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Dendritic cells overcome Cre/Lox induced gene deficiency by siphoning cytosolic material from surrounding cells.


ABSTRACT: In a previous report, keratinocytes were shown to share their gene expression profile with surrounding Langerhans cells (LCs), influencing LC biology. Here, we investigated whether transferred material could substitute for lost gene products in cells subjected to Cre/Lox conditional gene deletion. We found that in human Langerin-Cre mice, epidermal LCs and CD11b+CD103+ mesenteric DCs overcome gene deletion if the deleted gene was expressed by neighboring cells. The mechanism of material transfer differed from traditional antigen uptake routes, relying on calcium and PI3K, being susceptible to polyguanylic acid inhibition, and remaining unaffected by inflammation. Termed intracellular monitoring, this process was specific to DCs, occurring in all murine DC subsets tested and human monocyte-derived DCs. The transferred material was presented on MHC-I and MHC-II, suggesting a role in regulating immune responses.

SUBMITTER: Herbst CH 

PROVIDER: S-EPMC10879714 | biostudies-literature | 2024 Mar

REPOSITORIES: biostudies-literature

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Dendritic cells overcome Cre/Lox induced gene deficiency by siphoning cytosolic material from surrounding cells.

Herbst Christopher H CH   Bouteau Aurélie A   Menykő Evelin J EJ   Qin Zhen Z   Gyenge Ervin E   Su Qingtai Q   Cooper Vincent V   Mabbott Neil A NA   Igyártó Botond Z BZ  

iScience 20240206 3


In a previous report, keratinocytes were shown to share their gene expression profile with surrounding Langerhans cells (LCs), influencing LC biology. Here, we investigated whether transferred material could substitute for lost gene products in cells subjected to Cre/Lox conditional gene deletion. We found that in human Langerin-Cre mice, epidermal LCs and CD11b+CD103+ mesenteric DCs overcome gene deletion if the deleted gene was expressed by neighboring cells. The mechanism of material transfer  ...[more]

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