[89Zr]Zr-hCD103的研制。[68Ga]Ga-hCD103。Fab01A用于PET成像无创评估癌症反应性T细胞浸润:基于fab的CD103免疫PET

IF 3.1 3区医学 Q1 RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING

EJNMMI Research Pub Date : 2023-11-20 DOI:10.1186/s13550-023-01043-9

Xiaoyu Fan, Marta A Ważyńska, Arjan Kol, Noemi Perujo Holland, Bruna Fernandes, Sander M J van Duijnhoven, Annechien Plat, Hans van Eenennaam, Philip H Elsinga, Hans W Nijman, Marco de Bruyn

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引用次数: 0

摘要

背景:CD103是一种特异性表达于肿瘤反应性T细胞表面的整合素。在成功的免疫治疗过程中，CD103+ T细胞的数量显著增加，因此可能是免疫治疗反应的无创PET成像的一个有吸引力的生物标志物。由于抗体的长半衰期阻碍了在治疗早期对CD103+ T细胞动力学进行重复成像，因此，我们在这里探索了CD103 Fab片段用较长(89Zr)和较短寿命的放射性核素(68Ga)进行放射性标记的PET成像。方法:用89Zr或68Ga对抗人CD103 Fab片段Fab01A进行放射性标记，生成[89Zr]Zr-hCD103。[68Ga]Ga-hCD103。分别Fab01A。在雄性裸鼠(BALB/cOlaHsd-Foxn1nu)中对这些示踪剂进行体内评估，并建立表达cd103的CHO (CHO. cd103)或CHO野生型(CHO. k1)异种移植物，然后进行一系列PET成像和离体生物分布。结果:89年锆Zr-hCD103。早在注射后3小时，Fab01A就在CD103+异种移植物中显示出高的示踪剂摄取。然而，在3小时和6小时的扫描中，背景信号仍然很高。注射后24小时背景相对较低，肿瘤摄取充足。ga [68] Ga-hCD103。fab01cd103 +异种移植物在3小时后显示出可接受的摄取和信噪比，在随后的时间点下降。结论:89年锆Zr-hCD103。早在注射后6小时的扫描中，Fab01A就显示出相对较低的背景和较高的异种移植物摄取，可以在临床试验免疫治疗期间进行重复成像。18F或64Cu可以作为68Ga的替代品，优化示踪剂的半衰期和辐射负荷。

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Development of [⁸⁹Zr]Zr-hCD103.Fab01A and [⁶⁸Ga]Ga-hCD103.Fab01A for PET imaging to noninvasively assess cancer reactive T cell infiltration: Fab-based CD103 immunoPET.

Background: CD103 is an integrin specifically expressed on the surface of cancer-reactive T cells. The number of CD103+ T cells significantly increases during successful immunotherapy and might therefore be an attractive biomarker for noninvasive PET imaging of immunotherapy response. Since the long half-life of antibodies preclude repeat imaging of CD103+ T cell dynamics early in therapy, we therefore here explored PET imaging with CD103 Fab fragments radiolabeled with a longer (⁸⁹Zr) and shorter-lived radionuclide (⁶⁸Ga).

Methods: Antihuman CD103 Fab fragment Fab01A was radiolabeled with ⁸⁹Zr or ⁶⁸Ga, generating [⁸⁹Zr]Zr-hCD103.Fab01A and [⁶⁸Ga]Ga-hCD103.Fab01A, respectively. In vivo evaluation of these tracers was performed in male nude mice (BALB/cOlaHsd-Foxn1nu) with established CD103-expressing CHO (CHO.CD103) or CHO-wildtype (CHO.K1) xenografts, followed by serial PET imaging and ex vivo bio-distribution.

Results: [⁸⁹Zr]Zr-hCD103.Fab01A showed high tracer uptake in CD103+ xenografts as early as 3 h post-injection. However, the background signal remained high in the 3- and 6-h scans. The background was relatively low at 24 h after injection with sufficient tumor uptake. [⁶⁸Ga]Ga-hCD103.Fab01Ashowed acceptable uptake and signal-to-noise ratio in CD103+ xenografts after 3 h, which decreased at subsequent time points.

Conclusion: [⁸⁹Zr]Zr-hCD103.Fab01A demonstrated a relatively low background and high xenograft uptake in scans as early as 6 h post-injection and could be explored for repeat imaging during immunotherapy in clinical trials. ¹⁸F or ⁶⁴Cu could be explored as alternative to ⁶⁸Ga in optimizing half-life and radiation burden of the tracer.

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来源期刊

EJNMMI Research RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING&nb-

CiteScore

5.90

自引率

3.10%

发文量

审稿时长

13 weeks

期刊介绍： EJNMMI Research publishes new basic, translational and clinical research in the field of nuclear medicine and molecular imaging. Regular features include original research articles, rapid communication of preliminary data on innovative research, interesting case reports, editorials, and letters to the editor. Educational articles on basic sciences, fundamental aspects and controversy related to pre-clinical and clinical research or ethical aspects of research are also welcome. Timely reviews provide updates on current applications, issues in imaging research and translational aspects of nuclear medicine and molecular imaging technologies. The main emphasis is placed on the development of targeted imaging with radiopharmaceuticals within the broader context of molecular probes to enhance understanding and characterisation of the complex biological processes underlying disease and to develop, test and guide new treatment modalities, including radionuclide therapy.