Publication | Open Access
Blood Group O–Dependent Cellular Responses to Cholera Toxin: Parallel Clinical and Epidemiological Links to Severe Cholera
43
Citations
15
References
2016
Year
ImmunologyImmunologic MechanismO Blood GroupCellular PhysiologyParallel ClinicalCrisprInfection ControlSevere CholeraCholera ToxinMicrobial ToxinVirulence FactorBlood GroupCell BiologyClinical MicrobiologySignal TransductionPathogenesisMicrobiologyCrispr/cas9 EngineeringCellular Immune ResponseSystems BiologyMedicineGenome Editing
Because O blood group has been associated with more severe cholera infections, it has been hypothesized that cholera toxin (CT) may bind non-O blood group antigens of the intestinal mucosae, thereby preventing efficient interaction with target GM1 gangliosides required for uptake of the toxin and activation of cyclic adenosine monophosphate (cAMP) signaling in target epithelia. Herein, we show that after exposure to CT, human enteroids expressing O blood group exhibited marked increase in cAMP relative to cells derived from blood group A individuals. Likewise, using CRISPR/Cas9 engineering, a functional group O line (HT-29-A(-/-)) was generated from a parent group A HT-29 line. CT stimulated robust cAMP responses in HT-29-A(-/-) cells relative to HT-29 cells. These findings provide a direct molecular link between blood group O expression and differential cellular responses to CT, recapitulating clinical and epidemiologic observations.
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