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FAM168B identified as a novel candidate target for chimeric antigen receptor T cell-based cancer therapyopen access

Authors
Pramanik, SubrataThaker, ManishaInoue, NorikoKim, Pok-SonKutzner, ArneManavalan, ArulmaniPramanik, GopalHeese, Klaus
Issue Date
Jan-2026
Publisher
SPRINGER
Keywords
Cancer; CAR T cell; FAM168A; FAM168B; pMANI; TCRP1
Citation
DISCOVER ONCOLOGY, v.17, no.1, pp 1 - 19
Pages
19
Indexed
SCIE
SCOPUS
Journal Title
DISCOVER ONCOLOGY
Volume
17
Number
1
Start Page
1
End Page
19
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/211362
DOI
10.1007/s12672-025-03876-3
ISSN
2730-6011
2730-6011
Abstract
Aging-related diseases, particularly cancer, remain major health challenges that demand new therapeutic strategies. Chimeric antigen receptor (CAR) T cell therapy has emerged as a powerful modality in immuno-oncology, enabling patient-derived T cells to be engineered ex vivo to recognize and eliminate tumor antigens. Here, we identify FAM168B (family with sequence similarity 168 member B, also known as myelin-associated neurite-outgrowth inhibitor, MANI) and its homolog FAM168A (tongue cancer resistance-associated protein 1, TCRP1) as candidate membrane-associated proteins expressed on cancer cell surfaces. The unique characteristics of FAM168B suggest its potential as a tumor-specific target for CAR T cell development. This approach could expand the therapeutic repertoire of CAR T cell therapy and support the design of more precise and versatile treatment strategies for diverse cancer types.
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서울 의생명공학전문대학원 > 서울 의생명과학과 > 1. Journal Articles
서울 공과대학 > 서울 정보시스템학과 > 1. Journal Articles

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Heese, Klaus
GRADUATE SCHOOL OF BIOMEDICAL SCIENCE AND ENGINEERING (DEPARTMENT OF BIOMEDICAL SCIENCE)
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