1.Aneurysmal Bone Cyst:CT and MRI Diagnosis:A Report of 21 Cases
Renqi MOU ; Xiaofeng TANG ; Chentao ZHOU ; Xulin LIU ; Yongzhong XU ; Dianjing SUN
Journal of Practical Radiology 1992;0(11):-
Objective To analyze CT and MRI manifestations of the aneurysmal bone cyst and to evaluate the value of its imaging diagnosis.Methods The manifestations of CT and MRI of the aneurysmal bone cyst confirmed by operation or puncture were analysed retrospectively.Results On CT images,there were obvious liqued-liqued level within the lesions in 16 cases,in which,the CT values in up part was lower than that in low part,and there were obvious soft tissue mass in secondary aneurysmal bone cyst.While,on MRI,all lesions appeared obvious liqued-liqued level except one secondary example,and the soft tissue mass of secondary aneurysmal bone cyst was clear showed.Conclusion Most of aneurysmal bone cyst appear liqued-liqued level within the lesions on CT and MRI,it is a characteristic sign,but not the only one.
2.The radionuclide imaging and therapy for metastatic prostate cancer
Xuexin HE ; Jinyun ZHOU ; Haoran LI ; Chentao JIN ; Mei TIAN
Chinese Journal of Urology 2021;42(10):792-796
Metastatic prostate cancer is one of the most malignancies and do harm to the health and life expectancy of men. The popularization and application of 68Gallium or 18Fluorine labeled prostate-specific membrane antigen (PSMA) positron emission tomography/computed tomography (PET/CT) benefit for the excellent diagnostic efficacy, unique value in the diagnosis of metastatic prostate cancer, clinical decision-making guidance, efficacy in monitoring and prognosis evaluation. 223Radium and 177Lu-PSMA radioligand therapy (RLT) could effectively alleviate bone pain, and prolong the overall survival time (OS) as wellas progression-free survival time (PFS) with good safety. In addition, survival of patients with metastatic prostate cancer is expected to be further improved with the advance in the combination therapies with PSMA RLT, androgen-deprivation therapy (ADT), chemotherapy, targeted therapy and immunotherapy.
3. Structural, Functional, and Molecular Imaging of Autism Spectrum Disorder
Xiaoyi LI ; Xiao HE ; Jinyun ZHOU ; Chentao JIN ; Yuanxue GAO ; Mei TIAN ; Hong ZHANG ; Xiaoyi LI ; Xiao HE ; Jinyun ZHOU ; Chentao JIN ; Yuanxue GAO ; Mei TIAN ; Hong ZHANG ; Hong ZHANG ; Kai ZHANG ; Lesang SHEN ; Xiaoyi LI ; Xiao HE ; Jinyun ZHOU ; Chentao JIN ; Yuanxue GAO ; Mei TIAN ; Hong ZHANG ; Hong ZHANG
Neuroscience Bulletin 2021;37(7):1051-1071
Autism spectrum disorder (ASD) is a heterogeneous neurodevelopmental disorder associated with both genetic and environmental risks. Neuroimaging approaches have been widely employed to parse the neurophysiological mechanisms underlying ASD, and provide critical insights into the anatomical, functional, and neurochemical changes. We reviewed recent advances in neuroimaging studies that focused on ASD by using magnetic resonance imaging (MRI), positron emission tomography (PET), or single-positron emission tomography (SPECT). Longitudinal structural MRI has delineated an abnormal developmental trajectory of ASD that is associated with cascading neurobiological processes, and functional MRI has pointed to disrupted functional neural networks. Meanwhile, PET and SPECT imaging have revealed that metabolic and neurotransmitter abnormalities may contribute to shaping the aberrant neural circuits of ASD. Future large-scale, multi-center, multimodal investigations are essential to elucidate the neurophysiological underpinnings of ASD, and facilitate the development of novel diagnostic biomarkers and better-targeted therapy.
4.PET imaging on neurofunctional changes after optogenetic stimulation in a rat model of panic disorder.
Xiao HE ; Chentao JIN ; Mindi MA ; Rui ZHOU ; Shuang WU ; Haoying HUANG ; Yuting LI ; Qiaozhen CHEN ; Mingrong ZHANG ; Hong ZHANG ; Mei TIAN
Frontiers of Medicine 2019;13(5):602-609
Panic disorder (PD) is an acute paroxysmal anxiety disorder with poorly understood pathophysiology. The dorsal periaqueductal gray (dPAG) is involved in the genesis of PD. However, the downstream neurofunctional changes of the dPAG during panic attacks have yet to be evaluated in vivo. In this study, optogenetic stimulation to the dPAG was performed to induce panic-like behaviors, and in vivo positron emission tomography (PET) imaging with F-flurodeoxyglucose (F-FDG) was conducted to evaluate neurofunctional changes before and after the optogenetic stimulation. Compared with the baseline, post-optogenetic stimulation PET imaging demonstrated that the glucose metabolism significantly increased (P < 0.001) in dPAG, the cuneiform nucleus, the cerebellar lobule, the cingulate cortex, the alveus of the hippocampus, the primary visual cortex, the septohypothalamic nucleus, and the retrosplenial granular cortex but significantly decreased (P < 0.001) in the basal ganglia, the frontal cortex, the forceps minor corpus callosum, the primary somatosensory cortex, the primary motor cortex, the secondary visual cortex, and the dorsal lateral geniculate nucleus. Taken together, these data indicated that in vivo PET imaging can successfully detect downstream neurofunctional changes involved in the panic attacks after optogenetic stimulation to the dPAG.
5.Quantitative proteomics revealed extensive microenvironmental changes after stem cell transplantation in ischemic stroke.
Yao CHEN ; Fahuan SONG ; Mengjiao TU ; Shuang WU ; Xiao HE ; Hao LIU ; Caiyun XU ; Kai ZHANG ; Yuankai ZHU ; Rui ZHOU ; Chentao JIN ; Ping WANG ; Hong ZHANG ; Mei TIAN
Frontiers of Medicine 2022;16(3):429-441
The local microenvironment is essential to stem cell-based therapy for ischemic stroke, and spatiotemporal changes of the microenvironment in the pathological process provide vital clues for understanding the therapeutic mechanisms. However, relevant studies on microenvironmental changes were mainly confined in the acute phase of stroke, and long-term changes remain unclear. This study aimed to investigate the microenvironmental changes in the subacute and chronic phases of ischemic stroke after stem cell transplantation. Herein, induced pluripotent stem cells (iPSCs) and neural stem cells (NSCs) were transplanted into the ischemic brain established by middle cerebral artery occlusion surgery. Positron emission tomography imaging and neurological tests were applied to evaluate the metabolic and neurofunctional alterations of rats transplanted with stem cells. Quantitative proteomics was employed to investigate the protein expression profiles in iPSCs-transplanted brain in the subacute and chronic phases of stroke. Compared with NSCs-transplanted rats, significantly increased glucose metabolism and neurofunctional scores were observed in iPSCs-transplanted rats. Subsequent proteomic data of iPSCs-transplanted rats identified a total of 39 differentially expressed proteins in the subacute and chronic phases, which are involved in various ischemic stroke-related biological processes, including neuronal survival, axonal remodeling, antioxidative stress, and mitochondrial function restoration. Taken together, our study indicated that iPSCs have a positive therapeutic effect in ischemic stroke and emphasized the wide-ranging microenvironmental changes in the subacute and chronic phases.
Animals
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Cell Differentiation
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Disease Models, Animal
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Ischemic Stroke
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Proteomics
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Rats
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Stem Cell Transplantation/methods*
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Stroke/therapy*