(구)글로벌 핫이슈
핵의학
- [Clin Cancer Res.] Bone Marrow Cell Trafficking Analyzed by 89Zr-oxine Positron Emission Tomography in a Murine Transplantation Model.
NIH / Noriko Sato*
- 출처
- Clin Cancer Res.
- 등재일
- 2017 Jun 1
- 저널이슈번호
- 23(11):2759-2768. doi: 10.1158/1078-0432.CCR-16-1561. Epub 2016 Dec 13.
- 내용
Abstract
Purpose:
The success of hematopoietic stem cell transplantation (HSCT) depends on donor cell homing to the bone marrow. However, there is no reliable method of noninvasively monitoring the kinetics and distribution of transferred cells. Using zirconium-89 (89Zr)-oxine cell labeling combined with PET imaging, we sought to visualize and quantify donor cell homing in a mouse bone marrow transplantation model.
Experimental Design:
The effect of 89Zr-oxine labeling on bone marrow cell viability and differentiation was evaluated in vitro89Zr-labeled bone marrow cells (2 × 107 cells, 16.6 kBq/106 cells) were transferred intravenously, and serial microPET images were obtained (n = 5). The effect of a CXCR4 inhibitor, plerixafor (5 mg/kg) and G-CSF (2.5 μg) on bone marrow homing and mobilization were examined (n = 4). Engraftment of the transferred 89Zr-labeled cells was evaluated (n = 3).
Results:
89Zr-oxine-labeled bone marrow cells showed delayed proliferation, but differentiated normally. Transferred bone marrow cells rapidly migrated to the bone marrow, spleen, and liver (n = 5). Approximately 36% of donor cells homed to the bone marrow within 4 hours, irrespective of prior bone marrow ablation. Inhibition of CXCR4 by plerixafor alone or with G-CSF significantly blocked the bone marrow homing (P < 0.0001, vs. nontreated, at 2 hours), confirming a crucial role of the CXCR4-CXCL12 system. Mobilization of approximately 0.64% of pretransplanted bone marrow cells induced a 3.8-fold increase of circulating bone marrow cells. 89Zr-labeled donor cells engrafted as well as nonlabeled cells.
Conclusions:
89Zr-oxine PET imaging reveals rapid bone marrow homing of transferred bone marrow cells without impairment of their stem cell functions, and thus, could provide useful information for optimizing HSCT.
Author information
Asiedu KO1, Koyasu S1, Szajek LP2, Choyke PL1, Sato N3.
1 Molecular Imaging Program, NCI, NIH, Bethesda, Maryland.
2 Positron Emission Tomography Department, Warren Grant Magnuson Clinical Center, NIH, Bethesda, Maryland.
3 Molecular Imaging Program, NCI, NIH, Bethesda, Maryland. saton@mail.nih.gov.
- 덧글달기
- 이전글 [Clin Cancer Res.] Tumor-Specific Uptake of Fluorescent Bevacizumab-IRDye800CW Microdosing in Patients with Primary Breast Cancer: A Phase I Feasibility Study.
- 다음글 [Clin Cancer Res.] 18F-Fluoroestradiol PET/CT Measurement of Estrogen Receptor Suppression during a Phase I Trial of the Novel Estrogen Receptor-Targeted Therapeutic GDC-0810: Using an Imaging Biomarker to Guide Drug Dosage in Subsequent Trials.
- COPYRIGHT(C) 2015 한국원자력의학원 전략기획팀 All rights Reserved.
- 문의 : rmwebzine@kirams.re.kr 발행처 : 한국원자력의학원 전략기획팀
- 우) 01812 서울시 노원구 노원로 75 한국원자력의학원 전략기획팀