Your search keyword '"Nakayama, Jun"' showing total 129 results

1. Proteins and noncoding RNAs that promote homologous chromosome recognition and pairing in fission yeast meiosis undergo condensate formation in vitro.

Author

Ding, Da‐Qiao, Okamasa, Kasumi, Yoshimura, Yuriko, Matsuda, Atsushi, Yamamoto, Takaharu G., Hiraoka, Yasushi, and Nakayama, Jun‐ichi

Published

2024

2. Analysis of the responsiveness to antiandrogens in multiple breast cancer cell lines.

Author

Kuroiwa, Yuka, Ito, Kagenori, Nakayama, Jun, Semba, Kentaro, and Yamamoto, Yusuke

Subjects

CELL lines, BREAST cancer, ANDROGEN receptors, ANTIANDROGENS, CANCER cells

Abstract

Antiandrogens were originally developed as therapeutic agents for prostate cancer but are also expected to be effective for breast cancer. However, the role of androgen signaling in breast cancer has long been controversial due to the limited number of experimental models. Our study aimed to comprehensively investigate the efficacy of antiandrogens on breast cancer. In the present study, a total of 18 breast cancer cell lines were treated with the agonist or antagonists of the androgen receptor (AR). Among the 18 cell lines tested, only T‐47D cells proliferated in an androgen‐dependent manner, while the other cell lines were almost irresponsive to AR stimulation. On the other hand, treatment with AR antagonists at relatively high doses suppressed the proliferation of not only T‐47D cells but also some other cell lines including AR‐low/negative cells. In addition, expression of the full‐length AR and constitutively active AR splice variants, AR‐V7 and ARV567es, was not correlated with sensitivity to AR antagonists. These data suggest that the antiproliferative effect of AR antagonists is AR‐independent in some cases. Consistently, proliferation of AR‐knockout BT‐549 cells was inhibited by AR antagonists. Identification of biomarkers would be necessary to determine which breast cancer patients will benefit from these drugs. [ABSTRACT FROM AUTHOR]

Published

2024

3. Metastatic potentials classified with hypoxia‐inducible factor 1 downstream genes in pan‐cancer cell lines.

Author

Nakamichi, Kazuya, Yamamoto, Yusuke, Semba, Kentaro, and Nakayama, Jun

Subjects

HYPOXIA-inducible factor 1, CELL lines, WARBURG Effect (Oncology), STERNUM, POST-translational modification

Abstract

Hypoxia‐inducible factor 1 (HIF1) is a transcription factor that is stabilized under hypoxia conditions via post‐translational modifications. HIF1 regulates tumor malignancy and metastasis by gene transcriptions, such as Warburg effect and angiogenesis‐related genes, in cancer cells. However, the HIF1 downstream genes show varied expressional patterns in different cancer types. Herein, we performed the hierarchical clustering based on the HIF1 downstream gene expression patterns using 1406 cancer cell lines crossing 30 types of cancer to understand the relationship between HIF1 downstream genes and the metastatic potential of cancer cell lines. Two types of cancers, including bone and breast cancers, were classified based on HIF1 downstream genes with significantly altered metastatic potentials. Furthermore, different HIF1 downstream gene subsets were extracted to discriminate each subtype for these cancer types. HIF1 downstream subtyping classification will help to understand the novel insight into tumor malignancy and metastasis in each cancer type. [ABSTRACT FROM AUTHOR]

Published

2024

4. Osteoblast‐derived extracellular vesicles exert osteoblastic and tumor‐suppressive functions via SERPINA3 and LCN2 in prostate cancer.

Author

Ito, Kagenori, Yamamoto, Tomofumi, Hayashi, Yusuke, Sato, Shun, Nakayama, Jun, Urabe, Fumihiko, Shimasaki, Takeo, Nakamura, Eijiro, Matui, Yoshiyuki, Fujimoto, Hiroyuki, Kimura, Takahiro, Egawa, Shin, Ochiya, Takahiro, and Yamamoto, Yusuke

Abstract

Clinically, the osteolytic phenotype is rare in prostate cancer (PCa), and the prognosis is generally worse than that of the osteoblastic phenotype. Osteoblastic prostate cancer (BPCa) is a major type of bone metastasis. Several factors responsible for osteogenesis have been identified, but the molecular mechanism of osteoblastic bone metastasis in PCa is not fully understood. Here, we show the osteogenic and tumor‐suppressive roles of SERPINA3 and LCN2 in BPCa. In a co‐culture of osteoblasts (OBs) and BPCa cells, SERPINA3 and LCN2 were remarkably upregulated in BPCa via OB‐derived extracellular vesicles, while they were not in the co‐culture of OBs and osteolytic prostate cancer (LPCa) cells. In both the co‐culture system and mouse xenograft experiments with intracaudal injection, enhanced expression of SERPINA3 and LCN2 in PCa led to osteogenesis. Additionally, the addition of SERPINA3 and LCN2 to BPCa cells significantly suppressed the proliferative potential. Retrospective analysis also confirmed that high expression levels of SERPINA3 and LCN2 were significantly correlated with a better prognosis. Our results may partially explain how osteoblastic bone metastasis develops and why the prognosis for BPCa is relatively better than that for LPCa. [ABSTRACT FROM AUTHOR]

Published

2023

5. Increased GS‐II lectin binding and SATB2 downregulation are biological features for sessile serrated lesions and microvesicular hyperplastic polyps.

Author

Matoba, Hisanori, Iwaya, Mai, Sato, Yoshiko, Kobayashi, Noriyasu, Takemura, Haruka, Kouno, Yusuke, Karasawa, Ayumi, and Nakayama, Jun

Subjects

POLYPS, DOWNREGULATION, LECTINS, CARRIER proteins, AMINO acid sequence, IMMUNOSTAINING

Abstract

Sessile serrated lesions (SSLs) and microvesicular hyperplastic polyps (MVHPs) are colorectal lesions displaying gastric differentiation. Griffonia simplicifolia‐II (GS‐II) is a lectin specific to terminal α/βGlcNAc residues. Here, we assessed GS‐II binding and performed immunostaining for HIK1083 (specific to terminal αGlcNAc residues), MUC5AC, MUC6, and special AT‐rich sequence binding protein 2 (SATB2) in SSLs, MVHPs, and tubular adenomas (TAs). We observed MUC5AC positivity in 28 of 30 SSLs, but in only three of 23 TAs. Moreover, 24 of 30 SSLs were MUC6‐positive, while none of the 23 TAs were MUC6‐positive. None of the 30 SSLs or 23 TAs showed HIK1083 positivity. All 30 SSLs and 26 MVHPs were GS‐II‐positive, while only seven of 23 were in TAs. GS‐II staining was mainly distributed in the Golgi region, but SSLs and MVHPs showed goblet cell distribution, in 20 of 30 and 19 of 26 cases, respectively. All SSLs, MVHPs, and TAs were SATB2‐positive, but 21 of 30 SSLs and 12 of 26 MVHPs showed decreased staining intensity relative to adjacent mucosa, a decrease seen in only two of 23 in TAs. These results indicate overall that increased terminal βGlcNAc and decreased SATB2 expression are characteristics of SSLs and MVHPs. [ABSTRACT FROM AUTHOR]

Published

2023

6. Researchers support preprints and open access publishing, but with reservations: A questionnaire survey of MBSJ members.

Author

Ide, Kazuki and Nakayama, Jun‐ichi

Subjects

*OPEN access publishing, *PREPRINTS, *UNIVERSITY faculty, *SCHOLARLY publishing, *MOLECULAR biology

Abstract

Since the 1990s, journals have become increasingly online and open access. In fact, about 50% of articles published in 2021 were open access. The use of preprints (i.e., non‐peer‐reviewed articles) has also increased. However, there is limited awareness of these concepts among academics. Therefore, we conducted a questionnaire‐based survey among members of the Molecular Biology Society of Japan. The survey was conducted between September 2022 and October 2022, with 633 respondents, 500 of whom (79.0%) were faculty members. In total, 478 (76.6%) respondents had published articles as open access, and 571 (91.5%) wanted to publish their articles in open access. Although 540 (86.5%) respondents knew about preprints, only 183 (33.9%) had posted preprints before. In the open‐ended section of the questionnaire survey, several comments were made about the cost burdens associated with open access and the difficulty of how academic preprints are handled. Although open access is widespread, and recognition of preprints is increasing, some issues remain that need to be addressed. Academic and institutional support, and transformative agreement may help reduce the cost burden. Guidelines for handling preprints in academia are also important for responding to changes in the research environment. [ABSTRACT FROM AUTHOR]

Published

2023

7. HOXB7 induces STAT3‐mediated transformation and lung metastasis in immortalized mammary gland NMuMG cells.

Author

Azuma, Kazushi, Sakamoto, Mai, Katayama, Shota, Matsui, Atsuka, Nakamichi, Kazuya, Goshima, Naoki, Watanabe, Shinya, Nakayama, Jun, and Semba, Kentaro

Subjects

MAMMARY glands, HER2 positive breast cancer, LUNGS, EPITHELIAL-mesenchymal transition, BREAST, HOMEOBOX genes, BREAST cancer prognosis

Abstract

The homeobox family genes are often dysregulated in various cancer types. Particularly HOXB7 amplification and overexpression correlate with poor prognosis in various cancer such as gastric, pancreatic, and lung cancers. Moreover, HOXB7 is known to contribute to cancer progression by promoting epithelial to mesenchymal transition, anticancer drug resistance, and angiogenesis. In this study, we show that HOXB7 is coamplified with ERBB2 in a subset of breast cancer patients and HOXB7 expression correlates with poor prognosis in HER2‐positive breast cancer patients. This clinical observation is supported by the following results—HOXB7 overexpression in an immortalized murine mammary gland epithelial cell line NMuMG induces cellular transformation in vitro, tumorigenesis, and lung metastasis through the activation of JAK‐STAT signaling. [ABSTRACT FROM AUTHOR]

Published

2023

8. α1,4‐Linked N‐acetylglucosamine suppresses gastric cancer development by inhibiting Mucin‐1‐mediated signaling.

Author

Fujii, Chifumi, Harumiya, Satoru, Sato, Yoshiko, Kawakubo, Masatomo, Matoba, Hisanori, and Nakayama, Jun

Abstract

Gastric cancer is the second leading cause of cancer deaths worldwide, and more understanding of its molecular basis is urgently needed. Gastric gland mucin secreted from pyloric gland cells, mucous neck cells, and cardiac gland cells of the gastric mucosa harbors unique O‐glycans carrying terminal α1,4‐linked N‐acetylglucosamine (αGlcNAc) residues. We previously reported that αGlcNAc loss correlated positively with poor outcomes for patients with differentiated‐type gastric cancer. However, the molecular mechanisms underlying these outcomes remained poorly understood. Here, we examined the effects of upregulated αGlcNAc expression on malignant phenotypes of the differentiated‐type gastric cancer cell lines, AGS and MKN7. Upregulation of αGlcNAc following ectopic expression of its biosynthetic enzyme attenuated cell proliferation, motility, and invasiveness of AGS and MKN7 cells in vitro. Moreover, AGS cell tumorigenicity was significantly suppressed by αGlcNAc overexpression in a xenograft model. To define the molecular mechanisms underlying these phenotypes, we investigated αGlcNAc binding proteins in AGS cells and identified Mucin‐1 (MUC1) and podocalyxin. Both proteins were colocalized with αGlcNAc on human gastric cancer cells. We also found that αGlcNAc was bound to MUC1 in murine normal gastric mucosa. When we assessed the effects of αGlcNAc binding to MUC1, we found that αGlcNAc blocked galectin‐3 binding to MUC1, phosphorylation of the MUC1 C‐terminus, and recruitment of Src and β‐catenin to that C‐terminus. These results suggest that αGlcNAc regulates cancer cell phenotypes by dampening MUC1 signal transduction. [ABSTRACT FROM AUTHOR]

Published

2022

9. Mucin distribution in bronchiolar adenoma/ciliated muconodular papillary tumor reveals organoid differentiation simulating the normal lung.

Author

Matoba, Hisanori, Ikeyama, Meguru, Kobayashi, Noriyasu, Takemura, Haruka, Hanaoka, Takaomi, Sato, Yoshiko, and Nakayama, Jun

Subjects

ADENOMA, LUNGS, MUCINS, ADENOMATOUS polyps, LUNG tumors, TUMORS, BRONCHI

Abstract

Bronchiolar adenoma/ciliated muconodular papillary tumor is a lung neoplasm exhibiting various degrees of proximal and distal bronchiolar differentiation. Here, we evaluated distribution of MUC5AC and MUC5B in bronchiolar adenoma/ciliated muconodular papillary tumor for comparison with that seen in normal respiratory tract. In normal respiratory tract, MUC5AC was mainly distributed in large bronchi, while MUC5B was distributed in bronchi, bronchioles, and submucosal glands. In bronchiolar adenoma/ciliated muconodular papillary tumor, MUC5AC was primarily distributed in luminal cells of large airspaces, and MUC5B was distributed in luminal cells of small airspaces and mucinous glands, in addition to large airspaces, regardless of distal or proximal differentiation. In particular, MUC5B was distributed in non‐mucinous club and ciliated cells in both the normal respiratory tract and bronchiolar adenoma/ciliated muconodular papillary tumor. These results indicate that MUC5AC and MUC5B distribution in bronchiolar adenoma/ciliated muconodular papillary tumor is similar to that seen in normal respiratory tract, suggestive of organoid differentiation simulating the normal lung. [ABSTRACT FROM AUTHOR]

Published

2022

10. Glycosylation of MUC6 by α1,4‐linked N‐acetylglucosamine enhances suppression of pancreatic cancer malignancy.

Author

Yuki, Atsuko, Fujii, Chifumi, Yamanoi, Kazuhiro, Matoba, Hisanori, Harumiya, Satoru, Kawakubo, Masatomo, and Nakayama, Jun

Abstract

Biomarkers for early diagnosis of pancreatic cancer are greatly needed, as the high fatality of this cancer is in part due to delayed detection. α1,4‐linked N‐acetylglucosamine (αGlcNAc), a unique O‐glycan specific to gastric gland mucus, is biosynthesized by α1,4‐N‐acetylglucosaminyltransferase (α4GnT) and primarily bound at the terminal glycosylated residue to scaffold protein MUC6. We previously reported that αGlcNAc expression decreases at early stages of neoplastic pancreatic lesions, followed by decreased MUC6 expression, although functional effects of these outcomes were unknown. Here, we ectopically expressed α4GnT, the αGlcNAc biosynthetic enzyme, together with MUC6 in the human pancreatic cancer cell lines MIA PaCa‐2 and PANC‐1, neither of which expresses α4GnT and MUC6. We observed significantly suppressed proliferation in both lines following coexpression of α4GnT and MUC6. Moreover, cellular motility decreased following MUC6 ectopic expression, an effect enhanced by cotransduction with α4GnT. MUC6 expression also attenuated invasiveness of both lines relative to controls, and this effect was also enhanced by additional α4GnT expression. We found αGlcNAc‐bound MUC6 formed a complex with trefoil factor 2. Furthermore, analysis of survival curves of patients with pancreatic ductal adenocarcinoma using a gene expression database showed that samples marked by higher A4GNT or MUC6 mRNA levels were associated with relatively favorable prognosis. These results strongly suggest that αGlcNAc and MUC6 function as tumor suppressors in pancreatic cancer and that decreased expression of both may serve as a biomarker of tumor progression to pancreatic cancer. [ABSTRACT FROM AUTHOR]

Published

2022

11. Decreased alpha‐1,4‐linked N‐acetylglucosamine glycosylation in biliary tract cancer progression from biliary intraepithelial neoplasia to invasive adenocarcinoma.

Author

Okumura, Motohiro, Yamanoi, Kazuhiro, Uehara, Takeshi, and Nakayama, Jun

Abstract

Biliary tract cancer (BTC) is typically lethal due to the difficulty of early stage diagnosis. Thus, novel biomarkers of BTC precursors are necessary. Biliary intraepithelial neoplasia (BilIN) is a major precursor of BTC and is classified as low or high grade based on cell atypia. In normal gastric mucosa, gastric gland mucin‐specific O‐glycans are unique in having α1,4‐linked N‐acetylglucosamine (αGlcNAc) attached to MUC6. Previously, we reported that αGlcNAc functions as a tumor suppressor of differentiated‐type gastric adenocarcinoma and that decreased αGlcNAc glycosylation on MUC6 in gastric, pancreatic, and uterine cervical neoplasms occurs in cancer as well as in their precursor lesions. However, αGlcNAc and MUC6 expression patterns in biliary tract neoplasms have remained unclear. Here, we analyzed MUC5AC, MUC6, and αGlcNAc expression status in 51 BTC cases and compared the expression of each with progression from low‐grade BilIN to invasive adenocarcinoma (IAC). The frequency of αGlcNAc‐positive and MUC6‐positive lesions decreased with tumor progression. When we compared each marker's expression level with tumor progression, we found that the MUC6 expression score in IAC was significantly lower than in low‐grade or high‐grade BilIN (P < 0.001 or P < 0.01, respectively). However, the αGlcNAc expression score was low irrespective of histological grade, and also lower than that of MUC6 across all histological grades (P < 0.001 for low‐grade and high‐grade BilIN, and P < 0.01 for IAC). These results suggest that decreased expression of αGlcNAc relative to MUC6 marks the initiation of BTC progression. [ABSTRACT FROM AUTHOR]

Published

2020

12. Diffuse MIST1 expression and decreased α1,4‐linked N‐acetylglucosamine (αGlcNAc) glycosylation on MUC6 are distinct hallmarks for gastric neoplasms showing oxyntic gland differentiation.

Author

Yamada, Shigenori, Yamanoi, Kazuhiro, Sato, Yoshiko, and Nakayama, Jun

Subjects

GASTRIC mucosa, N-acetylglucosamine, GLANDS, TUMORS, GLYCOSYLATION, CHLOROGENIC acid, GLYCANS

Abstract

Aims: Gastric neoplasms showing oxyntic gland differentiation (GAOGs) constitute a gastric neoplasm subtype that shows low atypia, thus similar to non‐neoplastic gastric oxyntic glands. Therefore, their diagnosis in biopsy specimens is difficult. GAOGs were first described in 2007, and introduced in the latest World Health Organization classification book as gastric adenocarcinoma of the fundic gland type (GA‐FG) and oxyntic gland adenoma. Previously, we assessed α1,4‐linked N‐acetylglucosamine (αGlcNAc) residues attached to the MUC6 scaffold in gastric neoplasms, and observed decreased αGlcNAc glycosylation in both differentiated‐type gastric cancer and high‐grade pyloric gland adenoma (PGA), a gastric cancer precursor. GA‐FG and PGA often harbour the same mutations. However, the αGlcNAc status in GAOGs remained unknown. To elucidate αGlcNAc expression in GAOGs, we performed the study. Methods and results: We assessed the expression of αGlcNAc; the mucin markers MUC6, MUC5AC, and MUC2; the gastric gland cell markers MIST1, pepsinogen 1 (PG1), H/K‐ATPase and chromogranin‐A (CGA); and the proliferation marker Ki67 in 13 GAOG lesions. All 13 (100%) were MUC6‐positive, whereas 10 (76.2%) were αGlcNAc‐negative. Moreover, all 13 (100%) were MIST1‐ and PG1‐positive, three (23.1%) were MUC5AC‐positive, four (30.8%) were H/K‐ATPase‐positive, and one (7.7%) was CGA‐positive. Conclusions: GAOGs frequently lost αGlcNAc residues on MUC6, but expressed the gastric gland progenitor marker MIST1 and aberrantly expressed various types of gastric gland cell lineage marker, suggestive of immature differentiation to gastric gland cells. Thus, diffuse MIST1 positivity and decreased αGlcNAc glycosylation on MUC6‐positive cells could serve as important biomarkers for the histopathological diagnosis of GAOG. [ABSTRACT FROM AUTHOR]

Published

2020

13. Polyunsaturated fatty acid deficiency affects sulfatides and other sulfated glycans in lysosomes through autophagy‐mediated degradation.

Author

Wang, Yaping, Nakajima, Takero, Diao, Pan, Yamada, Yosuke, Nakamura, Kozo, Nakayama, Jun, Tanaka, Naoki, Aoyama, Toshifumi, and Kamijo, Yuji

Published

2020

14. Establishment and characterization of highly osteolytic luminal breast cancer cell lines by intracaudal arterial injection.

Author

Han, Yuxuan, Nakayama, Jun, Hayashi, Yusuke, Jeong, Seongmoon, Futakuchi, Mitsuru, Ito, Emi, Watanabe, Shinya, and Semba, Kentaro

Subjects

*CELL lines, *BREAST cancer, *METASTATIC breast cancer, *TRIPLE-negative breast cancer, *CANCER cells

Abstract

Bone is one of the most common metastatic sites of breast cancer, and bone metastasis profoundly affects the quality of life of breast cancer patients. Bone metastasis is commonly observed among all the subtypes of breast cancer; however, its molecular mechanism has been analyzed only in triple‐negative subtype of breast cancer (TNBC). To characterize the molecular mechanisms of bone metastasis of luminal breast cancer, we established a bone‐metastatic model of the MCF7, luminal breast cancer cell line, with enhanced osteolytic activity by intracaudal arterial injection (CAI). Pathological analysis of the established cell lines revealed that they exhibited fierce osteolytic ability by promoting osteoclast differentiation and activity. The signature genes extracted from highly osteolytic MCF7 cell lines were differed from those of bone‐metastatic TNBC cell lines. Our results suggest that unique mechanisms of osteolysis in bone‐metastatic lesions of luminal breast cancer. In addition, several up‐regulated genes in MCF7‐BM (Bone Metastasis) 02 cell lines correlated with poor prognosis with luminal breast cancer patients. Our findings support further study on the bone‐metastatic mechanisms of luminal breast cancer. [ABSTRACT FROM AUTHOR]

Published

2020

15. SNX9 determines the surface levels of integrin β1 in vascular endothelial cells: Implication in poor prognosis of human colorectal cancers overexpressing SNX9.

Author

Tanigawa, Kazufumi, Maekawa, Masashi, Kiyoi, Takeshi, Nakayama, Jun, Kitazawa, Riko, Kitazawa, Sohei, Semba, Kentaro, Taguchi, Tomohiko, Akita, Satoshi, Yoshida, Motohira, Ishimaru, Kei, Watanabe, Yuji, and Higashiyama, Shigeki

Subjects

VASCULAR endothelial cells, VASCULAR endothelial growth factor receptors, COLORECTAL cancer, INTEGRINS, VASCULAR endothelial growth factors, INTRACELLULAR membranes

Abstract

Angiogenesis, the formation of new blood vessels, is involved in a variety of diseases including the tumor growth. In response to various angiogenic stimulations, a number of proteins on the surface of vascular endothelial cells are activated to coordinate cell proliferation, migration, and spreading processes to form new blood vessels. Plasma membrane localization of these angiogenic proteins, which include vascular endothelial growth factor receptors and integrins, are warranted by intracellular membrane trafficking. Here, by using a siRNA library, we screened for the sorting nexin family that regulates intracellular trafficking and identified sorting nexin 9 (SNX9) as a novel angiogenic factor in human umbilical vein endothelial cells (HUVECs). SNX9 was essential for cell spreading on the Matrigel, and tube formation that mimics in vivo angiogenesis in HUVECs. SNX9 depletion significantly delayed the recycling of integrin β1, an essential adhesion molecule for angiogenesis, and reduced the surface levels of integrin β1 in HUVECs. Clinically, we showed that SNX9 protein was highly expressed in tumor endothelial cells of human colorectal cancer tissues. High‐level expression of SNX9 messenger RNA significantly correlated with poor prognosis of the patients with colorectal cancer. These results suggest that SNX9 is an angiogenic factor and provide a novel target for the development of new antiangiogenic drugs. [ABSTRACT FROM AUTHOR]

Published

2019

16. Cullin‐3/KCTD10 E3 complex is essential for Rac1 activation through RhoB degradation in human epidermal growth factor receptor 2‐positive breast cancer cells.

Author

Murakami, Akari, Maekawa, Masashi, Kawai, Katsuhisa, Nakayama, Jun, Araki, Nobukazu, Semba, Kentaro, Taguchi, Tomohiko, Kamei, Yoshiaki, Takada, Yasutsugu, and Higashiyama, Shigeki

Abstract

Rho GTPase Rac1 is a central regulator of F‐actin organization and signal transduction to control plasma membrane dynamics and cell proliferation. Dysregulated Rac1 activity is often observed in various cancers including breast cancer and is suggested to be critical for malignancy. Here, we showed that the ubiquitin E3 ligase complex Cullin‐3 (CUL3)/KCTD10 is essential for epidermal growth factor (EGF)‐induced/human epidermal growth factor receptor 2 (HER2)‐dependent Rac1 activation in HER2‐positive breast cancer cells. EGF‐induced dorsal membrane ruffle formation and cell proliferation that depends on both Rac1 and HER2 were suppressed in CUL3‐ or KCTD10‐depleted cells. Mechanistically, CUL3/KCTD10 ubiquitinated RhoB for degradation, another Rho GTPase that inhibits Rac1 activation at the plasma membrane by suppressing endosome‐to‐plasma membrane traffic of Rac1. In HER2‐positive breast cancers, high expression of Rac1 mRNA significantly correlated with poor prognosis of the patients. This study shows that this novel molecular axis (CUL3/KCTD10/RhoB) positively regulates the activity of Rac1 in HER2‐positive breast cancers, and our findings may lead to new treatment options for HER2‐ and Rac1‐positive breast cancers. CUL3/KCTD10/RhoB ubiquitin E3 protein complex is a novel regulator of Rac1 activation. The axis may be a promising target for development of novel anti‐cancer drugs to HER2‐positive breast cancers. [ABSTRACT FROM AUTHOR]

Published

2019

17. Annexin A1 expression is correlated with malignant potential of renal cell carcinoma.

Author

Yamanoi, Mariko, Yamanoi, Kazuhiro, Fujii, Chifumi, Nakayama, Jun, and Fukuda, Michiko N

Subjects

RENAL cell carcinoma, HYPOXIA-inducible factors, LOG-rank test, PROGRESSION-free survival, CELL lines

Abstract

Objectives: To evaluate the expression of annexin A1 protein in patients with renal cell carcinoma. Methods: Annexin A1 expression was examined in renal cell carcinoma specimens from 27 patients, and their disease‐free survival was analyzed using the log–rank test. Annexin A1 knockdown in the human renal cell carcinoma cell line Caki‐1 was carried out, and its proliferation, invasion, motility and adhesion were compared with those of control cells. Results: In 13 out of 27 patients, annexin A1 was highly expressed in the membrane of renal cell carcinoma tumor cells, whereas in the rest of the patients, annexin A1 expression was weak or negligible in the membrane of those cells. Patients with high annexin A1 expression had significantly poorer disease‐free survival than those with weak or negligible annexin A1 expression (P = 0.031). In the renal cell carcinoma cell line, annexin A1 knockdown cells showed significantly decreased proliferation, invasion, motility and adhesion relative to control cells, and expressed lower relative levels of membrane‐type 1 matrix metalloproteinase and hypoxia‐inducible factor 1‐alpha transcripts, showing a potential pathway regulated by annexin A1. Conclusion: Annexin A1 is associated with renal cell carcinoma malignant potential and could serve as a marker of poor prognosis. [ABSTRACT FROM AUTHOR]

Published

2019

18. Meiosis‐specific cohesin component, Rec8, promotes the localization of Mps3 SUN domain protein on the nuclear envelope.

Author

Bommi, Jagadeeswara Rao, Rao, Hanumanthu Bala Durga Prasada, Challa, Kiran, Higashide, Mika, Shinmyozu, Kaori, Nakayama, Jun‐ichi, Shinohara, Miki, and Shinohara, Akira

Subjects

MEIOSIS, COHESINS, NUCLEAR membranes, BUDDING (Zoology), GENE expression, CENTROSOMES

Abstract

Proteins in the nuclear envelope (NE) play a role in the dynamics and functions of the nucleus and of chromosomes during mitosis and meiosis. Mps3, a yeast NE protein with a conserved SUN domain, predominantly localizes on a yeast centrosome equivalent, spindle pole body (SPB), in mitotic cells. During meiosis, Mps3, together with SPB, forms a distinct multiple ensemble on NE. How meiosis‐specific NE localization of Mps3 is regulated remains largely unknown. In this study, we found that a meiosis‐specific component of the protein complex essential for sister chromatid cohesion, Rec8, binds to Mps3 during meiosis and controls Mps3 localization and proper dynamics on NE. Ectopic expression of Rec8 in mitotic yeast cells induced the formation of Mps3 patches/foci on NE. This required the cohesin regulator, WAPL ortholog, Rad61/Wpl1, suggesting that a meiosis‐specific cohesin complex with Rec8 controls NE localization of Mps3. We also observed that two domains of the nucleoplasmic region of Mps3 are essential for NE localization of Mps3 in mitotic as well as meiotic cells. We speculate that the interaction of Mps3 with the meiosis‐specific cohesin in the nucleoplasm is a key determinant for NE localization/function of Mps3. Expression of a meiosis‐specific cohesin component, Rec8, promotes the localization of Mps3 SUN domain protein of the budding yeast on nuclear envelope. [ABSTRACT FROM AUTHOR]

Published

2019

19. Spinal manifestations in 12 patients with musculocontractural Ehlers‐Danlos syndrome caused by CHST14/D4ST1 deficiency (mcEDS‐CHST14).

Author

Uehara, Masashi, Kosho, Tomoki, Yamamoto, Noriaki, Takahashi, Hideaki E., Shimakura, Taketoshi, Nakayama, Jun, Kato, Hiroyuki, and Takahashi, Jun

Abstract

Musculocontractural Ehlers‐Danlos syndrome caused by mutations in CHST14 (mcEDS‐CHST14) is a recently delineated disorder, characterized by craniofacial, skeletal, visceral, and ocular malformations; and progressive cutaneous, skeletal, vascular, and visceral fragility‐related manifestations. Spinal lesions, though one of the most serious complications, have not been investigated systematically. In this study, we report detailed and comprehensive information about spinal lesions of 12 patients with a mean age at the first visit of 13.4 years. Eight patients (66.7%) had scoliosis with a Cobb angle ≥10°, including one with severe scoliosis with a Cobb angle ≥45°. Five patients (41.7%) had kyphosis at the thoracolumbar junction with a kyphotic angle ≥20°. Three patients (25%) developed severe thoracolumbar kyphosis with a kyphotic angle ≥50° accompanied by thoracic lordosis with a wedge‐like vertebral deformity and anterior vertebral osteophyte at the thoracolumbar junction, and two of them underwent surgical correction: complicated by fistula formation in one and performed safely and effectively through two‐staged operation in the other. Six patients (50.0%) had cervical kyphosis, all of whom except one had kyphosis ≥20° at the thoracolumbar level. Two patients (16.7%) had atlantoaxial subluxation, and 10 patients (83.3%) had cervical vertebral malformations. Patients with mcEDS‐CHST14 are susceptible to develop scoliosis, thoracolumbar kyphosis, and cervical kyphosis; and are recommended to have regular surveillance including total spine radiology. The present findings also suggest the critical role of dermatan sulfate in the development and maintenance of the spine. [ABSTRACT FROM AUTHOR]

Published

2018

20. Upregulated expression of La ribonucleoprotein domain family member 6 and collagen type I gene following water‐filtered broad‐spectrum near‐infrared irradiation in a 3‐dimensional human epidermal tissue culture model as revealed by microarray analysis

Author

Tanaka, Yohei and Nakayama, Jun

Subjects

*GENETIC regulation, *NUCLEOPROTEIN genetics, *COLLAGEN genetics, *NEAR infrared radiation, *EPIDERMIS, *GENE expression, *DNA microarrays, *POLYMERASE chain reaction, *PHYSIOLOGY

Abstract

Abstract: Background/Objectives: Water‐filtered broad‐spectrum near‐infrared irradiation can induce various biological effects, as our previous clinical, histological, and biochemical investigations have shown. However, few studies that examined the changes thus induced in gene expression. The aim was to investigate the changes in gene expression in a 3‐dimensional reconstructed epidermal tissue culture exposed to water‐filtered broad‐spectrum near‐infrared irradiation. Methods: DNA microarray and quantitative real‐time polymerase chain reaction (PCR) analysis was used to assess gene expression levels in a 3‐dimensional reconstructed epidermal model composed of normal human epidermal cells exposed to water‐filtered broad‐spectrum near‐infrared irradiation. The water filter allowed 1000–1800 nm wavelengths and excluded 1400–1500 nm wavelengths, and cells were exposed to 5 or 10 rounds of near‐infrared irradiation at 10 J/cm2. Results: A DNA microarray with over 50 000 different probes showed 18 genes that were upregulated or downregulated by at least twofold after irradiation. Quantitative real‐time PCR revealed that, relative to control cells, the gene encoding La ribonucleoprotein domain family member 6 (LARP6), which regulates collagen expression, was significantly and dose‐dependently upregulated (P < 0.05) by water‐filtered broad‐spectrum near‐infrared exposure. Gene encoding transcripts of collagen type I were significantly upregulated compared with controls (P < 0.05). Conclusions: This study demonstrates the ability of water‐filtered broad‐spectrum near‐infrared irradiation to stimulate the production of type I collagen. [ABSTRACT FROM AUTHOR]

Published

2018

21. <italic>Cholesterol‐</italic>α<italic>‐glucosyltransferase</italic> gene is present in most <italic>Helicobacter</italic> species including gastric non‐<italic>Helicobacter pylori</italic> helicobacters obtained from Japanese patients

Author

Kawakubo, Masatomo, Horiuchi, Kazuki, Matsumoto, Takehisa, Nakayama, Jun, Akamatsu, Taiji, Katsuyama, Tsutomu, Ota, Hiroyoshi, and Sagara, Junji

Subjects

HELICOBACTER pylori, GLYCOSYLTRANSFERASES, POLYMERASE chain reaction, BACTERIA phylogeny, GENE expression in bacteria, GLYCOLIPIDS, JAPANESE people, HEALTH

Abstract

Abstract: Background: Non‐Helicobacter pylori helicobacters (NHPHs) besides H. pylori infect human stomachs and cause chronic gastritis and mucosa‐associated lymphoid tissue lymphoma. Cholesteryl‐α‐glucosides have been identified as unique glycolipids present in H. pylori and some Helicobacter species. Cholesterol‐α‐glucosyltransferase (αCgT), a key enzyme for the biosynthesis of cholesteryl‐α‐glucosides, plays crucial roles in the pathogenicity of H. pylori. Therefore, it is important to examine αCgTs of NHPHs. Materials and Methods: Six gastric NHPHs were isolated from Japanese patients and maintained in mouse stomachs. The αCgT genes were amplified by PCR and inverse PCR. We retrieved the αCgT genes of other Helicobacter species by BLAST searches in GenBank. Results: αCgT genes were present in most Helicobacter species and in all Japanese isolates examined. However, we could find no candidate gene for αCgT in the whole genome of Helicobacter cinaedi and several enterohepatic species. Phylogenic analysis demonstrated that the αCgT genes of all Japanese isolates show high similarities to that of a zoonotic group of gastric NHPHs including Helicobacter suis, Helicobacter heilmannii, and Helicobacter ailurogastricus. Of 6 Japanese isolates, the αCgT genes of 4 isolates were identical to that of H. suis, and that of another 2 isolates were similar to that of H. heilmannii and H. ailurogastricus. Conclusions: All gastric NHPHs examined showed presence of αCgT genes, indicating that αCgT may be beneficial for these helicobacters to infect human and possibly animal stomachs. Our study indicated that NHPHs could be classified into 2 groups, NHPHs with αCgT genes and NHPHs without αCgT genes. [ABSTRACT FROM AUTHOR]

Published

2018

22. Gastric gland mucin-specific O-glycan expression decreases with tumor progression from precursor lesions to pancreatic cancer.

Author

Ohya, Ayumi, Yamanoi, Kazuhiro, Shimojo, Hisashi, Fujii, Chifumi, and Nakayama, Jun

Abstract

Pancreatic cancer is lethal, as it is often detected late. Thus, novel biomarkers of precursor lesions are needed to devise timely therapies. Pancreatic intraepithelial neoplasia (Pan IN) and intraductal papillary mucinous neoplasm ( IPMN) are major precursors of pancreatic cancer. In normal gastric mucosa, gastric gland mucin-specific O-glycans are unique in having α1,4-linked N-acetylglucosamine (αGlc NAc) residues attached to MUC6. Recently we reported that αGlc NAc functions as a tumor suppressor for differentiated-type gastric adenocarcinoma (Karasawa et al., J Clin Invest 122, 923, 2012). MUC6 is also expressed in pancreatic neoplasms, including Pan IN and IPMN, but the role of αGlc NAc expression in pancreatic neoplasms remains unknown. Here, we analyze expression patterns of αGlc NAc, MUC6 and MUC5 AC in pancreatic neoplasms and compare them with progression from Pan IN to invasive ductal adenocarcinoma ( IDAC) (the Pan IN- IDAC sequence; 20 cases) and from IPMN to IPMN with associated invasive carcinoma ( IPMNAIC) (the IPMN- IPMNAIC sequence; 20 cases). At both sequences, the frequency of MUC6-positive and αGlc NAc-positive lesions decreased with tumor progression. We then compared expression levels of αGlc NAc and MUC6 at each step of the progression. At the Pan IN- IDAC sequence, αGlc NAc expression significantly decreased relative to MUC6 in low-grade Pan IN ( P = 0.021), high-grade Pan IN/intraductal spread of IDAC ( P = 0.031) and IDAC ( P = 0.013). At the IPMN- IPMNAIC sequence, decreased αGlc NAc expression was also observed in low-grade IPMN exhibiting gastric-type morphology ( P = 0.020). These results suggest that decreased expression of αGlc NAc relative to MUC6 occurs early and marks the initiation of tumor progression to pancreatic cancer. [ABSTRACT FROM AUTHOR]

Published

2017

23. Four domains of Ada1 form a heterochromatin boundary through different mechanisms.

Author

Kamata, Kazuma, Shinmyozu, Kaori, Nakayama, Jun‐ichi, Hatashita, Masanori, Uchida, Hiroyuki, and Oki, Masaya

Subjects

SACCHAROMYCES cerevisiae, EUKARYOTIC cell genetics, HETEROCHROMATIN, ACETYLTRANSFERASES, PROTEASOMES

Abstract

In eukaryotic cells, there are two chromatin states, silenced and active, and the formation of a so-called boundary plays a critical role in demarcating these regions; however, the mechanisms underlying boundary formation are not well understood. In this study, we focused on S. cerevisiae ADA1, a gene previously shown to encode a protein with a robust boundary function. Ada1 is a component of the histone modification complex Spt-Ada-Gcn5-acetyltransferase ( SAGA) and the SAGA-like ( SLIK) complex, and it helps to maintain the integrity of these complexes. Domain analysis showed that four relatively small regions of Ada1 (Region I; 66-75 aa, II; 232-282 aa, III; 416-436 aa and IV; 476-488 aa) have a boundary function. Among these, Region II could form an intact SAGA complex, whereas the other regions could not. Investigation of cellular factors that interact with these small regions identified a number of proteasome-associated proteins. Interestingly, the boundary functions of Region II and Region III were affected by depletion of Ump1, a maturation and assembly factor of the 20S proteasome. These results suggest that the boundary function of Ada1 is functionally linked to proteasome processes and that the four relatively small regions in ADA1 form a boundary via different mechanisms. [ABSTRACT FROM AUTHOR]

Published

2016

24. Decreased expression of gastric gland mucin-specific glycan α1,4-linked N-acetylglucosamine on its scaffold mucin 6 is associated with malignant potential of pyloric gland adenoma of the stomach.

Author

Yamanoi, Kazuhiro, Sekine, Shigeki, Higuchi, Kayoko, Kushima, Ryoji, and Nakayama, Jun

Subjects

GENE expression, N-acetylglucosamine, GLYCANS, GASTRIC mucosa, ADENOCARCINOMA, TUMOR suppressor genes, IMMUNOHISTOCHEMISTRY

Abstract

Aims: Pyloric gland adenoma (PGA) is a unique gastric neoplasm expressing mucin 6 (MUC6), and is often associated with high-grade dysplasia and/or adenocarcinoma. MUC6 secreted from the gastric gland mucous cells, such as pyloric gland cells, carries unique O-glycans with terminal α1,4-linked N-acetylglucosamine (αGlcNAc) residues on its molecule. As we recently demonstrated that αGlcNAc serves as a tumour suppressor for gastric adenocarcinoma, this study aimed to investigate the significance of αGlcNAc expression in PGA. Methods and results: Eighteen patients with PGA were examined with immunohistochemistry for αGlc- NAc and MUC6. αGlcNAc and MUC6 were coexpressed in 12 of 18 PGAs. However, reduced αGlcNAc expression relative to MUC6 expression was observed in six cases. When the MIB-1 labelling index (LI) of tumour cells was examined with respect to reduced αGlcNAc expression, the MIB-1 LI was significantly higher in PGAs showing decreased αGlcNAc expression relative to MUC6 expression than in PGAs with unchanged αGlcNAc expression (P = 0.023). Conclusions: The present study indicates that coexpression of αGlcNAc and MUC6 in PGA suggests the presence of fully glycosylated MUC6 on tumour cells, consistent with pyloric gland differentiation. However, the decreased glycosylation of αGlcNAc on MUC6 is associated with high mitotic activity of tumour cells, indicative of malignant potential of PGA. [ABSTRACT FROM AUTHOR]

Published

2015

25. Reduced gland mucin-specific O-glycan in gastric atrophy: A possible risk factor for differentiated-type adenocarcinoma of the stomach.

Author

Yamada, Shigenori, Okamura, Takuma, Kobayashi, Satoshi, Tanaka, Eiji, and Nakayama, Jun

Subjects

ATROPHY, ADENOCARCINOMA, STOMACH cancer, GASTRIC diseases, GASTRIC mucosa, DISEASE risk factors

Abstract

Background and Aims O-glycans exhibiting terminal α1,4-linked N-acetylglucosamine (α Glc NAc) are attached to MUC6 in gastric gland mucins and serve as a tumor suppressor for gastric adenocarcinoma. Gastric atrophy is associated with risk for gastric cancer. However, the significance of α Glc NAc expression in pyloric glands of chronic atrophic gastritis remains unknown. Here, we asked whether reduced α Glc NAc expression in chronic atrophic gastritis is associated with risk for gastric cancer. Methods We quantitatively analyzed expression of α Glc NAc relative to MUC6 in pyloric glands by immunohistochemistry in 67 patients with normal mucosa, 70 with chronic atrophic gastritis, 68 with intramucosal differentiated-type adenocarcinoma, and 11 with intramucosal undifferentiated-type adenocarcinoma. We also compared the Ki-67 labeling index in gastric epithelial cells between chronic atrophic gastritis and normal gastric mucosa with respect to α Glc NAc reduction. Results In normal pyloric mucosa, α Glc NAc was co-expressed with MUC6. By contrast, in chronic atrophic gastritis, pyloric gland α Glc NAc expression was significantly reduced relative to MUC6. In intramucosal gastric cancer, α Glc NAc expression in pyloric glands found just beneath differentiated-type adenocarcinoma was also reduced relative to MUC6. However, pyloric glands present beneath undifferentiated-type adenocarcinoma exhibited no α Glc NAc decrease. The Ki-67 labeling index in chronic atrophic gastritis showing α Glc NAc reduction was significantly increased relative to that in normal gastric mucosa. Conclusions Because α Glc NAc prevents the gastric cancer development, reduced α Glc NAc expression in chronic atrophic gastritis is a possible risk factor for differentiated-type adenocarcinoma of the stomach. [ABSTRACT FROM AUTHOR]

Published

2015

26. Malignant meningioma with adenocarcinoma-like metaplasia: Demonstration of intestinal phenotype.

Author

Takayama, Yoshiyasu, Nobusawa, Sumihito, Ochiai, Ikuo, Watanabe, Hitoshi, Ishigame, Hiroki, Ikota, Hayato, Hirato, Junko, Nakayama, Jun, and Yokoo, Hideaki

Subjects

METASTASIS, ADENOCARCINOMA, METAPLASIA, MENINGIOMA, EPITHELIUM

Abstract

Meningiomas show a diverse histopathologic appearance, often referred to as metaplastic changes; however, adenocarcinoma-like metaplasia is an extremely rare condition. Here, we present a novel case. A dura-based bulky mass located in the right frontotemporal region was identified radiologically in an 83-year-old woman. The tumor, yellow to ash-gray in color, was subtotally removed. Histopathological examination revealed robust adenocarcinoma-like structures within a conventional meningothelial neoplasm. Meningioma elements showed a WHO grade I to III histology. Morphological and immunophenotypic transition between meningothelial and columnar epithelial cells was confirmed on detailed observation. It was of note that the adenocarcinomatous components shared an immunophenotype with intestinal epithelium, expressing CDX2, MUC2 and cytokeratin 20. The present case could be differentiated from secretory meningioma based on distinct cellular atypia, lack of intracytoplasmic lumina and pseudosammoma bodies, and the intact status of the KLF4 gene. In addition, the morphological and immunophenotypic transition excluded the possibility of metastatic carcinoma within meningioma. This is the first reported case of meningioma with adenocarcinoma-like metaplasia harboring an intestinal immunophenotype. [ABSTRACT FROM AUTHOR]

Published

2015

27. 'Gliomatosis encephali' as a novel category of brain tumors by the first autopsy case report of gliomatosis cerebelli.

Author

Nakahara, Asa, Yoshida, Toshikazu, Yazawa, Masanobu, Ehara, Takashi, Nakayama, Jun, Kakita, Akiyoshi, Ogura, Ryosuke, Asakawa, Mika, Suzuki‐Kouyama, Emi, and Oyanagi, Kiyomitsu

Subjects

GLIOMAS, GLIAL fibrillary acidic protein, VIMENTIN, NECROSIS

Abstract

Gliomatosis cerebri is a rare diffuse glioma that is neither mass-forming nor necrotic, and does not disrupt existing structures. Gliomatosis occurring in the cerebellum is known as gliomatosis cerebelli, and only three such cases examined by biopsy have been reported. Here we describe the first autopsy findings of a patient who was diagnosed as having gliomatosis in the cerebellum. Neuropathological examination identified the tumor cells as being positive for glial fibrillary acidic protein, vimentin and nestin, with atypical nuclei that were cashew-nut- or dishcloth-gourd-shaped. These tumor cells were dense in the right cerebellum, but also spread broadly throughout the brain including the left cerebrum and optic nerve. Mitotic figures were frequently seen in the cerebellum, brain stem and cerebrum. Scherer's secondary structures were evident not only in the cerebellum but also the cerebrum. No necrosis, microvascular proliferation or destruction of anatomical structures was detected in the whole brain. Differences in the origin of the tumors of the gliomatoses cerbri and cerebelli suggests these tumors are different types of brain tumors. Thus the findings support that the gliomatosis cerebelli is a novel type of brain tumor classification. Furthermore, by the similarities of the histological features among the tumors, it appears appropriate to establish a novel category of 'gliomatosis encephali' which includes both gliomatosis cerebri and gliomatosis cerebelli. [ABSTRACT FROM AUTHOR]

Published

2014

28. Reduced expression of α Glc NAc in Barrett's oesophagus adjacent to Barrett's adenocarcinoma - a possible biomarker to predict the malignant potential of Barrett's oesophagus.

Author

Iwaya, Yugo, Hasebe, Osamu, Koide, Naohiko, Kitahara, Kei, Suga, Tomoaki, Shinji, Akihiro, Muraki, Takashi, Yokosawa, Shuichi, Yamada, Shigenori, Arakura, Norikazu, Tanaka, Eiji, and Nakayama, Jun

Subjects

ESOPHAGEAL cancer, BIOMARKERS, GLYCOASPARAGINASE, LABORATORY mice, ADENOCARCINOMA, SQUAMOUS cell carcinoma

Abstract

Aims Gastric gland mucin contains O-glycans exhibiting terminal α1,4-linked N-acetylglucosamine residues (αGlc NAc). Recently we demonstrated that mice deficient in αGlc NAc in gastric gland mucin develop gastric adenocarcinoma spontaneously, indicating that αGlc NAc is a tumour suppressor for gastric cancer. However, the role of αGlc NAc in Barrett's oesophagus ( BO) remains unknown. In this study, we investigated whether reduced αGlc NAc expression in BO is associated with development of Barrett's adenocarcinoma ( BAC). Methods and results Thirty-five BO lesions adjacent to BAC were examined by immunohistochemistry for αGlc NAc, MUC6 and CDX2. As controls, 35 BO lesions without BAC obtained from patients with oesophageal squamous cell carcinoma were also analysed. Expression of αGlc NAc relative to its scaffold MUC6 in BO adjacent to BAC was reduced significantly compared to control BO. Decreased αGlc NAc expression in BO adjacent to BAC was particularly significant in patients with smaller tumour size (<20 mm) and minimal invasion of tumour cells to the superficial muscularis mucosae. There was also a significant inverse correlation between αGlc NAc and CDX2 expression in BO adjacent to BAC. Conclusions Decreased expression of αGlc NAc compared with MUC6 in BO is a possible hallmark in predicting BAC development. [ABSTRACT FROM AUTHOR]

Published

2014

29. Loss of gastric gland mucin-specific O-glycan is associated with progression of differentiated-type adenocarcinoma of the stomach.

Author

Shiratsu, Kazuo, Higuchi, Kayoko, and Nakayama, Jun

Abstract

Gastric gland mucin secreted from the lower portion of the gastric mucosa contains unique O-linked oligosaccharides having terminal α1,4-linked N-acetylglucosamine (αGlc NAc) residues largely attached to a MUC6 scaffold. Previously, we generated A4gnt-deficient mice, which totally lack αGlc NAc, and showed that αGlc NAc functions as a tumor suppressor for gastric cancer. Here, to determine the clinicopathological significance of αGlc NAc in gastric carcinomas, we examined immunohistochemical expression of αGlc NAc and mucin phenotypic markers including MUC5 AC, MUC6, MUC2, and CD10 in 214 gastric adenocarcinomas and compared those expression patterns with clinicopathological parameters and cancer-specific survival. The αGlc NAc loss was evaluated in MUC6-positive gastric carcinoma. Thirty-three (61.1%) of 54 differentiated-type gastric adenocarcinomas exhibiting MUC6 in cancer cells lacked αGlc NAc expression. Loss of αGlc NAc was significantly correlated with depth of invasion, stage, and venous invasion by differentiated-type adenocarcinoma. Loss of αGlc NAc was also significantly associated with poorer patient prognosis in MUC6-positive differentiated-type adenocarcinoma. By contrast, no significant correlation between αGlc NAc loss and any clinicopathologic variable was observed in undifferentiated-type adenocarcinoma. Expression of MUC6 was also significantly correlated with several clinicopathological variables in differentiated-type adenocarcinoma. However, unlike the case with αGlc NAc, its expression showed no correlation with cancer-specific survival in patients. In undifferentiated-type adenocarcinoma, we observed no significant correlation between mucin phenotypic marker expression, including MUC6, and any clinicopathologic variable. These results together indicate that loss of αGlc NAc in MUC6-positive cancer cells is associated with progression and poor prognosis in differentiated, but not undifferentiated, types of gastric adenocarcinoma. [ABSTRACT FROM AUTHOR]

Published

2014

30. High Levels of FOXP3+ Regulatory T Cells in Gastric MALT Lymphoma Predict Responsiveness to Helicobacter pylori Eradication.

Author

Iwaya, Yugo, Kobayashi, Motohiro, Momose, Masanobu, Hiraoka, Nobuyoshi, Sakai, Yasuhiro, Akamatsu, Taiji, Tanaka, Eiji, Ohtani, Haruo, Fukuda, Minoru, and Nakayama, Jun

Subjects

HELICOBACTER pylori, MUCOSA-associated lymphoid tissue lymphoma, GASTRITIS, IMMUNE response, IMMUNOHISTOCHEMISTRY, LYMPHOMAS, T cells

Abstract

Background Although Helicobacter pylori eradication is a first-line treatment of gastric MALT lymphoma, roughly 25% of patients do not respond to treatment. CD4+ FOXP3+ regulatory T ( Treg) cells regulate immune responses in physiological conditions and various inflammatory conditions, including H. pylori-associated diseases. Our goal was to determine how Treg cells affect responsiveness to H. pylori eradication therapy. Materials and methods We performed dual immunohistochemistry for CD4 and FOXP3 to evaluate the prevalence of FOXP3+ Treg cells in the stomach of 63 patients with MALT lymphoma and 55 patients with chronic active gastritis. Receiver operating characteristic analysis was carried out to determine the best cut-off point in differentiating H. pylori eradication responders from nonresponders. Results Both the FOXP3+/ CD4+ cell ratio and the absolute number of FOXP3+ cells per high-power field in MALT lymphoma were significantly greater in H. pylori eradication responders compared with nonresponders, suggesting that Treg cells function in regression mechanisms of MALT lymphomas. Cut-off points with good sensitivities and specificities were obtained to predict eradication outcome. Conclusions A high number of Treg cells or a high ratio of Treg cells to the total number of CD4+ T cells in gastric MALT lymphoma could predict responsiveness to eradication therapy. [ABSTRACT FROM AUTHOR]

Published

2013

31. C-terminus of the Sgf73 subunit of SAGA and SLIK is important for retention in the larger complex and for heterochromatin boundary function.

Author

Kamata, Kazuma, Hatanaka, Akira, Goswami, Gayatri, Shinmyozu, Kaori, Nakayama, Jun‐ichi, Urano, Takeshi, Hatashita, Masanori, Uchida, Hiroyuki, and Oki, Masaya

Subjects

HETEROCHROMATIC genes, C-terminal residues, SACCHAROMYCES cerevisiae, GENOMICS, GENETIC testing, HISTONE acetyltransferase, UBIQUITINATION

Abstract

The budding yeast Saccharomyces cerevisiae contains active and inactive chromatin separated by boundary domains. Previously, we used genome-wide screening to identify 55 boundary-related genes. Here, we focus on Sgf73, a boundary protein that is a component of the Spt- Ada- Gcn5 acetyltransferase ( SAGA) and SLIK ( SAGA-like) complexes. These complexes have histone acetyltransferase ( HAT) and histone deubiquitinase activity, and Sgf73 is one of the factors necessary to anchor the deubiquitination module. Domain analysis of Sgf73 was carried out, and the minimum region (373-402 aa) essential for boundary function was identified. This minimum region does not include the domain involved in anchoring the deubiquitination module, suggesting that the histone deubiquitinase activity of Sgf73 is not important for its boundary function. Next, Sgf73-mediated boundary function was analyzed in disruption strains in which different protein subunits of the SAGA/ SLIK/ ADA complexes were deleted. Deletion of ada2, ada3 or gcn5 (a HAT module component) caused complete loss of the boundary function of Sgf73. The importance of SAGA or SLIK complex binding to the boundary function of Sgf73 was also analyzed. Western blot analysis detected both the full-length and truncated forms of Spt7, suggesting that SAGA and SLIK complex formation is important for the boundary function of Sgf73. [ABSTRACT FROM AUTHOR]

Published

2013

32. Immunohistochemical expression of core 2 β1,6- N-acetylglucosaminyl transferase 1 ( C2 Gn T1) in endometrioid-type endometrial carcinoma: a novel potential prognostic factor.

Author

Miyamoto, Tsutomu, Suzuki, Akihisa, Asaka, Ryoichi, Ishikawa, Kaori, Yamada, Yasushi, Kobara, Hisanori, Nakayama, Jun, and Shiozawa, Tanri

Subjects

TRANSFERASES, CANCER cells, CARCINOMA, UTERUS, MYOMETRIUM, HYPERPLASIA

Abstract

Aims It has been reported that the expression of core 2 β1,6- N-acetylglucosaminyl transferase 1 ( C2 Gn T1), which synthesizes the core 2 branching structure on O-glycans, may be associated with the biological aggressiveness of tumour cells. Therefore, the aim of this study was to examine the relationship between the expression of C2 Gn T1 and clinicopathological parameters of patients with endometrial carcinoma. Methods and results The immunohistochemical expression of C2 Gn T1 was examined in 84 cases of endometrioid-type endometrial carcinoma, 15 cases of endometrial hyperplasia, and 30 normal endometria. The staining intensity was reported according to a positivity index ( PI, full score 100), calculated from the percentage of positive cells. The expression of C2 Gn T1 was significantly higher in endometrial carcinoma ( PI = 8.31 ± 15.29) than in normal endometrium ( PI = 0.52 ± 1.24) ( P < 0.0005). In carcinomas, the PI was higher in high-grade or advanced-stage tumours, but not significantly. Topologically, C2 Gn T1 was strongly expressed at sites of deep myometrial invasion. In addition, patients with C2 Gn T1 overexpression ( PI ≥ 10) had significantly shorter survival ( P < 0.0005). Multivariable analysis also indicated that C2 Gn T1 overexpression was an independent prognostic factor ( P = 0.017). Conclusions C2 Gn T1 appears to be involved in the biological aggressiveness of endometrial carcinoma. C2 Gn T1 might become a novel prognostic factor for endometrial carcinoma. [ABSTRACT FROM AUTHOR]

Published

2013

33. Non-thermal DNA damage of cancer cells using near-infrared irradiation.

Author

Tanaka, Yohei, Tatewaki, Naoto, Nishida, Hiroshi, Eitsuka, Takahiro, Ikekawa, Nobuo, and Nakayama, Jun

Abstract

Previously, we reported that near-infrared irradiation that simulates solar near-infrared irradiation with pre- and parallel-irradiational cooling can non-thermally induce cytocidal effects in cancer cells. To explore these effects, we assessed cell viability, DNA damage response pathways, and the percentage of mitotic cancer cells after near-infrared treatment. Further, we evaluated the anti-cancer effects of near-infrared irradiation compared with doxorubicin in xenografts in nude mice by measuring tumor volume and assessing protein phosphorylation by immunoblot analysis. The cell viability of A549 lung adenocarcinoma cells was significantly decreased after three rounds of near-infrared irradiation at 20 J ⁄ cm2. Apoptotic cells were observed in near-infrared treated cells. Moreover, near-infrared treatment increased the phosphorylation of ataxia-telangiectasia mutated ( ATM) at Ser1981, H2 AX at Ser139, Chk1 at Ser317, structural maintenance of chromosome ( SMC) 1 at Ser966, and p53 at Ser15 in A549 cells compared with control. Notably, near-infrared treatment induced the formation of nucleic foci of γH2 AX. The percentage of mitotic A549 cells, as measured by histone H3 phosphorylation, decreased significantly after three rounds of near-infrared irradiation at 20 J ⁄cm2. Both near-infrared and doxorubicin inhibited the tumor growth of MDA- MB435 melanoma cell xenografts in nude mice and increased the phosphorylation of p53 at Ser15, Chk1 at Ser317, SMC1 at Ser966, and H2 AX at Ser139 compared with control mice. These results indicate that near-infrared irradiation can non-thermally induce cytocidal effects in cancer cells as a result of activation of the DNA damage response pathway. The near-infrared irradiation schedule used here reduces discomfort and side effects. Therefore, this strategy may have potential application in the treatment of cancer. ( Cancer Sci 2012; 103: 1467-1473) [ABSTRACT FROM AUTHOR]

Published

2012

34. Reduced glycosylation of α-dystroglycans on carcinoma cells contributes to formation of highly infiltrative histological patterns in prostate cancer.

Author

Shimojo, Hisashi, Kobayashi, Motohiro, Kamigaito, Takayuki, Shimojo, Yasuyo, Fukuda, Minoru, and Nakayama, Jun

Published

2011

35. Prominent expression of sialyl Lewis X-capped core 2-branched O-glycans on high endothelial venule-like vessels in gastric MALT lymphoma.

Author

Kobayashi, Motohiro, Mitoma, Junya, Hoshino, Hitomi, Yu, Shin-Yi, Shimojo, Yasuyo, Suzawa, Kenichi, Khoo, Kay-Hooi, Fukuda, Minoru, and Nakayama, Jun

Published

2011

36. Physiological Roles of Class I HDAC Complex and Histone Demethylase.

Author

Hayakawa, Tomohiro and Nakayama, Jun-ichi

Abstract

Epigenetic gene silencing is one of the fundamental mechanisms for ensuring proper gene expression patterns during cellular differentiation and development. Histone deacetylases (HDACs) are evolutionally conserved enzymes that remove acetyl modifications from histones and play a central role in epigenetic gene silencing. In cells, HDAC forms a multiprotein complex (HDAC complex) in which the associated proteins are believed to help HDAC carry out its cellular functions. Though each HDAC complex contains distinct components, the presence of isoforms for some of the components expands the variety of complexes and the diversity of their cellular roles. Recent studies have also revealed a functional link between HDAC complexes and specific histone demethylases. In this paper, we summarize the distinct and cooperative roles of four class I HDAC complexes, Sin3, NuRD, CoREST, and NCoR/SMRT, with respect to their component diversity and their relationship with specific histone demethylases. [ABSTRACT FROM AUTHOR]

Published

2011

37. Nasu-Hakola disease: The first case reported by Nasu and review.

Author

Kaneko, Minoru, Sano, Kenji, Nakayama, Jun, and Amano, Naoji

Subjects

NEUROLOGICAL disorders, PROTEINS, ORGANIC compounds, CEREBRAL atrophy, CEREBRAL cortex, NEUROLOGY, AMINO acids

Abstract

Nasu-Hakola disease (NHD) was first reported separately by Nasu and Hakola around the same time in the 1970s. It is an autosomal recessive inherited disorder characterized by progressive dementia and repeated pathological fractures during adolescence. It has recently been demonstrated that NHD is caused by a mutation in the TREM2 or DAP12 gene. The present paper demonstrates the first patient reported by Nasu and reviews NHD. The patient was a man who died at the age 38 years. His family history was unremarkable. There was no abnormal developmental history. At the age of 26, the patient suffered a pathological fracture of the right tibia, and X-ray confirmed bone resorption in the right tibia. As for mental status, the patient tended to be euphoric. After that, bone resorption was also seen in other long bones. At the age of 33, the patient could not walk after suffering a right femoral neck fracture. He was apathetic and exhibited behavioral abnormalities. At the age of 38, he could not move or speak and subsequently died. General pathological examination showed yellow opaque gelatinous substances in the medullary cavities, matching translucent cystic lesions in the femur, tibia, and fibula on X-rays. Light microscopy showed numerous membranocystic changes in the substances. The brain weighed 1050 g. Symmetric systemic cerebral atrophy, in particular atrophy of the cerebral white matter in the occipital and temporal lobes, was confirmed. Histological examination showed white matter degeneration and diffuse sclerosis accompanied by astroglial proliferation. Severe demyelination was confirmed. Axonal degeneration and destruction were marked. In demyelinated areas, fat granule cells appeared, and lipid granule-positive cells aggregated around vessels. Cerebral cortical neurons were relatively maintained. In the brain, no membranocystic lesions could be recognized. In the DAP12 gene, the patient had a conversion of nucleotide at position 116 resulting in serine 38 to asparagine substitution. [ABSTRACT FROM AUTHOR]

Published

2010

38. Non-thermal cytocidal effect of infrared irradiation on cultured cancer cells using specialized device.

Author

Tanaka, Yohei, Matsuo, Kiyoshi, Yuzuriha, Shunsuke, Yan, Huimin, and Nakayama, Jun

Abstract

As infrared penetrates the skin, thermal effects of infrared irradiation on cancer cells have been investigated in the field of hyperthermia. We evaluated non-thermal effects of infrared irradiation using a specialized device (1100–18000 nm with filtering of wavelengths between 1400 and 1500 nm and contact cooling) on cancer cells. In in vitro study, five kinds of cultured cancer cell lines (MCF7 breast cancer, HeLa uterine cervical cancer, NUGC-4 gastric cancer, B16F0 melanoma, and MDA-MB435 melanoma) were irradiated using the infrared device, and then the cell proliferation activity was evaluated by 3-(4,5-dimethylthiazol-2-yl)-5-(3-carboxymethoxyphenyl)-2-(4-sulfophenyl)-2H-tetrazolium (MTS) assay. Proliferation of all the cancer cell lines was significantly suppressed by infrared irradiation. Total infrared output appeared to be correlated with cell survival. Increased temperature during infrared irradiation appeared not to play a role in cell survival. The maximum temperature elevation in the wells after each shot in the 20 and 40 J/cm2 culture was 3.8°C and 6.9°C, respectively. In addition, we have shown that infrared irradiation significantly inhibited the tumor growth of MCF7 breast cancer transplanted in severe combined immunodeficiency mice and MDA-MB435 melanoma transplanted in nude mice in vivo. Significant differences between control and irradiated groups were observed in tumor volume and frequencies of TUNEL-positive and Ki-67-positive cells. These results indicate that infrared, independent of thermal energy, can induce cell killing of cancer cells. As this infrared irradiation schedule reduces discomfort and side effects, reaches the deep subcutaneous tissues, and facilitates repeated irradiations, it may have potential as an application for treating various forms of cancer. ( Cancer Sci 2010) [ABSTRACT FROM AUTHOR]

Published

2010

39. Critical roles of VEGF-C-VEGF receptor 3 in reconnection of the collecting lymph vessels in mice.

Author

Ikomi, Fumitaka, Kawai, Yoshiko, Nakayama, Jun, Ogiwara, Naoko, Sasaki, Katsunori, Mizuno, Risuke, and Ohhashi, Toshio

Subjects

VASCULAR endothelial growth factors, ENDOTHELIAL seeding, IMMUNOHISTOCHEMISTRY techniques, LABORATORY mice, CELL receptors

Abstract

Molecular mechanisms of reconnection of collecting lymph vessels were analyzed by using murine popliteal prenodal lymph vessels. At 1 and 2 weeks after being divided by cutting the lymph vessel, lymphatic reconnection was frequently observed accompanied by mesh-like lymphatic channels. Electron microscopic study also showed a monolayer of endothelial cells in the newly developed lymph vessels. Smooth muscle markers were immunofluorescently demonstrated in the wall of the new vessels. At 1 week after the procedure of cutting, augmented expressions of VEGF receptors 1, 2 and 3 were found immunohistochemically at the site of the reconnected lymph vessels. The expression of mRNA for VEGF receptor 3 was enhanced at 5 days and 1 week in small pieces of the tissues containing the reconnected lymph vessels, compared with that in the corresponding tissues obtained with sham operated ones. The administration of VEGF-C at the cutting site of the collecting lymph vessel significantly increased the rate of the reconnected lymph vessels, whereas additional treatment with Flt4/Fc chimera protein significantly reduced the rate of the reconnected ones. These results suggest that activation of VEGF-C-VEGF receptor 3 has critical roles in reconnection of the collecting lymph vessels in adult mice. [ABSTRACT FROM AUTHOR]

Published

2008

40. Induction of trophinin in human endometrial surface epithelia by CGβ and IL-1β

Author

Sugihara, Kazuhiro, Kabir-Salmani, Maryam, Byrne, James, Wolf, Don P., Lessey, Bruce, Iwashita, Mitsutoshi, Aoki, Daisuke, Nakayama, Jun, and Fukuda, Michiko N.

Subjects

ADHESION, COHESION, ADSORPTION (Chemistry), PLACENTA

Abstract

Abstract: During embryo implantation, trophinin mediates cell adhesion by homophilic binding at the apical surfaces of trophectoderm and endometrium. Trophinin is expressed on the human endometrial epithelia in rare occasions. We developed hCG-coated agarose beads that mimic the physical and physiological features of an implantation-stage human blastocyst. When hCG-coated beads were applied to human endometrial epithelial cells in the presence of IL-1β, endometrial cells acquired strong trophinin expression and the ability for apical cell adhesion with trophinin-expressing human trophoblastic cells. These results provide a mechanism for trophinin-mediated adhesion of human blastocyst to endometrium by a spatially and temporally restricted paracrine effect of hCG derived from the blastocyst. [Copyright &y& Elsevier]

Published

2008

41. The role of trophinin, an adhesion molecule unique to human trophoblasts, in progression of colorectal cancer.

Author

Harada, Oi, Suga, Tomoaki, Suzuki, Takefumi, Nakamoto, Katsuaki, Kobayashi, Motohiro, Nomiyama, Tetsuo, Nadano, Daita, Ohyama, Chikara, Fukuda, Michiko N., and Nakayama, Jun

Published

2007

42. RBP2 is an MRG15 complex component and down-regulates intragenic histone H3 lysine 4 methylation.

Author

Hayakawa, Tomohiro, Ohtani, Yasuko, Hayakawa, Noriyo, Shinmyozu, Kaori, Saito, Motoki, Ishikawa, Fuyuki, and Nakayama, Jun-ichi

Subjects

METHYLATION, HISTONES, LYSINE, PROTEINS, ACETYLTRANSFERASES, RNA polymerases

Abstract

MRG15 is a conserved chromodomain protein that associates with histone deacetylases (HDACs) and Tip60-containing histone acetyltransferase (HAT) complexes. Here we further characterize MRG15-containing complexes and show a functional link between MRG15 and histone H3K4 demethylase activity in mammalian cells. MRG15 was predominantly localized to discrete nuclear subdomains enriched for Ser2-phosphorylated RNA polymerase II, suggesting it is involved specifically with active transcription. Protein analysis of the MRG15-containing complexes led to the identification of RBP2, a JmjC domain-containing protein. Remarkably, over-expression of RBP2 greatly reduced the H3K4 methylation in culture human cells in vivo, and recombinant RBP2 efficiently removed H3K4 methylation of histone tails in vitro. Knockdown of RBP2 resulted in increased H3K4 methylation levels within transcribed regions of active genes. Our findings demonstrate that RBP2 associated with MRG15 complex to maintain reduced H3K4 methylation at transcribed regions, which may ensure the transcriptional elongation state. [ABSTRACT FROM AUTHOR]

Published

2007

43. RNA interference-mediated knock-down of transient receptor potential vanilloid 1 prevents forepaw inflammatory hyperalgesia in rat.

Author

Kasama, Susumu, Kawakubo, Masatomo, Suzuki, Takefumi, Nishizawa, Tomoko, Ishida, Akiko, and Nakayama, Jun

Subjects

ION channels, CELL receptors, HYPERALGESIA, INFLAMMATION, RNA

Abstract

Transient receptor potential vanilloid (TRPV)1 is a ligand-gated cation channel expressed by primary sensory neurons, including those in the dorsal root ganglia (DRG). TRPV1 plays an essential role in development of inflammatory thermal hyperalgesia after tissue injury and its expression in rat lumbar DRG is increased after hindpaw inflammation. However, the identity of factors mediating forepaw inflammatory hyperalgesia has remained elusive. Here, we examined behavioral responses to noxious thermal stimuli after forepaw inflammation in rats and found that inflammation induced by intraplantar injection of complete Freund's adjuvant significantly reduced hot-plate latency (HPL) at 50 °C. TRPV1 expression levels in the ipsilateral cervical DRG were also elevated after forepaw inflammation. By contrast, HPL at 56 °C was not shortened after forepaw inflammation and expression of TRPV2, a TRPV1 homolog, in the DRG was not increased. Paratracheal injection of short interfering RNA targeting TRPV1 blocked TRPV1 up-regulation in cervical DRG and abolished inflammation-mediated HPL reductions seen at 50 °C. However, thermal hyperalgesia previously established by inflammation was not reversed by short interfering RNA injection. These results indicate that: (i) enhanced TRPV1 expression in cervical DRG is closely associated with development of inflammatory thermal hyperalgesia in the forepaw after tissue injury and (ii) RNA interference targeting TRPV1 prevents inflammatory thermal hyperalgesia after forepaw injuries but does not ameliorate it when already established in a rat model of nociceptive pain representing upper limb injury in humans. [ABSTRACT FROM AUTHOR]

Published

2007

44. Acetylated YY1 regulates Otx2 expression in anterior neuroectoderm at two cis-sites 90 kb apart.

Author

Takasaki, Nobuyoshi, Kurokawa, Daisuke, Nakayama, Rika, Nakayama, Jun-ichi, and Aizawa, Shinichi

Subjects

ACETYLATION, HOMEOBOX genes, GENE expression, PROTEIN binding, HEAD

Abstract

The mouse homeobox gene Otx2 plays essential roles at each step and in every tissue during head development. We have previously identified a series of enhancers that are responsible for driving the Otx2 expression in these contexts. Among them the AN enhancer, existing 92 kb 5′ upstream, directs Otx2 expression in anterior neuroectoderm (AN) at the headfold stage. Analysis of the enhancer mutant Otx2ΔAN/− indicated that Otx2 expression under the control of this enhancer is essential to the development of AN. This study demonstrates that the AN enhancer is promoter-dependent and regulated by acetylated YY1. YY1 binds to both the AN enhancer and promoter region. YY1 is acetylated in the anterior head, and only acetylated YY1 can bind to the sequence in the enhancer. Moreover, YY1 binding to both of these two sites is essential to Otx2 expression in AN. These YY1 binding sites are highly conserved in AN enhancers in tetrapods, coelacanth and skate, suggesting that establishment of the YY1 regulation coincides with that of OTX2 function in AN development in an ancestral gnathostome. [ABSTRACT FROM AUTHOR]

Published

2007

45. Identification of oligopeptides binding to peritoneal tumors of gastric cancer.

Author

Akita, Noriyuki, Maruta, Fukuto, Seymour, Leonard W., Kerr, David J., Parker, Alan L., Asai, Tomohiro, Oku, Naoto, Nakayama, Jun, and Miyagawa, Shinichi

Subjects

PEPTIDES, TUMORS, MICE, HOMOLOGY (Biology), CANCER cells

Abstract

This is a report of in vivo intraperitoneal biopanning, and we successfully identified a novel peptide to target the multiple peritoneal tumors of gastric cancer. A phage display library was injected directly into the abdominal cavity of mice bearing peritoneal tumors of human gastric cancer, and phages associated with the tumors were subsequently reclaimed from isolated samples. The tumor-associated phages were amplified and the biopanning cycle was repeated five times to enrich for high affinity tumor-selective binding peptides. Finally, a tri-peptide motif, KLP, which showed homology with laminin 5 (a ligand for α3β1 integrin), was identified as a binding peptide for peritoneal tumors of gastric cancer. Phage clones displaying the sequence KLP showed 64-fold higher binding to peritoneal tumors than control phage and were preferentially distributed in tumors rather than in normal organs after intraperitoneal injection into mice. In addition, the KLP phages were more likely to bind to cancer cells in malignant ascites derived from a patient with recurrent gastric cancer. Synthesized peptide containing the motif KLP (SWKLPPS) also showed a strong binding activity to peritoneal tumors without cancer growth effect. Liposomes conjugated with SWKLPPS peptide appeared significantly more often in tumors than control liposomes after intraperitoneal injection into mice. Furthermore, modification of liposomes with SWKLPPS peptide enhanced the antitumor activity of adriamycin on gastric cancer cells. The peptide motif KLP seems a potential targeting ligand for the treatment of peritoneal metastasis of gastric cancer. ( Cancer Sci 2006; 97: 1075–1081) [ABSTRACT FROM AUTHOR]

Published

2006

46. Maintenance of self-renewal ability of mouse embryonic stem cells in the absence of DNA methyltransferases Dnmt1, Dnmt3a and Dnmt3b.

Author

Tsumura, Akiko, Hayakawa, Tomohiro, Kumak, Yuichi, Takebayashi, Shin-ichiro, Sakaue, Morito, Matsuoka, Chisa, Shimotohno, Kunitada, Ishikawa, Fuyuki, Li, En, Ueda, Hiroki R., Nakayama, Jun-ichi, and Okano, Masaki

Subjects

EMBRYONIC stem cells, MICE, DNA, METHYLTRANSFERASES, METHYLATION, GENOMES

Abstract

DNA methyltransferases Dnmt1, Dnmt3a and Dnmt3b cooperatively regulate cytosine methylation in CpG dinucleotides in mammalian genomes, providing an epigenetic basis for gene silencing and maintenance of genome integrity. Proper CpG methylation is required for the normal growth of various somatic cell types, indicating its essential role in the basic cellular function of mammalian cells. Previous studies using Dnmt1−/– or Dnmt3a−/– Dnmt3b−/– ES cells, however, have shown that undifferentiated embryonic stem (ES) cells can tolerate hypomethylation for their proliferation. In an attempt to investigate the effects of the complete loss of CpG DNA methyltransferase function, we established mouse ES cells lacking all three of these enzymes by gene targeting. Despite the absence of CpG methylation, as demonstrated by genome-wide methylation analysis, these triple knockout (TKO) ES cells grew robustly and maintained their undifferentiated characteristics. TKO ES cells retained pericentromeric heterochromatin domains marked with methylation at Lys9 of histone H3 and heterochromatin protein-1, and maintained their normal chromosome numbers. Our results indicate that ES cells can maintain stem cell properties and chromosomal stability in the absence of CpG methylation and CpG DNA methyltransferases. [ABSTRACT FROM AUTHOR]

Published

2006

47. Rotigaptide (ZP123) Improves Atrial Conduction Slowing in Chronic Volume Overload-Induced Dilated Atria.

Author

Haugan, Ketil, Miyamoto, Takuya, Takeishi, Yasuchika, Kubota, Isao, Nakayama, Jun, Shimojo, Hisashi, and Hirose, Masamichi

Subjects

TACHYARRHYTHMIAS, TACHYCARDIA, CELL communication, PROTEINS, BIOMOLECULES

Abstract

Chronic atrial dilation is associated with atrial conduction velocity slowing and an increased risk of developing atrial tachyarrhythmias. Rotigaptide (ZP123) is a selective gap junction modifier that increases cardiac gap junctional intercellular communication. We hypothesised that rotigaptide treatment would increase atrial conduction velocity and reduce the inducibility to atrial tachyarrhythmias in a model of chronic volume overload induced chronic atrial dilatation characterized by atrial conduction velocity slowing. Chronic volume overload was created in Japanese white rabbits by arterio-venous shunt formation. Atrial conduction velocity and atrial tachyarrhythmias inducibility were examined in Langendorff-perfused chronic volume overload hearts (n=12) using high-resolution optical mapping before and after treatment with rotigaptide. Moreover, expression levels of atrial gap junction proteins (connexin40 and connexin43) were examined in chronic volume overload hearts (n=6) and compared to sham-operated controls (n=6). Rotigaptide treatment significantly increased atrial conduction velocity in chronic volume overload hearts, however, rotigaptide did not decrease susceptibility to the induction of atrial tachyarrhythmias. Protein expressions of Cx40 and Cx43 were decreased by 32% and 72% (P<0.01), respectively, in chromic volume overload atria compared to control. To conclude, rotigaptide increased atrial conduction velocity in a rabbit model of chromic volume overload induced atrial conduction velocity slowing. The demonstrated effect of rotigaptide on atrial conduction velocity did not prevent atrial tachyarrhythmias inducibility. Whether rotigaptide may possess antiarrhythmic efficacy in other models of atrial fibrillation remains to be determined. [ABSTRACT FROM AUTHOR]

Published

2006

48. Female adnexal tumor of probable wolffian origin: Morphological, immunohistochemical, and ultrastructural study with c-kit gene analysis.

Author

Harada, Oi, Ota, Hiroyoshi, Takagi, Kimiyo, Matsuura, Hiroyuki, Hidaka, Eiko, and Nakayama, Jun

Subjects

TUMORS, WOLFFIAN body, FETUS, KIDNEYS, CANCER in women, IMATINIB, ANTINEOPLASTIC agents

Abstract

Female adnexal tumors of probable wolffian origin (FATWO) are rare neoplasms believed to originate from mesonephric (wolffian) remnants. Rarity and variable location of FATWO make the diagnosis difficult. Although most cases follow a benign clinical course, approximately 10% of them either recur or metastasize and are thought to be resistant to chemoradiation therapy. In 2004, imatinib therapy, a tyrosine kinase inhibitor known to be effective against gastrointestinal stromal tumors, was reported to be effective also in a case of KIT-positive FATWO. However, c-kit gene mutations in FATWO have never been studied. Herein is reported the case of a 50-year-old Japanese woman with FATWO arising in the right paratubal site. The tumor had typical characteristics of FATWO in both morphology and immunohistochemistry. KIT protein was diffusely and weakly expressed, but DNA analysis revealed no mutational change in exon 9 or 11 of the c-kit gene. It is believed that accumulation of such genetic data of FATWO are essential from a therapeutic standpoint, although the present case had no mutation. In addition, the cytological features of this rare tumor are presented, which have not been described previously. [ABSTRACT FROM AUTHOR]

Published

2006

49. Clinical utility of quantitative RT-PCR targeted to α1,4- N-acetylglucosaminyltransferase mRNA for detection of pancreatic cancer.

Author

Ishizone, Satoshi, Yamauchi, Kazuyoshi, Kawa, Shigeyuki, Suzuki, Takefumi, Shimizu, Fumiaki, Harada, Oi, Sugiyama, Atsushi, Miyagawa, Shinichi, Fukuda, Minoru, and Nakayama, Jun

Subjects

PANCREATIC cancer, CANCER patients, PANCREATIC blood vessels, MESSENGER RNA, BIOSYNTHESIS, CELLULAR pathology, ORGANIC synthesis, BIOCHEMICAL engineering, NUCLEIC acids

Abstract

α1,4- N-Acetylglucosaminyltransferase (α4GnT) is a glycosyltransferase responsible for the biosynthesis of α1,4-GlcNAc-capped O-glycans, and is frequently expressed in pancreatic cancer cells but not peripheral blood cells. In the present study, we tested the clinical utility of α4GnT mRNA expressed in the mononuclear cell fraction of peripheral blood as a biomarker of pancreatic cancer. Total RNA isolated from the peripheral blood mononuclear cells from 55 pancreatic cancer patients, 10 chronic pancreatitis patients, and 70 cancer-free volunteers was analyzed quantitatively by reverse transcription-polymerase chain reaction with primers specific for α4GnT, and the expression level of α4GnT mRNA relative to that of glyceraldehyde-3-phosphate dehydrogenase (GAPDH) was measured. When the ratio of α4GnT to GAPDH transcripts exceeded a defined cut-off value, patients were considered to have pancreatic cancer. By these standards, 76.4% of the pancreatic cancer patients were detected by this assay. A strong correlation was obtained between positivity in this assay and the expression of α4GnT protein detected immunohistochemically in pancreatic cancer tissues resected subsequently, suggesting that α4GnT mRNA detected in the peripheral blood is derived from circulating pancreatic cancer cells. Although increased levels of α4GnT mRNA was detected in 40.0% of chronic pancreatitis patients and 17.1% of cancer-free volunteers, the expression levels were significantly lower than those seen in pancreatic cancer patients. These results suggest that quantitative analysis of α4GnT mRNA expressed in the mononuclear cell fraction of peripheral blood will contribute to the detection of pancreatic cancer. ( Cancer Sci 2006; 97: 119 – 126) [ABSTRACT FROM AUTHOR]

Published

2006

50. Malignant myoepithelioma (myoepithelial carcinoma) of soft tissue.

Author

Harada, Oi, Ota, Hiroyoshi, and Nakayama, Jun

Subjects

TUMORS, CANCER cells, CANCER invasiveness, DIAGNOSIS, SYMPTOMS, PATHOLOGY

Abstract

Malignant myoepithelioma of soft tissue is extremely rare. Presented herein is a case arising in a 17-year-old man. The tumor was initially noticed as a painless deep soft-tissue mass in the right forearm when the patient was aged 3 years. Thereafter, it grew without remarkable symptoms, such as pain or tenderness, until his visit to the hospital because of swelling of his forearm when he was 17 years old. An excisional biopsy specimen disclosed an invasive tumor exhibiting a lobular architecture. The tumor cells were arranged in a reticular and/or trabecular fashion with a myxoid background, and nuclear atypia was evident. Mitoses and tumor necrosis were also observed. Immunohistochemically, S-100 protein and epithelial markers were diffusely positive. Faint intercellular junctions and basal laminae were identified by electronmicroscopy. On the basis of these findings, the tumor was diagnosed as a malignant myoepithelioma of soft tissue. Six months later, multiple lung metastases were observed, and an open biopsy revealed a neoplasm displaying the same histological feature as the previously biopsied specimens. The patient died of his disease 18 months after the lung biopsy. Malignant myoepithelioma shoud be kept in mind in diagnosis of deep soft-tissue tumors with epithelioid features. [ABSTRACT FROM AUTHOR]

Published

2005