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Olig2-Cre for oligodendrocyte conditional models

Conditional deletion of Target limits genetic change to the lineage you choose. That precision matters for oncology, immunology, and metabolic work where systemic loss would confound interpretation. After you confirm your Cre specificity, crossing to Target floxed stock yields interpretable cohorts. For oligodendrocyte work, plan Cre specificity, reporter crosses, and baseline phenotyping before you scale.

View all oligodendrocyte Cre lines

Driver pairing notes

Olig2-Cre biases recombination toward oligodendrocyte lineages. Inducible design: no, constitutive activity.

Conditional knockout keeps oligodendrocyte as the experimental theater while the rest of the animal retains a wild type allele. That pattern mirrors somatic mutation in patients and avoids systemic compensation that can erase subtle phenotypes. It is often preferred when a germline null is lethal, weak, or confounded by developmental rescue.

A conventional knockout answers whether the gene is required broadly. When oligodendrocyte is the organ of interest, a global null can still be informative if viability is acceptable and you want the simplest genotype. If the null is harsh, a floxed allele with a regional Cre is the safer long term platform.

Example conditional alleles to pair with Olig2-Cre

H2 with Olig2-CreStk11 with Olig2-CreCdkn2a with Olig2-CreFbn1 with Olig2-CreHbb with Olig2-Cre

Frequently asked questions

What animals express Olig2-Cre?

Olig2-Cre is used for oligodendrocyte biased recombination in community standard protocols. We recommend reporter validation on your background before large experiments.

Is Olig2-Cre inducible?

Some lines in the CreERT2 family need tamoxifen for nuclear access. Tell us your timing goals and we help pick tamoxifen versus constitutive strategies.

Which floxed genes pair with Olig2-Cre?

Top pairs depend on your disease model. We link common conditional alleles in our catalog and can suggest three to five references genes that match oligodendrocyte biology.

References

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