Establishment of Leptin-Responsive Cell Lines from Adult Mouse Hypothalamus.
Leptin resistance is considered to be the primary cause of obesity. However, the cause of leptin resistance remains incompletely understood, and there is currently no cure for the leptin-resistant state. In order to identify novel drug-target molecules that could overcome leptin resistance, it would...
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doaj-a49f5dfaa4444b91b5881f854b466ddd2020-11-25T01:50:25ZengPublic Library of Science (PLoS)PLoS ONE1932-62032016-01-01112e014863910.1371/journal.pone.0148639Establishment of Leptin-Responsive Cell Lines from Adult Mouse Hypothalamus.Hiroshi IwakuraKatsuko DoteMika BandoHiroyuki KoyamaKiminori HosodaKenji KangawaKazuwa NakaoLeptin resistance is considered to be the primary cause of obesity. However, the cause of leptin resistance remains incompletely understood, and there is currently no cure for the leptin-resistant state. In order to identify novel drug-target molecules that could overcome leptin resistance, it would be useful to develop in vitro assay systems for evaluating leptin resistance. In this study, we established immortalized adult mouse hypothalamus-derived cell lines, termed adult mouse hypothalamus (AMH) cells, by developing transgenic mice in which SV40 Tag was overexpressed in chromogranin A-positive cells in a tamoxifen-dependent manner. In order to obtain leptin-responsive clones, we selected clones based on the phosphorylation levels of STAT3 induced by leptin. The selected clones were fairly responsive to leptin in terms of STAT3, ERK, and Akt phosphorylation and induction of c-Fos mRNA induction. Pretreatment with leptin, insulin, and palmitate attenuated the c-Fos mRNA response to leptin, suggesting that certain aspects of leptin resistance might be reconstituted in this cellular model. These cell lines are useful tools for understanding the molecular nature of the signal disturbance in the leptin-resistant state and for identifying potential target molecules for drugs that relieve leptin resistance, although they have drawbacks including de-differentiated nature and lack of long-time stability.http://europepmc.org/articles/PMC4744015?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Hiroshi Iwakura Katsuko Dote Mika Bando Hiroyuki Koyama Kiminori Hosoda Kenji Kangawa Kazuwa Nakao |
spellingShingle |
Hiroshi Iwakura Katsuko Dote Mika Bando Hiroyuki Koyama Kiminori Hosoda Kenji Kangawa Kazuwa Nakao Establishment of Leptin-Responsive Cell Lines from Adult Mouse Hypothalamus. PLoS ONE |
author_facet |
Hiroshi Iwakura Katsuko Dote Mika Bando Hiroyuki Koyama Kiminori Hosoda Kenji Kangawa Kazuwa Nakao |
author_sort |
Hiroshi Iwakura |
title |
Establishment of Leptin-Responsive Cell Lines from Adult Mouse Hypothalamus. |
title_short |
Establishment of Leptin-Responsive Cell Lines from Adult Mouse Hypothalamus. |
title_full |
Establishment of Leptin-Responsive Cell Lines from Adult Mouse Hypothalamus. |
title_fullStr |
Establishment of Leptin-Responsive Cell Lines from Adult Mouse Hypothalamus. |
title_full_unstemmed |
Establishment of Leptin-Responsive Cell Lines from Adult Mouse Hypothalamus. |
title_sort |
establishment of leptin-responsive cell lines from adult mouse hypothalamus. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2016-01-01 |
description |
Leptin resistance is considered to be the primary cause of obesity. However, the cause of leptin resistance remains incompletely understood, and there is currently no cure for the leptin-resistant state. In order to identify novel drug-target molecules that could overcome leptin resistance, it would be useful to develop in vitro assay systems for evaluating leptin resistance. In this study, we established immortalized adult mouse hypothalamus-derived cell lines, termed adult mouse hypothalamus (AMH) cells, by developing transgenic mice in which SV40 Tag was overexpressed in chromogranin A-positive cells in a tamoxifen-dependent manner. In order to obtain leptin-responsive clones, we selected clones based on the phosphorylation levels of STAT3 induced by leptin. The selected clones were fairly responsive to leptin in terms of STAT3, ERK, and Akt phosphorylation and induction of c-Fos mRNA induction. Pretreatment with leptin, insulin, and palmitate attenuated the c-Fos mRNA response to leptin, suggesting that certain aspects of leptin resistance might be reconstituted in this cellular model. These cell lines are useful tools for understanding the molecular nature of the signal disturbance in the leptin-resistant state and for identifying potential target molecules for drugs that relieve leptin resistance, although they have drawbacks including de-differentiated nature and lack of long-time stability. |
url |
http://europepmc.org/articles/PMC4744015?pdf=render |
work_keys_str_mv |
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