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Clinical Trial
. 2016 May 15;22(10):2342-50.
doi: 10.1158/1078-0432.CCR-15-2594. Epub 2016 Jan 26.

Vaccination against Oncoproteins of HPV16 for Noninvasive Vulvar/Vaginal Lesions: Lesion Clearance Is Related to the Strength of the T-Cell Response

Mariëtte I E van Poelgeest  1 Marij J P Welters  2 Renee Vermeij  3 Linda F M Stynenbosch  2 Nikki M Loof  2 Dorien M A Berends-van der Meer  1 Margriet J G Löwik  1 Ineke L E Hamming  3 Edith M G van Esch  1 Bart W J Hellebrekers  4 Marc van Beurden  5 Henk W Schreuder  6 Marjolein J Kagie  7 J Baptist M Z Trimbos  1 Lorraine M Fathers  8 Toos Daemen  9 Harry Hollema  10 A Rob P M Valentijn  8 Jaap Oostendorp  8 J Hanneke N G Oude Elberink  11 Gertjan J Fleuren  12 Tjalling Bosse  12 Gemma G Kenter  13 Theo Stijnen  14 Hans W Nijman  3 Cornelis J M Melief  15 Sjoerd H van der Burg  16
Affiliations
Clinical Trial

Vaccination against Oncoproteins of HPV16 for Noninvasive Vulvar/Vaginal Lesions: Lesion Clearance Is Related to the Strength of the T-Cell Response

Mariëtte I E van Poelgeest et al. Clin Cancer Res. .

Abstract

Purpose: Therapeutic vaccination with human papillomavirus type 16 (HPV16) E6 and E7 synthetic long peptides (SLP) is effective against HPV16-induced high-grade vulvar and vaginal intraepithelial neoplasia (VIN/VaIN). However, clinical nonresponders displayed weak CD8(+) T-cell reactivity. Here, we studied if imiquimod applied at the vaccine site could improve CD8(+) T-cell reactivity, clinical efficacy, and safety of HPV16-SLP (ISA101).

Experimental design: A multicenter open-label, randomized controlled trial was conducted in patients with HPV16(+) high-grade VIN/VaIN. Patients received ISA101 vaccination with or without application of 5% imiquimod at the vaccine site. The primary objective was the induction of a directly ex vivo detectable HPV16-specific CD8(+) T-cell response. The secondary objectives were clinical responses (lesion size, histology, and virology) and their relation with the strength of vaccination-induced immune responses.

Results: Forty-three patients were assigned to either ISA101 with imiquimod (n = 21) or ISA101 only (n = 22). Imiquimod did not improve the outcomes of vaccination. However, vaccine-induced clinical responses were observed in 18 of 34 (53%; 95% CI, 35.1-70.2) patients at 3 months and in 15 of 29 (52%; 95% CI, 32.5-70.6) patients, 8 of whom displayed a complete histologic response, at 12 months after the last vaccination. All patients displayed vaccine-induced T-cell responses, which were significantly stronger in patients with complete responses. Importantly, viral clearance occurred in all but one of the patients with complete histologic clearance.

Conclusions: This new study confirms that clinical efficacy of ISA101 vaccination is related to the strength of vaccine-induced HPV16-specific T-cell immunity and is an effective therapy for HPV16-induced high-grade VIN/VaIN. Clin Cancer Res; 22(10); 2342-50. ©2016 AACRSee related commentary by Karaki et al., p. 2317.

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