CCL17:一種具有多生物學功能的趨化因子
日期:2025-06-09 09:38:02
1. CCL17概述
CCL17(也稱為TARC)是一種屬于CC亞家族的趨化因子,主要參與免疫細胞的遷移、激活和炎癥反應的調節。它由樹突狀細胞、內皮細胞、角質形成細胞和成纖維細胞等產生,并在胸腺中高表達,對T細胞的發育、遷移和成熟T細胞的激活起重要作用。CCL22和CCL17同屬于CC型趨化因子家族,二者具有高度同源性,具有共同的受體分子CCR4,都可以有效趨化CCR4表達陽性的細胞。
Figure 1. CCL17二聚體結構,來源于PDB:1NR4。球體部分為G7T突變位置,綠色部分為二硫鍵位置。
來源:DOI: 10.1016/j.bbrep.2017.11.005
2. CCL17與疾病的關聯
2.1 心血管疾病
CCL17在心血管疾病中起著關鍵作用,尤其是在年齡相關和血管緊張素II (Ang II)誘導的病理性心臟重塑和心力衰竭中。研究發現,隨著年齡的增長,血清中CCL17水平顯著增加,并與心臟功能障礙相關。在動物實驗中,CCL17基因敲除小鼠顯示出對年齡和Ang II誘導的心臟肥大和纖維化的抑制作用,并伴隨著T細胞亞群的可塑性和分化 [1]。此外,使用抗CCL17中和抗體的治療也顯著抑制了Ang II誘導的病理性心臟重塑 [2]。這些發現揭示了CCL17作為一種新的治療靶點的潛力,可用于年齡相關和Ang II誘導的病理性心臟肥大和心力衰竭。
2.2 炎癥與自身免疫性疾病
趨化因子受體CCR4是CCL17的高親和力受體,CCL17在炎癥中的作用主要體現在其通過與CCR4結合,參與調控炎癥反應和炎癥性疼痛。在炎癥模型中,CCL17能夠促進炎癥性T細胞的趨化和激活,尤其是在Th2型免疫反應中 [3]。在骨關節炎模型中,CCL17基因敲除小鼠顯示出對疼痛和疾病發展的抵抗性,表明CCL17在炎癥性疼痛的發病機制中起著關鍵作用 [4]。此外,在炎癥性關節炎和腸道炎癥模型中,CCL17的缺乏也能夠減輕疾病癥狀,進一步支持了CCL17在炎癥中的重要作用 [5][6]。
在自身免疫疾病中,CCL17同樣扮演著重要角色 [3]。在系統性紅斑狼瘡(SLE)中,CCL17的表達也有所增加,提示其可能參與SLE的免疫病理過程 [7][8]。此外,在多發性硬化癥(MS)的動物模型實驗性自身免疫性腦脊髓炎(EAE)中,CCL17基因敲除小鼠顯示出減輕的疾病癥狀 [9]。這些研究結果表明,CCL17在自身免疫疾病的發病機制中具有重要作用,并可能成為治療這些疾病的新靶點。
CCL17在過敏性哮喘中發揮著關鍵作用,它由樹突狀細胞(DCs)產生,能吸引Th2細胞到氣道,引發過敏性哮喘的炎癥反應。NOD1刺激的樹突狀細胞在體內能加重Th2肺部反應,且這種作用以CCL17依賴性方式發生 [10]。通過人源化SCID小鼠模型的研究發現,阻斷CCR4(CCL17的受體)能顯著減少氣道炎癥和支氣管高反應性,表明CCR4-CCL17軸在Th2細胞招募到氣道中起到關鍵作用 [11]。這些研究結果都暗示了CCL17可能是一個潛在的治療過敏性哮喘的靶點。
2.3 腫瘤及腫瘤微環境
CCL17在多種腫瘤細胞中高表達,能促進腫瘤細胞增殖、遷移和侵襲。在肝細胞癌中,與M2型巨噬細胞共培養或用CCL17處理,可增強腫瘤細胞的這些惡性生物學行為,還能提升細胞干性,促進腫瘤球形成,并上調腫瘤干細胞相關轉錄因子表達,助力腫瘤復發和轉移 [12]。此外,CCL17通過激活TGF-β1/Smad和Wnt/β-catenin信號通路,影響上皮-間質轉化過程,進一步加強腫瘤細胞的侵襲和轉移能力 [13]。
CCL17與多種免疫細胞浸潤相關。在胃癌和甲狀腺癌中,其高表達與Foxp3+調節性T細胞聚集有關,可能抑制抗腫瘤免疫 [13][14]。同時,CCR4-CCL17信號軸選擇性招募Th2細胞、Tregs、記憶T細胞至炎癥或腫瘤微環境,通過JAK/STAT6、PI3K/AKT通路激活免疫抑制程序。
3. 相關信號通路研究
| 信號通路/分子 | 作用描述 | 相關疾病/細胞類型 | 參考文獻 |
|---|---|---|---|
| CCL17/CCR4 | 促進腫瘤細胞遷移、侵襲、干性維持,調控免疫細胞遷移 | 多種腫瘤、干細胞 | 12, 15, 16, 17, 18 |
| ERK/PD-L1 | CCL17通過CCR4激活ERK/PD-L1信號,增強腫瘤細胞惡性行為 | 食管鱗癌 | 15 |
| mTORC1/mTORC2 | 乳酸誘導M2極化,M2分泌CCL17,CCL17/CCR4激活mTORC1促進腫瘤侵襲 | 垂體腺瘤 | 16, 19 |
| Wnt/β-catenin、TGF-β1 | CCL17促進腫瘤細胞EMT及干性,激活Wnt/β-catenin和TGF-β1信號 | 肝細胞癌 | 12 |
| STAT6/IRF4/JMJD3 | IL-4誘導CCL17表達依賴STAT6-IRF4-JMJD3通路,涉及表觀遺傳調控 | 單核細胞/巨噬細胞 | 7 |
| β-arrestin | CCL17激活CCR4主要招募β-arrestin而非G蛋白,提示其可能作為清道夫受體 | T細胞 | 20 |
4. 臨床意義與應用前景
4.1 生物標志物與預后預測
CCL17/CCL22高表達可預測頭頸鱗癌患者的免疫檢查點抑制劑療效及生存率 [19],在鼻型NK/T細胞淋巴瘤、肝癌等疾病中也有潛在的診斷和預后價值 [12][18]。
4.2 靶向治療潛力
抗CCR4單抗可介導NK細胞殺傷腫瘤細胞,CCL17/CCR4軸成為多種腫瘤的新型靶向治療候選 [18][21]。
5. 相關產品推薦
華美生物提供CCL17相關高質量重組蛋白和抗體,旨在幫助科研工作者進行CCL17作用機制與臨床轉化方向的研究:
● CCL17重組蛋白
Recombinant Human C-C motif chemokine 17 (CCL17) (Active); CSB-MP856406HU
Recombinant Macaca mulatta C-C motif chemokine 17 (CCL17) (Active); CSB-MP811562MOW
Recombinant Mouse C-C motif chemokine 17 (Ccl17) (Active); CSB-MP6512MO
● CCL17重組抗體
CCL17 Recombinant Monoclonal Antibody; CSB-RA856406MA1HU
Activity: Measured by its binding ability in a functional ELISA. Immobilized Anti-CCL17 recombinant antibody at 2 μg/mL can bind Human CCL17 protein (CSB-MP856406HU). The EC50 is 2.403-2.741 ng/mL.
● CCL17(TRAC) ELISA試劑盒
參考文獻:
[1] Zhang, Y., Ye, Y., Tang, X., Wang, H., Tanaka, T., Tian, R., Yang, X., Wang, L., Xiao, Y., Hu, X., Jin, Y., Pang, H., Du, T., Liu, H., Sun, L., Xiao, S., Dong, R., Ferrucci, L., Tian, Z., & Zhang, S. (2022). CCL17 acts as a novel therapeutic target in pathological cardiac hypertrophy and heart failure. The Journal of Experimental Medicine, 219(8).
[2] Zhang, Y., Tang, X., Wang, Z., Wang, L., Chen, Z., Qian, J. Y., Tian, Z., & Zhang, S. Y. (2023). The chemokine CCL17 is a novel therapeutic target for cardiovascular aging. Signal transduction and targeted therapy, 8(1), 157.
[3] Lupancu, T.J., Eivazitork, M., Hamilton, J.A., Achuthan, A.A. and Lee, K.M.-C. (2023), CCL17/TARC in autoimmunity and inflammation—not just a T-cell chemokine. Immunol Cell Biol, 101: 600-609.
[4] Lee, M.-C., Saleh, R., Achuthan, A., Fleetwood, A. J., F?rster, I., Hamilton, J. A., & Cook, A. D. (2018). CCL17 blockade as a therapy for osteoarthritis pain and disease. Arthritis Research & Therapy, 20(1), 62.
[5] Heiseke, A. F., Faul, A. C., Lehr, H., F?rster, I., Schmid, R. M., Krug, A. B., & Reindl, W. (2011). CCL17 Promotes Intestinal Inflammation in Mice and Counteracts Regulatory T Cell–Mediated Protection From Colitis. Gastroenterology, 142(2), 335–345.
[6] Achuthan, A., Cook, A. D., Kevin M.-C. Lee, Saleh, R., Hsu Wei Khiew, Melody Wei-Ning Chang, Louis, C., Fleetwood, A. J., Lacey, D., Anne Deen Christensen, Frye, A. T., Pui Yeng Lam, Kusano, H., Nomura, K., Steiner, N., F?rster, I., Nutt, S. L., Olshansky, M., Turner, S. J., & Hamilton, J. A. (2016). Granulocyte macrophage colony-stimulating factor induces CCL17 production via IRF4 to mediate inflammation. Journal of Clinical Investigation, 126(9), 3453–3466.
[7] Hsu, A. T., Lupancu, T. J., Lee, M.-C., Fleetwood, A. J., Cook, A. D., Hamilton, J. A., & Achuthan, A. (2018). Epigenetic and transcriptional regulation of IL4-induced CCL17 production in human monocytes and murine macrophages. Journal of Biological Chemistry, 293(29), 11415–11423.
[8] T R D J Radstake. (2004). Increased expression of CCL18, CCL19, and CCL17 by dendritic cells from patients with rheumatoid arthritis, and regulation by Fc gamma receptors. Annals of the Rheumatic Diseases, 64(3), 359–367.
[9] Dhaiban, S., Al-Ani, M., Elemam, N. M., & Maghazachi, A. A. (2020). Targeting Chemokines and Chemokine Receptors in Multiple Sclerosis and Experimental Autoimmune Encephalomyelitis. Journal of Inflammation Research, Volume 13, 619–633.
[10] Yahia, S. A., Imane Azzaoui, Laetitia Everaere, Vorng, H., Cécile Chenivesse, Philippe Marquillies, Duez, C., Delacre, M., Grandjean, T., Balsamelli, J., d’Andon, M. F., Fan, Y., Coline Ple, Werts, C., Ivo Gomperts Boneca, Wallaert, B., Mathias Chamaillard, & Tsicopoulos, A. (2014). CCL17 Production by Dendritic Cells Is Required for NOD1-mediated Exacerbation of Allergic Asthma. American Journal of Respiratory and Critical Care Medicine, 189(8), 899–908.
[11] Perros, F., Hoogsteden, H. C., Coyle, A. J., Lambrecht, B. N., & Hammad, H. (2009). Blockade of CCR4 in a humanized model of asthma reveals a critical role for DC-derived CCL17 and CCL22 in attracting Th2 cells and inducing airway inflammation. Allergy, 64(7), 995–1002.
[12] Zhu, F., Li, X., Chen, S., Zeng, Q., Zhao, Y., & Luo, F. (2016). Tumor-associated macrophage or chemokine ligand CCL17 positively regulates the tumorigenesis of hepatocellular carcinoma. Medical Oncology, 33(2).
[13] Mizukami, Y., Kono, K., Kawaguchi, Y., Akaike, H., Kamimura, K., Sugai, H., & Fujii, H. (2008). CCL17 and CCL22 chemokines within tumor microenvironment are related to accumulation of Foxp3+ regulatory T cells in gastric cancer. International Journal of Cancer, 122(10), 2286–2293.
[14] Gu, X., Chen, B., Zhang, S., Zhai, X., Hu, Y., & Ye, H. (2024). The expression of CCL17 and potential prognostic value on tumor immunity in thyroid carcinoma based on bioinformatics analysis. Scientific Reports, 14(1).
[15] Jin, C., Lu, L., Gao, J., & Chen, L. (2024). M2-like Macrophages-derived CCL17 Promotes Esophageal Squamous Cell Carcinoma Metastasis and Stemness via Activating CCR4-mediated ERK/PD-L1 Pathway.. Current molecular medicine.
[16] Zhang, A., Xu, Y., Xu, H., Ren, J., Meng, T., Ni, Y., Zhu, Q., Zhang, W., Pan, Y., Jin, J., Bi, Y., Wu, Z., Lin, S., & Lou, M. (2021). Lactate-induced M2 polarization of tumor-associated macrophages promotes the invasion of pituitary adenoma by secreting CCL17. Theranostics, 11, 3839 - 3852.
[17] Konno, K., Sasaki, T., Kulkeaw, K., & Sugiyama, D. (2020). Paracrine CCL17 and CCL22 signaling regulates hematopoietic stem/progenitor cell migration and retention in mouse fetal liver.. Biochemical and biophysical research communications.
[18] Kumai, T., Nagato, T., Kobayashi, H., Komabayashi, Y., Ueda, S., Kishibe, K., Ohkuri, T., Takahara, M., Celis, E., & Harabuchi, Y. (2015). CCL17 and CCL22/CCR4 signaling is a strong candidate for novel targeted therapy against nasal natural killer/T-cell lymphoma. Cancer Immunology, Immunotherapy, 64, 697-705.
[19] Zhou, W., Zhang, X., Feng, Y., Zhang, Y., & Liu, Z. (2022). The CC ligand chemokine family members CCL17/CCL22 predict the survival and response to immune checkpoint blockade therapy of patients with head and neck squamous cell carcinoma.. Current problems in cancer, 46 6, 100896 .
[20] Lim, H., Lane, J., Canals, M., & Stone, M. (2021). Systematic Assessment of Chemokine Signaling at Chemokine Receptors CCR4, CCR7 and CCR10. International Journal of Molecular Sciences, 22.
[21] Goenka, A., Khan, F., Verma, B., Sinha, P., Dmello, C., Jogalekar, M., Gangadaran, P., & Ahn, B. (2023). Tumor microenvironment signaling and therapeutics in cancer progression. Cancer Communications, 43, 525 - 561.
