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Dive into the research topics where Akie Takebayashi is active.

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Featured researches published by Akie Takebayashi.


Cancer Cell International | 2014

Metformin impairs growth of endometrial cancer cells via cell cycle arrest and concomitant autophagy and apoptosis

Akimasa Takahashi; Fuminori Kimura; Akiyoshi Yamanaka; Akie Takebayashi; Nobuyuki Kita; Kentaro Takahashi; Takashi Murakami

BackgroundEffective therapies for early endometrial cancer usually involve surgical excision and consequent infertility Therefore, new treatment approaches that preserve fertility should be developed. Metformin, a well-tolerated anti-diabetic drug, can inhibit cancer cell growth. However, the mechanism of metformin action is not well understood. Here we investigate the roles of autophagy and apoptosis in the anti-cancer effects of metformin on endometrial cancer cells.MethodsIshikawa endometrial cancer cells were treated with metformin. WST-8 assays, colony formation assays, flow cytometry, caspase luminescence measurement, immunofluorescence, and western blots were used to assess the effects of metformin on cell viability, proliferation, cell cycle progression, apoptosis, and autophagy.ResultsMetformin-treated cells exhibited significantly lower viability and proliferation and significantly more cell cycle arrest in G1 and G2/M than control cells. These cells also exhibited significantly more apoptosis via both intrinsic and extrinsic pathways. In addition, metformin treatment induced autophagy. Inhibition of autophagy, either by Beclin1 knockdown or by 3-methyladenine-mediated inhibition of caspase-3/7, suppressed the anti-proliferative effects of metformin on endometrial cancer cells. These findings indicate that the anti-proliferative effects and apoptosis caused by metformin are partially or completely dependent on autophagy.ConclusionsWe showed that metformin suppresses endometrial cancer cell growth via cell cycle arrest and concomitant autophagy and apoptosis.


PLOS ONE | 2014

The association between endometriosis and chronic endometritis

Akie Takebayashi; Fuminori Kimura; Yohei Kishi; Mitsuaki Ishida; Akimasa Takahashi; Akiyoshi Yamanaka; Kentaro Takahashi; Hiroshi Suginami; Takashi Murakami

Objective To evaluate the association between endometriosis and chronic endometritis. Methods Endometrial specimens were obtained from 71 patients, 34 with endometriosis (endometriosis group) and 37 without endometriosis (non-endometriosis group), who underwent hysterectomy, and the specimens were immunostained for the plasmacyte marker CD138. The rate of chronic endometritis was compared between the endometriosis group and the non-endometriosis group. Furthermore, the 71 patients were also divided into two groups, 28 with chronic endometritis (chronic endometritis group) and 43 without chronic endometritis (non-chronic endometritis group). Logistic regression analysis was performed with variables including age, body mass index (BMI), gravidity and parity, and diagnoses of leiomyoma, adenomyosis, and endometriosis on pathology to examine the independent effect of each variable on chronic endometritis. Patients suffering from cervical invasive carcinoma, endometrial carcinoma, and endometrial polyps or treated with gonadotropin-releasing hormone agonists, progestins, or oral contraceptives before surgery were excluded. Results Chronic endometritis was identified in 52.94% of the endometriosis group and 27.02% of the non-endometriosis group (p<0.05). Logistic regression analysis revealed that endometriosis was associated with chronic endometritis. Conclusions This result suggests a strong association between endometriosis and chronic endometritis.


American Journal of Reproductive Immunology | 2015

Subpopulations of macrophages within eutopic endometrium of endometriosis patients.

Akie Takebayashi; Fuminori Kimura; Yohei Kishi; Mitsuaki Ishida; Akimasa Takahashi; Akiyoshi Yamanaka; Di Wu; Luyi Zheng; Kentaro Takahashi; Hiroshi Suginami; Takashi Murakami

Endometriosis is recognized as a chronic inflammatory disease and is related to immune response. There have been reports that revealed the different distribution of macrophage within the eutopic endometrium of women with endometriosis. Macrophages are functionally polarized into M1 and M2 cell lineages. We studied a difference in the subpopulations of M1 and M2 macrophages within the eutopic endometrium in patients with or without endometriosis to investigate how the eutopic endometrium is stimulated immunologically.


Journal of Obstetrics and Gynaecology Research | 2018

Impact of hysteroscopic surgery for isthmocele associated with cesarean scar syndrome

Shunichiro Tsuji; Fuminori Kimura; Akiyoshi Yamanaka; Tetsuro Hanada; Kimiko Hirata; Akie Takebayashi; Akiko Takashima; Ayumi Seko‐Nitta; Takashi Murakami

Cesarean scar syndrome (CSS) is characterized by increased risk of postmenstrual abnormal uterine bleeding, dysmenorrhea, and infertility, due to a post‐cesarean scar defect known as an isthmocele. This study aimed to assess the impact of hysteroscopic surgery on isthmocele associated with CSS.


Experimental Animals | 2018

Protective effect of a mechanistic target of rapamycin inhibitor on an in vivo model of cisplatin-induced ovarian gonadotoxicity

Yuji Tanaka; Fuminori Kimura; Luyi Zheng; Shoji Kaku; Akie Takebayashi; Kyoko Kasahara; Shunichiro Tsuji; Takashi Murakami

This study aimed to evaluate the protective effect of everolimus, a mechanistic target of rapamycin (mTOR) inhibitor, on cisplatin chemotherapy-induced ovarian toxicity. Eighty sexually mature, virgin, female, 7-week-old C57BL/6J mice were divided into four groups: control, cisplatin (Cis), everolimus (mTORi), and everolimus plus cisplatin (mTORi+Cis). Mice in the Cis and mTORi+Cis groups were intraperitoneally injected with 2 mg/kg of cisplatin for 15 d. Mice in the mTORi and mTORi+Cis groups were orally administered 2.5 mg/kg of everolimus for 29 d, from one week before the first cisplatin injection to one week after the last cisplatin injection. Histological examinations were performed 24 h after the last everolimus administration. The primordial, primary, and antral follicles were significantly depleted in the Cis group compared with that in the control group, confirming the gonadotoxicity of cisplatin. The number of primordial, secondary, and antral follicles was significantly higher in the mTORi+Cis group than in the Cis group, thereby displaying the effect of mTORi-treatment on ovarian protection. Primordial, secondary, and antral follicle counts were similar in the mTORi+Cis and the control groups. The results of this study indicate a protective effect of an mTOR inhibitor against cisplatin chemotherapy-induced gonadotoxicity in the ovarian reserve in an in vivo mouse model.


Tohoku Journal of Experimental Medicine | 2012

Primate Model Research for Endometriosis

Akiyoshi Yamanaka; Fuminori Kimura; Akie Takebayashi; Nobuyuki Kita; Kentaro Takahashi; Takashi Murakami


Reproductive Biology and Endocrinology | 2017

Chronic endometritis modifies decidualization in human endometrial stromal cells

Di Wu; Fuminori Kimura; Luyi Zheng; Mitsuaki Ishida; Yoko Niwa; Kimiko Hirata; Akie Takebayashi; Akiko Takashima; Kentaro Takahashi; Ryoji Kushima; Guangmei Zhang; Takashi Murakami


Tohoku Journal of Experimental Medicine | 2013

Intake of Vinegar Beverage Is Associated with Restoration of Ovulatory Function in Women with Polycystic Ovary Syndrome

Di Wu; Fuminori Kimura; Akiko Takashima; Yoshihiko Shimizu; Akie Takebayashi; Nobuyuki Kita; Guangmei Zhang; Takashi Murakami


Gynecology and Minimally Invasive Therapy | 2013

Comparison of the outcome of in vitro fertilization after laparoscopic laser ablation surgery versus laparoscopic cystectomy for endometrioma

Akie Takebayashi; Yoshihiko Shimizu; Akimasa Takahashi; Akiyoshi Yamanaka; Akiko Takashima; Fuminori Kimura; Nobuyuki Kita; Kentaro Takahashi; Takashi Murakami


Tohoku Journal of Experimental Medicine | 2014

Exaggerated Placental Site, Consisting of Implantation Site Intermediate Trophoblasts, Causes Massive Postpartum Uterine Hemorrhage: Case Report and Literature Review

Akie Takebayashi; Fuminori Kimura; Akiyoshi Yamanaka; Akimasa Takahashi; Shunichiro Tsuji; Tetsuo Ono; Shoji Kaku; Nobuyuki Kita; Kentaro Takahashi; Hidetoshi Okabe; Takashi Murakami

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Takashi Murakami

Shiga University of Medical Science

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Fuminori Kimura

University of Massachusetts Amherst

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Kentaro Takahashi

Shiga University of Medical Science

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Akiyoshi Yamanaka

Shiga University of Medical Science

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Nobuyuki Kita

Shiga University of Medical Science

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Akiko Takashima

Shiga University of Medical Science

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Akimasa Takahashi

Shiga University of Medical Science

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Shoji Kaku

Shiga University of Medical Science

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Shunichiro Tsuji

Shiga University of Medical Science

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Yoshihiko Shimizu

Shiga University of Medical Science

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