Luman/CREB3 Recruitment Factor Regulates Glucocorticoid Receptor Activity and Is Essential for Prolactin-Mediated Maternal Instinct

Martyn, Amanda C.; Choleris, Elena; Gillis, Daniel; Armstrong, John N.; Amor, Talya R.; McCluggage, A.R.R.; Turner, Patricia V.; Liang, Guanxiang; Cai, Kimberly; Lu, Ray

doi:10.1128/mcb.01142-12

Cited by 35 publications

(41 citation statements)

References 68 publications

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“…Besides its cellular function, the biological role of LRF is largely unknown. Recently, we found a severe maternal behavioral defect in female LRF gene knockout mice accompanied by misregulation of glucocorticoid and prolactin signaling [23]. Our preliminary data also suggest a fertility deficit in these mutant mice (unpublished), suggesting a potential role for LRF in reproduction and related hormonal signaling.…”

supporting

confidence: 61%

Expression Pattern Implicates a Potential Role for Luman Recruitment Factor in the Process of Implantation in Uteri and Development of Preimplantation Embryos in Mice

et al. 2013

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Luman/CREB3 recruitment factor (LRF or CREBRF) was identified as a regulator of Luman (or CREB3) that is involved in the unfolded protein response during endoplasmic reticulum stress. Luman is implicated in a multitude of functions ranging from viral infection and immunity to cancer. The biological function of LRF, however, is unknown. In this paper, we report that uteri of pregnant mice and embryos displayed enhanced LRF expression at all stages, and the expressed LRF was found to be localized specifically at implantation sites. On the other hand, uteri of mice induced for delayed implantation or pseudopregnant mice showed low levels of LRF expression, suggesting that LRF mediates uterine receptivity during implantation. Further, expression of LRF was found to be modulated by steroid hormones such as progesterone and estradiol. This study thereby identifies a potential role for LRF in the process of implantation in uteri and development of preimplantation embryos in mice.

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confidence: 61%

Expression Pattern Implicates a Potential Role for Luman Recruitment Factor in the Process of Implantation in Uteri and Development of Preimplantation Embryos in Mice

et al. 2013

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“…However, the function of CREBRF is minimally characterized, so the mechanisms by which rs373863828 affects these phenotypes are currently unclear. Individual studies have indicated that this transcription factor impacts glucocorticoid signaling, autophagy, unfolded protein response, and starvation resistance, as well as murine decidualization, embryo implantation, and maternal behavior (Audas, Li, Liang, & Lu, 2008; Li et al, 2016; Martyn et al, 2012; Minster et al, 2016; Xue et al, 2016; Yang et al, 2013). Future studies should aim to refine the effect of this variation on the related phenotypes of height, weight, and BMI in other Pacific Island populations, as well as other anthropometric traits.…”

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confidence: 99%

A missense variant in CREBRF is associated with taller stature in Samoans

Carlson

Rosenthal

Russell

et al. 2019

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ObjectivesStudies have demonstrated that rs373863828, a missense mutation in CREBRF, is associated with a number of anthropometric traits including body mass index (BMI), obesity, percent body fat, hip circumference, and abdominal circumference. Given the biological relationship between height and adiposity, we hypothesized that the effect of this variant on BMI might be due in part to a previously untested association of this variant with height.MethodsWe tested the hypothesis that minor allele of rs373863828 is associated with height in a Samoan population in two adult cohorts and in a separate cohort of children (age 5 - 18 years old) using linear mixed modeling.ResultsWe found evidence of a strong relationship between rs373863828 and greater mean height in Samoan adults (0.77 cm greater average height for each copy of the minor allele) with the same direction of effect in Samoan children.ConclusionsThese results suggest that the missense variant rs373863828 in CREBRF, first identified through an association with larger BMI, may be related to an underlying biological mechanism affecting overall body size including stature.

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“…The potential importance of this variant in organismal energy homeostasis is further supported by the ‘lean’ phenotype of mice 30 and flies 26 lacking the ortholog for this gene. These data, in combination with evidence of positive selection, support a thrifty variant hypothesis for human obesity and underscore the value of examining unique populations to identify new genetic contributions to complex traits.…”

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confidence: 97%

“…In support of this hypothesis, expression of CREBRF orthologs is highly induced by starvation in all tissues of Drosophila 26,27 as well as in human lymphoblasts 28,29 . Moreover, REPTOR -knockout flies 26 and Crebrf -knockout mice 30 have lower total energy storage and body weight, respectively. Similarly, we found that nutrient starvation of 3T3-L1 preadipocytes rapidly increased Crebrf mRNA levels, which peaked by 4 h at levels 13-fold higher than those seen at 0 h ( P = 1.1 × 10 −16 ) and remained elevated by 5-fold at 24 h after the start of starvation ( P = 4.1 × 10 −14 ) (Fig.…”

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confidence: 99%

A thrifty variant in CREBRF strongly influences body mass index in Samoans

et al. 2016

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Samoans are a unique founder population with a high prevalence of obesity1–3, making them well suited for identifying new genetic contributors to obesity4. We conducted a genome-wide association study (GWAS) in 3,072 Samoans, discovered a variant, rs12513649, strongly associated with body mass index (BMI) (P = 5.3 × 10−14), and replicated the association in 2,102 additional Samoans (P = 1.2 × 10−9). Targeted sequencing identified a strongly associated missense variant, rs373863828 (p.Arg457Gln), in CREBRF (meta P = 1.4 × 10−20). Although this variant is extremely rare in other populations, it is common in Samoans (frequency of 0.259), with an effect size much larger than that of any other known common BMI risk variant (1.36–1.45 kg/m2 per copy of the risk-associated allele). In comparison to wild-type CREBRF, the Arg457Gln variant when overexpressed selectively decreased energy use and increased fat storage in an adipocyte cell model. These data, in combination with evidence of positive selection of the allele encoding p.Arg457Gln, support a ‘thrifty’ variant hypothesis as a factor in human obesity.

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Luman/CREB3 Recruitment Factor Regulates Glucocorticoid Receptor Activity and Is Essential for Prolactin-Mediated Maternal Instinct

Cited by 35 publications

References 68 publications

Expression Pattern Implicates a Potential Role for Luman Recruitment Factor in the Process of Implantation in Uteri and Development of Preimplantation Embryos in Mice

Expression Pattern Implicates a Potential Role for Luman Recruitment Factor in the Process of Implantation in Uteri and Development of Preimplantation Embryos in Mice

A missense variant in CREBRF is associated with taller stature in Samoans

A thrifty variant in CREBRF strongly influences body mass index in Samoans

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