상세 보기
- Kwon, Kee Woong;
- Kang, Tae Gun;
- Lee, Jii Bum;
- Choi, Eunsol;
- Kim, Hagyu;
- 외 8명
WEB OF SCIENCE
3SCOPUS
3초록
Cancers are a risk factor for active tuberculosis (TB), and anti-cancer drugs can independently cause TB progression. To understand the underlying mechanisms, mice infected with Mycobacterium tuberculosis (Mtb) were treated with gemcitabine (Gem), cisplatin, or paclitaxel. These treatments delay Mtb-specific T cell responses, increase bacterial loads, and cause hyperinflammation with permissive neutrophils in the lungs. However, depleting Mtb-permissive neutrophils reduce bacterial levels and G-CSF production, thereby attenuating lung immunopathology. Additionally, Mtb-specific T cell responses generated by BCG vaccination inhibit bacterial growth and neutrophil infiltration even after Gem treatment. Gem induces granulocyte-biased generation in the bone marrow via G-CSF signaling, which led to lung neutrophil inflammation. However, pre-existing Mtb-specific T cell responses from BCG vaccination normalizes granulopoiesis by restricting G-CSF production. These findings show the mechanism of anti-cancer drug-induced neutrophilic lung inflammation in TB and highlight the role of Mtb-specific T cell responses in maintaining balanced hematopoiesis against Gem-induced TB immunopathogenesis.
키워드
- 제목
- Mycobacterium tuberculosis-specific T cells restrain anti-cancer drug-induced neutrophilic lung inflammation in tuberculosis
- 저자
- Kwon, Kee Woong; Kang, Tae Gun; Lee, Jii Bum; Choi, Eunsol; Kim, Hagyu; Park, Min Chul; Choi, Sangwon; Kim, Kyungmin; Kim, Hyeong Woo; Jeong, Su Jin; Kim, Hye Ryun; Shin, Sung Jae; Ha, Sang-Jun
- 발행일
- 2025-10
- 유형
- Article
- 권
- 16
- 호
- 1