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1. P171 Peripheral monocyte fraction in patients with infective endocarditis

Author

K. Ise, T. Tomono, K. Kida, Y. Nagata, N. Sakai, N. Mitsuya, T. Ohno, M. Okuda, and T. Makiishi

Subjects
Microbiology (medical), Pathology, medicine.medical_specialty, business.industry, Monocyte, Fraction (chemistry), General Medicine, medicine.disease, Peripheral, Infectious Diseases, medicine.anatomical_structure, Infective endocarditis, medicine, Pharmacology (medical), In patient, business
Published
2013
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2. Status of NAT screening for HCV, HIV and HBV: experience in Japan

Author

T, Tomono, H, Murokawa, K, Minegishi, R, Yamanaka, H Y, Lizuka, M, Miyamoto, S, Satoh, S, Nakahira, T, Murozuka, H, Emura, Y, Doi, H, Mine, S, Yokoyama, H, Ohnuma, T, Tanaka, A, Yoshikawa, and K, Nishioka

Subjects
Hepatitis B virus, Blood Donors, Hepacivirus, Red Cross, Blood, Japan, DNA, Viral, Hepatitis Viruses, HIV-1, Humans, Mass Screening, RNA, Viral, Blood Transfusion, Viremia, Nucleic Acid Amplification Techniques
Abstract

The first nationwide nucleic acid amplification testing (NAT) for hepatitis B virus (HBV), hepatitis C virus (HCV), and human immunodeficiency virus type 1 (HIV-1) of voluntarily donated blood after serological pre-screening and before release of cellular components and plasma for fractionation was implemented by the Japanese Red Cross Blood Transfusion Services. The NAT screening assay using multiplex reagent is time-saving, cost effective, and labour-saving procedure for all blood and blood products including short-shelf life platelets. During the 50-mini-pool NAT screening of serologically negative donations (February 1, 2001-April 30, 2001), we were able to screen out 112 HBV-positive, 25 HCV-positive, and 4 HIV-1 positive units from blood and blood components.

Published
2002

3. A pilot study on developing a new ambiguity tolerance scale

Author

T. Tomono

Subjects
Correlation, Scale (social sciences), media_common.quotation_subject, Construct validity, Trait anxiety, Ambiguity, Psychology, Social psychology, General Psychology, Reliability (statistics), Exploratory factor analysis, Ambiguity tolerance, media_common
Abstract

In this study, the author developed a new ambiguity tolerance scale (ATS), which could assess ambiguity tolerance more positively than similar ambiguity tolerance scales developed previously. Scale items were created by referring to past studies. All items were designed to end with phrases implying ‘can’ tolerate ambiguity instead of implying ‘cannot’ tolerate ambiguity. The participants were 205 male and female college students, who completed the ATS and a trait anxiety scale. Two factors were extracted in an exploratory factor analysis of the ATS ‘the ability to control ambiguity’ and ‘the ability to enjoy ambiguity’. In addition, each subscale’s internal consistency was sufficiently high. The correlation coefficients between both scales were statistically significant. These results suggested that the reliability and validity of the ATS were partly confirmed. However, this study did not examine test–retest reliability and another view of construct validity. Further studies should address this.

Published
2014
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6. Reconstruction of late laryngo-tracheal stenosis in a one stage operation by cervical flap and cartilage transplantation

Author

Kiyoshi Matsuo, T. Tomono, Katsura Yamamoto, and T. Hirose

Subjects
Larynx, medicine.medical_specialty, business.industry, medicine.medical_treatment, Lumen (anatomy), Stent, Costal cartilage, medicine.disease, Surgery, Tracheal Stenosis, Plastic surgery, Stenosis, medicine.anatomical_structure, Cartilage transplantation, medicine, Radiology, business
Abstract

An operation has been devised to produce a one stage correction of cases with stenosis of the larynx and trachea. The scar tissue of the stenotic area is resected. To reconstruct the inner lining of the lumen, a cervical pedicle flap is inserted. To insure a stable structural framework, costal cartilage is usually used. A stent is inserted into the lumen by using a rubber glove finger packed with silicon sponge to maintain an adequate air passage for about four weeks. The external covering is achieved by direct closure. The tracheostome should remain open for four to six months. In ten cases, all obtained satisfactory results by this method.

Published
1986
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7. Synthesis and esterolytic reactions of linear and cross-linked asymmetric imidazole-containing polymers

Author

R. J. Schiavone, T. Tomono, and C. G. Overberger

Subjects
chemistry.chemical_classification, Polymers and Plastics, Organic Chemistry, Polymer, Hydrophobic effect, Solvent, chemistry.chemical_compound, chemistry, Nucleophile, Polymer chemistry, Materials Chemistry, Imidazole, Solvolysis, Enantiomer, Alkyl
Abstract

Asymmetric linear and cross-linked imidazole-containing polymers were prepared from 1-[2(S)-methylbutyl]-4-vinylimidazole and 1-[2(S)-methylbutyl]-5-vinylimidazole. The esterolytic reactions of these linear and cross-linked asymmetric polymers with the enantiomeric substrates (R)- and (S)-4-(3-methylpentadecanoyl)-3-nitrobenzoic acid, (R)- and (S)-S, were studied by measuring the pseudo-first order kinetics of the solvolysis of these enantiomeric substrates in the presence of these asymmetric polymers. The linear homopolymers and copolymers of 1-[2(S)-methylbutyl]-4- and 5-vinylimidazole showed hydrophobic and electrostatic effects in the solvolysis of the enantiomeric substrates with these linear asymmetric polymers. Cross-links were introduced into these asymmetric polymers to increase the rigidity and reduce the number of conformations available to the polymer. The reduced conformational mobility was expected to enhance any enantioselectivity in the solvolysis of the enantiomeric substrates with these polymers. Using these cross-linked polymers, hydrophobic interactions were observed in the solvolysis of a series of substrates with increasing alkyl chain length. Also, on changing the polarity of the solvent, a bell-shaped rate profile was observed in the solvolysis of the long chain substrate S. This effect was attributed to a combination of the coiling of the cross-linked polymer chains and hydrophobic interactions with the substrate on changing solvent polarity. Even with the increased rigidity of these cross-linked polymers, no significant enantioselectivity in the solvolysis of the enantiomeric substrates was observed. So, neither the linear nor the cross-linked asymmetric polyvinylimidazoles showed enantioselectivity in the solvolysis of these enantiomeric substrates. In this case, the hydrophobic interactions and the reduced conformational mobility through crosslinking were not strong enough to bring about enantioselectivity in the solvolysis of these enantiomeric substrates.

Published
1987
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8. General lectures (II)

Author

Y. Karasawa, H. Ōnuma, H. Suzuki, T. Okazaki, A. Yasui, T. Murakami, K. Furuya, M. Ohtsuki, H. Sata, T. Kondo, H. Takada, K. Kawaguchi, S. Sai, S. Takeda, M. Kitagawa, T. Morooka, T. Shiraishi, M. Namiki, H. Kawauchi, K. Nakagawa, H. Kuramata, Y. Yamaguchi, T. Kabakino, T. Inokuchi, J. Wakisaka, Y. Yamauchi, T. Debuchi, W. Ogo, C. Yamasaki, M. Sigemori, K. Hashimoto, T. Shirozu, N. Kaibara, K. Inokuchi, K. Soejima, T. Hiyama, M. Wakita, T. Ikemoto, H. Hayasaka, S. Fukui, T. Takeda, N. Aoyama, Y. Takada, Y. Saheki, Y. Yoshida, K. Minagawa, T. Okuyama, S. Yamamitsu, Y. Konishi, N. Ishimatsu, S. Murai, A. Nukaga, S. Toyama, Y. Watanabe, N. Mizushima, M. Abe, K. Maruyama, K. Yoshino, T. Suzuki, K. Akisato, M. Kitajima, T. Tabata, M. Hashimoto, T. Tanaka, Y. Nakagawa, Y. Ishii, M. Inoue, S. Katayama, Y. Nakano, M. Fukuda, M. Takaki, H. Hyodo, J. Kobayashi, H. Nishikawa, K. Morimoto, T. Takagi, S. Sako, H. Tomoda, M. Furusawa, R. Sassa, T. Unuma, T. Iwase, T. Yoshioka, M. Kusakabe, M. Iio, S. Kobayashi, M. Kizu, T. Kasugai, K. Yoshida, T. Kembo, T. Yoshida, Y. Suga, T. Suguro, Y. Kono, S. Mitsui, Y. Nagamachi, T. Nakamura, H. Suto, T. Higuchi, M. Onai, K. Isizuka, A. Takei, M. Simoda, T. Sekiguchi, K. Shichijo, Y. Akashi, K. Mori, K. Ogasawara, R. Tanaka, K. Yoshikawa, T. Takahashi, T. Ogata, S. Tanaka, T. Seito, H. Matsuda, T. Imajo, K. Moriyasu, Y. Takata, H. Kamei, H. Murai, T. Takemitsu, T. Kanemitsu, M. Ishii, M. Imaizumi, M. Inada, G. B. J. Glass, K. Ebata, N. Yamanaka, S. Watanabe, H. Mori, S. Tsukasa, H. Sato, Y. Chuman, N. Nakahara, H. Taniguchi, S. Ehira, M. Hori, T. Irisa, H. Yokoyama, T. Kunieda, Y. Ogushi, K. Kawakami, M. Kuroda, D. Sasaki, S. SŌma, S. Yanagiya, A. Munakata, F. Matsunaga, M. Abiko, H. Ohuchi, C. Tai, T. Kawashima, W. Oosawa, H. Asakura, H. Senba, T. Hatayama, K. Yukawa, T. Konishi, M. Miyata, H. Shimazu, T. Kinoshita, K. Nukada, T. Yamagishi, K. Harada, S. Nakano, T. Sakai, K. Shindo, K. Fukushima, S. Odagiri, K. Tarao, Y. Saito, K. Ohara, S. Sasaki, T. Tomoda, N. Kaneda, H. Yamaguchi, T. Hayashi, J. Suzuki, Y. Kofune, A. Urase, A. Yamagata, N. Sugino, M. Hatano, K. Oshima, T. Tanabe, M. Ohto, K. Okuda, E. Mitani, S. Yamamoto, K. Kobayashi, T. Ono, T. Kamata, S. Mohri, H. Makiishi, A. Kitano, S. Tatumi, S. Mizuno, K. Tsumori, T. Shimizu, K. Nomatsu, H. Hiratsuka, M. Ichinose, T. Morishita, A. Morita, S. Matsuzaki, M. Oda, K. Kamegaya, M. Tuchiya, K. Sambe, Y. Murakami, A. Machii, Y. Nitta, Y. Aiso, N. Kitahara, M. Sato, Y. Yoshizawa, Y. Hishinuma, H. Nagasako, Y. Nao, H. Harada, K. Mishima, Y. Yamagata, M. Mandai, Y. Kondo, Y. Uchida, S. Takizawa, S. Kinoshita, T. Kurihara, K. Sakumoto, H. Okamoto, S. Sakurai, S. Ishitobi, H. Tanaka, K. Ishihara, N. Kuno, I. Aoki, Y. Horiguchi, K. Kitamura, M. Miwa, K. Okada, Y. Endo, M. Tatsuta, T. Morii, S. Okuda, H. Tamura, K. Fukuda, K. Sato, K. Koizumi, T. Takebe, S. Yamagata, S. Noda, Y. Toda, T. Hayakawa, S. Nakajima, S. Hitokawa, N. Sawabu, S. Hirose, A. Takada, J. Takeuchi, Y. Kuniyasu, H. Kakehi, G. Uchiyama, N. Arimizu, T. Kuroda, H. Saishyo, T. Takashima, M. Shin, M. Akashi, T. Moriyama, M. Uchimura, R. Tsuchiya, G. Kakizaki, N. Noto, T. Oizumi, T. Soeno, T. Maeta, T. Saito, S. Naito, K. Shimizu, T. Nakajima, M. Tanaka, T. Kin, S. Sugiyama, H. Takayama, T. Tomono, N. Kamijo, Y. Kimura, T. Matsuo, M. Shimada, B. Terashima, S. Furuta, K. Kashiwabara, S. Oka, M. Sugiura, M. Karasawa, K. Ito, K. Takei, Y. Ishihara, A. Kuroda, N. Sato, T. Noro, H. Ishikawa, Y. Tajima, S. Hashihira, T. Nishii, R. Mori, Y. Takeda, T. Yamadori, A. Wakabayashi, S. Iwata, M. Shiraso, K. Tokutake, S. Matsuno, N. Haga, Y. Suda, T. Sato, T. Tsunoda, H. Kanno, Y. Aneha, K. Kikuchi, K. Imamura, O. Kondo, Y. Yuki, S. Omata, S. Okamoto, H. Nagahara, H. Motoyama, H. Watanabe, T. Maekawa, T. Miyakawa, Y. Anazawa, T. Motoyama, T. Kawamura, Y. Kusaka, F. Shima, S. Abe, S. Ichihara, M. Nomura, T. Ushiyama, S. Futagawa, M. Ishida, G. Obata, Y. Sugiyama, K. Suzuki, M. Abo, M. Takeuchi, E. Tann, K. Kimura, A. Iwaya, H. Takahashi, K. Ono, J. Inoue, S. Miyaishi, T. Sasaki, Y. Kuroyanagi, H. Kato, C. Kido, K. Hibino, M. Kishikawa, T. Takeuchi, H. Murate, A. Tanabe, M. Kozuka, M. Ito, N. Kato, Y. Yazaki, K. Goto, M. Miyaji, J. Yokoi, I. Endo, S. Kato, M. Miyazaki, N. Murayama, A. Kawamura, B. Murohisa, S. Hirai, M. Furukawa, G. Nakashima, H. Furuse, T. Fukuda, F. Hanyu, N. Sakakibara, H. Ide, K. Momma, H. Nagashima, T. Matsushiro, N. Suzuki, T. Saitoh, N. Nakamura, W. Takahashi, T. Hatanaka, N. Kobayashi, M. Hagano, T. Furusawa, T. Osuga, O. W. Portman, K. Takahashi, H. Kibayashi, H. Yamazaki, K. Komaki, H. Tanimura, Y. Hikasa, R. Ogawa, H. Nakagawa, M. Osada, H. Koizumi, M. Katayama, H. Sakamoto, T. Manome, M. Sesoko, M. Kobayashi, Y. Komine, N. Watanabe, Y. Okabe, M. Ogino, T. Naruke, T. Hoshika, T. Miyano, K. Tsuneoka, S. Kitajima, I. Nakada, Y. Sasamori, H. Munakata, K. Tanaka, H. Oguro, T. Numata, K. Oh-Uti, S. Goto, K. Takashina, G. Sasaki, A. Kimura, T. Sasagawa, G. Takahashi, H. Sugiyama, K. Iwaki, S. Okada, M. Iwasaki, Y. Kawashima, H. Kaneda, T. Honda, K. Ariga, Woo pak Sa, H. Hozawa, T. Susuki, Y. Kato, T. Mizuno, H. Oya, S. Yoshino, and T. Hattori

Subjects
Gastroenterology
Published
1973
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9. Studies on Toxoplasmosis

Author

K. Shinohara, S. Kobayashi, O. Kinoshita, M. Ikeda, T. Tomono, S. Semba, Hisao Iwasaki, N. Kaneko, H. Takashino, N. Watanabe, K. Utsuki, G. Kosuge, S. Kawashima, S. Akane, H. Naito, T. Sudo, S. Yoshida, K. Tanaka, H. Tomioka, M. Suzuki, and T. Iwasaki

Subjects
business.industry, Immunology, Medicine, business, medicine.disease, Toxoplasmosis
Published
1964
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12. [One-stage resected case of dumbbell type tumor of the posterior mediastinum]

Author

K, Nagai, H, Hiyoshi, T, Tomono, Y, Matsushima, R, Amamiya, K, Oho, and Y, Hayata

Subjects
Adult, Male, Spinal Neoplasms, Humans, Mediastinal Neoplasms, Neurilemmoma
Abstract

We reported a dumbbell type tumor of the posterior mediastinum. The patient was an asymptomatic 40-year-old male. An abnormal shadow in the right lower lung field was pointed out in a mass survey. We recognized a dumbbell type tumor in the posterior mediastinum by chest CT and MRI. The tumor invaded the intervertebral canal through the spinal foramen. It was most clearly seen by MRI myelography. Operation was performed with the patient in a prone position and with an L-shaped skin incision of the back and 11th intracostal thoracotomy and Th11 laminectomy. The dumbbell type tumor was completely removed by this operation. The pathological diagnosis was Schwannoma. The post operative course was good. The one-stage operation is useful for dumbbell type tumors of the posterior mediastinum.

Published
1989

15. [A cytologic diagnosis of breast secretions--application of cytology to the mass survey of breast cancer]

Author

M, Fujii, Y, Ishii, M, Nagao, T, Wakabayashi, S, Fukahori, A, Goto, T, Tomono, and K, Hagiwara

Subjects
Adult, Breast Diseases, Cytodiagnosis, Nipples, Humans, Breast Neoplasms, Female, Breast, Middle Aged
Abstract

From January 1982 to March 1987, an exfoliative cytological examination of abnormal nipple discharge was carried out on 790 patients. Of 22 histologically confirmed mammary carcinomas, 7 cases (31.8%) were diagnosed as positive by conventional cytologic techniques. By using the concentration method, in which the nipple secretion was collected in a series of testings that lasted 3 to 5 days and stored in a glass tube containing a fixative, the diagnostic accuracy was seen to increase significantly and 9 out of 15 malignant cases (60.0%) were accurately diagnosed as having cancer. Moreover, all 5 cases without any palpable mass were found to be positive by the smears made by this procedure.

Published
1988

19. RECENT DEVELOPMENTS IN THE USE OF POLYMERS AS REACTANTS IN ORGANIC REACTIONS

Author

Yusuke Kawakami, C. G. Overberger, A. Meenakshi, A. C. Guterl, T. Tomono, and L. J. Mathias

Subjects
chemistry.chemical_classification, Polymer science, Organic reaction, Chemistry, Reactivity (chemistry), Polymer
Abstract

In a review article [Accounts Chem. Res., 2, 217 (1969)] is a summation of our work up to 1968. In this review we summarized the activity of polyvinylimidazole and copolymers in esterolytic reactions. We explained the increased reactivity of these polymeric reactants in terms of cooperative effects and electrostatic factors. In 1967, we blundered into the extremely interesting discovery that long-chain esters provided us with enormous acceleration of rates at room temperature and we have attributed this in “general” terminology to apolar bonding as a third factor to understand the high reactivity of these synthetic macromolecules. Reference 1 describes our recent published work. We are heavily emphasizing the apolar bonding concept. Related work which conceptually can be regarded as similar to our own discovery was carried out by the group of Professor Irving M. Klotz at Northwestern (2), the group of Professor Kabanov at the University of Moscow (3), and the group of Professor Kunitake (4).

Published
1979
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21. Effectiveness of HPD and radiation therapy in lung cancer

Author

H, Kato, C, Konaka, J, Ono, Y, Matsushima, K, Nishimiya, J, Lay, H, Sawa, H, Shinohara, T, Saito, K, Kinoshita, T, Tomono, M, Aida, and Y, Hayata

Subjects
Adult, Male, Lung Neoplasms, Adenocarcinoma, Middle Aged, Hematoporphyrins, Photochemotherapy, Carcinoma, Squamous Cell, Humans, Female, Hematoporphyrin Derivative, Carcinoma, Small Cell, Melanoma, Aged, Neoplasm Staging
Published
1983

24. [ON VOLVULUS OF THE GALLBLADDER]

Author

A, SHIROTA, K, TOMITA, and T, TOMONO

Subjects
Radiography, Torsion Abnormality, Adolescent, Japan, Geriatrics, Surgical Procedures, Operative, Humans, Gallbladder Diseases, Child, Intestinal Volvulus
Published
1964

25. Immunoserogical studies on the production of cholecystitis

Author

T. Tomono, K. Tomita, M. Matsunaga, Akiro Shirota, Yasuhito Shimizu, K. Iioka, Masahiko Onda, M. Miki, H. Yokota, S. Matsukura, M. Endo, E. Wada, Y. Ichikawa, Y. Iida, H. Hattori, G. Fujishima, T. Hakozaki, and T. Tanaka

Subjects
medicine.medical_specialty, Surgical oncology, business.industry, General surgery, Internal medicine, Gastroenterology, medicine, Cholecystitis, Hepatology, medicine.disease, business, Colorectal surgery, Abdominal surgery
Published
1966
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27. Studies on diagnoses of pancreas diseases by the universal coelomoscope : (V)

Author

Y. Kimura, K. Shimada, Masayuki Oda, T. Matsuo, N. Kamijo, H. Takayama, T. Tomono, K. Takei, H. Takahashi, M. Sugiura, S. Oka, K. Ito, M. Karasawa, and Y. Hagiwara

Subjects
medicine.medical_specialty, business.industry, General surgery, Gastroenterology, Hepatology, Colorectal surgery, Pancreas diseases, Surgical oncology, Internal medicine, medicine, Medical diagnosis, business, Abdominal surgery
Published
1972
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29. Validation of the Absorption-Enhancing Ability of Oligoarginines Grafted onto a Backbone of Hyaluronic Acid through Animal Studies from Rodents to Primates.

Author

Yagi H, Tomono T, Abe K, Tsutsumi Y, Makabe M, Mitsuhashi H, Kimura T, Kobayashi H, Miyata K, Shigeno K, and Sakuma S

Subjects
Animals, Mice, Male, Administration, Intranasal, Nasal Mucosa metabolism, Nasal Mucosa drug effects, Macaca fascicularis, Nasal Absorption drug effects, Arginine chemistry, Hyaluronic Acid chemistry
Abstract

The purpose of our research is to develop functional additives that enhance mucosal absorption of biologics, such as peptide/protein and antibody drugs, to provide their non-to-poor invasive dosage forms self-managed by patients. Our previous in vivo and in vitro studies demonstrated that the intranasal absorption of biologics in mice was significantly improved when coadministered with oligoarginines anchored chemically to hyaluronic acid via a glycine spacer, presumably through syndecan-4-mediated macropinocytosis under activation by oligoarginines. The present mouse experiments first revealed that diglycine-L-tetraarginine-linked hyaluronic acid significantly enhanced the intranasal absorption of sulpiride, which is a poor-absorptive organic compound with a low molecular weight. However, similar enhancement was not observed for levofloxacin, which has a similarly low molecular weight but is a well-absorptive organic compound, probably because its absorption was mostly dominated by passive diffusion. The subsequent monkey experiments revealed that there was no species difference in the absorption-enhancing ability of diglycine-L-tetraarginine-linked hyaluronic acid for not only organic compounds but also biologics. This was presumably because the expression levels of endocytosis-associated membrane proteins on the nasal mucosa in monkeys were almost equivalent to those in mice, and poorly membrane-permeable/membrane-impermeable drugs were mainly absorbed via syndecan-4-mediated macropinocytosis, regardless of animal species. Drug concentrations in the brain assessed in mice and monkeys and those in the cerebral spinal fluids (CSFs) assessed in monkeys indicated that drugs would be delivered from the systemic circulation to the central nervous system by crossing the blood-brain and the blood-CSF barriers under coadministration with the hyaluronic acid derivative. In line with our original hypothesis, this new set of data supported that our oligoarginine-linked hyaluronic acid would locally perform on the mucosal surface and enhance the membrane permeation of drugs under its colocalization.

Published
2024
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30. The Improved Antigen Uptake and Presentation of Dendritic Cells Using Cell-Penetrating D-octaarginine-Linked PNVA-co-AA as a Novel Dendritic Cell-Based Vaccine.

Author

Fujioka Y, Ueki H, A R, Sasajima A, Tomono T, Ukawa M, Yagi H, Sakuma S, Kitagawa K, and Shirakawa T

Subjects
Animals, Mice, Cell Line, Tumor, Oligopeptides chemistry, Female, Mice, Inbred C57BL, Cell-Penetrating Peptides chemistry, Dendritic Cells immunology, Cancer Vaccines immunology, Antigen Presentation immunology
Abstract

Cancer immunotherapy using antigen-pulsed dendritic cells can induce strong cellular immune responses by priming cytotoxic T lymphocytes. In this study, we pulsed tumor cell lysates with VP-R8, a cell-penetrating D-octaarginine-linked co-polymer of N-vinylacetamide and acrylic acid (PNVA-co-AA), into the DC2.4 murine dendritic cell line to improve antigen uptake and then determined the anti-tumor effect in tumor-bearing mice. DC2.4 cells were pulsed with the cell lysate of EL4, a murine lymphoma cell line, and VP-R8 to generate the DC2.4 vaccine. For the in vivo study, DC2.4 cells pulsed with EL4 lysate and VP-R8 were subcutaneously injected into the inguinal lymph node to investigate the anti-tumor effect against EL4 and EL4-specific T cell immune responses. VP-R8 significantly improved antigen uptake into DC2.4 compared to conventional keyhole limpet hemocyanin ( p < 0.05). The expression of MHC class I, MHC class II, and CD86 in DC2.4 cells significantly increased after pulsing tumor lysates with VP-R8 compared to other treatments ( p < 0.05). The intra-lymph node injection of DC2.4 pulsed with both VP-R8 and EL4 lysate significantly decreased tumor growth compared to DC2.4 pulsed with KLH and lysates ( p < 0.05) and induced tumor-infiltrating CD8T cells. The DC2.4 vaccine also remarkably increased the population of IFN-gamma-producing T cells and CTL activity against EL4 cells. In conclusion, we demonstrated that VP-R8 markedly enhances the efficiency of dendritic cell-based vaccines in priming robust anti-tumor immunity, suggesting its potential as a beneficial additive for dendritic cell-based immunotherapy.

Published
2024
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31. Approaching Process in Walking through an Aperture for Individuals with Stroke.

Author

Muroi D, Kodama K, Tomono T, Saito Y, Koyake A, and Higuchi T

Subjects
Humans, Walking, Biomechanical Phenomena, Stroke complications, Stroke Rehabilitation methods
Abstract

Muroi et al. show that individuals with stroke have improved collision avoidance behavior when passing through an aperture while entering from the paretic-side of the body. However, the underlying mechanism remains unknown. We reanalyzed Muroi et al.'s data to reveal how individuals with stroke walk through an aperture by examining changes in walking velocity and behavioral complexity (i.e., sample entropy, an index of (ir)regularity of time series, regarded lower entropy as more regular and less complex) by focusing on the approaching process. The results showed that individuals with stroke reduced their walking velocity and behavioral complexity before passing through the narrow aperture when approaching from the paretic side. We interpreted that the improved obstacle avoidance when penetrating from the paretic side may be due to careful body rotation and adjusting the walking velocity in advance.

Published
2024
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32. Mucosal absorption of antibody drugs enhanced by cell-penetrating peptides anchored to a platform of polysaccharides.

Author

Tomono T, Yagi H, Igi R, Tabaru A, Fujimoto K, Enomoto K, Ukawa M, Miyata K, Shigeno K, and Sakuma S

Subjects
Rats, Mice, Animals, Hyaluronic Acid pharmacology, Ranibizumab, Nasal Mucosa metabolism, Antibodies, Drug Carriers chemistry, Administration, Intranasal, Cell-Penetrating Peptides chemistry
Abstract

Our previous studies demonstrated that L-octaarginine grafted onto hyaluronic acid via a tetraglycine spacer significantly enhanced intranasal absorption of protein drugs with a molecular weight (Mw) of 22 kDa or less. The present study focused on its potential as an absorption enhancer for antibody drugs with a larger Mw and the enhancement mechanism. When ranibizumab (48 kDa) alone was intranasally administered in mice, its absolute bioavailability was 0.67% on average. The mean bioavailability elevated to 6.2% under coadministration with tetraglycine-L-octaarginine-linked hyaluronic acid. A similar result was observed under substitution of ranibizumab with certolizumab pegol (91 kDa), although bioavailability itself decreased with the Mw increase, irrespective of coadministration with the hyaluronic acid derivative. Rat experiments also revealed that coadministration with the polysaccharide derivative resulted in significant enhancement of intranasal absorption of trastuzumab (148 kDa). In vitro studies using gene-knocked down cells indicated that syndecan-4-induced macropinocytosis played a crucial role on acceleration of antibody uptake into epithelial cells on the nasal mucosa, irrespective of their Mw. It appeared that neither clathrin heavy chain nor caveolin-1 involved in cellular uptake of antibodies. Tetraglycine-L-octaarginine-linked hyaluronic acid was concluded to be a promising delivery tool that possessed universal absorption-enhancing abilities independent to Mw of biologics., Competing Interests: Declaration of Competing Interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Takumi Tomono reports financial support was provided by Japan Society for the Promotion of Science. Takumi Tomono reports financial support was provided by Mochida Memorial Foundation for Medical and Pharmaceutical Research. Shinji Sakuma reports a relationship with Japan Society for the Promotion of Science that includes: funding grants. Takumi Tomono reports a relationship with Kurata Grants that includes: funding grants., (Copyright © 2023. Published by Elsevier B.V.)

Published
2023
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33. Performance of Cell-Penetrating Peptides Anchored to Polysaccharide Platforms Applied via Various Mucosal Routes as an Absorption Enhancer.

Author

Yagi H, Tomono T, Handa Y, Saito N, Ukawa M, Miyata K, Shigeno K, and Sakuma S

Subjects
Mice, Animals, Nasal Mucosa metabolism, Dextrans pharmacology, Hyaluronic Acid metabolism, Administration, Intranasal, Cell-Penetrating Peptides chemistry, Human Growth Hormone metabolism, Human Growth Hormone pharmacology
Abstract

We have been investigating the potential of cell-penetrating peptides anchored to polymeric platforms as a novel absorption enhancer which delivers biologics into systemic circulation via mucosal routes. Our previous mouse experiments demonstrated that hyaluronic acid modified with l-octaarginine, a typical cell-penetrating peptide, via a tetraglycine spacer significantly enhanced the mucosal absorption of protein drugs applied into the nasal cavities, irrespective of the molecular weights ( M w ) of the drugs. The present study evaluated the performance of tetraglycine-l-octaarginine-linked hyaluronic acid applied via various mucosal routes. Somatropin ( M w : ca. 22.1 kDa) was moderately absorbed from the lung mucosa, and the mean absolute bioavailability (BA) reached 19% under enhancer-free conditions; nevertheless, its BA under intranasal administration was approximately 1% or less. Its BA significantly elevated to 46% on average through intrapulmonary coadministration with tetraglycine-l-octaarginine-linked hyaluronic acid. When the administration site was replaced with the oral cavities, an extreme reduction in somatropin absorption was observed with a mean BA of 0.056% under enhancer-free conditions. Intraoral coadministration with tetraglycine-l-octaarginine-linked hyaluronic acid resulted in a 6.3-fold elevation of somatropin absorption with statistical significance. A similar enhancement was observed under intrarectal administration with a further reduction in BA. On the other hand, the hyaluronic acid derivative did not exhibit the absorption-enhancing ability under intragastric administration, probably due to the lack of stabilization effects against enzyme-susceptible biologics. The results indicated that the intrapulmonary route was suitable for maximizing the mucosal absorption of biologics, and that there was a likelihood of the intraoral route with user convenience. When somatropin was substituted with fluorescein isothiocyanate-conjugated dextran with an average M w range of 4-70 kDa, similar phenomena were observed under intrapulmonary and intranasal administration. BA decreased with an increase in the M w of dextran; however, the ratio of BA under enhancer-present conditions to that under enhancer-free conditions was consistently around 3, indicating that the performance of the hyaluronic acid derivative was M w -independent, irrespective of the administration route.

Published
2023
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34. Enzyme-embedded electrospun fiber sensor of hydrophilic polymer for fluorometric ethanol gas imaging in vapor phase.

Author

Iitani K, Nakaya M, Tomono T, Toma K, Arakawa T, Tsuchido Y, Mitsubayashi K, and Takeda N

Subjects
Alcohol Dehydrogenase chemistry, Breath Tests methods, Ethanol metabolism, Gases, Humans, Polymers, Biosensing Techniques methods, Volatile Organic Compounds
Abstract

Non-invasive measurement of volatile organic compounds (VOCs) emitted from living organisms is a powerful technique for diagnosing health conditions or diseases in humans. Bio-based gas sensors are suitable for the sensitive and selective measurement of a target VOC from a complex mixture of VOCs. Conventional bio-based sensors are normally prepared as wet-type probes to maintain proteins such as enzymes in a stable state, resulting in limitations in the commercialization of sensors, their operating environment, and performance. In this study, we present an enzyme-based fluorometric electrospun fiber sensor (eFES) mesh as a gas-phase biosensor in dry form. The eFES mesh targeting ethanol was fabricated by simple one-step electrospinning of polyvinyl alcohol with an alcohol dehydrogenase and an oxidized form of nicotinamide adenine dinucleotide. The enzyme embedded in the eFES mesh worked actively in a dry state without pretreatment. Substrate specificity was also maintained, and the sensor responded well to ethanol with a sufficient dynamic range. Adjustment of the pH and coenzyme quantity in the eFES mesh also affected enzyme activity. The dry-form biosensor-eFES mesh-will open a new direction for gas-phase biosensors because of its remarkable performance and simple fabrication, which is advantageous for commercialization., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published
2022
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35. A PCR-amplified transgene fragment flanked by a single copy of a truncated inverted terminal repeat for recombinant adeno-associated virus production prevents unnecessary plasmid DNA packaging.

Author

Adachi K, Tomono T, Okada H, Shiozawa Y, Yamamoto M, Miyagawa Y, and Okada T

Subjects
DNA Packaging, Plasmids genetics, Polymerase Chain Reaction, Terminal Repeat Sequences genetics, Transgenes, Dependovirus genetics, Genetic Vectors genetics
Abstract

The application of recombinant adeno-associated viruses (rAAVs) for gene therapy faces certain challenges, including genome packaging of non-vector sequences. Inverted terminal repeats (ITRs) flanking the rAAV genome, comprising three inverted repeat regions (A, B, and C) and a non-inverted repeat region (D), contribute to non-vector genome packaging. We aimed to circumvent this issue by comparing the properties of rAAV containing DNA plasmids and PCR-amplified transgenes, including a single copy of the AD sequence (rAAV-pAD/L-AD, respectively), which is a truncated form of ITR, with those of wild-type ITR genome (single-stranded and self-complementary AAV; ssAAV and scAAV). The packaging efficiency of rAAV-pAD/L-AD was found to be comparable to that of scAAV, whereas the transduction efficiency of rAAV-pAD/L-AD was lower than that of ss/scAAV. Remarkably, rAAV-L-AD reduced the plasmid backbone packaging contamination compared to ss/scAAV. Furthermore, to confirm the functionality of this system, we generated a rAAV-L-AD harboring a short hairpin RNA targeting ATP5B (rAAV-L-AD-shATP5B) and found that it caused a significant decrease in ATP5B mRNA levels when transduced into HEK293EB cells, suggesting that it was functional. Thus, our system successfully packaged L-AD into capsids with minimal contamination of plasmid DNA, offering a novel functional packaging platform without causing plasmid backbone encapsidation., (© 2021. The Author(s), under exclusive licence to Springer Nature Limited.)

Published
2022
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36. Evaluation of parameters for efficient purification and long-term storage of herpes simplex virus-based vectors.

Author

Kuroda S, Miyagawa Y, Sukegawa M, Tomono T, Yamamoto M, Adachi K, Verlengia G, Goins WF, Cohen JB, Glorioso JC, and Okada T

Abstract

Replication competent oncolytic herpes simplex virus (HSV) vectors have been used extensively to treat solid tumors with promising results. However, highly defective HSV vectors will be needed for applications that require sustained therapeutic gene expression in the absence of vector-related toxicity or inflammation. These vectors require complementing cell lines for their manufacture, creating significant challenges to achieve high yields of infectious virus particles. We recently described an improved upstream process for the production of a non-cytotoxic HSV vector for gene therapy applications. Here, we sought to optimize the downstream conditions for purification and long-term storage of the same vector, JΔNI5. We compared different methods to remove cellular impurities and concentrate the vector by monitoring both physical and biological titers, resulting in the establishment of optimal conditions for vector production. To optimize the long-term storage parameters for non-cytotoxic HSV vectors, we evaluated vector stability at low temperature and sensitivity to freeze-thaw cycles. We report that suboptimal purification and storage methods resulted in loss of vector viability. Our results describe effective and reproducible protocols for purification and storage of HSV vectors for pre-clinical studies., Competing Interests: Y.M., J.B.C., and J.C.G. are co-inventors of intellectual property licensed to Replay Therapeutics, Inc. J.B.C., and J.C.G. are co-inventors of intellectual property licensed to Oncorus, Inc. J.C.G. is a founder and consultant of Coda Biotherapeutics and Oncorus, Inc. W.F.G. is a consultant of Oncorus, Inc., (© 2022 The Author(s).)

Published
2022
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37. Evaluation of a D -Octaarginine-linked polymer as a transfection tool for transient and stable transgene expression in human and murine cell lines.

Author

Sakuma S, Okamoto M, Matsushita N, Ukawa M, Tomono T, Kawamoto K, Ikeda T, and Sakuma S

Subjects
Animals, Cell Line, Green Fluorescent Proteins genetics, Green Fluorescent Proteins metabolism, Humans, Mice, Oligopeptides, Plasmids genetics, Transfection veterinary, Transgenes, DNA, Polymers
Abstract

Poly(N-vinylacetamide-co-acrylic acid) coupled with d-octaarginine (VP-R8) promotes the cellular uptake of peptides/proteins in vitro; however, details of the transfection efficacy of VP-R8, such as the cell types possessing high gene transfer, are not known. Herein, we compared the ability of VP-R8 to induce the cellular uptake of plasmid DNA in mouse and human cell lines from different tissues and organs. A green fluorescent protein (GFP)-expression plasmid was used as model genetic material, and fluorescence as an indicator of uptake and plasmid-derived protein expression. Three mouse and three human cell lines were incubated with a mixture of plasmid and VP-R8, and fluorescence analysis were performed two days after transfection. To confirm stable transgene expression, we performed drug selection three days after transfection. A commercially available polymer-based DNA transfection reagent (PTR) was used as the transfection control and standard for comparing transgene expression efficiency. In the case of transient transgene expression, slight-to-moderate GFP expression was observed in all cell lines transfected with plasmid via VP-R8; however, transfection efficiency was lower than using the PTR for gene delivery. In the case of stable transgene expression, VP-R8 promoted drug-resistance acquisition more efficiently than the PTR did. Cells that developed drug resistance after VP-R8-mediated gene transfection expressed GFP more efficiently than cells that developed drug resistance after transfection with the PTR. Thus, VP-R8 shows potential as an in vitro or ex vivo nonviral transfection tool for generating cell lines with stable transgene expression.

Published
2022
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38. Acquisition of absorption-enhancing abilities of cationic oligopeptides with short chain arginine residues through conjugation to hyaluronic acid.

Author

Tomono T, Yagi H, Kanemoto S, Ukawa M, Miyata K, Shigeno K, and Sakuma S

Subjects
Animals, Arginine chemistry, Exenatide, Mice, Oligopeptides chemistry, Cell-Penetrating Peptides chemistry, Cell-Penetrating Peptides metabolism, Hyaluronic Acid chemistry
Abstract

Cell-penetrating peptides such as oligoarginines are one of promising tools that improve mucosal absorption of poorly membrane-permeable biologics. We have already demonstrated that conjugation of L-octaarginine to hyaluronic acid via a tetraglycine spacer resulted in a 3-fold enhancement of nasal absorption of somatropin (Mw: ca. 22.1 kDa) in mice when compared with the unmodified peptide. Here, we evaluated absorption-enhancing abilities and safety profiles of oligopeptides with short chain arginine residues conjugated to hyaluronic acid. Somatropin absorption was hardly ever enhanced by diglycine-L-tetraarginine. The peptide acquired the absorption-enhancing ability through the conjugation; however, it disappeared when arginine residues were halved. In vivo data were consistent to in vitro cellular uptake of somatropin. When somatropin was substituted with exendin-4 (Mw: ca. 4.2 kDa), cellular uptake was significantly enhanced by diglycine-L-diarginine conjugated to hyaluronic acid under comparison with the unmodified peptide. The conjugate also exhibited the enhancement ability in mice, as observed for hyaluronic acid derivatives with four and more arginine residues. Another cell studies revealed that oligoarginine-linked hyaluronic acid tended to be less toxic as arginine residues were reduced. Results indicated that diglycine-L-tetraarginine-linked hyaluronic acid was the most suitable candidate as an absorption enhancer whose Mw-independent enhancement ability and safety were well-balanced., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published
2022
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39. Concordance of the histological diagnosis of type 1 autoimmune pancreatitis and its distinction from pancreatic ductal adenocarcinoma with endoscopic ultrasound-guided fine needle biopsy specimens: an interobserver agreement study.

Author

Notohara K, Kamisawa T, Furukawa T, Fukushima N, Uehara T, Kasashima S, Iwasaki E, Kanno A, Kawashima A, Kubota K, Kuraishi Y, Motoya M, Naitoh I, Nishino T, Sakagami J, Shimizu K, Tomono T, Aishima S, Fukumura Y, Hirabayashi K, Kojima M, Mitsuhashi T, Naito Y, Ohike N, Tajiri T, Yamaguchi H, Fujiwara H, Ibuki E, Kobayashi S, Miyaoka M, Nagase M, Nakashima J, Nakayama M, Oda S, Taniyama D, Tsuyama S, Watanabe S, Ikeura T, Kawa S, and Okazaki K

Subjects
Biopsy, Fine-Needle methods, Fibrosis, Humans, Observer Variation, Ultrasonography, Interventional, Pancreatic Neoplasms, Autoimmune Diseases diagnosis, Autoimmune Diseases pathology, Autoimmune Pancreatitis diagnosis, Carcinoma, Pancreatic Ductal diagnosis, Carcinoma, Pancreatic Ductal pathology, Pancreatic Neoplasms diagnosis, Pancreatic Neoplasms pathology, Phlebitis pathology
Abstract

The histological diagnosis of type 1 autoimmune pancreatitis (AIP) based on the findings obtained by an endoscopic ultrasound-guided fine needle biopsy (EUS-FNB) is feasible, but the diagnostic consistency of this method has not been confirmed. We determined the interobserver agreement among 20 pathologists regarding the diagnosis of type 1 AIP, including the distinction from pancreatic ductal adenocarcinoma (PDAC) using large tissue samples obtained by EUS-FNB. After guidance for diagnosing AIP with biopsy tissues was provided, a round 2 was performed. The median sensitivity and specificity for diagnosing PDAC vs. non-neoplastic diseases were 95.2% and 100%, respectively. In groups of specialists (n = 7) and the generalists (n = 13), Fleiss' к-values increased from 0.886 to 0.958 and from 0.750 to 0.816 in round 2. The concordance was fair or moderate for obliterative phlebitis and storiform fibrosis but slight for ductal lesion of type 1 AIP. Discordant results were due to ambiguous findings and biopsy tissue limitations. Among the specialists, the ratio of cases with perfect agreement regarding the presence of storiform fibrosis increased in round 2, but agreement regarding obliterative phlebitis or ductal lesions was not improved. Although the histological definite diagnosis of type 1 AIP was achieved by most observers in > 60% of the cases, the confidence levels varied. Because some ambiguities exist, the histological diagnostic levels based on the diagnostic criteria of type 1 AIP should not be taken for granted. Guidance is effective for improving accurate PDAC diagnoses (notably by recognizing acinar-ductal metaplasia) and for evaluating storiform fibrosis., (© 2021. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published
2022
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40. Mechanism on antigen delivery under mucosal vaccination using cell-penetrating peptides immobilized at multiple points on polymeric platforms.

Author

Ukawa M, Endo R, Yagi H, Tomono T, Miyata K, Shigeno K, Tobita E, Uto T, Baba M, and Sakuma S

Subjects
Adjuvants, Vaccine, Animals, Mice, Nasal Mucosa, Polymers, Vaccination, Cell-Penetrating Peptides
Abstract

We have developed an aggregate of D-octaarginine immobilized at multiple points on a co-polymer of N-vinylacetamide and acrylic acid. Previous studies revealed that immunoglobulin G and A were induced when mice were inoculated with influenza virus antigens under coadministration with the D-octaarginine-immobilized polymers as a mucosal vaccine adjuvant. Infection experiments demonstrated that mice vaccinated with a mixture of inactivated influenza viruses and the polymers were protected from infection with mouse-adapted infectious viruses. In the present study, we investigated the mechanism on antigen delivery under mucosal vaccination using the polymers. Two-hour retention of fluorescein-labeled ovalbumin (F-OVA) on the nasal mucosa was observed when applied with the polymers; nevertheless F-OVA was eliminated less than 10 min under polymer-free conditions. F-OVA mixed with the polymers was vigorously taken up into murine dendritic cells. Electrophoresis and dynamic light scattering analysis indicated that OVA interacted with the polymers. The uptake of F-OVA was hardly ever inhibited by the addition of an excess amount of intact OVA. The results suggested that viral antigens were accumulated on the mucosa and delivered into dendritic cells under basolateral membranes via dendrites extending to the mucosal surface and/or subsequent to their permeation through epithelial cells, when they were coadministered with D-octaarginine-immobilized polymers., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published
2022
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41. Drug resistance via radixin-mediated increase of P-glycoprotein membrane expression during SNAI1-induced epithelial-mesenchymal transition in HepG2 cells.

Author

Kamioka H, Edaki K, Kasahara H, Tomono T, Yano K, and Ogihara T

Subjects
ATP Binding Cassette Transporter, Subfamily B metabolism, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Antineoplastic Agents therapeutic use, Genetic Vectors, Hep G2 Cells, Humans, Membrane Glycoproteins metabolism, Microfilament Proteins metabolism, Neoplasms drug therapy, Paclitaxel therapeutic use, RNA, Messenger metabolism, RNA, Small Interfering, Rhodamine 123 metabolism, Transfection, Cell Membrane metabolism, Cytoskeletal Proteins metabolism, Drug Resistance, Neoplasm, Epithelial-Mesenchymal Transition, Membrane Proteins metabolism, Neoplasms metabolism, Snail Family Transcription Factors metabolism
Abstract

Objectives: Epithelial-mesenchymal transition (EMT) plays a role in cancer metastasis as well as in drug resistance through various mechanisms, including increased drug efflux mediated by P-glycoprotein (P-gp). In this study, we investigated the activation mechanism of P-gp, including its regulatory factors, during EMT in hepatoblastoma-derived HepG2 cells., Methods: HepG2 cells were transfected with SNAI1 using human adenovirus serotype 5 vector. We quantified mRNA and protein expression levels using qRT-PCR and western blot analysis, respectively. P-gp activity was evaluated by uptake assay, and cell viability was assessed by an MTT assay., Key Findings: P-gp protein expression on plasma membrane was higher in SNAI1-transfected cells than in Mock cells, although there was no difference in P-gp protein level in whole cells. Among the scaffold proteins such as ezrin, radixin and moesin (ERM), only radixin was increased in SNAI1-transfected cells. Uptake of both Rho123 and paclitaxel was decreased in SNAI1-transfected cells, and this decrease was blocked by verapamil, a P-gp inhibitor. The reduced susceptibility of SNAI1-transfected cells to paclitaxel was reversed by elacridar, another P-gp inhibitor., Conclusions: Increased expression of radixin during SNAI1-induced EMT leads to increased P-gp membrane expression in HepG2 cells, enhancing P-gp function and thereby increasing drug resistance., (© The Author(s) 2021. Published by Oxford University Press on behalf of the Royal Pharmaceutical Society. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published
2021
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42. Essential role of Notch/Hes1 signaling in postnatal pancreatic exocrine development.

Author

Kuriyama K, Kodama Y, Shiokawa M, Nishikawa Y, Marui S, Kuwada T, Sogabe Y, Kakiuchi N, Tomono T, Matsumori T, Mima A, Morita T, Ueda T, Tsuda M, Yamauchi Y, Sakuma Y, Ota Y, Maruno T, Uza N, Kageyama R, Chiba T, and Seno H

Subjects
Animals, Cell Differentiation drug effects, Cell Differentiation physiology, Disease Models, Animal, Mice, Signal Transduction physiology, Stem Cells metabolism, Stem Cells physiology, Pancreas metabolism, Transcription Factor HES-1 pharmacology
Abstract

Background: Notch/Hes1 signaling has been shown to play a role in determining the fate of pancreatic progenitor cells. However, its function in postnatal pancreatic maturation is not fully elucidated., Methods: We generated conditional Hes1 knockout and/or Notch intracellular domain (NICD) overexpression mice in Ptf1a- or Pdx1-positive pancreatic progenitor cells and analyzed pancreatic tissues., Results: Both Ptf1a cre/+ ; Hes1 f/f and Ptf1a cre/+ ; Rosa26 NICD mice showed normal pancreatic development at P0. However, exocrine tissue of the pancreatic tail in Ptf1a cre/+ ; Hes1 f/f mice atrophied and was replaced by fat tissue by 4 weeks of age, with increased apoptotic cells and fewer centroacinar cells. This impaired exocrine development was completely rescued by NICD overexpression in Ptf1a cre/+ ; Hes1 f/f ; Rosa26 NICD mice, suggesting compensation by a Notch signaling pathway other than Hes1. Conversely, Pdx1-Cre; Hes1 f/f mice showed impaired postnatal exocrine development in both the pancreatic head and tail, revealing that the timing and distribution of embryonic Hes1 expression affects postnatal exocrine tissue development., Conclusions: Notch signaling has an essential role in pancreatic progenitor cells for the postnatal maturation of exocrine tissue, partly through the formation of centroacinar cells., (© 2021. Japanese Society of Gastroenterology.)

Published
2021
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44. Reconstruction of Geometric and Optical Parameters of Non-Planar Objects with Thin Film.

Author

Kobayashi Y, Morimoto T, Sato I, Mukaigawa Y, Tomono T, and Ikeuchi K

Abstract

Here, we propose a novel method to estimate the parameters of non-planar objects with thin film surfaces. Being able to estimate the optical parameters of objects with thin film surfaces has a wide range of applications from industrial inspections to biological and archaeology research. However, there are many challenging issues that need to be overcome to model such parameters. The appearance of thin film objects is highly dependent on the surface orientation and optical parameters such as the refractive index and film thickness. First, we therefore analyzed the optical parameters of non-planar objects with thin film surfaces. Next, we proposed and implemented an analysis procedure and demonstrated its effectiveness for studying planar objects with thin film surfaces. Finally, we developed a device to acquire the shapes and optical parameters of objects with thin film surfaces using a camera and demonstrated the effectiveness of our method experimentally. Then, we surveyed the errors caused by the light source. We discussed the difference between the theoretically obtained parameters and experimental data obtained using a hyper spectral camera.

Published
2021
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45. Functional Alterations of Multidrug Resistance-Associated Proteins 2 and 5, and Breast Cancer Resistance Protein upon Snail-Induced Epithelial-Mesenchymal Transition in HCC827 Cells.

Author

Yano K, Todokoro I, Kamioka H, Tomono T, and Ogihara T

Subjects
Cell Line, Tumor, Epithelial-Mesenchymal Transition drug effects, Humans, Multidrug Resistance-Associated Protein 2, ATP Binding Cassette Transporter, Subfamily G, Member 2 metabolism, Epithelial-Mesenchymal Transition physiology, Multidrug Resistance-Associated Proteins metabolism, Neoplasm Proteins metabolism, Snail Family Transcription Factors pharmacology
Abstract

Our previous report indicated that Snail-induced epithelial-mesenchymal transition (EMT) enhanced P-glycoprotein (P-gp) function and drug resistance to P-gp substrate anticancer drug in a human non-small cell lung cancer (NSCLC) cell line, HCC827. Our objective is to evaluate the changes in the mRNA and protein expression levels and the functions of multidrug resistance-associated protein (MRP) 2, MRP5 and breast cancer resistance protein (BCRP). Snail-expressing HCC827 cells showed increased mRNA levels of Snail and a mesenchymal marker vimentin, and decreased mRNA levels of an epithelial marker E-cadherin after transduction, indicating that Snail had induced EMT consistent with our previous reports. The mRNA level of MRP2 was significantly decreased, while that of MRP5 remained unchanged, in Snail-expressing cells. The expression levels of MRP2 and MRP5 proteins in whole-cell homogenate were unchanged in Snail-expressing cells, but MRP5 protein showed significantly increased membrane localization. Snail-transduction increased the efflux transport of 5-(and-6)-carboxy-2',7'-dichlorofluorescein (CDCF), a substrate of MRP2, 3 and 5. This increase was blocked by MK571, which inhibits MRP1, 2, and 5. Toxicity of cisplatin, a substrate of MRP2 and 5, was significantly decreased in Snail-expressing cells. BCRP mRNA and protein levels were both decreased in Snail-expressing cells, which showed an increase in the intracellular accumulation of 7-ethyl-10-hydroxycamptothecin (SN-38), a BCRP substrate, resulting in reduced viability. These results suggested that MRP5 function appears to be increased via an increase in membrane localization, whereas the BCRP function is decreased via a decrease in the expression level in HCC827 cells with Snail-induced EMT.

Published
2021
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46. Hes1 Is Essential in Proliferating Ductal Cell-Mediated Development of Intrahepatic Cholangiocarcinoma.

Author

Matsumori T, Kodama Y, Takai A, Shiokawa M, Nishikawa Y, Matsumoto T, Takeda H, Marui S, Okada H, Hirano T, Kuwada T, Sogabe Y, Kakiuchi N, Tomono T, Mima A, Morita T, Ueda T, Tsuda M, Yamauchi Y, Kuriyama K, Sakuma Y, Ota Y, Maruno T, Uza N, Marusawa H, Kageyama R, Chiba T, and Seno H

Subjects
Animals, Bile Duct Neoplasms genetics, Bile Duct Neoplasms metabolism, Cholangiocarcinoma genetics, Cholangiocarcinoma metabolism, Diet adverse effects, Humans, Mice, Knockout, Mice, Transgenic, Proto-Oncogene Proteins p21(ras) genetics, Receptors, Notch metabolism, Bile Duct Neoplasms pathology, Bile Ducts, Intrahepatic pathology, Cholangiocarcinoma pathology, Transcription Factor HES-1 genetics, Transcription Factor HES-1 metabolism
Abstract

Intrahepatic cholangiocarcinoma (ICC) is frequently driven by aberrant KRAS activation and develops in the liver with chronic inflammation. Although the Notch signaling pathway is critically involved in ICC development, detailed mechanisms of Notch-driven ICC development are still unknown. Here, we use mice whose Notch signaling is genetically engineered to show that the Notch signaling pathway, specifically the Notch/Hes1 axis, plays an essential role in expanding ductular cells in the liver with chronic inflammation or oncogenic Kras activation. Activation of Notch1 enhanced the development of proliferating ductal cells (PDC) in injured livers, while depletion of Hes1 led to suppression. In correlation with PDC expansion, ICC development was also regulated by the Notch/Hes1 axis and suppressed by Hes1 depletion. Lineage-tracing experiments using Epcam creERT2 mice further confirmed that Hes1 plays a critical role in the induction of PDC and that ICC could originate from PDC. Analysis of human ICC specimens showed PDC in nonneoplastic background tissues, confirming HES1 expression in both PDC and ICC tumor cells. Our findings provide novel direct experimental evidence that Hes1 plays an essential role in the development of ICC via PDC. SIGNIFICANCE: This study contributes to the identification of the cells of origin that initiate ICC and suggests that HES1 may represent a therapeutic target in ICC., (©2020 American Association for Cancer Research.)

Published
2020
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47. CXCR4 in Tumor Epithelial Cells Mediates Desmoplastic Reaction in Pancreatic Ductal Adenocarcinoma.

Author

Morita T, Kodama Y, Shiokawa M, Kuriyama K, Marui S, Kuwada T, Sogabe Y, Matsumori T, Kakiuchi N, Tomono T, Mima A, Ueda T, Tsuda M, Yamauchi Y, Nishikawa Y, Sakuma Y, Ota Y, Maruno T, Uza N, Nagasawa T, Chiba T, and Seno H

Subjects
Animals, Carcinoma, Pancreatic Ductal genetics, Carcinoma, Pancreatic Ductal metabolism, Cell Differentiation genetics, Cell Movement, Chemokine CXCL12 metabolism, Epithelial Cells pathology, Epithelial-Mesenchymal Transition genetics, Gene Expression Regulation, Neoplastic, Humans, Liver Neoplasms, Experimental pathology, Liver Neoplasms, Experimental secondary, Mice, Inbred C57BL, Mice, Knockout, Myofibroblasts metabolism, Myofibroblasts pathology, Pancreatic Neoplasms genetics, Pancreatic Neoplasms metabolism, Receptors, CXCR4 genetics, Carcinoma, Pancreatic Ductal pathology, Pancreatic Neoplasms pathology, Receptors, CXCR4 metabolism
Abstract

Pancreatic ductal adenocarcinoma (PDAC) features abundant stromal cells with an excessive extracellular matrix (ECM), termed the desmoplastic reaction. CXCR4 is a cytokine receptor for stromal cell-derived factor-1 (CXCL12) expressed in PDAC, but its roles in PDAC and the characteristic desmoplastic reaction remain unclear. Here, we generated a mouse model of PDAC with conditional knockout of Cxcr4 (KPC-Cxcr4-KO) by crossing Cxcr4 flox mice with Pdx1-Cre;KrasLSL-G12D/+;Trp53LSL-R172H/+ (KPC-Cxcr4-WT) mice to assess the development of pancreatic intraepithelial neoplasia (PanIN) and pancreatic cancers. Tumor cell characteristics of those two types were analyzed in vitro . In addition, CXCR4 expression in human pancreatic cancer specimens was evaluated by IHC staining. In KPC-Cxcr4-KO mice, the number and pathologic grade of PanIN lesions were reduced, but the frequency of pancreatic cancers did not differ from that in KPC-Cxcr4-WT mice. The pancreatic tumor phenotype in KPC-Cxcr4-KO mice was significantly larger and undifferentiated, characterized by abundant vimentin-expressing cancer cells, significantly fewer fibroblasts, and markedly less deposition of ECM. In vitro , KPC-Cxcr4-KO tumor cells exhibited higher proliferative and migratory activity than KPC-Cxcr4-WT tumor cells. Myofibroblasts induced invasion activity in KPC-Cxcr4-WT tumor cells, showing an epithelial-mesenchymal interaction, whereas KPC-Cxcr4-KO tumor cells were unaffected by myofibroblasts, suggesting their unique nature. In human pancreatic cancer, undifferentiated carcinoma did not express CXCR4 and exhibited histologic and IHC features similar to those in KPC-Cxcr4-KO mice. In summary, the CXCL12/CXCR4 axis may play an important role in the desmoplastic reaction in PDAC, and loss of CXCR4 induces phenotype changes in undifferentiated carcinoma without a desmoplastic reaction. SIGNIFICANCE: The current study uncovers CXCR4 as a key regulator of desmoplastic reaction in PDAC and opens the way for new therapeutic approaches to overcome the chemoresistance in patients with PDAC., (©2020 American Association for Cancer Research.)

Published
2020
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48. Nasal absorption enhancement of protein drugs independent to their chemical properties in the presence of hyaluronic acid modified with tetraglycine-L-octaarginine.

Author

Tomono T, Yagi H, Ukawa M, Ishizaki S, Miwa T, Nonomura M, Igi R, Kumagai H, Miyata K, Tobita E, Kobayashi H, and Sakuma S

Subjects
Administration, Intranasal, Animals, Exenatide administration & dosage, Exenatide chemistry, Exenatide pharmacokinetics, Human Growth Hormone administration & dosage, Human Growth Hormone chemistry, Human Growth Hormone pharmacokinetics, Hyaluronic Acid chemistry, Hyaluronic Acid pharmacokinetics, Mice, Nasal Absorption physiology, Nasal Mucosa drug effects, Nasal Mucosa metabolism, Octreotide administration & dosage, Octreotide chemistry, Octreotide pharmacokinetics, Oligopeptides chemistry, Oligopeptides pharmacokinetics, Peptides chemistry, Peptides pharmacokinetics, Hyaluronic Acid administration & dosage, Nasal Absorption drug effects, Oligopeptides administration & dosage, Peptides administration & dosage
Abstract

Our previous mouse studies demonstrated that mean bioavailability of exendin-4, which is an injectable glucagon-like peptide-1 (GLP-1) analogue whose molecular weight (Mw) and isoelectric point (pI) are ca. 4.2 kDa and 4.5, respectively, administered nasally with poly(N-vinylacetamide-co-acrylic acid) (PNVA-co-AA) bearing D-octaarginine, which is a typical cell-penetrating peptide, was 20% relative to subcutaneous administration even though it was less than 1% when exendin-4 alone was given nasally. The studies also revealed that the absorption-enhancing ability of D-octaarginine-linked PNVA-co-AA for exendin-4 was statistically equivalent to that of sodium salcaprozate (SNAC), which is an absorption enhancer formulated in tablets of semaglutide approved recently as an orally available GLP-1 analogue. From a perspective of clinical application of our technology, we have separately developed hyaluronic acid modified with L-octaarginine via a tetraglycine spacer which would be degraded in biological conditions. The present study revealed that tetraglycine-L-octaarginine-linked hyaluronic acid enhanced nasal absorption of exendin-4 in mice, as did D-octaarginine-linked PNVA-co-AA. There was no significant difference in absorption-enhancing abilities between the hyaluronic acid derivative and SNAC when octreotide (Mw: ca. 1.0 kDa, pI: 8.3) and lixisenatide (Mw: ca. 4.9 kDa, pI: 9.5) were used as a model protein drug. On the other hand, SNAC did not significantly enhance nasal absorption of somatropin (Mw: ca. 22.1 kDa, pI: 5.3) when compared with absorption enhancer-free conditions. Substitution of SNAC with tetraglycine-L-octaarginine-linked hyaluronic acid resulted in a 5-fold increase in absolute bioavailability of somatropin with statistical significance. It appeared that pI hardly ever influenced absorption-enhancing abilities of both enhancers. Results indicated that our polysaccharide derivative would be a promising absorption enhancer which delivers biologics applied on the nasal mucosa into systemic circulation and was of greater advantage than SNAC for enhancing nasal absorption of protein drugs with a larger Mw., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published
2020
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49. Rb and p53 Execute Distinct Roles in the Development of Pancreatic Neuroendocrine Tumors.

Author

Yamauchi Y, Kodama Y, Shiokawa M, Kakiuchi N, Marui S, Kuwada T, Sogabe Y, Tomono T, Mima A, Morita T, Matsumori T, Ueda T, Tsuda M, Nishikawa Y, Kuriyama K, Sakuma Y, Ota Y, Maruno T, Uza N, Masuda A, Tatsuoka H, Yabe D, Minamiguchi S, Masui T, Inagaki N, Uemoto S, Chiba T, and Seno H

Subjects
Animals, Mice, Mice, Transgenic, Cell Transformation, Neoplastic genetics, Neuroendocrine Tumors genetics, Pancreatic Neoplasms genetics, Retinoblastoma Protein genetics, Tumor Suppressor Protein p53 genetics
Abstract

Pancreatic neuroendocrine tumors (PanNET) were classified into grades (G) 1 to 3 by the World Health Organization in 2017, but the precise mechanisms of PanNET initiation and progression have remained unclear. In this study, we used a genetically engineered mouse model to investigate the mechanisms of PanNET formation. Although pancreas-specific deletion of the Rb gene ( Pdx1-Cre;Rb f/f ) in mice did not affect pancreatic exocrine cells, the α-cell/β-cell ratio of islet cells was decreased at 8 months of age. During long-term observation (18-20 months), mice formed well-differentiated PanNET with a Ki67-labeling index of 2.7%. In contrast, pancreas-specific induction of a p53 mutation ( Pdx1-Cre;Trp53 R172H ) had no effect on pancreatic exocrine and endocrine tissues, but simultaneous induction of a p53 mutation with Rb gene deletion ( Pdx1-Cre;Trp53 R172H ;Rb f/f ) resulted in the formation of aggressive PanNET with a Ki67-labeling index of 24.7% over the short-term (4 months). In Pdx1-Cre;Trp53 R172H ;Rb f/f mice, mRNA expression of Pten and Tsc2 , negative regulators of the mTOR pathway, significantly decreased in the islet cells, and activation of the mTOR pathway was confirmed in subsequently formed PanNET. Thus, by manipulating Rb and p53 genes, we established a multistep progression model from dysplastic islet to indolent PanNET and aggressive metastatic PanNET in mice. These observations suggest that Rb and p53 have distinct roles in the development of PanNET. SIGNIFICANCE: Pancreas-specific manipulation of Rb and p53 genes induced malignant transformation of islet cells, reproducing stepwise progression from microadenomas to indolent (grade 1) and subsequent aggressive PanNETs (grade 2-3)., (©2020 American Association for Cancer Research.)

Published
2020
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50. Utility of laser-cut covered self-expandable metal stents for unresectable malignant distal biliary obstruction: a single-center experience.

Author

Marui S, Uza N, Yamazaki H, Ota S, Nakamura T, Yoshida H, Okada H, Hirano T, Kuwada T, Sogabe Y, Tomono T, Matsumori T, Morita T, Nishikawa Y, Tsuda M, Maruno T, Shiokawa M, Kodama Y, and Seno H

Subjects
Device Removal, Humans, Lasers, Retrospective Studies, Stents, Cholestasis etiology, Cholestasis surgery, Self Expandable Metallic Stents
Abstract

Background: Few reports have evaluated the effectiveness of laser-cut, covered, self-expandable metal stents (LC-CSEMS) for unresectable malignant distal biliary obstruction (MDBO) and whether reintervention is feasible after placement. We describe our experience with LC-CSEMS placement for unresectable MDBO., Methods: Patients undergoing LC-CSEMS placement for unresectable MDBO from November 2014 to December 2018 were reviewed. Recurrent biliary obstruction (RBO), median time to RBO (TRBO), and reintervention were analyzed., Results: 52 patients who underwent LC-CSEMS placement for unresectable MDBO were included in the analysis. The RBO rate was 15 % and the median TRBO was 445 days. Reintervention was attempted in nine patients and stent removal was successful in eight patients., Conclusions: Our experience suggests the effectiveness of LC-CSEMS in patients with unresectable MDBO in terms of stent patency and feasibility of reintervention., Competing Interests: The authors declare that they have no conflicts of interest., (© Georg Thieme Verlag KG Stuttgart · New York.)

Published
2020
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