Back

Pembrolizumab, Temozolomide and HSPPC-96 Vaccine in Newly Diagnosed Glioblastoma Post-Chemoradiation: Results from a Multi-institutional, Phase 2, Randomized, Placebo-Controlled Trial

Ozer, B. H.; Lindhorst, S. M.; Merrell, R. T.; Trevino, C. R.; Rudnick, J. D.; Avgeropoulos, N. G.; Ramakrishna, N.; Khagi, S.; Rauf, Y.; Walbert, T.; Pan, E.; Youssef, M.; Fink, K. L.; Mandel, J. J.; Taylor, L. P.; Colman, H.; Dunbar, E. M.; Paleologos, N.; Burton, E. C.; Wu, J.; Leeper, H. E.; Gonzalez, J.; Penas-Prado, M.; Raizer, J. J.; Veglia, E.; Craig, S.; Yuan, Y.; Chambers, C.; Wall, K.; Grajkowska, E.; Mendoza, T.; Armstrong, T. S.; Gilbert, M. R.

2026-06-24 oncology
10.64898/2026.06.22.26354817 medRxiv
Show abstract

Background: GBM is one of the most common and most aggressive brain tumors in adults, and upfront standard of care treatment has limited efficacy. Immune checkpoint inhibitor strategies have significantly improved outcomes in various solid tumors but have not proven effective in GBM, suggesting other strategies may be needed to realize their full potential. Methods: GBM patients were treated with upfront standard of care chemoradiation with temozolomide and pembrolizumab, followed by adjuvant temozolomide and pembrolizumab for six nine-week cycles. Depending on production of sufficient vaccine, patients were randomized into HSPPC-96 vaccine or placebo group (q4 weeks) while those with failed vaccine production continued on study unblinded as an ancillary group. The primary objective was overall survival at one year, and secondary endpoints were progression-free survival at six months, overall and progression-free survival, radiographic response, and tolerability by patient-reported outcomes and adverse event documentation. Results: 90 patients were screened, 32 were treated (8 vaccine, 9 placebo, 15 ancillary), and 26 were evaluable for radiographic responses prior to accrual termination. The study did not meet its primary endpoint of overall survival at one year (65.5% in vaccine group, 75% in placebo). Progression-free endpoints were mildly improved in the vaccine group but were not significant, and response rates were not significantly different. The regimen was well-tolerated and safe. Conclusions: Though limited by early discontinuation, these findings do not support the combination of pembrolizumab and HSPPC-96 vaccine with standard of care therapy. Trials Registration: ClinicalTrials.gov identifier: NCT03018288

Matching journals

The top 8 journals account for 50% of the predicted probability mass.

1
Neuro-Oncology
36 papers in training set
Top 0.1%
11.9%
2
Clinical Cancer Research
64 papers in training set
Top 0.2%
7.3%
3
Journal of Neuro-Oncology
10 papers in training set
Top 0.1%
6.8%
4
JAMA Network Open
130 papers in training set
Top 0.4%
6.3%
5
Neuro-Oncology Advances
25 papers in training set
Top 0.1%
6.3%
6
PLOS ONE
5266 papers in training set
Top 28%
5.5%
7
Journal of the Neurological Sciences
18 papers in training set
Top 0.1%
5.5%
8
JCO Precision Oncology
14 papers in training set
Top 0.1%
4.9%
50% of probability mass above
9
International Journal of Radiation Oncology*Biology*Physics
25 papers in training set
Top 0.2%
4.3%
10
BMC Cancer
67 papers in training set
Top 0.7%
3.1%
11
Frontiers in Oncology
103 papers in training set
Top 1%
2.5%
12
Cancer Medicine
26 papers in training set
Top 0.4%
2.1%
13
BMJ Open
601 papers in training set
Top 9%
1.9%
14
Journal for ImmunoTherapy of Cancer
75 papers in training set
Top 1%
1.9%
15
Brain and Behavior
43 papers in training set
Top 0.6%
1.7%
16
The Lancet Regional Health - Americas
22 papers in training set
Top 0.3%
1.7%
17
Cancer Cell
42 papers in training set
Top 1.0%
1.1%
18
Clinical and Translational Radiation Oncology
10 papers in training set
Top 0.2%
1.1%
19
FEBS Open Bio
31 papers in training set
Top 0.5%
1.1%
20
eClinicalMedicine
77 papers in training set
Top 2%
1.0%
21
Scientific Reports
3612 papers in training set
Top 71%
1.0%
22
Journal of Clinical Investigation
179 papers in training set
Top 5%
1.0%
23
Nature Communications
5641 papers in training set
Top 55%
0.9%
24
Oncotarget
18 papers in training set
Top 0.5%
0.8%
25
Pharmacological Research
18 papers in training set
Top 0.5%
0.8%
26
PLOS Medicine
110 papers in training set
Top 3%
0.8%
27
British Journal of Cancer
49 papers in training set
Top 2%
0.8%
28
JCI Insight
277 papers in training set
Top 7%
0.8%
29
BMJ Health & Care Informatics
15 papers in training set
Top 1%
0.6%