A novel approach using C. elegans DNA damage-induced apoptosis to characterize the dynamics of uptake transporters for therapeutic drug discoveries

Abstract: Organic cation transporter (OCT) function is critical for cellular homeostasis. C. elegans lacking OCT-1 displays a shortened lifespan and increased susceptibility to oxidative stress. We show that these phenotypes can be rescued by downregulating the OCT-1 paralogue, OCT-2. Herein, we delineate a biochemical pathway in C. elegans where uptake of genotoxic chemotherapeutics such as doxorubicin and cisplatin, and subsequent DNA damage-induced apoptosis of germ cells, are dependent exclusively upon OCT-2. We cha… Show more

“…We used the gst::gfp reporter animals to monitor oxidative stress caused by toxic compounds and showed that these animals expressed a basal level of GST-4::GFP in the intestine. However, the expression level of the GST-4::GFP was greatly stimulated following RNAi downregulation of oct-1 that led to the upregulation of oct-2 [33]. Consistent with this observation, downregulation of the oct-2 transporter gene by RNAi lowered the basal levels of GST-4::GFP expression in the reporter strain [33].…”

“…First, unlike the oct-1 null animals, downregulation of oct-2 did not affect the lifespan of the animals. Second, perhaps most interesting, the depletion of OCT-2 rescued the shortened lifespan of animals already deleted for the oct-1 gene [33]. This striking observation prompted the possibility that OCT-1 might influence OCT-2 function, whereby oct-1 downregulation leads to oct-2 upregulation.…”

“…This notion is based on the fact that OCT1 knockout mice manifest upregulation of two related transporter genes, OCT2 and OCT3 [34]. And third, quantitative PCR analysis indeed revealed that downregulation of oct-1 led to the upregulation of oct-2 expression in several tissues of the animals, while several control genes, such as act-1 encoding actin, were unaffected [33]. As such, we proposed that OCT-2 upregulation could be responsible for triggering uptake of toxic environmental compounds into the animals and thus account for the shortened lifespan displayed by the oct-1 animals.…”

“…However, the existence of another related member of the organic cation transporter family, namely OCT-2, in C. elegans, suggests that there needs to be a strategy to test the contribution of each transporter towards doxorubicin uptake. Prior to our work, there was no function assigned to this putative transporter OCT-2 [33]. Moreover, there are no animals in the consortiums, USA or Japan, carrying either partial or complete deletion of the oct-2 gene, as in the case of oct-1.…”

“…Moreover, there are no animals in the consortiums, USA or Japan, carrying either partial or complete deletion of the oct-2 gene, as in the case of oct-1. Thus, to examine whether OCT-1 or OCT-2 or both have roles in the uptake of doxorubicin in C. elegans, we used RNA-interference (RNAi) feeding bacteria to generate animals with different genotypes, in particular, either downregulated for one or both transporters [33].…”

The tales of two organic cation transporters, OCT-1 and OCT-2, in C. elegans

“…We used the gst::gfp reporter animals to monitor oxidative stress caused by toxic compounds and showed that these animals expressed a basal level of GST-4::GFP in the intestine. However, the expression level of the GST-4::GFP was greatly stimulated following RNAi downregulation of oct-1 that led to the upregulation of oct-2 [33]. Consistent with this observation, downregulation of the oct-2 transporter gene by RNAi lowered the basal levels of GST-4::GFP expression in the reporter strain [33].…”

“…First, unlike the oct-1 null animals, downregulation of oct-2 did not affect the lifespan of the animals. Second, perhaps most interesting, the depletion of OCT-2 rescued the shortened lifespan of animals already deleted for the oct-1 gene [33]. This striking observation prompted the possibility that OCT-1 might influence OCT-2 function, whereby oct-1 downregulation leads to oct-2 upregulation.…”

“…This notion is based on the fact that OCT1 knockout mice manifest upregulation of two related transporter genes, OCT2 and OCT3 [34]. And third, quantitative PCR analysis indeed revealed that downregulation of oct-1 led to the upregulation of oct-2 expression in several tissues of the animals, while several control genes, such as act-1 encoding actin, were unaffected [33]. As such, we proposed that OCT-2 upregulation could be responsible for triggering uptake of toxic environmental compounds into the animals and thus account for the shortened lifespan displayed by the oct-1 animals.…”

“…However, the existence of another related member of the organic cation transporter family, namely OCT-2, in C. elegans, suggests that there needs to be a strategy to test the contribution of each transporter towards doxorubicin uptake. Prior to our work, there was no function assigned to this putative transporter OCT-2 [33]. Moreover, there are no animals in the consortiums, USA or Japan, carrying either partial or complete deletion of the oct-2 gene, as in the case of oct-1.…”

“…Moreover, there are no animals in the consortiums, USA or Japan, carrying either partial or complete deletion of the oct-2 gene, as in the case of oct-1. Thus, to examine whether OCT-1 or OCT-2 or both have roles in the uptake of doxorubicin in C. elegans, we used RNA-interference (RNAi) feeding bacteria to generate animals with different genotypes, in particular, either downregulated for one or both transporters [33].…”

The tales of two organic cation transporters, OCT-1 and OCT-2, in C. elegans

Potent anticancer activity of a novel iridium metallodrug via oncosis

Molecular basis for stereoselective transport of fenoterol by the organic cation transporters 1 and 2