2014
DOI: 10.1371/journal.pone.0106923
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Modulation of Gene Expression by 3-Iodothyronamine: Genetic Evidence for a Lipolytic Pattern

Abstract: 3-Iodothyronamine (T1AM) is an endogenous biogenic amine, structurally related to thyroid hormone, which is regarded as a novel chemical messenger. The molecular mechanisms underlying T1AM effects are not known, but it is possible to envisage changes in gene expression, since delayed and long-lasting phenotypic effects have been reported, particularly with regard to the modulation of lipid metabolism and body weight. To test this hypothesis we analysed gene expression profiles in adipose tissue and liver of ei… Show more

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Cited by 30 publications
(30 citation statements)
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“…Mitchel et al [30] performed RT-PCR with rat TAAR1 specific primers and noticed that TAAR1 mRNA was present in various rat tissues including adipose tissue and that T1AM induced some of its lipolytic effects by activating this receptor [30]. This is further supported by Marrioti et al [18], who used chronic T1AM treatment (the same dose as our study twice a day for five days) in a rat model and looked for gene expression changes [18]. They discovered elevated lipolysis and gene expression of beta-oxidation markers coupled with the decreased expression of adipogenesis markers in adipose tissue.…”
Section: Is Sc Cu Us Ss Si Io On Nmentioning
confidence: 87%
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“…Mitchel et al [30] performed RT-PCR with rat TAAR1 specific primers and noticed that TAAR1 mRNA was present in various rat tissues including adipose tissue and that T1AM induced some of its lipolytic effects by activating this receptor [30]. This is further supported by Marrioti et al [18], who used chronic T1AM treatment (the same dose as our study twice a day for five days) in a rat model and looked for gene expression changes [18]. They discovered elevated lipolysis and gene expression of beta-oxidation markers coupled with the decreased expression of adipogenesis markers in adipose tissue.…”
Section: Is Sc Cu Us Ss Si Io On Nmentioning
confidence: 87%
“…The subchronic T1AM treatment causes ketonuria and a significant loss of body fat indicating a shift in the metabolic pathways from carbohydrate to lipid oxidation. The treatment also triggers lipolytic pattern in rat adipose tissue and modulates mitochondrial FoF1-ATP synthase activity [16][17][18][19][20]. Taken together, these modulations in lipid metabolism provide a balance in energy homeostasis and thus have a great potential in therapeutic applications (especially for treating obesity).…”
Section: Introductionmentioning
confidence: 94%
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“…Uptake of T1AM appears to be mediated via facilitated diffusion, but the specific transporters which are responsible for this have yet to be identified [26], however due to its association with ApoB100 in circulation, LDL receptors may likely facilitate for cellular internalization of T1AM [25]. This internalization, and subsequent unknown intracellular interaction, may mediate long term alterations in gene expression patterns, as confirmed by Mariotti et al in rat adipose and liver [27], and possibly account for the persistence of effects observed in chronic T1AM administration [3] (Figure 2). …”
Section: Distribution and Transportmentioning
confidence: 89%
“…This response was thought to be mediated through α2A adrenergic receptor interaction, whereby T1AM possesses adrenergicblocking properties [31]. This interaction with α2A may present an additional ubiquitous receptor target of T1AM than just GCPRs as it has also been speculated that T1AM interacts with α2A in pancreatic beta-cells [27]. ICV administration of T1AM was able to improve learning capacity and served as a memory enhancer in mice [28].…”
Section: Brainmentioning
confidence: 99%