Projects per year
Abstract
Background: The growth factor receptor bound protein 7 (Grb7) family of signalling adaptor proteins comprises Grb7, Grb10 and Grb14. Each can interact with the insulin receptor and other receptor tyrosine kinases, where Grb10 and Grb14 inhibit insulin receptor activity. In cell culture studies they mediate functions including cell survival, proliferation, and migration. Mouse knockout (KO) studies have revealed physiological roles for Grb10 and Grb14 in glucose-regulated energy homeostasis. Both Grb10 KO and Grb14 KO mice exhibit increased insulin signalling in peripheral tissues, with increased glucose and insulin sensitivity and a modestly increased ability to clear a glucose load. In addition, Grb10 strongly inhibits fetal growth such that at birth Grb10 KO mice are 30% larger by weight than wild type littermates.
Results: Here, we generate a Grb7 KO mouse model. We show that during fetal development the expression patterns of Grb7 and Grb14 each overlap with that of Grb10. Despite this, Grb7 and Grb14 did not have a major role in influencing fetal growth, either alone or in combination with Grb10. At birth, in most respects both Grb7 KO and Grb14 KO single mutants were indistinguishable from wild type, while Grb7:Grb10 double knockout (DKO) were near identical to Grb10 KO single mutants and Grb10:Grb14 DKO mutants were slightly smaller than Grb10 KO single mutants. In the developing kidney Grb7 had a subtle positive influence on growth. An initial characterisation of Grb7 KO adult mice revealed sexually dimorphic effects on energy homeostasis, with females having a significantly smaller renal white adipose tissue depot and an enhanced ability to clear glucose from the circulation, compared to wild type littermates. Males had elevated fasted glucose levels with a trend towards smaller white adipose depots, without improved glucose clearance.
Conclusions: Grb7 and Grb14 do not have significant roles as inhibitors of fetal growth, unlike Grb10, and instead Grb7 may promote growth of the developing kidney. In adulthood, Grb7 contributes subtly to glucose mediated energy homeostasis, raising the possibility of redundancy between all three adaptors in physiological regulation of insulin signalling and glucose handling.
Results: Here, we generate a Grb7 KO mouse model. We show that during fetal development the expression patterns of Grb7 and Grb14 each overlap with that of Grb10. Despite this, Grb7 and Grb14 did not have a major role in influencing fetal growth, either alone or in combination with Grb10. At birth, in most respects both Grb7 KO and Grb14 KO single mutants were indistinguishable from wild type, while Grb7:Grb10 double knockout (DKO) were near identical to Grb10 KO single mutants and Grb10:Grb14 DKO mutants were slightly smaller than Grb10 KO single mutants. In the developing kidney Grb7 had a subtle positive influence on growth. An initial characterisation of Grb7 KO adult mice revealed sexually dimorphic effects on energy homeostasis, with females having a significantly smaller renal white adipose tissue depot and an enhanced ability to clear glucose from the circulation, compared to wild type littermates. Males had elevated fasted glucose levels with a trend towards smaller white adipose depots, without improved glucose clearance.
Conclusions: Grb7 and Grb14 do not have significant roles as inhibitors of fetal growth, unlike Grb10, and instead Grb7 may promote growth of the developing kidney. In adulthood, Grb7 contributes subtly to glucose mediated energy homeostasis, raising the possibility of redundancy between all three adaptors in physiological regulation of insulin signalling and glucose handling.
| Original language | English |
|---|---|
| Article number | 221 |
| Journal | BMC Biology |
| Volume | 22 |
| Issue number | 1 |
| Early online date | 30 Sept 2024 |
| DOIs | |
| Publication status | Published - 30 Sept 2024 |
Data Availability Statement
All data generated or analysed during this study are included in this published article and its supplementary information files. The Grb10 KO (full designation Grb10Gt(β−geo)1Ward) [17] and Grb14 KO [33] mouse strains were generated as previously described and can be obtained from us. The Grb7 KO strain we describe here can be obtained with permission from Benjamin Margolis (University of Michigan, USA).Acknowledgements
For generously supplying the Grb7 KO mouse strain we thank Benjamin Margolis (University of Michigan, USA). We are grateful to University of Bath Biological Services Unit staff for outstanding animal care.Funding
This work was supported by Medical Research Council grants [MR/S00002X/1, MR/S008233/1]. The funder had no specific role in the conceptualization, design, data collection, analysis, decision to publish, or preparation of the manuscript.
| Funders | Funder number |
|---|---|
| Medical Research Council | MR/S008233/1, MR/S00002X/1 |
Keywords
- Cell signalling
- Developmental biology
- Epistasis
- Fetal growth
- Genomic imprinting
- Growth factor receptor
- Insulin
- Mouse genetics
- mTORC1
ASJC Scopus subject areas
- Biotechnology
- Structural Biology
- Ecology, Evolution, Behavior and Systematics
- Physiology
- General Biochemistry,Genetics and Molecular Biology
- General Agricultural and Biological Sciences
- Plant Science
- Developmental Biology
- Cell Biology
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Dive into the research topics of 'Grb7, Grb10 and Grb14, encoding the growth factor receptor-bound 7 family of signalling adaptor proteins have overlapping functions in the regulation of fetal growth and post-natal glucose metabolism'. Together they form a unique fingerprint.Projects
- 2 Finished
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Imprinted genes defining a novel mammalian growth regulatory axis
Ward, A. (PI) & Urrutia, A. (CoI)
28/05/19 → 29/12/22
Project: Research council
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MRC adipose regulation
Ward, A. (PI) & Moorwood, K. (Researcher)
3/01/19 → 30/11/22
Project: Research council