Multimodal and Multiscale Analysis Reveals Distinct Vascular, Metabolic and Inflammatory Components of the Tissue Response to Limb Ischemia

Tamar Kapanadze Jens P. Bankstahl; Alexander Wittneben; Wolfgang Koestner; Matthias Ballmaier; Jaba Gamrekelashvili; Kashyap Krishnasamy; Anne Limbourg; Tobias L. Ross; Geerd-Jürgen Meyer; Hermann Haller; Frank M. Bengel; Florian P. Limbourg

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Multimodal and Multiscale Analysis Reveals Distinct Vascular, Metabolic and Inflammatory Components of the Tissue Response to Limb Ischemia

机译：多模式和多尺度分析揭示了肢体缺血组织反应的不同血管，代谢和炎性成分

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Ischemia triggers a complex tissue response involving vascular, metabolic and inflammatory changes. Methods: We combined hybrid SPECT/CT or PET/CT nuclear imaging studies of perfusion, metabolism and inflammation with multicolor flow cytometry-based cell population analysis to comprehensively analyze the ischemic tissue response and to elucidate the cellular substrate of noninvasive molecular imaging techniques in a mouse model of hind limb ischemia. Results: Comparative analysis of tissue perfusion with [sup99m/supTc]-Sestamibi and arterial influx with [sup99m/supTc]-labeled albumin microspheres by SPECT/CT revealed a distinct pattern of response to vascular occlusion: an early ischemic period of matched suppression of tissue perfusion and arterial influx, a subacute ischemic period of normalized arterial influx but impaired tissue perfusion, and a protracted post-ischemic period of hyperdynamic arterial and normalized tissue perfusion, indicating coordination of macrovascular and microvascular responses. In addition, the subacute period showed increased glucose uptake by [sup18/supF]-FDG PET/CT scanning as the metabolic response of viable tissue to hypoperfusion. This was associated with robust macrophage infiltration by flow cytometry, and glucose uptake studies identified macrophages as major contributors to glucose utilization in ischemic tissue. Furthermore, imaging with the TSPO ligand [sup18/supF]-GE180 showed a peaked response during the subacute phase due to preferential labeling of monocytes and macrophages, while imaging with [sup68/supGa]-RGD, an integrin ligand, showed prolonged post-ischemic upregulation, which was attributed to labeling of macrophages and endothelial cells by flow cytometry. Conclusion: Combined nuclear imaging and cell population analysis reveals distinct components of the ischemic tissue response and associated cell subsets, which could be targeted for therapeutic interventions.

机译：缺血引发复杂的组织反应，涉及血管，代谢和炎症变化。方法：我们将基于SPECT / CT或PET / CT混合核磁共振成像的灌注，代谢和炎症研究与基于多色流式细胞仪的细胞群体分析相结合，以全面分析缺血性组织反应并阐明无创分子成像技术的细胞底物。后肢缺血的小鼠模型。结果：通过SPECT / CT对[ 99m Tc]-司他他比的组织灌流和[ 99m Tc]标记的白蛋白微球的动脉灌注进行比较分析，发现了明显的应答模式到血管闭塞：相匹配的组织灌注和动脉血流抑制的早期缺血期，归一化动脉血流的亚急性缺血期，但组织灌注受损，高动力动脉和归一化组织血流的缺血后长期期，表明大血管的协调和微血管反应。此外，[ 18 F] -FDG PET / CT扫描显示亚急性期葡萄糖摄取增加，这是活组织对灌注不足的代谢反应。这与流式细胞仪检测到的巨噬细胞浸润有关，葡萄糖摄取研究发现巨噬细胞是缺血组织中葡萄糖利用的主要贡献者。此外，由于单核细胞和巨噬细胞的优先标记，使用TSPO配体[ 18 F] -GE180进行的成像在亚急性阶段反应达到峰值，而使用[ 68 Ga ] -RGD，一种整合素配体，显示出缺血后的上调时间延长，这归因于通过流式细胞术标记巨噬细胞和内皮细胞。结论：核成像和细胞群体分析相结合，揭示了缺血性组织反应和相关细胞亚群的不同组成部分，可将其用于治疗干预。

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《Theranostics》 |2019年第1期|共15页
作者
Tamar Kapanadze Jens P. Bankstahl; Alexander Wittneben; Wolfgang Koestner; Matthias Ballmaier; Jaba Gamrekelashvili; Kashyap Krishnasamy; Anne Limbourg; Tobias L. Ross; Geerd-Jürgen Meyer; Hermann Haller; Frank M. Bengel; Florian P. Limbourg;
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中图分类医药、卫生;
关键词
ischemiavascularmetabolicinflammatory;

机译：缺血性血管代谢性炎症;

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1. Society for Vascular Surgery Wound, Ischemia, foot Infection (WIfI) score correlates with the intensity of multimodal limb treatment and patient-centered outcomes in patients with threatened limbs managed in a limb preservation center [J] . Robinson William P., Loretz Lorraine, Hanesian Colleen, Journal of vascular surgery . 2017,第2期

机译：血管外科伤口的社会，缺血，脚部感染（WiFi）得分与肢体保存中心管理威胁肢体患者的多模式肢体治疗和患者中心结果的强度相关
2. The Society for Vascular Surgery Wound, Ischemia, and foot Infection (WIfI) Score Correlates With the Intensity of Multimodal Limb Treatment and Patient-Centered Outcomes in Patients With Threatened Limbs Managed in a Limb Preservation Center [J] . Robinson William P., Loretz Lorraine, Hanesian Colleen, Journal of vascular surgery . 2016,第4期

机译：肢体保存中心管理的肢体受威胁肢体患者的多模式肢体治疗强度和以患者为中心的结果与血管外科手术学会伤口，缺血和足部感染（WIfI）评分相关
3. DISTINCT EXPRESSION PROFILE AND HISTOLOGICAL DISTRIBUTION OF NLRP3 INFLAMMASOME COMPONENTS IN THE TISSUES OF HAINAN BLACK GOAT SUGGEST A SITE-SPECIFIC ROLE IN THE INFLAMMATORY RESPONSE [J] . Zhang Kaizhao, Tao Pan, Liu Jianxin, Acta Veterinaria Hungarica . 2017,第3期

机译：海南黑山羊组织中NLRP3炎症组分的明显表达谱和组织学分布表明炎症反应中的特异性作用
4. Probabilistic independent component analysis for laser speckle contrast images reveals in vivo multi - component vascular responses to forepaw stimulation [C] . Li Nan, Pelled Galit, Thakor Nitish V. 32nd Annual International Conference of the IEEE Engineering in Medicine and Biology Society . 2010

机译：激光散斑对比图像的概率独立成分分析揭示了对前爪刺激的体内多成分血管反应
5. An ex vivo femoral artery model to demonstrate inflammatory response and monocyte response following increased vascular wall shear stress. [D] . Baldwin, Aparna Kadam. 2013

机译：一个离体的股动脉模型表现出炎症反应和单核细胞反应后增加血管壁剪切应力。
6. Multimodal and Multiscale Analysis Reveals Distinct Vascular Metabolic and Inflammatory Components of the Tissue Response to Limb Ischemia [O] . Tamar Kapanadze, Jens P. Bankstahl, Alexander Wittneben, 2019

机译：多峰和多尺度分析揭示了组织对肢体缺血的不同血管代谢和炎性成分
7. Multimodal and Multiscale Analysis Reveals Distinct Vascular, Metabolic and Inflammatory Components of the Tissue Response to Limb Ischemia [O] . Tamar Kapanadze, Jens P. Bankstahl, Alexander Wittneben, 2019

机译：多模式和多尺度分析显示出对肢体缺血的组织反应的不同血管，代谢和炎症组分

Multimodal and Multiscale Analysis Reveals Distinct Vascular, Metabolic and Inflammatory Components of the Tissue Response to Limb Ischemia

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