Inducible Programming of CAR T Cell Intrinsic Properties for Cancer Immunotherapy

Code

J3-3084 (D) - included in ARIS records

Head

PhD Anže Smole

Period

10/1/2021 - 9/30/2024

Range in 2023

0.41 FTE

Science

Medical sciences (8)
Biotechnical sciences (4)
Other (1)

Reseacher status

Researcher (12)
Junior expert or technical associate (1)

Education

Doctor's degree (12)
Other (1)

Sex

Woman (10)
Man (3)

Status

Employed at RO and RRD (12)
No data on employment in RO (1)

No. of publications

10–99 (9)
100–999 (3)
1,000–9,999 (1)

Projects / Programmes source: ARIS

source: ARIS

Inducible Programming of CAR T Cell Intrinsic Properties for Cancer Immunotherapy

Research activity

Code	Science	Field	Subfield
3.04.00	Medical sciences	Oncology

Code	Science	Field
3.02	Medical and Health Sciences	Clinical medicine

Keywords

Cancer, Immunotherapy, Cell therapy, CAR T cells, Chimeric Antigen Receptors, Transcription factor, Inducible expression, Lentiviral vectors, Gene-engineered immune cells, CRISPR/Cas9, CD19, Xenograft and Syngeneic mouse models, Hematologic Malignancies, CAR T cell dysfunction persistence expansion.

Evaluation (rules)

source: COBISS

Evaluation of bibliographic research performance indicators according to ARIS methodology

Points

4,356.93

A''

430.89

A'

1,940.72

A1/2

2,580.55

CI10

9,376

CImax

450

h10

47

A1

13.73

A3

8.55

Data for the last 5 years (citations for the last 10 years) on April 19, 2024; A3 for period 2018-2022

Data for ARIS tenders ( 04.04.2019 – Programme tender, archive )

Citations Citations for bibliographic records in COBIB.SI that are linked to records in citation databases

source: WoS

source: Scopus

source: COBISS

Database	Linked records	Citations	Pure citations	Average pure citations
WoS	513	14,198	10,586	20.64
Scopus	523	16,540	12,524	23.95

Researchers (13)

no.	Code	Name and surname	Research area	Role	Period	No. of publicationsNo. of publications
1.	51848	PhD Tim Božič	Medical sciences	Researcher	2022 - 2023	52
2.	37380	PhD Karen Butina Ogorelec	Microbiology and immunology	Researcher	2021	34
3.	14575	PhD Maja Čemažar	Oncology	Researcher	2021 - 2024	1,425
4.	05236	PhD Vladka Čurin Šerbec	Microbiology and immunology	Researcher	2021 - 2024	261
5.	10412	PhD Simon Horvat	Biotechnical sciences	Researcher	2021 - 2024	561
6.	36366	PhD Špela Kos	Medical sciences	Researcher	2021 - 2022	81
7.	35344	PhD Valerija Kovač	Medical sciences	Researcher	2021 - 2024	20
8.	36367	PhD Urša Lampreht Tratar	Oncology	Researcher	2021 - 2024	125
9.	39112	PhD Katja Leben	Biotechnology	Researcher	2023 - 2024	13
10.	32113	PhD Jelka Pohar	Biotechnology	Researcher	2022 - 2024	97
11.	38858	Katja Skulj		Technical associate	2021 - 2024	14
12.	33201	PhD Anže Smole	Biotechnology	Head	2021 - 2024	74
13.	37534	PhD Katarina Žnidar	Medical sciences	Researcher	2021 - 2024	69

Organisations (4)

no.	Code	Research organisation	City	Registration number	No. of publicationsNo. of publications
1.	0105	National Institute of Biology	Ljubljana	5055784	13,256
2.	0302	Institute of Oncology Ljubljana	Ljubljana	5055733000	15,455
3.	0311	Blood Transfusion Centre of Slovenia	Ljubljana	5053960	1,737
4.	0481	University of Ljubljana, Biotechnical Faculty	Ljubljana	1626914	66,295

Abstract

Chimeric Antigen Receptor (CAR) T cell therapy is clinically approved advanced cancer immunotherapy approach with genetically engineered autologous (patient’s own) T cells. Although CAR T cell immunotherapy is a paradigm-shifting approach to treat cancer, the therapy is not always successful as evident from non-responding or relapsed disease. CAR T cell therapy is limited in solid tumors and in hematologic malignancies that induce dysfunctional T cell phenotypes and differentiation states. Additionally, dysfunctional T cells prevent successful manufacturing of CAR T cells in a substantial number of patients seeking CD19 CAR therapy. Genetic integration of relevant accessory molecules into CAR T cells is a promising approach to improve T cell functions and therapy outcomes. However, there remain both knowledge and translational gaps in (i) understanding which accessory molecules will provide optimal therapeutic efficacy when overexpressed in CAR T cells and (ii) how to genetically integrate them into CAR T cells in a clinically feasible manner. My proposal aims to address these issues to improve CAR T cells targeting CD19+ hematologic malignancies by (i) integrating the key transcription factor (TFs) that we identified through our preliminary studies as important candidates to improve T cell intrinsic properties and (ii) genetically integrate them into CAR T cells in an inducible manner (iTF-CAR T cells). In Objective 1, we will utilize a novel genetic platform called Uni-Vect that I developed at the University of Pennsylvania (UPenn). Uni-Vect will enable transient expression of TFs in CAR T cells, while we will also test the constitutive expression of the same TFs (cTF-CAR T cells). We will create CD19 targeting CAR T cells upgraded with ectopic expression of two key transcription factors and their variants to generate CAR T cell products with fitness profiles associated with a capacity to expand, persist and mediate cancer regression after infusion. i/cTF-CAR T cell approach will be further optimized for clinical translation with the use of a single step CRISPR/Cas9-mediated targeted gene integration approach that will simultaneously improve the safety and manufacturing of i/cTF-CAR T cells. In Objective 2 we will develop and validate comprehensive in vitro systems to evaluate and compare functional and phenotypic properties of i/cTF-CAR T cells. Utilizing advanced immunological methods including deep profiling of i/cTF-CAR T cells with RNA sequencing we will examine mechanisms leading to augmented fitness. Finally, we will investigate whether i/cTF-CAR T cells can improve activity against primary chronic lymphocytic leukemia (CLL) cells from patients treated with CART19 at UPenn and whether they can improve “expansion failure” T cells. Objective 3 is designed to test i/cTF-CAR T cell products in both xenograft and syngeneic preclinical mouse models. We will determine the impact of ectopic expression of variants of TFs on CAR T cell expansion, persistence, and anti-tumor activity in vivo. Then we will perform a comprehensive analysis of CAR T cells isolated from mice and examine CAR T cell phenotype, gene expression profiles and function to gain a better understanding of which key factors contribute to improved intrinsic properties. This will inform further developments of i/cTF-CAR T cell approaches. Together, the project aims at developing i/cTF-CAR T cells genetically equipped for improved expansion, persistence, and anti-tumor activity, and improving clinical CAR T cell manufacturing. Finally, we will investigate mechanisms by which TFs may improve CAR T cells and with this new understanding of CAR T cell biology, we will establish a foundation for the development of more effective cellular immunotherapies.