| ID | 112882 |
| Title Alternative | 小腸のリン恒常性における小腸型アルカリホスファターゼ(Akp3)の役割について
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| Author |
Sasaki, Shohei
University of Tokushima
Segawa, Hiroko
University of Tokushima
Tokushima University Educator and Researcher Directory
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Hanazaki, Ai
University of Tokushima
Kirino, Ruri
University of Tokushima
Fujii, Toru
University of Tokushima
Ikuta, Kayo
University of Tokushima
Noguchi, Miwa
University of Tokushima
Sasaki, Sumire
University of Tokushima
Koike, Megumi
University of Tokushima
Tanifuji, Kazuya
University of Tokushima
Kaneko, Ichiro
University of Tokushima
Tokushima University Educator and Researcher Directory
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Narisawa, Sonoko
Sanford Burnham Prebys Medical Discovery Institute
Millán, José Luis
Sanford Burnham Prebys Medical Discovery Institute
Miyamoto, Ken-ichi
University of Tokushima
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|
| Keywords | Hyperphosphatemia
CKD-MBD
Phosphate transporter
|
| Content Type |
Thesis or Dissertation
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| Description | Background/Aims: Hyperphosphatemia is a serious complication of late-stage chronic kidney disease (CKD). Intestinal inorganic phosphate (Pi) handling plays an important role in Pi homeostasis in CKD. We investigated whether intestinal alkaline phosphatase 3 (Akp3), the enzyme that hydrolyzes dietary Pi compounds, is a target for the treatment of hyperphosphatemia in CKD. Methods: We investigated Pi homeostasis in Akp3 knockout mice (Akp3-/-). We also studied the progression of renal failure in an Akp3-/- mouse adenine treated renal failure model. Plasma, fecal, and urinary Pi and Ca concentration were measured with commercially available kit, and plasma fibroblast growth factor 23, parathyroid hormone, and 1,25(OH)2D3 concentration were measured with ELISA. Brush border membrane vesicles were prepared from mouse intestine using the Ca2+ precipitation method and used for Pi transport activity and alkaline phosphatase activity. In vivo intestinal Pi absorption was measured with oral 32P administration. Results: Akp3-/- mice exhibited reduced intestinal type II sodium-dependent Pi transporter (Npt2b) protein levels and Na-dependent Pi co-transport activity. In addition, plasma active vitamin D levels were significantly increased in Akp3-/- mice compared with wild-type animals. In the adenine-induced renal failure model, Akp3 gene deletion suppressed hyperphosphatemia. Conclusion: The present findings indicate that intestinal Akp3 deletion affects Na+-dependent Pi transport in the small intestine. In the adenine-induced renal failure model, Akp3 is predicted to be a factor contributing to suppression of the plasma Pi concentration.
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| Journal Title |
Kidney and Blood Pressure Research
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| ISSN | 14204096
14230143
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| NCID | AA11085044
AA12783818
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| Publisher | S. Karger AG
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| Volume | 43
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| Issue | 5
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| Start Page | 1409
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| End Page | 1424
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| Published Date | 2018-09-10
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| Remark | 内容要旨・審査要旨・論文本文の公開
本論文は, 著者Shohei Sasakiの学位論文として提出され, 学位審査・授与の対象となっている。 |
| Rights | This article is licensed under the Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License (CC BY-NC-ND) (http://www.karger.com/Services/OpenAccessLicense). Usage and distribution for commercial purposes as well as any distribution of modified material requires written permission.
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| EDB ID | |
| DOI (Published Version) | |
| URL ( Publisher's Version ) | |
| FullText File | |
| language |
eng
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| TextVersion |
ETD
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| MEXT report number | 甲第3220号
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| Diploma Number | 甲栄第260号
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| Granted Date | 2018-09-27
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| Degree Name |
Doctor of Nutritional Science
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| Grantor |
Tokushima University
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| departments |
Medical Sciences
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