Hiring in life sciences? Share your open positions with our professional community. Read more Close

Your cookie settings

This site uses cookies. Some cookies are essential to make the site work and others help us to improve our services. Read more about cookies in our Privacy policy.

Choose your cookie preferences:

Advertisement

Short-term manufacturing of IL-7/CCL19-expressing CAR-T cells enhances and prolongs therapeutic effects in solid tumor models.

Created on 15 Jun 2026

Authors

Kohei Sakai, Yukimi Sakoda, Keishi Adachi, Yasuharu Ohta, Koji Tamada

Published in

Molecular cancer therapeutics. Jun 15, 2026. Epub Jun 15, 2026.

Abstract

CAR-T cell therapy has achieved remarkable success in the treatment of certain blood cancers, but its efficacy against solid tumors remains limited. One of the key strategies is the improvement of manufacturing methods for the rapid production of high-functioning CAR-T cells. We have improved the manufacturing method for CAR-T cells simultaneously expressing IL-7 and CCL19 (referred to as 7×19 CAR-T cells), armored CAR-T cells which we developed for treating solid tumors. We generated 7×19 CAR-T cells using a short-term culture method without expansion phase (referred to as Swift 7×19 CAR-T cells), then compared them with regular culture methods (referred to as Standard 7×19 CAR-T cells). Swift CAR-T cells are distinguished by a high frequency of early memory phenotypes, including stem cell memory and central memory T cells, which showed superior effector functions over Standard CAR-T cells. In a stress test in which effector cells are repeatedly stimulated by target-positive tumor cells, Swift 7×19 CAR-T cells and Swift conventional CAR-T cells initially exhibited similar antitumor effects. However, after repetitive stimulations, only Swift 7×19 CAR-T cells maintained a robust response. Furthermore, Swift 7×19 CAR-T cells demonstrated in vivo antitumor activity by substantially fewer cells compared to Standard 7×19 CAR-T cells, and conferred a long-term resistance to tumor rechallenge without autonomous proliferation indicative of malignant transformation. These results highlight the potential of the innovative "Swift" short-term culture methods combined with 7×19 CAR-T technology to provide a new treatment option for refractory solid tumors.

PMID:
42295209
Bibliographic data and abstract were imported from PubMed on 15 Jun 2026.

Read full publication at:
Please sign in to see all details.

Advertisement

Stats

  • Community rating n/a 0 votes
  • Reviewers' rating n/a 0 votes
  • Sign in to post a review. Add review
  • Your rating

1-terrible, 9-excellent. How would you rate this publication? Sign in in to submit your rating.

  • Recommendations n/a n/a positive of 0 vote(s)
  • Views 3
  • Comments 0

Recommended by

  • No recommendations yet.

Do you recommend this? Please sign in. Yes No

Recommended

Post a comment

You need to be signed in to post comments. You can sign in here.

Comments

There are no comments yet.

Advertisement