AI Article Synopsis
- Researchers found a specific genetic variant (Dock2) that affects immune function in a common mouse strain (C57BL/6) used in experiments, which originated from a colony of Irf5 knockout mice.
- This variant was unintentionally introduced into various mutant mouse lines, complicating the understanding of their immune responses because the strain shows several immune deficiencies typical of Dock2 loss.
- As a result, previous studies that relied on these mice for immunological research may require reevaluation due to the potential misinterpretation of data linked to the Dock2 disruption.
Article Abstract
We describe a homozygous copy-number variant that disrupts the function of Dock2 in a commercially available C57BL/6 mouse strain that is widely used for backcrossing. This Dock2 allele was presumed to have spontaneously arisen in a colony of Irf5 knockout mice. We discovered that this allele has actually been inadvertently backcrossed into multiple mutant mouse lines, including two engineered to be deficient in Siae and Cmah. This particular commercially obtained subline of C57BL/6 mice also exhibits several striking immune phenotypes that have been previously described in the context of Dock2 deficiency. Inadvertent backcrossing of a number of gene-targeted mice into this background has complicated the interpretation of several immunological studies. In light of these findings, published studies involving immune or hematopoietic phenotypes in which these C57BL/6 mice have been used as controls, as experimental animals, or for backcrossing will need to be reinterpreted.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4892502 | PMC |
| http://dx.doi.org/10.1016/j.celrep.2016.04.080 | DOI Listing |
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