The tyrosine kinase receptor Tyro3 enhances lifespan and neuropeptide y (Npy) neuron survival in the mouse anorexia (anx) mutation

Kim, Dennis Y.; Yu, Joanna; Mui, Ryan K.; Niibori, Rieko; Taufique, Hamza Bin; Aslam, Rukhsana; Semple, John W.; Cordes, Sabine P.

The tyrosine kinase receptor Tyro3 enhances lifespan and neuropeptide y (Npy) neuron survival in the mouse anorexia (anx) mutation

Mark

Kim, Dennis Y. ; Yu, Joanna ; Mui, Ryan K. ; Niibori, Rieko ; Taufique, Hamza Bin ; Aslam, Rukhsana ; Semple, John W. ^LU and Cordes, Sabine P. (2017) In DMM Disease Models and Mechanisms 10(5). p.581-595

Abstract: Severe appetite and weight loss define the eating disorder anorexia nervosa, and can also accompany the progression of some neurodegenerative disorders such as amyotrophic lateral sclerosis (ALS). Although acute loss of hypothalamic neurons that produce appetite-stimulating neuropeptide Y (Npy) and agouti-related peptide (Agrp) in adult mice or in mice homozygous for the anorexia (anx) mutation causes aphagia, our understanding of the factors that help maintain appetite regulatory circuitry is limited. Here we identify a mutation (C19T) that converts an arginine to a tryptophan (R7W) in the TYRO3 protein tyrosine kinase 3 (Tyro3) gene, which resides within the anx critical interval, as contributing to the severity of anx phenotypes. Our... (More); Severe appetite and weight loss define the eating disorder anorexia nervosa, and can also accompany the progression of some neurodegenerative disorders such as amyotrophic lateral sclerosis (ALS). Although acute loss of hypothalamic neurons that produce appetite-stimulating neuropeptide Y (Npy) and agouti-related peptide (Agrp) in adult mice or in mice homozygous for the anorexia (anx) mutation causes aphagia, our understanding of the factors that help maintain appetite regulatory circuitry is limited. Here we identify a mutation (C19T) that converts an arginine to a tryptophan (R7W) in the TYRO3 protein tyrosine kinase 3 (Tyro3) gene, which resides within the anx critical interval, as contributing to the severity of anx phenotypes. Our observation that, like Tyro3^-/- mice, anx/anx mice exhibit abnormal secondary platelet aggregation suggested that the C19T Tyro3 variant might have functional consequences. Tyro3 is expressed in the hypothalamus and other brain regions affected by the anx mutation, and its mRNA localization appeared abnormal in anx/anx brains by postnatal day 19 (P19). The presence of wild-type Tyro3 transgenes, but not an R7W-Tyro3 transgene, doubled the weight and lifespans of anx/anx mice and near-normal numbers of hypothalamic Npy-expressing neurons were present in Tyro3-transgenic anx/anx mice at P19. Although no differences in R7W-Tyro3 signal sequence function or protein localization were discernible in vitro, distribution of R7W-Tyro3 protein differed from that of Tyro3 protein in the cerebellum of transgenic wild-type mice. Thus, R7W-Tyro3 protein localization deficits are only detectable in vivo. Further analyses revealed that the C19T Tyro3 mutation is present in a few other mouse strains, and hence is not the causative anx mutation, but rather an anx modifier. Our work shows that Tyro3 has prosurvival roles in the appetite regulatory circuitry and could also provide useful insights towards the development of interventions targeting detrimental weight loss.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/4626fc75-d8fd-4f15-b0a5-4a33acfa0a3d

author

Kim, Dennis Y. ; Yu, Joanna ; Mui, Ryan K. ; Niibori, Rieko ; Taufique, Hamza Bin ; Aslam, Rukhsana ; Semple, John W. ^LU and Cordes, Sabine P.

publishing date

2017-05-01

type

Contribution to journal

publication status

published

keywords

Appetite regulation, Eating disorder, Modifier, Neurodegeneration, Npy, RNA localization, Transgenic rescue

in

DMM Disease Models and Mechanisms

volume

10

issue

5

pages

581 - 595

publisher

The Company of Biologists Ltd

external identifiers

scopus:85019560784
pmid:28093506

ISSN

1754-8403

DOI

10.1242/dmm.027433

language

English

LU publication?

no

id

4626fc75-d8fd-4f15-b0a5-4a33acfa0a3d

date added to LUP

2019-12-03 10:15:02

date last changed

2024-04-02 20:44:37

@article{4626fc75-d8fd-4f15-b0a5-4a33acfa0a3d,
  abstract     = {{<p>Severe appetite and weight loss define the eating disorder anorexia nervosa, and can also accompany the progression of some neurodegenerative disorders such as amyotrophic lateral sclerosis (ALS). Although acute loss of hypothalamic neurons that produce appetite-stimulating neuropeptide Y (Npy) and agouti-related peptide (Agrp) in adult mice or in mice homozygous for the anorexia (anx) mutation causes aphagia, our understanding of the factors that help maintain appetite regulatory circuitry is limited. Here we identify a mutation (C19T) that converts an arginine to a tryptophan (R7W) in the TYRO3 protein tyrosine kinase 3 (Tyro3) gene, which resides within the anx critical interval, as contributing to the severity of anx phenotypes. Our observation that, like Tyro3<sup>-/-</sup> mice, anx/anx mice exhibit abnormal secondary platelet aggregation suggested that the C19T Tyro3 variant might have functional consequences. Tyro3 is expressed in the hypothalamus and other brain regions affected by the anx mutation, and its mRNA localization appeared abnormal in anx/anx brains by postnatal day 19 (P19). The presence of wild-type Tyro3 transgenes, but not an R7W-Tyro3 transgene, doubled the weight and lifespans of anx/anx mice and near-normal numbers of hypothalamic Npy-expressing neurons were present in Tyro3-transgenic anx/anx mice at P19. Although no differences in R7W-Tyro3 signal sequence function or protein localization were discernible in vitro, distribution of R7W-Tyro3 protein differed from that of Tyro3 protein in the cerebellum of transgenic wild-type mice. Thus, R7W-Tyro3 protein localization deficits are only detectable in vivo. Further analyses revealed that the C19T Tyro3 mutation is present in a few other mouse strains, and hence is not the causative anx mutation, but rather an anx modifier. Our work shows that Tyro3 has prosurvival roles in the appetite regulatory circuitry and could also provide useful insights towards the development of interventions targeting detrimental weight loss.</p>}},
  author       = {{Kim, Dennis Y. and Yu, Joanna and Mui, Ryan K. and Niibori, Rieko and Taufique, Hamza Bin and Aslam, Rukhsana and Semple, John W. and Cordes, Sabine P.}},
  issn         = {{1754-8403}},
  keywords     = {{Appetite regulation; Eating disorder; Modifier; Neurodegeneration; Npy; RNA localization; Transgenic rescue}},
  language     = {{eng}},
  month        = {{05}},
  number       = {{5}},
  pages        = {{581--595}},
  publisher    = {{The Company of Biologists Ltd}},
  series       = {{DMM Disease Models and Mechanisms}},
  title        = {{The tyrosine kinase receptor Tyro3 enhances lifespan and neuropeptide y (Npy) neuron survival in the mouse anorexia (anx) mutation}},
  url          = {{http://dx.doi.org/10.1242/dmm.027433}},
  doi          = {{10.1242/dmm.027433}},
  volume       = {{10}},
  year         = {{2017}},
}

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The tyrosine kinase receptor Tyro3 enhances lifespan and neuropeptide y (Npy) neuron survival in the mouse anorexia (anx) mutation