So technically, we don’t have a lot of very insightful studies on sequencing. If you take, for instance, PSMA lutetium, you know that giving it before or after the taxol doesn’t make a big difference. If you look at PSMA Vision and PSMA 4, it’s roughly the same response rate and PSMA 4 tells you you can delay a little bit. For radium-223, what we know is that it shouldn’t be given too late, otherwise it doesn’t work...
So technically, we don’t have a lot of very insightful studies on sequencing. If you take, for instance, PSMA lutetium, you know that giving it before or after the taxol doesn’t make a big difference. If you look at PSMA Vision and PSMA 4, it’s roughly the same response rate and PSMA 4 tells you you can delay a little bit. For radium-223, what we know is that it shouldn’t be given too late, otherwise it doesn’t work. In terms of sequencing, the only certainty we have is that as soon as possible, this patient should be tested for DNA repair and the PARP inhibitor should be fed in as soon as possible, probably even in the metastatic or more naive setting. So that we know. For the rest, you have three drugs, radium, PSMA ligand, two chemotherapies. So the best strategy is the strategy you manage to give everything to everybody so I would recommend giving it very early when the patient has a time to monitor PSMA expression on a regular basis because if your patient has a very high PSMA expression that’s the time to give PSMA therapy and feed in docetaxel early. There was a beautiful trial from Kim Chi, Vancouver, Canada, comparing docetaxel to PSMA lutetium and actually showing that if you start with docetaxel first, you have a benefit in overall survival. So that’s a very strong message in terms of sequencing.
This transcript is AI-generated. While we strive for accuracy, please verify this copy with the video.