Your search keyword '"Kamiya, Mako"' showing total 5 results

1. Rapid fluorescence imaging of human hepatocellular carcinoma using the β-galactosidase-activatable fluorescence probe SPiDER-βGal.

Author

Ogawa, Soichiro, Kubo, Hidemasa, Murayama, Yasutoshi, Kubota, Takeshi, Yubakami, Masayuki, Matsumoto, Tatsuya, Yamamoto, Yusuke, Morimura, Ryo, Ikoma, Hisashi, Okamoto, Kazuma, Kamiya, Mako, Urano, Yasuteru, and Otsuji, Eigo

Subjects

HEPATOCELLULAR carcinoma, GALACTOSIDASES, FLUORESCENT probes, LIVER surgery, LABORATORY mice

Abstract

Fluorescence imaging of tumours facilitates rapid intraoperative diagnosis. Thus far, a promising activatable fluorescence probe for hepatocellular carcinoma (HCC) has not been developed. Herein, the utility of the fluorescence imaging of HCC using a β-galactosidase (β-Gal)-activatable fluorescence probe SPiDER-βGal was examined. β-Gal activity was measured in cryopreserved tissues from 68 patients. Live cell imaging of HCC cell lines and imaging of tumour-bearing model mice were performed using SPiDER-βGal. Furthermore, fluorescence imaging was performed in 27 freshly resected human HCC specimens. In cryopreserved samples, β-Gal activity was significantly higher in tumour tissues than in non-tumour tissues. Fluorescence was observed in HCC cell lines. In mouse models, tumours displayed stronger fluorescence than normal liver tissue. In freshly resected specimens, fluorescence intensity in the tumour was significantly higher than that in non-tumour liver specimens as early as 2 min after spraying. Receiver operating characteristic curves were generated to determine the diagnostic value of SPiDER-βGal 10 min after its spraying; an area under the curve of 0.864, sensitivity of 85.2%, and specificity of 74.1% were observed for SPiDER-βGal. SPiDER-βGal is useful for the rapid fluorescence imaging of HCC. Fluorescence imaging guided by SPiDER-βGal would help surgeons detect tumours rapidly and achieve complete liver resection. [ABSTRACT FROM AUTHOR]

Published

2021

2. β-Galactosidase is a target enzyme for detecting peritoneal metastasis of gastric cancer.

Author

Kubo, Hidemasa, Murayama, Yasutoshi, Ogawa, Soichiro, Matsumoto, Tatsuya, Yubakami, Masayuki, Ohashi, Takuma, Kubota, Takeshi, Okamoto, Kazuma, Kamiya, Mako, Urano, Yasuteru, and Otsuji, Eigo

Subjects

GALACTOSIDASES, STOMACH cancer, METASTASIS, GASTRECTOMY, GAMMA-glutamyltransferase

Abstract

Diagnosis of peritoneal metastasis in gastric cancer (GC) is essential for determining appropriate therapeutic strategies and avoiding non-essential laparotomy or gastrectomy. Recently, a variety of activatable fluorescence probes that can detect enzyme activities have been developed for cancer imaging. The aim of this study was to identify the key enzyme involved in peritoneal metastasis in GC. The enzymatic activity of gamma-glutamyl transpeptidase, dipeptidyl peptidase IV, and β-galactosidase (β-Gal) was assessed in lysates prepared from preserved human GC (n = 89) and normal peritoneal (NP; n = 20) samples. β-Gal activity was significantly higher in the human GC samples than in NP samples, whereas no differences were observed in the activities of the other enzymes. Therefore, we used SPiDER-βGal, a fluorescent probe that can be activated by β-Gal, for imaging GC cell lines, peritoneal metastasis in a mouse model, and fresh human resected GC samples (n = 13). All cell lines showed fluorescence after applying SPiDER-βGal, and metastatic nodules in the mice gradually developed high fluorescence that could be visualized with SPiDER-βGal. The human GC samples showed significantly higher fluorescence than NP samples. β-Gal is a useful target enzyme for fluorescence imaging of peritoneal metastasis in GC. [ABSTRACT FROM AUTHOR]

Published

2021

3. Red‐Shifted Fluorogenic Substrate for Detection of lacZ‐Positive Cells in Living Tissue with Single‐Cell Resolution.

Author

Ito, Hiroki, Kawamata, Yu, Kamiya, Mako, Tsuda‐Sakurai, Kayoko, Tanaka, Shinji, Ueno, Tasuku, Komatsu, Toru, Hanaoka, Kenjiro, Okabe, Shigeo, Miura, Masayuki, and Urano, Yasuteru

Subjects

SUBSTRATES (Materials science), FLUORESCENCE, ESCHERICHIA coli, GALACTOSIDASES, GREEN fluorescent protein

Abstract

The Escherichia coli lacZ gene encoding β‐galactosidase is a widely used reporter, but few synthetic substrates are available for detecting its activity with single‐cell resolution in living samples. Our recently reported fluorogenic substrate SPiDER‐βGal is suitable for this purpose, but its hydrolysis product shows green fluorescence emission, and a red‐shifted analogue is therefore required for use in combination with green fluorescent protein (GFP) markers. Herein, we describe the development of a red‐shifted fluorogenic substrate for β‐galactosidase, SPiDER‐Red‐βGal, based on a silicon rhodol scaffold and a carboxylic group as the intramolecular nucleophile. LacZ‐positive cells were successfully labeled with SPiDER‐Red‐βGal at single‐cell resolution in living samples, which enabled us to visualize different cell types in combination with GFP markers. SPiDER and the fly: A new fluorogenic β‐galactosidase substrate, SPiDER‐Red‐βGal, based on a silicon rhodol scaffold and a carboxylic group as the intramolecular nucleophile, exhibited simultaneous activation of red fluorescence and labeling ability for intracellular proteins via a quinone methide intermediate. The probe can label lacZ‐positive cells at single‐cell resolution in vivo with perfect orthogonality to green fluorescent protein (GFP) markers. [ABSTRACT FROM AUTHOR]

Published

2018

4. Detection of LacZ-Positive Cells in Living Tissue with Single-Cell Resolution.

Author

Doura, Tomohiro, Kamiya, Mako, Obata, Fumiaki, Yamaguchi, Yoshifumi, Hiyama, Takeshi Y., Matsuda, Takashi, Fukamizu, Akiyoshi, Noda, Masaharu, Miura, Masayuki, and Urano, Yasuteru

Subjects

*ESCHERICHIA coli, *GALACTOSIDASES, *GENE expression, *FLUORESCENCE, *NEURONS, *LIGANDS (Chemistry)

Abstract

The LacZ gene, which encodes Escherichia coli β-galactosidase, is widely used as a marker for cells with targeted gene expression or disruption. However, it has been difficult to detect lacZ-positive cells in living organisms or tissues at single-cell resolution, limiting the utility of existing lacZ reporters. Herein we present a newly developed fluorogenic β-galactosidase substrate suitable for labeling live cells in culture, as well as in living tissues. This precisely functionalized fluorescent probe exhibited dramatic activation of fluorescence upon reaction with the enzyme, remained inside cells by anchoring itself to intracellular proteins, and provided single-cell resolution. Neurons labeled with this probe preserved spontaneous firing, which was enhanced by application of ligands of receptors expressed in the cells, suggesting that this probe would be applicable to investigate functions of targeted cells in living tissues and organisms. [ABSTRACT FROM AUTHOR]

Published

2016

5. Selective Ablation of β-Galactosidase-Expressing Cells with a Rationally Designed Activatable Photosensitizer.

Author

Ichikawa, Yuki, Kamiya, Mako, Obata, Fumiaki, Miura, Masayuki, Terai, Takuya, Komatsu, Toru, Ueno, Tasuku, Hanaoka, Kenjiro, Nagano, Tetsuo, and Urano, Yasuteru

Subjects

*LASER ablation, *GALACTOSIDASES, *PHOTOSENSITIZERS, *CELL death, *PHYSIOLOGICAL effects of radiation

Abstract

We have developed an activatable photosensitizer capable of specifically inducing the death of β-galactosidase-expressing cells in response to photoirradiation. By using a selenium-substituted rhodol scaffold bearing β-galactoside as a targeting substituent, we designed and synthesized HMDESeR-βGal, which has a non-phototoxic spirocyclic structure owing to the presence of the galactoside moiety. However, β-galactosidase efficiently converted HMDESeR-βGal into phototoxic HMDESeR, which exists predominantly in the open xanthene form. This structural change resulted in drastic recovery of visible-wavelength absorption and the ability to generate singlet oxygen (1O2). When HMDESeR-βGal was applied to larval Drosophila melanogaster wing disks, which express β-galactosidase only in the posterior region, photoirradiation induced cell death in the β-galactosidase-expressing region with high specificity. [ABSTRACT FROM AUTHOR]

Published

2014