靶向 RHOA 通路可改善 Kctd13 和 16p11.2 缺失小鼠模型成年期的学习和记忆能力。

Targeting the RHOA pathway improves learning and memory in adult Kctd13 and 16p11.2 deletion mouse models.

机构信息

Université de Strasbourg, CNRS, INSERM, Institut de Génétique Biologie Moléculaire et Cellulaire - UMR 7104 - U1258, IGBMC, 1 rue Laurent Fries, 67404, Illkirch Cedex, France.

Université de Strasbourg, CNRS, INSERM, CELPHEDIA-PHENOMIN-ICS, Institut Clinique de La Souris, 1 rue Laurent Fries, 67404, Illkirch Cedex, France.

出版信息

Mol Autism. 2021 Jan 13;12(1):1. doi: 10.1186/s13229-020-00405-7.

DOI:10.1186/s13229-020-00405-7

PMID:33436060

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7805198/

Abstract

BACKGROUND

Gene copy number variants play an important role in the occurrence of neurodevelopmental disorders. Particularly, the deletion of the 16p11.2 locus is associated with autism spectrum disorder, intellectual disability, and several other features. Earlier studies highlighted the implication of Kctd13 genetic imbalance in 16p11.2 deletion through the regulation of the RHOA pathway.

METHODS

Here, we generated a new mouse model with a small deletion of two key exons in Kctd13. Then, we targeted the RHOA pathway to rescue the cognitive phenotypes of the Kctd13 and 16p11.2 deletion mouse models in a pure genetic background. We used a chronic administration of fasudil (HA1077), an inhibitor of the Rho-associated protein kinase, for six weeks in mouse models carrying a heterozygous inactivation of Kctd13, or the deletion of the entire 16p11.2 BP4-BP5 homologous region.

RESULTS

We found that the small Kctd13 heterozygous deletion induced a cognitive phenotype similar to the whole deletion of the 16p11.2 homologous region, in the Del/+ mice. We then showed that chronic fasudil treatment can restore object recognition memory in adult heterozygous mutant mice for Kctd13 and for 16p11.2 deletion. In addition, learning and memory improvement occurred in parallel to change in the RHOA pathway.

LIMITATIONS

The Kcdt13 mutant line does not recapitulate all the phenotypes found in the 16p11.2 Del/+ model. In particular, the locomotor activity was not altered at 12 and 18 weeks of age and the object location memory was not defective in 18-week old mutants. Similarly, the increase in locomotor activity was not modified by the treatment in the 16p11.2 Del/+ mouse model, suggesting that other loci were involved in such defects. Rescue was observed only after four weeks of treatment but no long-term experiment has been carried out so far. Finally, we did not check the social behaviour, which requires working in another hybrid genetic background.

CONCLUSION

These findings confirm KCTD13 as one target gene causing cognitive deficits in 16p11.2 deletion patients, and the relevance of the RHOA pathway as a therapeutic path for 16p11.2 deletion. In addition, they reinforce the contribution of other gene(s) involved in cognitive defects found in the 16p11.2 models in older mice.

摘要

背景

基因拷贝数变异在神经发育障碍的发生中起着重要作用。特别是，16p11.2 基因座的缺失与自闭症谱系障碍、智力障碍和其他几个特征有关。早期研究强调了 Kctd13 遗传失衡通过调节 RHOA 途径在 16p11.2 缺失中的作用。

方法

在这里，我们构建了一个新的小鼠模型，该模型中 Kctd13 的两个关键外显子发生了小缺失。然后，我们针对 RHOA 途径，在纯遗传背景下拯救 Kctd13 和 16p11.2 缺失小鼠模型的认知表型。我们使用 Rho 相关蛋白激酶抑制剂 fasudil（HA1077）进行六周的慢性给药，该抑制剂用于携带 Kctd13 杂合失活或整个 16p11.2 BP4-BP5 同源区缺失的小鼠模型。

结果

我们发现，在 Del/+ 小鼠中，Kctd13 杂合性小缺失诱导的认知表型类似于整个 16p11.2 同源区的缺失。然后，我们表明慢性 fasudil 治疗可以恢复成年杂合突变小鼠的物体识别记忆，无论是 Kctd13 还是 16p11.2 缺失。此外，学习和记忆的改善与 RHOA 途径的改变平行发生。

局限性

Kcdt13 突变系不能重现 16p11.2 Del/+ 模型中发现的所有表型。特别是，在 12 和 18 周龄时，运动活性没有改变，在 18 周龄的突变体中，物体位置记忆没有缺陷。同样，16p11.2 Del/+ 小鼠模型中，运动活性的增加也没有因治疗而改变，这表明其他基因座也参与了这种缺陷。仅在治疗四周后观察到挽救，但迄今为止尚未进行长期实验。最后，我们没有检查社会行为，这需要在另一个杂交遗传背景下进行。