Striking Immune Phenotypes in Gene-Targeted Mice Are Driven by a Copy-Number Variant Originating from a Commercially Available C57BL/6 Strain

Mahajan, Vinay S.; Demissie, Ezana; Mattoo, Hamid; Viswanadham, Vinay; Varki, Ajit; Morris, Robert; Pillai, Shiv

doi:10.1016/j.celrep.2016.04.080

Cited by 70 publications

(61 citation statements)

References 31 publications

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“…Six to eight weeks old male C57BL/6 wild-type and Cmah −/− mice with a human-like deletion in the exon 6 of the Cmah gene (Hedlund et al, 2007) were used. The Cmah −/− mice were negatively tested for a dock2 mutation, recently shown to be present in some of these mice due to backcrossing into commercially available C57BL/6 mice (Mahajan et al, 2016). Sedation was performed by inhalation of 4% isoflurane or by intraperitoneal injection of 80 mg kg −1 Ketamin and 5 mg kg −1 Rompun (Bayer AG) according to their body weight.…”

Section: Methodsmentioning

confidence: 99%

Streptococcus pneumoniae Senses a Human-like Sialic Acid Profile via the Response Regulator CiaR

Hentrich

Löfling

Pathak

et al. 2016

Cell Host & Microbe

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Summary Streptococcus pneumoniae is a human-adapted pathogen that encounters terminally sialylated glycoconjugates and free sialic acid (Sia) in the airways. Upon scavenging by the bacterial sialidase NanA, Sia products serve as carbon sources for the bacteria. Unlike most animals in which cytidine-monophosphate-N-acetylneuraminic acid hydroxylase (CMAH) converts Sia N-acetylneuraminic acid (Neu5Ac) into N-glycolylneuraminic acid (Neu5Gc), humans have an inactive CMAH, causing an absence of Neu5Gc and excess Neu5Ac. We find that pneumococcal challenge in Cmah−/− mice leads to heightened bacterial loads, virulence, and NanA expression. In vitro, NanA is upregulated in response to Neu5Ac compared to Neu5Gc, a process controlled by two-component response regulator CiaR and requiring Sia uptake by the transporter SatABC. Additionally, compared to Neu5Gc, Neu5Ac increases pneumococcal resistance to antimicrobial reactive oxygen species in a CiaR-dependant manner. Thus, S. pneumoniae senses and responds to Neu5Ac, leading to CiaR activation and increased virulence and potentially explaining greater susceptibility in humans.

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Section: Methodsmentioning

confidence: 99%

Streptococcus pneumoniae Senses a Human-like Sialic Acid Profile via the Response Regulator CiaR

Hentrich

Löfling

Pathak

et al. 2016

Cell Host & Microbe

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“…Most of the genetic variability among mouse strains has been focused on SNPs; however, variation in structure of DNA regions affecting DNA sequence length and/or orientation that includes deletions, insertions, copy-number gains, inversions, and transposable elements, may also underpin susceptibility traits [26]. In addition, while inbred mouse strains are considered isogenic, intra-strain differences and their influence on experimental outcomes have been identified [27, 28]. …”

Section: Genetic Variabilitymentioning

confidence: 99%

Genetic and epigenetic determinants of inter-individual variability in responses to toxicants

Lewis

Crawford

Furey

et al. 2017

Current Opinion in Toxicology

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It is well established that genetic variability has a major impact on susceptibility to common diseases, responses to drugs and toxicants, and influences disease-related outcomes. The appreciation that epigenetic marks also vary across the population is growing with more data becoming available from studies in humans and model organisms. In addition, the links between genetic variability, toxicity outcomes and epigenetics are being actively explored. Recent studies demonstrate that gene-by-environment interactions involve both chromatin states and transcriptional regulation, and that epigenetics provides important mechanistic clues to connect expression-related quantitative trait loci (QTL) and disease outcomes. However, studies of Gene×Environment×Epigenetics further extend the complexity of the experimental designs and create a challenge for selecting the most informative epigenetic readouts that can be feasibly performed to interrogate multiple individuals, exposures, tissue types and toxicity phenotypes. We propose that among the many possible epigenetic experimental methodologies, assessment of chromatin accessibility coupled with total RNA levels provides a cost-effective and comprehensive option to sufficiently characterize the complexity of epigenetic and regulatory activity in the context of understanding the inter-individual variability in responses to toxicants.

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“…As illustrated in Table 2, some immune relevant genetic variations among C57BL/6 substrains include a Nlrp12 mutation in C57BL/6J mice and a Dock2 mutation in C57BL/6NHsd mice from certain colonies. 55,77 The Nlrp12 gene primarily controls neutrophil chemotaxis in response to bacterial invasion. C57BL/6J mice carry a missense, loss of function mutation (Nlrp12 C57BL/6J ) and are more susceptible to certain bacterial infections compared with other C57BL/6 substrains harboring the wild-type Nlrp12 allele.…”

Section: Immune Relevant Variations Among Substrainsmentioning

confidence: 99%

“…The Dock2 Hsd mutation was revealed when reduced splenic marginal zone B cells and increased numbers of CD8+ T cells were identified in C57BL/6NHsd (and derived mutant mice) relative to other C57BL/6N mice. [77][78][79] Subsequently, Envigo tested their mice and reported that this mutation (Dock2 Hsd ) was present in 6 of their 19 C57BL/6NHsd colonies (http://www.envigo.com/ assets/docs/c57-customer-communication-2-final-9jun16.pdf). Many research programs maintain in-house colonies of genetically engineered animals and "wild-type" background strains that warrant genetic quality assurance (QA) testing and breeding strategies to minimize effects of random mutations and genetic drift.…”

Section: Immune Relevant Variations Among Substrainsmentioning

confidence: 99%

Immune Relevant and Immune Deficient Mice: Options and Opportunities in Translational Research

Radælli

Santagostino²,

Sellers

et al. 2018

ILAR Journal

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In 1989 ILAR published a list and description of immunodeficient rodents used in research. Since then, advances in understanding of molecular mechanisms; recognition of genetic, epigenetic microbial, and other influences on immunity; and capabilities in manipulating genomes and microbiomes have increased options and opportunities for selecting mice and designing studies to answer important mechanistic and therapeutic questions. Despite numerous scientific breakthroughs that have benefitted from research in mice, there is debate about the relevance and predictive or translational value of research in mice. Reproducibility of results obtained from mice and other research models also is a well-publicized concern. This review summarizes resources to inform the selection and use of immune relevant mouse strains and stocks, aiming to improve the utility, validity, and reproducibility of research in mice. Immune sufficient genetic variations, immune relevant spontaneous mutations, immunodeficient and autoimmune phenotypes, and selected induced conditions are emphasized.

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Striking Immune Phenotypes in Gene-Targeted Mice Are Driven by a Copy-Number Variant Originating from a Commercially Available C57BL/6 Strain

Cited by 70 publications

References 31 publications

Streptococcus pneumoniae Senses a Human-like Sialic Acid Profile via the Response Regulator CiaR

Streptococcus pneumoniae Senses a Human-like Sialic Acid Profile via the Response Regulator CiaR

Genetic and epigenetic determinants of inter-individual variability in responses to toxicants

Immune Relevant and Immune Deficient Mice: Options and Opportunities in Translational Research

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