, IL-25 is known to suppress development of experimental autoimmune encephalitis, which is an IL-17-mediated autoimmune disease in mice. However, the role of IL-25 in development of IL-17-mediated arthritis is not fully understood. Therefore, we investigated this using IL-1 receptor antagonist-deficient (IL-1Ra-/-) mice, which spontaneously develop IL-17-dependent arthritis. However, development of spontaneous arthritis (incidence rate, disease severity, proliferation of synovial cells, infiltration of PMNs, and bone erosion in joints) and differentiation of Th17 cells in draining lymph nodes in IL-25-/-IL-1Ra-/-mice were similar to in control IL-25+/+IL-1Ra-/-mice. These observations indicate that IL-25 does not exert any inhibitory and/or pathogenic effect on development of IL-17-mediated spontaneous arthritis in IL-1Ra-/-mice.

Published

2017

5. TIM-3 is not essential for development of airway inflammation induced by house dust mite antigens

Author

Hiraishi, Yoshihisa, Nambu, Aya, Shibui, Akiko, Nakanishi, Wakako, Yamaguchi, Sachiko, Morita, Hideaki, Iikura, Motoyasu, McKenzie, Andrew N.J., Matsumoto, Kenji, Sudo, Katsuko, Yamasoba, Tatsuya, Nagase, Takahide, and Nakae, Susumu

Abstract

T cell immunoglobulin domain and mucin domain-containing molecule 3 (TIM-3), which is preferentially expressed on Th1 cells rather than Th2 cells, is considered to be a negative regulator of Th1 cell function. This suggests that TIM-3 indirectly enhances Th2-type immune responses by suppressing Th1 cell function.

Published

2016

6. TSLP receptor is not essential for house dust mite-induced allergic rhinitis in mice

Author

Nakanishi, Wakako, Hiraishi, Yoshihisa, Yamaguchi, Sachiko, Takamori, Ayako, Morita, Hideaki, Matsumoto, Kenji, Saito, Hirohisa, Sudo, Katsuko, Yamasoba, Tatsuya, and Nakae, Susumu

Abstract

TSLP induces Th2 cytokine production by Th2 cells and various other types of cells, thereby contributing to Th2-type immune responses and development of allergic disorders. We found that house dust mite (HDM) extract induced TSLP production by nasal epithelial cells, suggesting that TSLP may be involved in development of HDM-induced allergic rhinitis (AR). To investigate that possibility in greater detail, wild-type and TSLP receptor-deficient (TSLPR−/−) mice on the C57BL/6J background were repeatedly treated intranasally with HDM extract. The frequency of sneezing, numbers of eosinophils and goblet cells, thickness of submucosal layers, serum levels of total IgE and HDM-specific IgG1, and levels of IL-4, IL-5 and IL-13 in the culture supernatants of HDM-stimulated LN cells were comparable in the two mouse strains. Those findings indicate that, in mice, TSLPR is not crucial for development of HDM-induced AR.

Published

2016

7. Development of Novel Small Hairpin RNAs That do not Require Processing by Dicer or AGO2

Author

Ohno, Shin-ichiro, Itano, Karen, Harada, Yuichirou, Asada, Koutaro, Oikawa, Keiki, Kashiwazako, Mikie, Okuyama, Hikaru, Kumagai, Katsuyoshi, Takanashi, Masakatsu, Sudo, Katsuko, Ikeda, Norihiko, and Kuroda, Masahiko

Abstract

The innate cytokine response to nucleic acid is the most challenging problem confronting the practical use of nucleic acid medicine. The degree of stimulation of the innate cytokine response strongly depends on the length of the nucleic acid. In this study, we developed a 30-nucleotide single-strand RNA, termed “guide hairpin RNA (ghRNA, ghR)”, that has a physiological function similar to that of miRNA and siRNA. The ghR caused no innate cytokine response either in vitroor in vivo. In addition, its structure does not contain a passenger strand seed sequence, reducing the unwanted gene repression relative to existing short RNA reagents. Systemic and local injection of ghR-form miR-34a (ghR-34a) suppressed tumor growth in a mouse model of RAS-induced lung cancer. Furthermore, Dicer and AGO2 are not required for ghR-34a function. This novel RNA interference (RNAi) technology may provide a novel, safe, and effective nucleic acid drug platform that will increase the clinical usefulness of nucleic acid therapy.

Published

2016

8. IL-25, IL-33 and TSLP receptor are not critical for development of experimental murine malaria

Author

Shibui, Akiko, Takamori, Ayako, Tolba, Mohammed E.M., Nambu, Aya, Shimura, Eri, Yamaguchi, Sachiko, Sanjoba, Chizu, Suto, Hajime, Sudo, Katsuko, Okumura, Ko, Sugano, Sumio, Morita, Hideaki, Saito, Hirohisa, Matsumoto, Kenji, and Nakae, Susumu

Abstract

IL-25, IL-33 and TSLP, which are produced predominantly by epithelial cells, can induce production of Th2-type cytokines such as IL-4, IL-5 and/or IL-13 by various types of cells, suggesting their involvement in induction of Th2-type cytokine-associated immune responses. It is known that Th2-type cytokines contribute to host defense against malaria parasite infection in mice. However, the roles of IL-25, IL-33 and TSLP in malaria parasite infection remain unclear. Thus, to elucidate this, we infected wild-type, IL-25−/−, IL-33−/−and TSLP receptor (TSLPR)−/−mice with Plasmodium berghei(P. berghei) ANKA, a murine malaria strain. The expression levels of IL-25, IL-33 and TSLP mRNA were changed in the brain, liver, lung and spleen of wild-type mice after infection, suggesting that these cytokines are involved in host defense against P. bergheiANKA. However, the incidence of parasitemia and survival in the mutant mice were comparable to in the wild-type mice. These findings indicate that IL-25, IL-33 and TSLP are not critical for host defense against P. bergheiANKA.

Published

2016

9. ST2 Requires Th2-, but Not Th17-, Type Airway Inflammation in Epicutaneously Antigen-Sensitized Mice

Author

Morita, Hideaki, Arae, Ken, Ohno, Tatsukuni, Kajiwara, Naoki, Oboki, Keisuke, Matsuda, Akio, Suto, Hajime, Okumura, Ko, Sudo, Katsuko, Takahashi, Takao, Matsumoto, Kenji, and Nakae, Susumu

Abstract

IL-33 is known to induce Th2-type cytokine production by various types of cells through its receptors, ST2 and IL-1RAcP. Polymorphism in the ST2 and/or IL-33 genes was found in patients with atopic dermatitis and asthma, implying that the IL-33/ST2 pathway is closely associated with susceptibility to these diseases. Exposure to allergens through damaged skin is suspected to be a trigger for allergen sensitization, resulting in development of such allergic disorders as asthma and atopic dermatitis.

Published

2012

10. Generation of Transgenic Mice on an NOD/SCID Background Using the Conventional Microinjection Technique1

Author

Kumagai, Katsuyoshi, Kubota, Naoto, Saito, Toshiki I., Sasako, Takayoshi, Takizawa, Rumi, Sudo, Katsuko, Kurokawa, Mineo, and Kadowaki, Takashi

Abstract

Humanized mice, which refers to immunodeficient mice repopulated with the human immune system, are powerful tools for study in the field of immunology. It has been difficult, however, to generate these transgenic (Tg) mice directly from such strains as the NOD/SCID mouse. In this study, we describe a method developed by us for the generation of Tg mice on an NOD/SCID background. First, we obtained fertilized eggs efficiently by means of in vitro fertilization (IVF); then, we attempted to generate CAG-EGFP Tg mice on an NOD/SCID background, finding that delayed timing of the microinjection after the IVF improved the time to development of the two-cell-stage embryos and the obtainment of newborns. We successfully generated Tg mice and confirmed the germ-line transmission in the offspring. In conclusion, we established a novel system for directly generating transgenic mice on an NOD/SCID background. This novel system is expected to allow improved efficiency of the generation of humanized mice.

Published

2011

11. Abnormal T cell activation caused by the imbalance of the IL-1/IL-1R antagonist system is responsible for the development of experimental autoimmune encephalomyelitis

Author

Matsuki, Taizo, Nakae, Susumu, Sudo, Katsuko, Horai, Reiko, and Iwakura, Yoichiro

Abstract

IL-1 is a pro-inflammatory cytokine that plays an important role in inflammation and host responses to infection. We have previously shown that imbalances in the IL-1 and IL-1R antagonist (IL-1Ra) system cause the development of inflammatory diseases. To explore the role of the IL-1/IL-1Ra system in autoimmune disease, we analyzed myelin oligodendrocyte glycoprotein (MOG)-induced experimental autoimmune encephalomyelitis (EAE) in mice bearing targeted disruptions of the IL-1α, IL-1β, IL-1α and IL-1β (IL-1) or IL-1Ra genes. IL-1α/β double-deficient (IL-1−/−) mice exhibited significant resistance to EAE induction with a significant reduction in disease severity, while IL-1α−/− or IL-1β−/− mice developed EAE in a manner similar to wild-type mice. IL-1Ra−/− mice also developed MOG-induced EAE normally with pertussis toxin (PTx) administration. In contrast to wild-type mice, however, these mice were highly susceptible to EAE induction in the absence of PTx administration. We found that both IFN-γ and IL-17 production and proliferation were reduced in IL-1−/− T cells upon stimulation with MOG, while IFN-γ, IL-17 and tumor necrosis factor-α production and proliferation were enhanced in IL-1Ra−/− T cells. These observations suggest that the IL-1/IL-1Ra system is crucial for auto-antigen-specific T cell induction and contributes to the development of EAE.

Published

2006

12. Role of Dok-1 and Dok-2 in Myeloid Homeostasis and Suppression of Leukemia

Author

Yasuda, Tomoharu, Shirakata, Masaki, Iwama, Atsushi, Ishii, Asuka, Ebihara, Yasuhiro, Osawa, Mitsujiro, Honda, Kazuho, Shinohara, Hisaaki, Sudo, Katsuko, Tsuji, Kohichiro, Nakauchi, Hiromitsu, Iwakura, Yoichiro, Hirai, Hisamaru, Oda, Hideaki, Yamamoto, Tadashi, and Yamanashi, Yuji

Abstract

Dok-1 and Dok-2 are closely related rasGAP-associated docking proteins expressed preferentially in hematopoietic cells. Although they are phosphorylated upon activation of many protein tyrosine kinases (PTKs), including those coupled with cytokine receptors and oncogenic PTKs like Bcr-Abl, their physiological roles are largely unidentified. Here, we generated mice lacking Dok-1 and/or Dok-2, which included the double-deficient mice succumbed to myeloproliferative disease resembling human chronic myelogenous leukemia (CML) and chronic myelomonocytic leukemia. The double-deficient mice displayed medullary and extramedullary hyperplasia of granulocyte/macrophage progenitors with leukemic potential, and their myeloid cells showed hyperproliferation and hypo-apoptosis upon treatment and deprivation of cytokines, respectively. Consistently, the mutant myeloid cells showed enhanced Erk and Akt activation upon cytokine stimulation. Moreover, loss of Dok-1 and/or Dok-2 induced blastic transformation of chronic phase CML-like disease in mice carrying the bcr-abl gene, a cause of CML. These findings demonstrate that Dok-1 and Dok-2 are key negative regulators of cytokine responses and are essential for myeloid homeostasis and suppression of leukemia.

Published

2004

13. IL-1 Plays an Important Role in Lipid Metabolism by Regulating Insulin Levels under Physiological Conditions

Author

Matsuki, Taizo, Horai, Reiko, Sudo, Katsuko, and Iwakura, Yoichiro

Abstract

IL-1 is a proinflammatory cytokine that plays important roles in inflammation. However, the role of this cytokine under physiological conditions is not known completely. In this paper, we analyzed the role of IL-1 in maintaining body weight because IL-1 receptor antagonist–deficient (IL-1Ra−/−) mice, in which excess IL-1 signaling may be induced, show a lean phenotype. Body fat accumulation was impaired in IL-1Ra−/− mice, but feeding behavior, expression of hypothalamic factors involved in feeding control, energy expenditure, and heat production were normal. When IL-1Ra−/− mice were treated with monosodium glutamate (MSG), which causes obesity in wild-type mice by ablating cells in the hypothalamic arcuate nucleus, they were resistant to obesity, indicating that excess IL-1 signaling antagonizes the effect of MSG-sensitive neuron deficiency. IL-1Ra−/− mice showed decreased weight gain when they were fed the same amount of food as wild-type mice, and lipid accumulation remained impaired even when they were fed a high-fat diet. Interestingly, serum insulin levels and lipase activity were low in IL-1Ra−/− mice, and the insulin levels were low in contrast to wild-type mice after MSG treatment. These observations suggest that IL-1 plays an important role in lipid metabolism by regulating insulin levels and lipase activity under physiological conditions.

Published

2003

14. IL-1 is required for allergen-specific Th2 cell activation and the development of airway hypersensitivity response.

Author

Nakae, Susumu, Komiyama, Yutaka, Yokoyama, Hiroshi, Nambu, Aya, Umeda, Masaomi, Iwase, Michiko, Homma, Ikuo, Sudo, Katsuko, Horai, Reiko, Asano, Masahide, and Iwakura, Yoichiro

Abstract

IL-1 is a pro-inflammatory cytokine consisted of two molecular species, IL-1alpha and IL-1beta, and the IL-1 receptor antagonist (IL-1Ra) is a natural inhibitor of both molecules. Although it is suggested that IL-1 potentiates immune responses mediated by T(h)2 cells, the role of IL-1 in asthma still remains unclear. In this study, we demonstrate that the ovalbumin (OVA)-induced airway hypersensitivity response (AHR) in IL-1alpha/beta-deficient (IL-1alpha/beta(-/-)) mice was significantly reduced from the levels seen in wild-type mice, whereas the responses seen in IL-1Ra(-/-) mice were profoundly exacerbated, suggesting that IL-1 is required for T(h)2 cell activation during AHR. OVA-specific T cell proliferation, IL-4 and IL-5 production by T cells, and IgG1 and IgE production by B cells in IL-1alpha/beta(-/-) mice were markedly reduced compared with these responses in wild-type mice; such responses were enhanced in IL-1Ra(-/-) mice. Using IL-1alpha(-/-) and IL-1beta(-/-) mice, we determined that both IL-1alpha and IL-1beta are involved in this reaction. Both IgG1 and IgE levels were reduced in IL-1beta(-/-) mice, while only IgE levels were affected in IL-1alpha(-/-) mice, indicating a functional difference between IL-1alpha and IL-1beta. These observations indicate that IL-1 plays important roles in the development of AHR.

Published

2003

15. IL-1-induced tumor necrosis factor-alpha elicits inflammatory cell infiltration in the skin by inducing IFN-gamma-inducible protein 10 in the elicitation phase of the contact hypersensitivity response.

Author

Nakae, Susumu, Komiyama, Yutaka, Narumi, Shosaku, Sudo, Katsuko, Horai, Reiko, Tagawa, Yoh-Ichi, Sekikawa, Kenji, Matsushima, Koji, Asano, Masahide, and Iwakura, Yoichiro

Abstract

Contact hypersensitivity (CHS) is a typical inflammatory response against contact allergens. Inflammatory cytokines, including IL-1 and tumor necrosis factor (TNF)-alpha, are implicated in the reaction, although the precise roles of each cytokine have not been completely elucidated. In this report, we dissected the functional roles of IL-1 and TNF-alpha during CHS. CHS induced by 2,4,6-trinitorochlorobenzene as well as oxazolone was suppressed in both IL-1alpha/beta(-/-) and TNF-alpha(-/-) mice. Hapten-specific T cell activation, as examined by T cell proliferation, OX40 expression and IL-17 production, was reduced in IL-1alpha/beta(-/-) mice, but not in TNF-alpha(-/-) mice, suggesting that IL-1 but not TNF-alpha is required for hapten-specific T cell priming in the sensitization phase. On the other hand, TNF-alpha, induced by IL-1, was necessary for the induction of local inflammation during the elicitation phase. We also found that the expression of IFN-gamma-inducible protein 10 (IP-10) was augmented at the inflammatory site. Although IP-10 mRNA expression was abrogated in TNF-alpha(-/-) mice, both CHS development and TNF-alpha mRNA expression occurred normally in IFN-gamma(-/-) mice, indicating that the induction of IP-10 during CHS was primarily controlled by TNF-alpha. Interestingly, CHS was suppressed by treatment with anti-IP-10 mAb, suggesting a critical role for IP-10 in CHS. Reduced CHS in TNF-alpha(-/-) mice was reversed by IP-10 injection during the elicitation phase. Thus, it was shown that the roles for IL-1 and TNF-alpha are different, although both cytokines are crucial for the development of CHS.

Published

2003

16. Mice Deficient in Nervous System-specific Carbohydrate Epitope HNK-1 Exhibit Impaired Synaptic Plasticity and Spatial Learning*

Author

Yamamoto, Shoji, Oka, Shogo, Inoue, Mitsuhiro, Shimuta, Misa, Manabe, Toshiya, Takahashi, Hideki, Miyamoto, Masaomi, Asano, Masahide, Sakagami, Junko, Sudo, Katsuko, Iwakura, Yoichiro, Ono, Katsuhiko, and Kawasaki, Toshisuke

Abstract

The HNK-1 carbohydrate epitope, a sulfated glucuronic acid at the non-reducing terminus of glycans, is expressed characteristically on a series of cell adhesion molecules and is synthesized through a key enzyme, glucuronyltransferase (GlcAT-P). We generated mice with a targeted deletion of the GlcAT-P gene. The GlcAT-P −/− mice exhibited normal development of gross anatomical features, but the adult mutant mice exhibited reduced long term potentiation at the Schaffer collateral-CA1 synapses and a defect in spatial memory formation. This is the first evidence that the loss of a single non-reducing terminal carbohydrate residue attenuates brain higher functions.

Published

2002

17. Requirement for MD-1 in cell surface expression of RP105/CD180 and B-cell responsiveness to lipopolysaccharide

Author

Nagai, Yoshinori, Shimazu, Rintaro, Ogata, Hirotaka, Akashi, Sachiko, Sudo, Katsuko, Yamasaki, Hidetoshi, Hayashi, Shin-Ichi, Iwakura, Yoichiro, Kimoto, Masao, and Miyake, Kensuke

Abstract

RP105 is a B-cell surface molecule that has been recently assigned as CD180. RP105 ligation with an antibody induces B-cell activation in humans and mice, leading to proliferation and up-regulation of a costimulatory molecule, B7.2/CD86. RP105 is associated with an extracellular molecule, MD-1. RP105/MD-1 has structural similarity to Toll-like receptor 4 (TLR4)/MD-2. TLR4 signals a membrane constituent of Gram-negative bacteria, lipopolysaccharide (LPS). MD-2 is indispensable for TLR4-dependent LPS responses because cells expressing TLR4/MD-2, but not TLR4 alone, respond to LPS. RP105 also has a role in LPS responses because B cells lacking RP105 show hyporesponsiveness to LPS. Little is known, however, regarding whether MD-1 is important for RP105-dependent LPS responses, as MD-2 is for TLR4. To address the issue, we developed mice lacking MD-1 and generated monoclonal antibodies (mAbs) to the protein. MD-1–null mice showed impairment in LPS-induced B-cell proliferation, antibody production, and B7.2/CD86 up-regulation. These phenotypes are similar to those of RP105-null mice. The similarity was attributed to the absence of cell surface RP105 on MD-1–null B cells. MD-1 is indispensable for cell surface expression of RP105. A role for MD-1 in LPS responses was further studied with anti–mouse MD-1 mAbs. In contrast to highly mitogenic anti-RP105 mAbs, the mAbs to MD-1 were not mitogenic but antagonistic on LPS-induced B-cell proliferation and on B7.2 up-regulation. Collectively, MD-1 is important for RP105 with respect to B-cell surface expression and LPS recognition and signaling.

Published

2002

18. Requirement for MD-1 in cell surface expression of RP105/CD180 and B-cell responsiveness to lipopolysaccharide

Author

Nagai, Yoshinori, Shimazu, Rintaro, Ogata, Hirotaka, Akashi, Sachiko, Sudo, Katsuko, Yamasaki, Hidetoshi, Hayashi, Shin-Ichi, Iwakura, Yoichiro, Kimoto, Masao, and Miyake, Kensuke

Abstract

RP105 is a B-cell surface molecule that has been recently assigned as CD180. RP105 ligation with an antibody induces B-cell activation in humans and mice, leading to proliferation and up-regulation of a costimulatory molecule, B7.2/CD86. RP105 is associated with an extracellular molecule, MD-1. RP105/MD-1 has structural similarity to Toll-like receptor 4 (TLR4)/MD-2. TLR4 signals a membrane constituent of Gram-negative bacteria, lipopolysaccharide (LPS). MD-2 is indispensable for TLR4-dependent LPS responses because cells expressing TLR4/MD-2, but not TLR4 alone, respond to LPS. RP105 also has a role in LPS responses because B cells lacking RP105 show hyporesponsiveness to LPS. Little is known, however, regarding whether MD-1 is important for RP105-dependent LPS responses, as MD-2 is for TLR4. To address the issue, we developed mice lacking MD-1 and generated monoclonal antibodies (mAbs) to the protein. MD-1–null mice showed impairment in LPS-induced B-cell proliferation, antibody production, and B7.2/CD86 up-regulation. These phenotypes are similar to those of RP105-null mice. The similarity was attributed to the absence of cell surface RP105 on MD-1–null B cells. MD-1 is indispensable for cell surface expression of RP105. A role for MD-1 in LPS responses was further studied with anti–mouse MD-1 mAbs. In contrast to highly mitogenic anti-RP105 mAbs, the mAbs to MD-1 were not mitogenic but antagonistic on LPS-induced B-cell proliferation and on B7.2 up-regulation. Collectively, MD-1 is important for RP105 with respect to B-cell surface expression and LPS recognition and signaling.

Published

2002

19. IL-1α, but not IL-1β, is required for contact-allergen-specific T cell activation during the sensitization phase in contact hypersensitivity

Author

Nakae, Susumu, Naruse-Nakajima1, Chie, Sudo, Katsuko, Horai, Reiko, Asano, Masahide, and Iwakura, Yoichiro

Abstract

Contact hypersensitivity (CHS) is a T cell-mediated cellular immune response caused by epicutaneous exposure to contact allergens. In this reaction, after the first epicutaneous allergen sensitization, Langerhans cells (LC) catch allergens and migrate from the skin to draining lymph nodes (LN) and activate naive T cells. Although IL-1 is suggested to be involved in these processes, the mechanisms have not been elucidated completely. In this report, to elucidate roles of IL-1α and IL-1β in CHS, we analyzed ear swelling in 2,4,6-trinitrochlorobenzene (TNCB)-induced CHS using gene-targeted mice. We found that ear swelling was suppressed in IL-1α-deficient (IL-1α–/–) mice but not in IL-1β–/– mice. LC migration from the skin into LN was delayed in both IL-1α–/– and IL-1β–/– mice, suggesting that this defect was not the direct cause for the reduced CHS in these mice. However, we found that the proliferative response of trinitrophenyl (TNP)-specific T cells after sensitization with TNCB was specifically reduced in IL-1α–/– mice. Furthermore, adoptive transfer of TNP-conjugated IL-1-deficient epidermal cells (EC) into wild-type mice indicated that only IL-1α, but not IL-1β, produced by antigen-presenting cells in EC could prime allergen-specific T cells. These observations indicate that IL-1α, but not IL-1β, plays a crucial role in TNCB-induced CHS by sensitizing TNP-specific T cells.

Published

2001

20. Six4, a Putative myogeninGene Regulator, Is Not Essential for Mouse Embryonal Development

Author

Ozaki, Hidenori, Watanabe, Yoko, Takahashi, Katsumasa, Kitamura, Ken, Tanaka, Akira, Urase, Koko, Momoi, Takashi, Sudo, Katsuko, Sakagami, Junko, Asano, Masahide, Iwakura, Yoichiro, and Kawakami, Kiyoshi

Abstract

ABSTRACTSix4is a member of the Sixfamily genes, homologues of Drosophila melanogaster sine oculis. The gene is thought to be involved in neurogenesis, myogenesis, and development of other organs, based on its specific expression in certain neuronal cells of the developing embryo and in adult skeletal muscles. To elucidate the biological roles of Six4, we generatedSix4-deficient mice by replacing the Sixhomologous region and homeobox by the β-galactosidase gene. 5-Bromo-4-chloro-3-indolyl-β-d-galactopyranoside staining of the heterozygous mutant embryos revealed expression ofSix4in cranial and dorsal root ganglia, somites, otic and nasal placodes, branchial arches, Rathke's pouch, apical ectodermal ridges of limb buds, and mesonephros. The expression pattern was similar to that of Six1except at the early stage of embryonic day 8.5. Six4-deficient mice were born according to the Mendelian rule with normal gross appearance and were fertile. No hearing defects were detected. Six4-deficient embryos showed no morphological abnormalities, and the expression patterns of several molecular markers, e.g., myogeninandNeuroD3(neurogenin1), were normal. Our results indicate that Six4is not essential for mouse embryogenesis and suggest that other members of the Sixfamily seem to compensate for the loss of Six4.

Published

2001

21. Six4, a Putative myogeninGene Regulator, Is Not Essential for Mouse Embryonal Development

Author

Ozaki, Hidenori, Watanabe, Yoko, Takahashi, Katsumasa, Kitamura, Ken, Tanaka, Akira, Urase, Koko, Momoi, Takashi, Sudo, Katsuko, Sakagami, Junko, Asano, Masahide, Iwakura, Yoichiro, and Kawakami, Kiyoshi

Abstract

Six4is a member of the Sixfamily genes, homologues of Drosophila melanogaster sine oculis. The gene is thought to be involved in neurogenesis, myogenesis, and development of other organs, based on its specific expression in certain neuronal cells of the developing embryo and in adult skeletal muscles. To elucidate the biological roles of Six4, we generatedSix4-deficient mice by replacing the Sixhomologous region and homeobox by the β-galactosidase gene. 5-Bromo-4-chloro-3-indolyl-β-d-galactopyranoside staining of the heterozygous mutant embryos revealed expression ofSix4in cranial and dorsal root ganglia, somites, otic and nasal placodes, branchial arches, Rathke's pouch, apical ectodermal ridges of limb buds, and mesonephros. The expression pattern was similar to that of Six1except at the early stage of embryonic day 8.5. Six4-deficient mice were born according to the Mendelian rule with normal gross appearance and were fertile. No hearing defects were detected. Six4-deficient embryos showed no morphological abnormalities, and the expression patterns of several molecular markers, e.g., myogeninandNeuroD3(neurogenin1), were normal. Our results indicate that Six4is not essential for mouse embryogenesis and suggest that other members of the Sixfamily seem to compensate for the loss of Six4.

Published

2001

22. TAG-1-Deficient Mice Have Marked Elevation of Adenosine A1 Receptors in the Hippocampus

Author

Fukamauchi, Fumihiko, Aihara, Okihiko, Wang, Yi-Jun, Akasaka, Keiko, Takeda, Yasuo, Horie, Masao, Kawano, Hitoshi, Sudo, Katsuko, Asano, Masahide, Watanabe, Kazutada, and Iwakura, Yoichiro

Abstract

TAG-1 is a neural recognition molecule in the immunoglobulin superfamily that is predominantly expressed in the developing brain. Several lines of evidence suggest that TAG-1 is involved in the outgrowth, guidance, and fasciculation of neurites. To directly assess the function of TAG-1 in vivo, we have generated mice with a deletion in the gene encoding TAG-1 using homologous recombination in embryonic stem cells. Gross morphological analysis of the cerebellum, the spinal cord, and the hippocampus appeared normal in TAG-1-deficient mice. However, TAG-1 (−/−) mice showed the upregulation of the adenosine A1 receptors determined by [3H]cyclopentyl-1,3-dipropylxanthine in the hippocampus, and their greater sensitivity to convulsant stimuli than that in TAG-1 (+/+) mice. We suspect that the subtle changes in neural plasticity induced by TAG-1 deficiency during development cause the selective vulnerability of specific brain regions and the epileptogenicity in TAG-1 (−/−) mice.

Published

2001

23. Development of Chronic Inflammatory Arthropathy Resembling Rheumatoid Arthritis in Interleukin 1 Receptor Antagonist–Deficient Mice

Author

Horai, Reiko, Saijo, Shinobu, Tanioka, Hidetoshi, Nakae, Susumu, Sudo, Katsuko, Okahara, Akihiko, Ikuse, Toshimi, Asano, Masahide, and Iwakura, Yoichiro

Abstract

Interleukin (IL)-1 is a proinflammatory cytokine that plays important roles in inflammation, host defense, and the neuro-immuno-endocrine network. IL-1 receptor antagonist (ra) is an endogenous inhibitor of IL-1 and is supposed to regulate IL-1 activity. However, its pathophysiological roles in a body remain largely unknown. To elucidate the roles of IL-1ra, IL-1ra–deficient mice were produced by gene targeting, and pathology was analyzed on different genetic backgrounds. We found that all of the mice on a BALB/cA background, but not those on a C57BL/6J background, spontaneously developed chronic inflammatory polyarthropathy. Histopathology showed marked synovial and periarticular inflammation, with articular erosion caused by invasion of granulation tissues closely resembling that of rheumatoid arthritis in humans. Moreover, elevated levels of antibodies against immunoglobulins, type II collagen, and double-stranded DNA were detected in these mice, suggesting development of autoimmunity. Proinflammatory cytokines such as IL-1β, IL-6, and tumor necrosis factor α were overexpressed in the joints, indicating regulatory roles of IL-1ra in the cytokine network. We thus show that IL-1ra gene deficiency causes autoimmunity and joint-specific inflammation and suggest that IL-1ra is important in maintaining homeostasis of the immune system. Possible involvement of IL-1ra gene deficiency in RA will be discussed.

Published

2000

24. Adenocarcinoma and carcinoid developing spontaneously in the stomach of mutant strains of Mastomys natalensis

Author

Kumazawa, Heiji, Takagi, Hiroshi, Sudo, Katsuko, Nakamura, Wataru, and Hosoda, Syun

Abstract

Summary Neoplastic and nonneoplastic lesions developing spontaneously in antral and fundic mucosae of stomachs of mutant chamois-coloured Z (130 animals) and Y (67 animals) strains of Mastomys aged 18 to 24 months were examined histologically and histochemically. The Z strain developed both antral lesions (hyperplasia 29.2%; dysplasia 23.8%; adenocarcinoma 17.7%) and fundic carcinoid(s) (72.3%). The antral lesions were limited to the lesser curvature near the pyloric ring. Macroscopically, adenocarcinomas resembled human gastric carcinomas of either Borrmann's type I or II. Histochemically, adenocarcinoma cells were characterised by marked reduction of total mucins produced and predominance of mucins with both periodic acid-Schiff and Alcian blue reactivities (neutral and sialated class II mucins). An infiltrating adenocarcinoma was successfully transplanted into nude mice, reaching the 7th generation of transplantations over 4 years, and retained histological features of the primary tumour. The ultrastructural appearance of growing transplanted tumours supported the reduced production of mucins by adenocarcinoma cells with scarcity of mucin granules and intracellular cysts.

Published

1989

25. Immunological properties of athymic nude mice born from homozygous (nu/nu) parents

Author

Kuhara, T., Fujiwara, M., Sudo, Katsuko, Suzuki, K., and Kawamura, A.

Abstract

No significant differences were observed between nude mice (nu/nu) born of homozygous (nu/nu) parents and those born of heterozygous (nu/+) mothers in the percentage of Thy-1-positive cells or immunoglobulin (Ig)-bearing cells in the spleen as assessed by immunofluorescence. There were no significant differences in the antibody response to thymus-dependent antigen or in the number of background plaque-forming cells to this antigen. The antibody response to thymus-independent antigen was not impaired at all in mice born from homozygous parents as compared with other nude mice or euthymic mice. It was concluded that the Thy-1-bearing (T) cells observed in nu/numice and the capacity of these mice to respond to thymus-dependent antigens arose independently of maternal T cells and of the influence of the maternal thymus.

Published

1980

26. Structural polymorphism of murine factor B controlled by a locus closely linked to the H-2 complex and demonstration of multiple alleles

Author

Natsuume-Sakai, Shunnosuke, Moriwaki, Kazuo, Migita, Shunsuke, Sudo, Katsuko, Suzuki, Kiyoshi, Lu, De-Yuan, Wang, Changhuai, and Takahashi, Morinobu

Abstract

New alleles of murine factor B (Bf) protein were demonstrated. When ethylenediaminetetraacetic acid (EDTA)-plasmas from inbred and wild mice were analyzed by isoelectro-focusing (IEF) and immunofixation, murine Bf proteins were visualized as distinct protein bands in all mice tested. Four variants of murine Bf could be demonstrated in a large number of tested mice: Bf 1 (isoelectro-focusing point (P.I.) range of 5.8–6.1) exemplified by B10 and B10.BR, Bf 2 (P.I. range of 5.8–6.0) exemplified by B10.MOL (OHM), Bf 3 (P.I. range of 5.6–5.9) exemplified by B10.MOL (TEN2) and Mus musculus (Mus m.) subspecies Chc, Bf4 (P.I. range of 6.0–6.3) exemplified by Mus m. subspecies Shh. The genetic linkage between S locus and Bf locus was studied with two backcross progenies — [B 10.BR × (B10.BR × Mus m. subspecies Chc)F1] and [B 10.BR × (B10.BR × Mus m. subspecies Shh)F1]. Totally, 256 backcross progenies were typed for Bf type and for Ss type (plasma level of the fourth complement protein regulated by S locus). The results indicated that murine Bf was controlled by a single codominant locus located close to the H-2 complex because no mouse showing recombination between Bf locus and S locus was found.

Published

1983

27. Two Families of Murine Carbohydrate Ligands for E-Selectin

Author

Osanai, Taka, Feizi, Ten, Chai, Wengang, Lawson, Alexander M., Gustavsson, Mikael L., Sudo, Katsuko, Araki, Masatake, Araki, Kimi, and Yuen, Chun-Ting

Abstract

In search of endogenous oligosaccharide ligands for the endothelial adhesion molecule E-selectin in mouse, glycolipids from tissues and the neutrophilic cell line 32D c13 were tested for E-selectin binding. Kidneys of BALB/c and NMRI mice (but not CBA) and the 32D c13 cells were found to contain minor glycolipid populations that support strongly the binding of murine E-selectin. By chromatogram binding experiments andin situliquid secondary ion mass spectrometry (LSIMS) with neoglycolipids derived from their endoglycoceramidase-released oligosaccharides, in conjunction with compositional and linkage analyses, one of the glycolipid ligands in kidney was identified as the Lex-active extended globo-glycolipid:

Published

1996

28. Production of Mice Deficient in Genes for Interleukin (IL)-1α, IL-1β, IL-1α/β, and IL-1 Receptor Antagonist Shows that IL-1β Is Crucial in Turpentine-induced Fever Development and Glucocorticoid Secretion

Author

Horai, Reiko, Asano, Masahide, Sudo, Katsuko, Kanuka, Hirotaka, Suzuki, Masatoshi, Nishihara, Masugi, Takahashi, Michio, and Iwakura, Yoichiro

Abstract

Interleukin (IL)-1 is a major mediator of inflammation and exerts pleiotropic effects on the neuro-immuno-endocrine system. To elucidate pathophysiological roles of IL-1, we have first produced IL-1α/β doubly deficient (KO) mice together with mice deficient in either the IL-1α, IL-1β, or IL-1 receptor antagonist (IL-1ra) genes. These mice were born healthy, and their growth was normal except for IL-1ra KO mice, which showed growth retardation after weaning. Fever development upon injection with turpentine was suppressed in IL-1β as well as IL-1α/β KO mice, but not in IL-1α KO mice, whereas IL-1ra KO mice showed an elevated response. At this time, expression of IL-1β mRNA in the diencephalon decreased 1.5-fold in IL-1α KO mice, whereas expression of IL-1α mRNA decreased >30-fold in IL-1β KO mice, suggesting mutual induction between IL-1α and IL-1β. This mutual induction was also suggested in peritoneal macrophages stimulated with lipopolysaccharide in vitro. In IL-1β KO mice treated with turpentine, the induction of cyclooxygenase-2 (EC 1.14.99.1) in the diencephalon was suppressed, whereas it was enhanced in IL-1ra KO mice. We also found that glucocorticoid induction 8 h after turpentine treatment was suppressed in IL-1β but not IL-1α KO mice. These observations suggest that IL-1β but not IL-1α is crucial in febrile and neuro-immuno-endocrine responses, and that this is because IL-1α expression in the brain is dependent on IL-1β. The importance of IL-1ra both in normal physiology and under stress is also suggested.

Published

1998

29. Prenatal aqueductal stenosis as a cuase of congenital hydrocephalus in the inbred at LEW/Jms

Author

Yamada, Hiroshi, Oi, Shizuo, Tamaki, Norihiko, Matsumoto, Satoshi, and Sudo, Katsuko

Abstract

We studied the microscopic morphological changes in congenital hydrocephalus in the inbred rat, LEW/Jms, on gestational days 17, 18, and 20 and during the neonatal period to clarify the etiopathogenesis, focusing particularly on the aqueductal changes. At 1 day of age, ventriculomegaly was limited to the lateral and III ventricles, and the aqueduct was obstructed, with the appearance of simple stenosis. On gestational days 20 and 18, the hydrocephalic rats showed occluded aqueducts, which paralleled the finding of hydrocephalus in the newborn rats. On gestational day 17, all eight models examined showed the same size ventricles. However, an aqueductal obstruction was observed in one of them. The other seven rats showed the aqueduct patent. From these observations, it can be concluded that the rat shows an aqueductal obstruction on gestational day 17 and appears to develop hydrocephalus with age. The aqueductal obstruction was considered to be the primary change and not a secondary phenomenon. The site of obstruction was the anterior part of the aqueduct (level of anterior colliculus) at every stage. Aqueductal obstruction following the developmental anomaly of the midbrain in the embryonic stage might thus be the primary cause of congenital hydrocephalus in rats LEW/Jms.

Published

1991

30. Histological changes in the midbrain around the aqueduct in congenital hydrocephalic rat LEW/Jms

Author

Yamada, Hiroshi, Oi, Shizuo, Tamaki, Norihiko, Matsumoto, Satoshi, and Sudo, Katsuko

Abstract

Primary aqueductal stenosis is one of the main causes of congenital hydrocephalus in humans and experimental models. The congenitally hydrocephalic rat strain LEW/Jms is one such model. In this report, we describe further detailed histological features of periaqueductal structure, including the posterior commissure, subcommissural organ (SCO), and ependyma, and discuss the changes in these structures in relation to the cause of hydrocephalus. Coronal sections of the aqueduct in normal rats showed that the usual ependyma was absent in the center of the base facing the dorsal side, which was replaced by tall columnar cells. On the other hand, in hydrocephalic rats the ependyma encircled the aqueductal cavity. In midline sagittal sections, normal and hydrocephalic rats showed the SCO, although the SCO in hydrocephalic rats was shorter than in normal rats. There was also a marked difference between normal and hydrocephalic rats in the dorsoventral dimension of the rostral midbrain. In hydrocephalus, this dimension was large in comparison with normal rats. The superior collicular commissure located caudal to the posterior commissure ran along the ventral side of the midbrain in rats with hydrocephalus, and there was a cell-depleted area just dorsal to the superior collicular commissure. The same findings were observed from the 17th day of gestation until the postnatal period. Although the role of the SCO has been widely discussed from the viewpoint of secretory function, the present study indicated that this organ might be involved in the formation of the shape of the aqueduct.

Published

1992

31. Cloned origin of DNA replication in c-myc gene can function and be transmitted in transgenic mice in an episomal state

Author

Sudo, Katsuko, Ogata, Masaaki, Sato, Yoshinari, Iguchi-Ariga, Sanae M.M., and Ariga, Hiroyoshi

Abstract

The c-myc protein has recently been shown to interact with a region possessing putative origin of DNA replication and enhancer activities located 2 kb upstream of the c-myc gene itself. Transgenic mice were obtained by injecting constructs containing this region, termed pmyc(H-P), into fertilized mouse eggs. The transgenic elements were capable of efficient replication in all mouse tissues examined and were maintained in an episomal state even in highly differentiated cells. Moreover, pmyc(H-P) was transmittable to the progeny throughout several generations, which suggests that the fragment derived from the region upstream of the c-myc gene possesses sequences necessary for partition, stability and DNA replication of the plasmid in the cells. In addition, we have shown that the plasmid might be captured only by eggs, not by sperm.

Published

1990