Indoxyl sulfate is one of the numerous uremic toxins. Since 90% of indoxyl sulfate in the serum is bound to albumin, it is difficult for chronic kidney disease (CKD) patients to excrete it in urine. The difficulty is due to the deteriorated glomerular filtration rate in kidney of CKD patients. Accumulation of high concentration of indoxyl sulfate has not only been found to accelerate the progression of CKD, but also found to affect other organs via circulation system. For example, it has been suggested that 40-50% of death in end stage CKD patients are related cardiovascular diseases. However, despite the conspicuous awareness of this phenomenon, current knowledge on the correlation between CKD and CVD is still limited. Therefore, in order to elucidate the underlying effects of indoxyl sulfate on cardiomyocytes, this study was designed to investigate the molecular change of gap junction under indoxyl sulfate treatment. No cell death has been observed after indoxyl sulfate treatment, implying indoxyl sulfate does not affect cardiomyocyte survival. In addition, indoxyl sulfate induced reduction in total connexin43 level and the effects are reversible. Gap junction intercellular communication (GJIC) of cardiomyocyte was assessed with scrape loading and was found with reduced communication. Immunofluorescence staining showed the expression pattern and morphology of Cx43 was altered in indoxyl sulfate treated cardiomyocytes, which appeared to correlate with reduced Cx43 protein and mRNA expression. Inhibition of PKC alpha and JNK blocked indoxyl sulfate -induced down-regulation of Cx43 protein and mRNA expression. Furthermore, PKC alpha inhibition prevented the indoxyl sulfate induced JNK activation. Thus, the down regulation of Cx43 protein induced by indoxyl sulfate was mediated by the PKC alpha-JNK signaling cascade. The present study provides, for the first time, the effects of indoxyl sulfate on gap junction connexin43 in neonatal rat cardiomyocytes.