Wednesday, September 9, 2020

Adding ADT to external beam radiation only benefits unfavorable risk patients

In 2013, Zumsteg et al. proposed a refinement in the NCCN "intermediate risk" classification into two subcategories, "favorable intermediate-risk (FIR)" and "unfavorable intermediate-risk (UIR)." Based on retrospective studies with short follow-up, they discerned that the two subgroups had divergent prognoses when treated with external beam radiation and adjuvant androgen deprivation therapy (ADT). Since then, others have found that it is also a useful division for deciding whether brachy boost therapy is beneficial (see this link), or whether it is beneficial to add ADT to brachytherapy (see this link). Some FIR patients may be suitable candidates for active surveillance.

It has also been found to be a useful division in terms of prognosis following surgery, brachytherapy, and SBRT (see this link). Some clinical trials use the definition to distinguish  "favorable risk" (low risk or FIR) from "unfavorable risk" (UIR or high risk).  Since 2016, NCCN has incorporated the distinction in its risk stratification system.

The NCCN definitions are as follows:

The NCCN intermediate-risk group is currently defined as having any of the following:
- Stage T2b or T2c, or
- PSA 10- 20 ng/ml, or
- Gleason score = 7 
(If multiple risk factors are present, the clinician may optionally deem it high risk)

Unfavorable Intermediate Risk (UIR):
- NCCN intermediate risk, as defined above, plus
- Predominant Gleason grade 4 (i.e., Gleason score 4+3), or
- Percentage of positive biopsy cores≥ 50%, or
- Multiple NCCN intermediate risk factors

Favorable Intermediate Risk (FIR):
- NCCN intermediate risk, as defined above, but only those with
- Predominant Gleason grade 3 (i.e., Gleason score 3+4 or 3+3), and
- Percentage of positive biopsy cores <50%, and
- No more than one NCCN intermediate risk factor

Now, it has been found to be a useful distinction in an unplanned secondary analysis of a randomized clinical trial, with 17.8 years of median follow-up. Such a long follow-up is unusual for a clinical trial and gives us the ability to see significant numbers of mortality and metastases even in intermediate-risk patients. The trial, RTOG 9408, was originally conducted among 1,068 intermediate-risk patients who received 66.6 Gy to the prostate (low by today's standards) and 46.8 Gy to the pelvic lymphatics. Half the patients received 4 months of adjuvant ADT, and half received none. They lacked biopsy core information on 16%, who are excluded from their analysis. Zumsteg et al. found that adding 4 months of ADT:

  • more than doubled 15-year metastasis-free survival and prostate cancer-specific survival among UIR patients. Mean overall survival was 0.7 years longer with ADT.
  • had no statistically significant effect on 15-year metastasis-free survival, prostate cancer-specific survival, or overall survival among FIR patients
  • it took about 6 years for the differences to start to be noticeable.

Given all the retrospective studies we've seen before that all point to FIR vs UIR as a useful and significant distinction, this is not surprising. It did take a lot of work to review pathology reports on almost a thousand patients, and the authors are to be commended for doing so. If it spares some FIR men from being overtreated, it was a worthwhile effort.

Tuesday, August 11, 2020

PSMA-targeted radiopharmaceutical clinical trials in the US

(frequently updated)

Now that the VISION trial of Lu-177-PSMA-617 is no longer recruiting, some patients are wondering if they can still get PSMA-targeted radiopharmaceuticals in the US, without traveling to Germany, Australia, India, etc. Here is a list of trials that are active, still open to recruitment, or will soon be recruiting. 

Unless otherwise noted, they are all for men who are: 

  • metastatic
  • castration-resistant 
  • have had at least one taxane chemotherapy
  • at least one of the advanced androgen receptor therapies (e.g., Zytiga, Xtandi, Erleada, or Nubeqa)
  • no Xofigo
  • PSMA-avid on a PSMA PET/CT scan

Radiopharmaceutical

Adjuvant drugs

Extra criteria

Recruitment status/ contact

Locations

Lu-177-PSMA-617 

LuCarbo

Carboplatin


Not yet recruiting

Dana-Farber, Boston


Lu-rhPSMA-10.1


•Recurrent postRP

•regionally positive on PSMA PET

recruiting

Emory,  Atlanta

Lu-177-JH20002


•Advanced PCa

recruiting

•California

•Florida

•Michigan

Lu-177-PSMA-617

PSMACare

1. ADT

2.ARSi+ADT (ARSi=Zytiga, Xtandi,Erleada or Nubeqa)

•Metastatic with PSMA PET, but not with conventional imaging

•CRPC

•No prior ARSi or chemo

recruiting

TBD

Lu-177-PNT2002

LUNAR

Before SBRT

Recurrent and oligometastatic

recruiting

UCLA

Ac-225-J591

ACTION

SBRT,

ADT if polymetastatic

Recurrent

# mets 

recruiting

Weill Cornell

Lu-177-rhPSMA-10.1


±previous chemo

recruiting 

•Maryland

•St.Louis

•Omaha

•Mt Sinai-NYC

Lu-177-PSMA-I&T


Chemo naïve, failed one hormonal

recruiting

• 56 locations

Ac-225-PSMA-I&T

TATCIST



Recruiting

• Houston

Ac-225-J591

 

 

recruiting

• Weill Cornell

• Brooklyn Methodist

Pluvicto+ONC392 (a CTL4 blocking immunotherapy)



recruiting

• NYU Langone

• Columbia


Ac-225-J591 + Lu-177-PSMA- I&T

 

 

recruiting

• Weill Cornell

• Brooklyn Methodist

Ac-225-J591

Keytruda

No chemo since castration resistant

recruiting

• Weill Cornell

• Brooklyn Methodist

• Dana Farber

• Columbia

Cu-67-SAR-bisPSMA

SECuRE

 

Previous chemo OK, not required

recruiting

• Johns Hopkins

•Mayo Rochester

•Mayo, AZ

•Tulane, N.O.

•Barnes Jewish, St. Louis

•Omaha, NE

•Weill Cornell

Lu-177-PSMA-617

PSMAddition


mHSPC

(M1 or N1)

Treatment naive

Recruiting

• 174  sites

Lu-177-PSMA-617

Keytruda

No chemo since castration resistant

active, not recruiting

UCSF

Lu-177-CTT1403

 

No Jevtana

active, not recruiting

UCSF

Lu-177-PSMA-617

 

 

Active, not recruiting

•Weill Cornell

•Tulane

Th-227-Antibody

(see article)

 

 

active, not recruiting

• Royal Marsden (UK)

• Finland

• Tulane

• MSK

• Omaha, NE

Lu-177-J591

Ketoconazole

Prior RP or RT

CRPC

Non-metastatic

active, not recruiting

• Weill Cornell

• USC

• Georgetown

• IU

• U of Iowa

• UPMC

Lu-177-PSMA-R2

 

 

Active, not recruiting

• Stanford

• Yale

• Tulane

• Johns Hopkins

• Mt Sinai

• MD Anderson

• U of Wisconsin

• Phoenix

Lu-177-PSMA-617

PSMAfore

 

Chemo and immunotherapy naïve, failed one hormonal

Active, not recruiting

(Phase 3 RCT)

• 72  sites

Lu-177-PSMA-617

(VISION)

 

 

Active, not recruiting

• 84 locations

Results expected August 2020

I-131-1095-MIPS

(see article)

Xtandi

Chemo naïve

Failed Zytiga

Active, not recruiting

• 17 locations

Results expected December 2021