We are testing a new system for linking grants to scientists.
The funding information displayed below comes from the
NIH Research Portfolio Online Reporting Tools and the
NSF Award Database.
The grant data on this page is limited to grants awarded in the United States and is thus partial. It can nonetheless be used to understand how funding patterns influence mentorship networks and vice-versa, which has deep implications on how research is done.
You can help! If you notice any innacuracies, please
sign in and mark grants as correct or incorrect matches.
Sign in to see low-probability grants and correct any errors in linkage between grants and researchers.
High-probability grants
According to our matching algorithm, Carlos A. Toro is the likely recipient of the following grants.
| Years |
Recipients |
Code |
Title / Keywords |
Matching
score |
| 2016 — 2018 |
Toro, Carlos Alejandro |
F32Activity Code Description:
To provide postdoctoral research training to individuals to broaden their scientific background and extend their potential for research in specified health-related areas. |
Metabolic Control of Puberty Via Epigenetics @ Oregon Health & Science University
? DESCRIPTION (provided by applicant): A number of studies have documented that energy balance can be enduringly affected by nutritional changes taking place during the essential period of developmental programming, which in humans occurs during late gestation and in rodents during the course of their early post-natal life. These alterations have been shown to severely affect female neuroendocrine reproductive development. An excess of nutrients availability advances the timing of puberty; nutritional deficiency delays it. Possibly due to the complexity of the systems involved and absence of precise candidates, neither the molecules linking nutritional programming to pubertal development nor the puberty-related genes they may regulate have been identified. Recently studies performed in our laboratory have demonstrated that female puberty is regulated by an epigenetic mechanism, of transcriptional repression that involves the Polycomb group (PcG) of transcriptional silencers. Our studies showed that this repression is imposed on downstream genes implicated in the stimulatory control of GnRH secretion (epitomized by Kiss gene). By discovering a novel epigenetic mechanism controlling the timing of puberty and identifying its basic components, we have now unveiled the existence of a regulatory system that may not only fulfill the long-sought out role of linking nutrition to neuroendocrine reproductive development, but is also amenable to experimental analysis. Accordingly, this proposal will test the hypothesis that alterations in the developmental programing of energy balance affect the timing of puberty by regulating the mechanism of epigenetic silencing that keeps GnRH secretion in check during prepubertal maturation. To this end, two main hypotheses will be tested: 1) Altering nutrient availability during early postnatal life affects puberty by regulating an epigenetic repressive tone imposed by the PcG complex on puberty-activating (PA) genes; and 2) Additional PcG target genes potentially relevant to the timing of puberty and to the nutritional regulation of this process can be identified by epigenome-wide anlaysis using RNA-and ChIP- massively parallel sequencing technology. I anticipate that a successful outcome of the proposed studies will provide major insights into the integrative mechanisms linking energy homeostasis, the neuroendocrine brain and the control of puberty. I also foresee that these studies will substantially contribute to our understanding on how disorders in energy balance influence the timing and progression of puberty, and will make researchers and clinicians aware of the epigenetics contribution to these disorders.
|
1 |