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| Czech study Results on using uPSA to determine when to use radiation after Radical Prostatectomy |
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| Radiation Decision pints |
definitions of some commonly used terms and abbreviations:
- Aggressive pathology means that the post-op pathology report indicates that cancer was found in one or more of the following places:
- Outside of the prostate capsule (pathological stage T3a), or
- In the seminal vesicles (pathological stage T3b), or
- Locally, but at a distance from the prostate (pathological stage T4), or
- At the surgical margin, where the surgeon has cut through the cancer — a “positive surgical margin” (PSM).
- Adjuvant radiation therapy (aRT) start right away.
- Salvage radiation therapy (sRT) start after BCR.
- Early salvage radiation therapy (early sRT) after aRT, but before sRT .
- Wait-and-see .
- Biochemical recurrence (BCR) post-surgery is now defined as a confirmed PSA ≥ 0.2 ng/ml. .
- An ultrasensitive PSA (uPSA) test is any PSA test that can reliably detect PSAs below 0.1 ng/ml. While the definition of biochemical recurrence has not been changed, detectable levels of PSA are now as low as 0.001 ng/ml on some commercially available ultrasensitive tests.
Ultrasensitive PSA reliably predicts eventual biochemical recurrence (a UCLA study)
Kang et al. found that a uPSA ≥ 0.03 ng/ml was the optimal threshold value for predicting biochemical recurrence (BCR). Other findings included:- uPSA ≥ 0.03 ng/ml was the most important and reliable predictor of BCR. It predicted all relapses (no false negatives: no one was under-treated), and hardly ever predicted relapses incorrectly. Only 2 percent would be over-treated by waiting for this cut-off.
- It was especially prognostic if found on the first uPSA test after surgery.
- Even if the first uPSA test was undetectable, any subsequent test where uPSA ≥ 0.03 ng/ml predicted BCR.
- Other lesser predictors of recurrence were pathologic Gleason grade, pathologic T stage, initial PSA before surgery, and surgical margin status.
- At 5 years of follow-up, 46 percent of patients had a BCR using the “standard” PSA ≥ 0.2 definition, 76 percent using the PSA ≥ 0.03 definition.
- Treating when an ultrasensitive PSA level reached 0.03 ng/ml gave a median lead time advantage of 18 months over waiting until PSA reached 0.2 ng/ml.
- It was necessary to monitor PSA for at least 5 years post-op, and to test at least every 6 months.
Ultrasensitive PSA can reliably predict eventual biochemical recurrence at 2 months after surgery (a Czech study)
A Czech study (Vesely et al.) looked at a group of 116 patients who had PSMs after surgery. Unlike the UCLA study, staging was not a selection criterion. The two studies’ goals were somewhat different. While the UCLA study didn’t start uPSA testing until 3 months after prostatectomy, in this study uPSA testing was begun at 2 weeks post-surgery. Most urologists wait for 3 months because surgery sheds a lot of PSA into the serum, and it takes a while for that excess to clear out. The goal in this study was to find out just how early in time after prostatectomy they could detect a uPSA prognostic for BCR, whereas the UCLA study sought to find out how late in uPSA progression they could detect a PSA prognostic for progression. The Czech cohort had the following characteristics:- Only patients with PSMs were included
- Patients who received aRT or hormone therapy were excluded
- Pathological stage T3/T4 in 54 percent of patients
- Gleason score ≥ 7 in 51 percent of patients
- Initial, pre-surgical PSA ≥ 9.2 in 50 percent of patients
- Time to first post-op PSA, 14 days
Vesely et al. found that the uPSA on day 30 had predictive accuracy of 74 percent for recurrence, and reached a maximum of 84 percent by day 60, when the uPSA was 0.04 ng/ml (increases in accuracy afterwards were not statistically significant). The following table summarizes their findings:
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