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Image of Sensory and motor physiological functions are impaired in gastric inhibitory polypeptide receptor-deficient mice
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Sensory and motor physiological functions are impaired in gastric inhibitory polypeptide receptor-deficient mice

Inagaki, Nobuya - Personal Name; Oiso, Yutaka - Personal Name; Seino, Yutaka - Personal Name; Yamada, Yuichiro - Personal Name; Hayashi, Yoshitaka - Personal Name; Tsunekawa, Shin - Personal Name; Seino, Yusuke - Personal Name; Himeno, Tatsuhito - Personal Name; Kamiya, Hideki - Personal Name; Okawa, Tetsuji - Personal Name; Nakamura, Jiro - Personal Name;

Aims/Introduction: Gastric inhibitory polypeptide (GIP) is an incretin secreted from the gastrointestinal tract after an ingestion of nutrients, and stimulates an insulin secretion from the pancreatic islets. Additionally, GIP has important roles in extrapancreatic tissues: fat accumulation in adipose tissue, neuroprotective effects in the central nervous system and an inhibition of bone resorption. In the current study, we investigated the effects of GIP signaling on the peripheral nervous system (PNS). Materials and Methods: First, the presence of the GIP receptor (GIPR) in mouse dorsal root ganglion (DRG) was evaluated utilizing immunohistochemical analysis, western blotting and reverse transcription polymerase chain reaction. DRG neurons of male wild-type mice (WT) were cultured with or without GIP, and their neurite lengths were quantified. Functions of the PNS were evaluated in GIPR-deficient mice (gipr-/-) and WT by using current perception thresholds (CPTs), Thermal Plantar Test (TPT), and motor (MNCV) and sensory nerve conduction velocity (SNCV, respectively). Sciatic nerve blood flow (SNBF) and plantar skin blood flow (PSBF) were also evaluated. Results: We confirmed the expression of GIPR in DRG neurons. The neurite outgrowths of DRG neurons were promoted by the GIP administrations. The gipr-/- showed impaired perception functions in the examination of CPTs and TPT. Both MNCV and SNCV were delayed in gipr-/- compared with these in WT. There was no difference in SNBF and PSBF between WT and gipr-/-. Conclusions: Our findings show that the GIP signal could exert direct physiological roles in the PNS, which might be directly exerted on the PNS.


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Detail Information
Series Title
JDI Jurnal of Diabetes Investigation Volume 5, Issue 1 January 2014
Call Number
(05) 616.46 WIL j
Publisher
Australia : Wiley., 2014
Collation
Hlm. 31-37
Language
English
ISBN/ISSN
2040-1124
Classification
(05) 616.46 WIL j
Content Type
-
Media Type
-
Carrier Type
-
Edition
Volume 5, Issue 1
Subject(s)
Gastric inhibitory polypeptide
Incretins
Peripheral nervous system
Specific Detail Info
-
Statement of Responsibility
-
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Perpustakaan STIKep PPNI Jawa Barat
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Perpustakaan STIKep PPNI Jawa Barat
Kampus 2 STIKep PPNI Jabar
Jl. Muhammad No. 34 Bandung - 40173
Telp. (022) 6004498
http://www.perpus.stikep-ppnijabar.ac.id/

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