Détail du document
Identifiant

oai:pubmedcentral.nih.gov:9738...

Sujet
Article
Auteur
Omland, Silje Haukali Ejlertsen, Jacob Secher Krustrup, Dorrit Christensen, Rikke Louise Svane, Inge Marie Olesen, Uffe Hoegh Hædersdal, Merete
Langue
en
Editeur

MDPI

Catégorie

Cancers

Année

2022

Date de référencement

13/01/2023

Mots clés
non-aggressive basal ablative fractional laser injection local safety broaden ratio immune keratinocyte monotherapy study tumor response afl anti-pd1 carcinoma cell
Métrique

Résumé

SIMPLE SUMMARY: The use of immune checkpoint inhibitors (ICI) is expanding with the approval for locally advanced and metastasizing keratinocyte carcinoma.

Most cases, however, are non-aggressive.

Systemic therapy remains limited by severe side effects.

Local administration could broaden ICI, but an adequate immune response might require an immune-attractive adjuvant such as ablative fractional laser (AFL).

Accordingly, aiming to broaden the field of ICI to keratinocyte carcinoma, this study investigates the intratumoral injection of anti-PD1 with and without AFL in basal cell carcinoma (BCC), exploring anti-PD1 concentration, immune cell infiltration, tumor response, and safety.

With the results of the study showing the feasibility of intratumoral anti-PD1 and increase in immune cell infiltration and tumor reduction upon combined anti-PD1 and AFL, local, hence broader, application of anti-PD1 holds potential for future treatment of non-aggressive keratinocyte carcinomas.

ABSTRACT: The use of immune checkpoint inhibitors (ICI) is expanding with the approval for advanced/metastatic keratinocyte carcinoma; however, most tumors are non-aggressive.

Local administration could broaden ICI, but adequate immune response might require an immune-attractive adjuvant such as ablative fractional laser (AFL).

Accordingly, this study aimed to explore intratumoral injection of anti-PD1 with and without AFL in basal cell carcinoma (BCC), exploring anti-PD1 concentration, immune cell infiltration, tumor response, and safety.

This open-label, proof-of-concept trial investigated intratumoral anti-PD1 + AFL combination therapy versus anti-PD1 or AFL monotherapy in 28 BCC patients.

The primary endpoints were immune cell infiltration evaluated immunohistochemically and clinical tumor response after 3 months.

The secondary outcomes were tumoral drug concentration and safety.

The most robust response was obtained following intervention with combined anti-PD1+AFL, leading to a ~2.5-fold increase in CD3+ cells (p = 0.027), and tumor reduction ≥25% in 73%, including two tumors with complete remission.

Upon anti-PD1 monotherapy, a slight decrease in CD3+ cells was observed while a non-significant increase following AFL was seen.

Tumor reduction ≥25% was seen in 45% and 50%, respectively, after anti-PD1 and AFL monotherapy.

The CD8/CD3 ratio remained unchanged after anti-PD1+AFL and anti-PD1 monotherapy, while AFL led to a decreased ratio.

A non-significant decline in the Foxp3/CD3 ratio was observed for all groups.

Side-effects were mild with no systemic drug concentration detected.

Intratumoral anti-PD1 injection is feasible, and a single exposure to locally injected anti-PD1 with adjuvant AFL increased immune cell infiltration and reduction in BCC with limited side-effects.

Omland, Silje Haukali,Ejlertsen, Jacob Secher,Krustrup, Dorrit,Christensen, Rikke Louise,Svane, Inge Marie,Olesen, Uffe Hoegh,Hædersdal, Merete, 2022, Feasibility of Intratumoral Anti-PD1 as Treatment of Human Basal Cell Carcinoma: An Explorative Study with Adjuvant Ablative Fractional Laser, MDPI

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