Kynurenine‐Induced Aryl Hydrocarbon Receptor Signaling in Mice Causes Body Mass Gain, Liver Steatosis, and Hyperglycemia

Rojas, Itzel Y.; Moyer, Benjamin J.; Ringelberg, Carol S.; Wilkins, Owen M.; Pooler, Darcy B.; Ness, Dylan B; Coker, Shodeinde; Tosteson, Tor D.; Lewis, Lionel D.; Chamberlin, Mary D.; Tomlinson, Craig R.

doi:10.1002/oby.23065

Cited by 34 publications

(27 citation statements)

References 44 publications

(86 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Consequently, Moyer et al (2016) proposed that a sustained increase in Kyn-induced AHR activity derived from the excess consumption of Western diet helped to promote the obese phenotype. This hypothesis was further tested rigorously in vivo by the Tomlinson group, who subsequently showed that the addition of Kyn to a low-fat diet induced AHR activity in mice to cause weight gain, fatty liver, and hyperglycemia (Rojas et al 2020, in press) [89]. Consistent with their previous findings, cytochrome P450 1B1 (CYP1B1) and stearoyl-coA desaturase 1 (SCD1) appeared to act as downstream effectors of Kyn-induced AHR signaling.…”

Section: Part Iii: Antagonist Theory: Ahr Inhibition As a Means For Treating Obesitymentioning

confidence: 79%

“…Having shown that activation of the AHR promoted obesity, and AHR inhibition prevented obesity, a remaining key question was whether AHR inhibition could also reverse obesity and its associated comorbidities. This question was answered recently in a study by Rojas et al (2020). Their data specifically demonstrated that obese C57BL6/J mice maintained on a Western diet, when switched to a Western diet containing the AHR antagonist αNF, lost body mass to a degree in which the mass of these mice nearly matched that of control mice maintained on a low-fat diet [90].…”

Section: Part Iii: Antagonist Theory: Ahr Inhibition As a Means For Treating Obesitymentioning

confidence: 99%

See 1 more Smart Citation

The Aryl Hydrocarbon Receptor in Energy Balance: The Road from Dioxin-Induced Wasting Syndrome to Combating Obesity with Ahr Ligands

Girer

Tomlinson

Elferink

2020

IJMS

Self Cite

View full text Add to dashboard Cite

The aryl hydrocarbon receptor (AHR) has been studied for over 40 years, yet our understanding of this ligand-activated transcription factor remains incomplete. Each year, novel findings continually force us to rethink the role of the AHR in mammalian biology. The AHR has historically been studied within the context of potent activation via AHR agonist 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD), with a focus on how the AHR mediates TCDD toxicity. Research has subsequently revealed that the AHR is actively involved in distinct physiological processes ranging from the development of the liver and reproductive organs, to immune system function and wound healing. More recently, the AHR was implicated in the regulation of energy metabolism and is currently being investigated as a potential therapeutic target for obesity. In this review, we re-trace the steps through which the early toxicological studies of TCDD led to the conceptual framework for the AHR as a potential therapeutic target in metabolic disease. We additionally discuss the key discoveries that have been made concerning the role of the AHR in energy metabolism, as well as the current and future directions of the field.

show abstract

Section: Part Iii: Antagonist Theory: Ahr Inhibition As a Means For Treating Obesitymentioning

confidence: 79%

Section: Part Iii: Antagonist Theory: Ahr Inhibition As a Means For Treating Obesitymentioning

confidence: 99%

The Aryl Hydrocarbon Receptor in Energy Balance: The Road from Dioxin-Induced Wasting Syndrome to Combating Obesity with Ahr Ligands

Girer

Tomlinson

Elferink

2020

IJMS

Self Cite

View full text Add to dashboard Cite

show abstract

“… 37 have indicated that KYN caused body mass gain in mice with a low-fat diet, developed a fatty liver and hyperglycaemia and increased liver Cyp1b1 and Scd1 gene expression. The authors concluded that AhR activation by KYN may be necessary but insufficient for the development of obesity and that excess caloric consumption is also required for a full manifestation of obesity 37 . The above results are in agreement with our results in which we did not observe any weight gain in the animals administered KYN and fed a normal diet.…”

Section: Discussionmentioning

confidence: 99%

Unexpected content of kynurenine in mother’s milk and infant formulas

Marszałek‐Grabska

Stachniuk

Iwaniak

et al. 2022

Sci Rep

View full text Add to dashboard Cite

Mother’s milk is widely recommended as complete food for the offspring in earliest postnatal time. However, the knowledge about detailed composition and the physiological role of bioactive components of breast milk is incomplete. Therefore, the aim of our study was to determine the content of kynurenine (KYN) in human breast milk during lactation and to explore the effects exerted by intragastric KYN administration from birth to weaning on physical and psychomotor development of adult rats. We found that KYN is consistently present in human milk and its content gradually increased from day 4 to 28 after delivery and that it is present in commercial baby formulas in amounts noticeably exceeding its physiological range. Animal studies showed that KYN supplementation resulted in a marked elevation of absorptive surface of rat intestine and in enhanced expression of both, aryl hydrocarbon receptor and G protein-coupled receptor 35 in the intestinal tissue in rats. Moreover, we discovered that KYN administration from birth to weaning resulted in neurobehavioral changes in adult rats. Therefore, we postulate that further research is required to thoroughly understand the function of KYN in early developmental stages of mammals and to ensure the safety of its presence in baby food products.

show abstract

“…Within the cell, unique components of clozapine's chemical structure, that is a halogenated diazepine, might trigger specific cellular responses such as activation of the aryl hydrocarbon receptor (AhR). Our assumption that this ligand-activated transcription factor plays a key role in clozapine-triggered adverse effects is supported by the fact that AhR signaling causes weight gain, hyperglycemia, and hypertension (Chang et al, 2017;Rojas et al, 2021) too. Besides activation of detoxification processes, the AhR is also involved in cell differentiation, angiogenesis, and stress responses.…”

Section: Introductionmentioning

confidence: 93%

“…Beside transcriptional upregulation of drug-metabolizing enzymes, the receptor activates multiple genomic as well as non-genomic pathways involved in stem cell differentiation, cell plasticity, and immunosuppression (Abel and Haarmann-Stemmann, 2010;Matsumura, 2009). In addition, PAH exposure as well as clozapine treatment increase the risk of bone marrow toxicity (Lee et al, 2004;Luster et al, 1985) and liver steatosis (Rojas et al, 2021;Von Wilmsdorff et al, 2014) as well as the incidence of diabetes, abdominal obesity (Lee et al, 2014;Teff and Kim, 2011), and hypertension (Alberich et al, 2019;Lee et al, 2012).…”

Section: Introductionmentioning

confidence: 99%

Activation of the aryl hydrocarbon receptor by clozapine induces preadipocyte differentiation and contributes to endothelial dysfunction

et al. 2022

View full text Add to dashboard Cite

Background: The superior therapeutic benefit of clozapine is often associated with metabolic disruptions as obesity, insulin resistance, tachycardia, higher blood pressure, and even hypertension. Aims: These adverse vascular/ metabolic events under clozapine are similar to those caused by polycyclic aromatic hydrocarbons (PAHs), and clozapine shows structural similarity to well-known ligands of the aryl hydrocarbon receptor (AhR). Therefore, we speculated that the side effects caused by clozapine might rely on AhR signaling. Methods: We examined clozapine-induced AhR activation by luciferase reporter assays in hepatoma HepG2 cells and we proved upregulation of the prototypical AhR target gene Cyp1A1 by realtime-PCR (RT-PCR) analysis and enzyme activity. Next we studied the physiological role of AhR in clozapine’s effects on human preadipocyte differentiation and on vasodilatation by myography in wild-type and AhR-/- mice. Results: In contrast to other antipsychotic drugs (APDs), clozapine triggered AhR activation and Cyp1A1 expression in HepG2 cells and adipocytes. Clozapine induced adipogenesis via AhR signaling. After PGF2α-induced constriction of mouse aortic rings, clozapine strongly reduced the maximal vasorelaxation under acetylcholine in rings from wild-type mice, but only slightly in rings from AhR-/- mice. The reduction was also prevented by pretreatment with the AhR antagonist CH-223191. Conclusion: Identification of clozapine as a ligand for the AhR opens new perspectives to explain common clozapine therapy-associated adverse effects at the molecular level.

show abstract

Kynurenine‐Induced Aryl Hydrocarbon Receptor Signaling in Mice Causes Body Mass Gain, Liver Steatosis, and Hyperglycemia

Cited by 34 publications

References 44 publications

The Aryl Hydrocarbon Receptor in Energy Balance: The Road from Dioxin-Induced Wasting Syndrome to Combating Obesity with Ahr Ligands

The Aryl Hydrocarbon Receptor in Energy Balance: The Road from Dioxin-Induced Wasting Syndrome to Combating Obesity with Ahr Ligands

Unexpected content of kynurenine in mother’s milk and infant formulas

Activation of the aryl hydrocarbon receptor by clozapine induces preadipocyte differentiation and contributes to endothelial dysfunction

Contact Info

Product

Resources

About