Genomic imprinting results in preferential expression of the paternal, or maternal allele of certain genes. We have performed a genome-wide characterization of imprinting in the mouse embryonic and adult brain. This approach uncovered parent-of-origin allelic effects in over 1300 loci. We identified parental bias in the expression of individual genes and of specific transcript isoforms, with differences between brain regions. Many imprinted genes are expressed in neural systems associated with feeding and motivated behaviors, and parental biases preferentially target genetic pathways governing metabolism and cell adhesion. We observed a preferential maternal contribution to gene expression in the developing brain and a major paternal contribution in the adult brain. Thus, parental expression bias emerges as a major mode of epigenetic regulation in the brain.Parent-of-origin effects influence gene expression and trait inheritance in offspring. Genomic imprinting is a form of epigenetic regulation that results in the preferential expression of the paternally or maternally inherited allele of certain genes (1). Currently, fewer than 100 imprinted genes have been identified, and the evolutionary pressures that underlie imprinting are debated (2,3). Clinical and experimental data suggest roles for imprinting in regulating brain development and function (4). In humans, Prader-Willi Syndrome (PWS) and Angelman Syndrome (AS) result from a deletion of the paternal or maternal copy of 15q11-13, respectively. PWS is associated with hyperphagia, stubbornness and compulsive traits (5), whereas AS is associated with absent speech, happy affect and inappropriate laughter (6). Further, studies of parthenogenetic (PG)-and androgenetic (AG)-chimeras in the mouse have suggested preferential maternal contribution to the development of the cortex, but preferential paternal contribution to the hypothalamus (7,8). Such biased roles have yet to be clearly demonstrated. Moreover, despite tantalizing reports, our understanding of the neural systems governed by imprinted genes, and of the scope and features of imprinted loci expressed in the brain is very limited.6 Address correspondance to Dr. Catherine Dulac: dulac@fas.harvard.edu or Dr. Christopher Gregg: cgregg@mcb.harvard.edu. 7 These authors contributed equally to this study. HHMI Author Manuscript HHMI Author Manuscript HHMI Author ManuscriptImprinting refers to functional differences between the maternal and paternal chromosomes or alleles (9), and is also used more strictly to define complete allele-specific silencing (10). Known imprinted genes have been shown to display all-or-none and biased allelic expression according to the gene and tissue considered (11,12). We report here a genomewide analysis of parental allelic effects involving complete silencing or parental biases in gene expression in the murine embryonic day 15 (E15) brain, and in the adult male and female cortex (medial prefrontal cortex (mPFC)) and hypothalamus (preoptic area (POA)). Together with a compa...
A well known, epidemiologically reproducible risk factor for human carcinomas is the long-term consumption of "red meat" of mammalian origin. Although multiple theories have attempted to explain this human-specific association, none have been conclusively proven. We used an improved method to survey common foods for free and glycosidically bound forms of the nonhuman sialic acid N-glycolylneuraminic acid (Neu5Gc), showing that it is highly and selectively enriched in red meat. The bound form of Neu5Gc is bioavailable, undergoing metabolic incorporation into human tissues, despite being a foreign antigen. Interactions of this antigen with circulating anti-Neu5Gc antibodies could potentially incite inflammation. Indeed, when human-like Neu5Gc-deficient mice were fed bioavailable Neu5Gc and challenged with anti-Neu5Gc antibodies, they developed evidence of systemic inflammation. Such mice are already prone to develop occasional tumors of the liver, an organ that can incorporate dietary Neu5Gc. Neu5Gc-deficient mice immunized against Neu5Gc and fed bioavailable Neu5Gc developed a much higher incidence of hepatocellular carcinomas, with evidence of Neu5Gc accumulation. Taken together, our data provide an unusual mechanistic explanation for the epidemiological association between red meat consumption and carcinoma risk. This mechanism might also contribute to other chronic inflammatory processes epidemiologically associated with red meat consumption.
Genetically modified organisms (GMOs) are increasingly deployed at large scales and in open environments. Genetic biocontainment strategies are needed to prevent unintended proliferation of GMOs in natural ecosystems. Existing biocontainment methods are insufficient either because they impose evolutionary pressure on the organism to eject the safeguard, because they can be circumvented by environmentally available compounds, or because they can be overcome by horizontal gene transfer (HGT). Here we computationally redesign essential enzymes in the first organism possessing an altered genetic code to confer metabolic dependence on nonstandard amino acids for survival. The resulting GMOs cannot metabolically circumvent their biocontainment mechanisms using environmentally available compounds, and they exhibit unprecedented resistance to evolutionary escape via mutagenesis and HGT. This work provides a foundation for safer GMOs that are isolated from natural ecosystems by reliance on synthetic metabolites.
Genomic imprinting results in preferential gene expression from paternally versus maternally inherited chromosomes. We used a genome-wide approach to uncover sex-specific parent-of-origin allelic effects in the adult mouse brain. Our study identified preferential selection of the maternally inherited X chromosome in glutamatergic neurons of the female cortex. Moreover, analysis of the cortex and hypothalamus identified 347 autosomal genes with sex-specific imprinting features. In the hypothalamus, sex-specific imprinted genes were mostly found in females, which suggests parental influence over the hypothalamic function of daughters. We show that interleukin-18, a gene linked to diseases with sex-specific prevalence, is subject to complex, regional, and sex-specific parental effects in the brain. Parent-of-origin effects thus provide new avenues for investigation of sexual dimorphism in brain function and disease.
Although the genetic code is redundant, synonymous codons for the same amino acid are not used with equal frequencies in genomes, a phenomenon termed "codon usage bias." Previous studies have demonstrated that synonymous changes in a coding sequence can exert significant cis effects on the gene's expression level. However, whether the codon composition of a gene can also affect the translation efficiency of other genes has not been thoroughly explored. To study how codon usage bias influences the cellular economy of translation, we massively converted abundant codons to their rare synonymous counterpart in several highly expressed genes in Escherichia coli. This perturbation reduces both the cellular fitness and the translation efficiency of genes that have high initiation rates and are naturally enriched with the manipulated codon, in agreement with theoretical predictions. Interestingly, we could alleviate the observed phenotypes by increasing the supply of the tRNA for the highly demanded codon, thus demonstrating that the codon usage of highly expressed genes was selected in evolution to maintain the efficiency of global protein translation. codon usage evolution | tRNA | codon-to-tRNA balance | translation efficiency | genome engineering S ince there are 61 sense codons but only 20 amino acids, most amino acids are encoded by more than a single codon. However, synonymous codons for the same amino acid are not utilized to the same extent across different genes or genomes. This phenomenon, termed "codon usage bias," has been the subject of intense research and was shown to affect gene expression and cellular function through varied processes in bacteria, yeast, and mammals (1-4).Although differential codon usage can result from neutral processes of mutational biases and drift (5-7), certain codon choices could be specifically favored as they increase the efficiency (8-12) or accuracy (13-17) of protein synthesis. These forces would typically lead to codon biases in a gene because they locally exert their effect on the gene in which the codons reside. Indeed, there is a positive correlation between a gene's expression level and the degree of its codon bias (1). Various systems have demonstrated how altering the codon usage synonymously can alter the expression levels of the manipulated genes (18-21), an effect that could reach more than 1,000-fold (22).In addition to such cis effects, it is possible that codon usage also acts in trans, namely, that the codon choice of some genes would affect the translation of others due to a "shared economy" of the entire translation apparatus (23-25). Previous theoretical works have suggested that an increase in the elongation rate may reduce the number of ribosomes on mRNAs and therefore may indirectly increase the rate of initiation of other transcripts due to an increase in the pool of free ribosomes (6,26). In addition, a recent computational study in yeast has also examined the indirect effects of synonymous codon changes on the translation of the entire transcriptome (2...
Here, we describe an RNA-sequencing (RNA-seq)-based approach that accurately detects even modest maternal or paternal allele expression biases at the tissue level, which we call noncanonical genomic imprinting effects. We profile imprinting in the arcuate nucleus (ARN) and dorsal raphe nucleus of the female mouse brain as well as skeletal muscle (mesodermal) and liver (endodermal). Our study uncovers hundreds of noncanonical autosomal and X-linked imprinting effects. Noncanonical imprinting is highly tissue-specific and enriched in the ARN, but rare in the liver. These effects are reproducible across different genetic backgrounds and associated with allele-specific chromatin. Using in situ hybridization for nascent RNAs, we discover that autosomal noncanonical imprinted genes with a tissue-level allele bias exhibit allele-specific expression effects in subpopulations of neurons in the brain in vivo. We define noncanonical imprinted genes that regulate monoamine signaling and determine that these effects influence the impact of inherited mutations on offspring behavior.
Engineering radically altered genetic codes will allow for genomically recoded organisms that have expanded chemical capabilities and are isolated from nature. We have previously reassigned the translation function of the UAG stop codon; however, reassigning sense codons poses a greater challenge because such codons are more prevalent, and their usage regulates gene expression in ways that are difficult to predict. To assess the feasibility of radically altering the genetic code, we selected a panel of 42 highly expressed essential genes for modification. Across 80 Escherichia coli strains, we removed all instances of 13 rare codons from these genes and attempted to shuffle all remaining codons. Our results suggest that the genome-wide removal of 13 codons is feasible; however, several genome design constraints were apparent, underscoring the importance of a strategy that rapidly prototypes and tests many designs in small pieces.
The nonhuman sialic acid N-glycolylneuraminic acid (Neu5Gc) is metabolically incorporated into human tissues from certain mammalian-derived foods, and this occurs in the face of an anti-Neu5Gc “xeno-autoantibody” response. Given evidence that this process contributes to chronic inflammation in some diseases, it is important to understand when and how these antibodies are generated in humans. We show here that human anti-Neu5Gc antibodies appear during infancy and correlate with weaning and exposure to dietary Neu5Gc. However, dietary Neu5Gc alone cannot elicit anti-Neu5Gc antibodies in mice with a humanlike Neu5Gc deficiency. Other postnatally appearing anti-carbohydrate antibodies are likely induced by bacteria expressing these epitopes; however, no microbe is known to synthesize Neu5Gc. Here, we show that trace exogenous Neu5Gc can be incorporated into cell surface lipooligosaccharides (LOS) of nontypeable Haemophilus influenzae (NTHi), a human-specific commensal/pathogen. Indeed, infant anti-Neu5Gc antibodies appear coincident with antibodies against NTHi. Furthermore, NTHi that express Neu5Gc-containing LOS induce anti-Neu5Gc antibodies in Neu5Gc-deficient mice, without added adjuvant. Finally, Neu5Gc from baby food is taken up and expressed by NTHi. As the flora residing in the nasopharynx of infants can be in contact with ingested food, we propose a novel model for how NTHi and dietary Neu5Gc cooperate to generate anti-Neu5Gc antibodies in humans.
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