Your search keyword '"Abe, Hideharu"' showing total 11 results

1. Clinical characteristics associated with 1-year tolvaptan efficacy in autosomal dominant polycystic kidney disease with a wide range of kidney functions

Author

Murakami, Taichi, Nishimura, Kenji, Ono, Hiroyuki, Ueta, Sayo, Shibata, Eriko, Kishi, Seiji, Tamaki, Masanori, Miya, Keiko, Shima, Hisato, Tashiro, Manabu, Inoue, Tomoko, Kawahara, Kazuhiko, Nagai, Kojiro, Abe, Hideharu, Minakuchi, Jun, and Doi, Toshio

Subjects

theraputic efficacy, autosomal dominant polycystic kidney disease, urogenital system, tolvaptan, urologic and male genital diseases, female genital diseases and pregnancy complications

Abstract

Autosomal dominant polycystic kidney disease (ADPKD) develops into end-stage kidney disease by 65 years of age in an estimated 45%-70% of patients. Recent trials revealed that tolvaptan inhibits disease progression both in early-stage or late-stage ADPKD ; however, stratified analysis showed a difference of favorable factors correlated with tolvaptan efficacy between early-stage and late-stage ADPKD. Thus, we examined the efficacy of tolvaptan in ADPKD with a wide range of estimated glomerular filtration rates (eGFR). We enrolled 24 patients with eGFR 35.3 (28.0-65.5) ml / min / 1.73m2 and evaluated treatment effect as ΔΔeGFR (ml / min / 1.73m2 / year) or ΔΔtotal kidney volume (TKV) (% / year) that was calculated as post-treatment annual change - pre-treatment annual change. Pre ΔeGFR was significantly low in eGFR responders, defined as ΔΔeGFR > 0 ml / min / 1.73m2 / year. In eGFR responders, pre ΔeGFR, post ΔeGFR, eGFR, TKV, and proteinuria were significantly correlated with ΔΔeGFR. In TKV responders defined as ΔΔTKV > 5 % / year, we identified hypertension history, proteinuria, TKV, and post ΔTKV as significantly correlated factors with ΔΔTKV. In conclusion, pre ΔeGFR may be a predictive factor of therapeutic efficacy on kidney function. Tolvaptan may have greater efficacy in early-stage ADPKD with rapid GFR decline or with well-controlled blood pressure.

Published

2020

2. Urinary Exosomal mRNA of WT1 as Diagnostic and Prognostic Biomarker for Diabetic Nephropathy

Author

Abe, Hideharu, Sakurai, Akiko, Ono, Hiroyuki, Hayashi, Sanae, Yoshimoto, Sakiya, Ochi, Arisa, Ueda, Sayo, Nishimura, Kenji, Shibata, Eriko, Tamaki, Masanori, Kishi, Fumi, Kishi, Seiji, Murakami, Taichi, Nagai, Kojiro, and Doi, Toshio

Subjects

diabetic nephropathy, exosome, biomarker, urologic and male genital diseases, PDSTF, WT1

Abstract

Diabetic nephropathy (DN) is the major cause of end-stage renal failure and is associated with increased morbidity and mortality as compared to other causes of renal disease. Albuminuria is often the first clinical indicator of the presence of DN. However, albuminuria or proteinuria is a common symptom in patients with various renal disorders. Therefore, specific biomarkers for the diagnosis of DN are required. A primary hallmark of DN is the progressive damage and death of glomerular podocytes, resulting in the leaking of proteins into the urine. Urinary exosomes released by podocytes are microvesicles containing information of the originated cells. Podocyte-derived signal transduction factors (PDSTFs) are good candidates to assess podocyte injuries. The profile of PDSTFs in urinary exosomes from patients with DN is different from that from patients with minimal change nehrotic syndrome. In addition, PDSTFs molecules in exosomes were derived from primary murine podocytes under high glucose conditions. Among PDSTFs in urinary exosomes, Wilms tumor 1 (WT1) levels reflected damage of diabetic glomeruli in the patients. Urinary exosomal WT1 can predict the decline in eGFR for the following several years. In conclusion, urinary exosomal WT1 is a useful biomarker to improve risk stratification in patients with DN.

Published

2018

3. Diagnosis of renal AL amyloidosis using DAPI

Author

Matsuura, Motokazu, Abe, Hideharu, Tominaga, Tatsuya, Sakurai, Akiko, Murakami, Taichi, Kishi, Seiji, Bando, Yoshimi, Minakuchi, Jun, Nagai, Kojiro, and Doi, Toshio

Subjects

mental disorders, AA amyloidosis, Amyloidosis, AL amyloidosis, Renal amyloidosis, DAPI

Abstract

Amyloidosis is often overlooked because its clinical manifestations can mimic those of more-common diseases. It is important to get a precise diagnosis as early as possible for the prevention of further organ damages. Amyloidosis is a disorder caused by deposition of insoluble abnormal amyloid. The kidney is a frequent site of amyloid deposition. The amyloid fibrils have a characteristic appearance and generate birefringence under polarized light when stained with the Congo red dye. Classification of amyloidosis is based on the precursor protein that forms the amyloid fibrils and the distribution of amyloid deposits as either systemic or localized. Involvement of amyloid fibrils in kidneys mainly occurs as amyloid light-chain (AL) or amyloid A (AA) amyloidosis. The potassium permanganate method with Congo red staining was once used widely to discriminate AL and AA amyloidoses, but thismethod has a problem of false positive results. We found that extracellular and cytoplasmic glomerular 4’,6-diamidino-2-phenylindole (DAPI)-positive areas were clearly consistent with amyloid deposition in AL amyloidosis. In contrast, the overlapping staining was not seen in AA amyloidosis. Therefore, we propose that DAPI staining readily distinguishes AL renal amyloidosis from AA renal amyloidosis as a simple and reproducible histochemical method.

Published

2017

4. 至適透析や溶血回避のための血液ポンプ前の動脈圧の再評価 : 血液透析患者における血液ポンプ前の動脈圧モニタリングの重要性

Author

Shibata, Eriko, Nagai, Kojiro, Takeuchi, Risa, Noda, Yasuhiro, Makino, Tomomi, Chikata, Yusuke, Hann, Michael, Yoshimoto, Sakiya, Ono, Hiroyuki, Ueda, Sayo, Tamaki, Masanori, Murakami, Taichi, Matsuura, Motokazu, Abe, Hideharu, and Doi, Toshio

Subjects

Vacuum monitor, Prepump arterial pressure, Blood flow, pressure pillow, Hemolysis, Dialysis

Abstract

Pre-pump arterial pressure (PreAP) is monitored to avoid generating excessive negative pressure. National Kidney Foundation K/DOQI clinical practice guidelines for vascular access recommend that PreAP should not fall below-250 mmHg because excessive negative PreAP can lead to a decrease in the delivery of blood flow, inadequate dialysis, and hemolysis. Nonetheless, these recommendations are consistently disregarded in clinical practice and pressure sensors are often removed from the dialysis circuit.Thus far,delivered blood flow has been reported to decrease at values more negative than -150 mmHg of PreAP. These values have been analyzed by an ultrasonic flowmeter and not directly measured. Furthermore, no known group has evaluated whether PreAP-induced hemolysis occurs at a particular threshold. Therefore, the aim of this study was to clarify the importance of PreAP in the prediction of inadequate dialysis and hemolysis. By using different diameter needles, human blood samples from healthy volunteers were circulated in a closed dialysis circuit. The relationship between PreAP and delivered blood flow or PreAP and hemolysis was investigated. We also investigated the optimal value for PreAP using several empirical monitoring methods, such as a pressure pillow. Our investigation indicated that PreAP is a critical factor in the determination of delivered blood flow and hemolysis,both of which occured at pressure values more negative than -150 mmHg. With the exception of direct pressure monitoring, commonly used monitoring methods for PreAP were determined to be ineffective. We propose that the use of a vacuum monitor would permit regular measurement of PreAP.

Published

2015

5. 入院慢性腎臓病患者における血清アルブミン濃度に影響を与える因子

Author

Yoshimoto, Sakiya, Nagai, Kojiro, Shibata, Eriko, Ueda, Sayo, Ono, Hiroyuki, Tamaki, Masanori, Nishimura, Kenji, Obata, Fumiaki, Inagaki, Taizo, Minato, Masanori, Kishi, Fumi, Matsuura, Motokazu, Matsui, Naoko, Endo, Itsuro, Hann, Michael, Kishi, Seiji, Murakami, Taichi, Abe, Hideharu, and Doi, Toshio

Subjects

Hospitalization, Proteinuria, Postural change, Serum albumin concentration, Chronic kidney disease

Published

2017

6. 循環アポリポプロテインL1はインスリン抵抗性が引き起こす脂質代謝異常に関連する

Author

Nishimura, Kenji, Murakami, Taichi, Sakurai, Toshihiro, Miyoshi, Masashi, Kurahashi, Kiyoe, Kishi, Seiji, Tamaki, Masanori, Tominaga, Tatsuya, Yoshida, Sumiko, Nagai, Kojiro, Abe, Hideharu, Hui, Shu-Ping, Kotani, Kazuhiko, and Doi, Toshio

Subjects

insulin, insulin resistance, abnormal lipid metabolism, ApoL1, Apolipoprotein L1

Abstract

Circulating ApolipoproteinL1 (ApoL1) is a component of pre-β-high-density lipoprotein (HDL), however little is known about the relationship of ApoL1 with cardiometabolic factors. Considering previous studies reporting the correlation of ApoL1 to triglyceride, we have hypothesized that ApoL1 associates with insulin-related metabolism. The current study examined their associations in 126 non-diabetic subjects and 36 patients with type 2 diabetes (T2DM). Non-diabetic subjects demonstrated triglyceride (standardized coefficients [s.c.] = 0.204, p < 0.05), body mass index (s.c. =0.232, p < 0.05) and HDL cholesterol (s.c. = −0.203, p < 0.05) as independent determinant of ApoL1 levels, and the significant elevation of ApoL1 in metabolic syndrome. Lipoprotein fractionation analysis revealed the predominant distribution of ApoL1 in large HDL fraction, and the significant increase of ApoL1 in large LDL fraction in high ApoL1 samples with insulin resistance. In T2DM, ApoL1 was higher in T2DM with metabolic syndrome, however ApoL1 was lower with β cell dysfunction. Insulin significantly promotes ApoL1 synthesis and secretion in HepG2 cells. In conclusion, circulating ApoL1 may be associated with abnormal HDL metabolism in insulin resistant status. This may suggest a regulation of insulin signal on the ApoL1 level, leading to offer a novel insight to the ApoL1 biology.

Published

2019

7. An adjustment in BMP4 function represents a treatment for diabetic nephropathy and podocyte injury

Author

Fujita, Yui, Tominaga, Tatsuya, Abe, Hideharu, Kangawa, Yumi, Fukushima, Naoshi, Ueda, Otoya, Jishage, Kou-ichi, Kishi, Seiji, Murakami, Taichi, Saga, Yumiko, Kanwar, Yashpal S., Nagai, Kojiro, and Doi, Toshio

Subjects

animal structures, diabetic nephropathy, embryonic structures, cytokine, CKD, Podocyte, BMP4

Abstract

Podocyte injury has been proposed to play an important role in diabetic nephropathy; however, its pathological mechanism remains unclear. We have shown that bone morphogenetic protein 4 (BMP4) signaling leads to the glomerular changes characteristic of this disorder. To analyze the molecular mechanism of podocyte injury, the effect of BMP4 was investigated using streptozotocin (STZ)- induced, Bmp4 heterozygous knockout (Bmp4+/−) and podocyte-specific Bmp4 knockout mice. Mice with STZ-induced diabetes exhibited glomerular matrix hyperplasia and decreased numbers of podocyte nucleus-specific WT1-positive cells. The number of podocytes and proteinuria were improved in both diabetic Bmp4 knockout mouse models compared to the effects observed in the control mice. The effect of BMP4 overexpression on Bmp4-induced or podocyte-specific transgenic mice was examined. Tamoxifen-induced Bmp4-overexpressing mice exhibited mesangial matrix expansion and decreased numbers of WT1-positive cells. Podocyte-specific Bmp4-overexpressing mice displayed increased kidney BMP4 expression and mesangial matrix expansion but decreased nephrin expression and numbers of WT1-positive cells. Both lines of Bmp4-overexpressing mice exhibited increased albuminuria. In cultured podocytes, BMP4 increased phospho-p38 levels. BMP4 decreased nephrin expression but increased cleaved caspase-3 levels. p38 suppression inhibited caspase-3 activation. Apoptosis was confirmed in STZ-diabetic glomeruli and Bmp4-overexpressing mice. Bmp4 +/− mice with diabetes displayed reduced apoptosis. Based on these data, the BMP4 signaling pathway plays important roles in the development of both podocyte injury and mesangial matrix expansion in diabetic nephropathy.

Published

2018

8. Novel Interplay Between Smad1 and Smad3 Phosphorylation via AGE Regulates the Progression of Diabetic Nephropathy

Author

Ono, Hiroyuki, Abe, Hideharu, Sakurai, Akiko, Ochi, Arisa, Tominaga, Tatsuya, Tamaki, Masanori, Kishi, Seiji, Murakami, Taichi, Nagai, Kojiro, Kohashi, Masayuki, and Doi, Toshio

Subjects

collagen, animal structures, integumentary system, phosphorylation, diabetic nephropathy, embryonic structures, Smad1, biological phenomena, cell phenomena, and immunity, Smad3

Abstract

Diabetic nephropathy (DN) is the major cause of end-stage renal failure and is associated with increased morbidity and mortality compared with other causes of renal diseases. We previously found that Smad1 plays a critical role in the development of DN both in vitro and in vivo. However, functional interaction between Smad1 and Smad3 signaling in DN is unclear. Here, we addressed the molecular interplay between Smad1 and Smad3 signaling under a diabetic condition by using Smad3-knockout diabetic mice. Extracellular matrix (ECM) protein overexpression and Smad1 activation were observed in the glomeruli of db/db mice but were suppressed in the glomeruli of Smad3+/−; db/db mice. Smad3 activation enhanced the phosphorylation of Smad1 C-terminal domain but decreased the phosphorylation of linker domain, thus regulating Smad1 activation in advanced glycation end product-treated mesangial cells (MCs). However, forced phosphorylation of the Smad1 linker domain did not affect Smad3 activation in MCs. Phosphorylation of the Smad1 linker domain increased in Smad3+/−; db/db mice and probucol-treated db/db mice, which was consistent with the attenuation of ECM overproduction. These results indicate that Smad3 expression and activation or probucol treatment alters Smad1 phosphorylation, thus suggesting new molecular mechanisms underlying DN development and progression.

Published

2018

9. 尿中IV型コラーゲン排泄は非糖尿病日本人一般住民の推定糸球体濾過量の低下に関与する : 5年間の観察研究

Author

Kishi, Fumi, Nagai, Kojiro, Takamatsu, Norimichi, Tominaga, Tatsuya, Tamaki, Masanori, Shibata, Eriko, Murakami, Taichi, Kishi, Seiji, Abe, Hideharu, Koezuka, Yasuhiko, Minagawa, Naoto, Ichien, Go, and Doi, Toshio

Subjects

Japanese general population, Chronic Kidney Desease, eGFR, Urinary type IV collagen, without diabetes

Abstract

Urinary type IV collagen (U-Col4) and albumin excretion is evaluated to monitor the development of diabetic kidney disease. However, U-Col4 excretion in the general population without diabetes has not yet been fully elucidated. In this study, 1067 participants without diabetes and with urinary albumin-creatinine ratio

Published

2018

10. Conditional Deletion of Smad1 Ameliorates Glomerular Injury in Progressive Glomerulonephritis

Author

Araki, Makoto, Matsubara, Takeshi, Abe, Hideharu, Torikoshi, Kazuo, Mima, Akira, Iehara, Noriyuki, Fukatsu, Atsushi, Kita, Toru, Arai, Hidenori, and Doi, Toshio

Subjects

animal structures, Glomerulonephritis, Glomerulosclerosis, embryonic structures, Collagen type IV, Smad1, biological phenomena, cell phenomena, and immunity

Abstract

Matrix expansion and cell proliferation are concomitantly observed in various glomerular injuries. However, the molecular mechanisms responsible for these changes have not been fully elucidated. We have reported that Smad1 is a key signalling molecule that regulates the transcription of type IV collagen (Col4) in mesangial matrix expansion and is thereby involved in glomerular injury in an acute model of glomerulonephritis. In this study, we addressed the role of Smad1 signalling in accelerated nephrotoxic nephritis (NTN), a model of progressive glomerulonephritis, using conditional deletion of Smad1 in Rosa26CreERT2 mice (Smad1-CKO). Mesangial matrix expansion in the Smad1-CKO mice with NTN was significantly inhibited compared with that in wild type mice with NTN, which was consistent with the decrease in Col4 expression level. On the other hand, STAT3 activation and cell proliferation were not influenced by Smad1 deletion in the NTN model. Therefore, we investigated another factor that activates cell proliferation in the absence of Smad1. Id2 induced VEGF secretion and subsequent STAT3 activation, independently of Smad1 expression in mouse mesangial cells. Here we show that Smad1 plays an important role in the development of glomerular injury without affecting cell proliferation, in progressive glomerulonephritis.

Published

2016

11. ビタミン D ユウドウタイ ガ メサンギウム サイボウ ノ ヘイカツキン ケイシツ オ Transforming Growth Factor - ベータ 2ガタ ジュヨウタイ オ カイシテ セイギョ スル

Author

Abe, Hideharu, 中尾, 一和, 小川, 修, and 北, 徹

Abstract

許諾条件により本文は公開していません : 本文は「THE JOURNAL OF BIOLOGICAL CHEMISTRY Vol.274, No.30, pp.20874-20878」に掲載, 本文データは平成22年度国立国会図書館の学位論文(博士)のデジタル化実施により作成された画像ファイルを基にpdf変換したものである

Published

2001