11 results on '"Jian-ping, Xiang"'
Search Results
2. Classification and hemodynamic characteristics of delayed intracerebral hemorrhage following stent-assisted coil embolism in unruptured intracranial aneurysms
- Author
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Zeng-Bao Wu, Xue-Yan Wan, Ming-Hui Zhou, Yan-Chao Liu, Ali Abdi Maalim, Zhuang-Zhuang Miao, Xiao Guo, Ying Zeng, Pu Liao, Li-Ping Gao, Jian-Ping Xiang, Hua-Qiu Zhang, Kai Shu, Ting Lei, and Ming-Xin Zhu
- Subjects
delayed intracerebral hemorrhage ,hemodynamics ,stent-assisted coil embolization ,intracranial aneurysms ,endovascular treatment ,Neurology. Diseases of the nervous system ,RC346-429 - Abstract
Background and objectiveStent-assisted coil (SAC) embolization is a commonly used endovascular treatment for unruptured intracranial aneurysms (UIAs) but can be associated with symptomatic delayed intracerebral hemorrhage (DICH). Our study aimed to investigate the hemodynamic risk factors contributing to DICH following SAC embolization and to establish a classification for DICH predicated on hemodynamic profiles.MethodsThis retrospective study included patients with UIAs located in the internal carotid artery (ICA) treated with SAC embolization at our institution from January 2021 to January 2022. We focused on eight patients who developed postoperative DICH and matched them with sixteen control patients without DICH. Using computational fluid dynamics, we evaluated the hemodynamic changes in distal arteries [terminal ICA, the anterior cerebral artery (ACA), and middle cerebral artery (MCA)] pre-and post-embolization. We distinguished DICH-related arteries from unrelated ones (ACA or MCA) and compared their hemodynamic alterations. An imbalance index, quantifying the differential in flow velocity changes between ACA and MCA post-embolization, was employed to gauge the flow distribution in distal arteries was used to assess distal arterial flow distribution.ResultsWe identified two types of DICH based on postoperative flow alterations. In type 1, there was a significant lower in the mean velocity increase rate of the DICH-related artery compared to the unrelated artery (−47.25 ± 3.88% vs. 42.85 ± 3.03%; p
- Published
- 2024
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3. Virtual simulation with AneuShape™ software for microcatheter shaping in intracranial aneurysm coiling: a validation study
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Zeng-Bao Wu, Ying Zeng, Hua-Qiu Zhang, Kai Shu, Gao-Hui Li, Jian-Ping Xiang, Ting Lei, and Ming-Xin Zhu
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virtual simulation ,microcatheter shaping ,cerebral aneurysm ,coil embolization ,treatment outcome ,Neurology. Diseases of the nervous system ,RC346-429 - Abstract
BackgroundThe shaping of an accurate and stable microcatheter plays a vital role in the successful embolization of intracranial aneurysms. Our study aimed to investigate the application and the role of AneuShape™ software in microcatheter shaping for intracranial aneurysm embolization.MethodsFrom January 2021 to June 2022, 105 patients with single unruptured intracranial aneurysms were retrospectively analyzed with or without AneuShape™ software to assist in microcatheter shaping. The rates of microcatheter accessibility, accurate positioning, and stability for shaping were analyzed. During the operation, fluoroscopy duration, radiation dose, immediate postoperative angiography, and procedure-related complications were evaluated.ResultsCompared to the manual group, aneurysm-coiling procedures involving the AneuShape™ software exhibited superior results. The use of the software resulted in a lower rate of reshaping microcatheters (21.82 vs. 44.00%, p = 0.015) and higher rates of accessibility (81.82 vs. 58.00%, p = 0.008), better positioning (85.45 vs. 64.00%, p = 0.011), and higher stability (83.64 vs. 62.00%, p = 0.012). The software group also required more coils for both small (
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- 2023
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4. Microstructure Analysis and Reconstruction of a Meniscus
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Shuang Zhu, Ge Tong, Jian‐ping Xiang, Shuai Qiu, Zhi Yao, Xiang Zhou, and Li‐jun Lin
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3D printing ,Freeze‐drying ,Meniscus ,Micro‐CT ,Micro‐MRI ,Orthopedic surgery ,RD701-811 - Abstract
Objective To analyze the characteristics of menicus microstructure and to reconstruct a microstructure‐mimicing 3D model of the menicus. Methods Human and sheep meniscus were collected and prepared for this study. Hematoxylin–eosin staining (HE) and Masson staining were conducted for histological analysis of the meniscus. For submicroscopic structure analysis, the meniscus was first freeze‐dried and then scanned by scanning electron microscopy (SEM). The porosity of the meniscus was determined according to SEM images. A micro‐MRI was used to scan each meniscus, immersed in distilled water, and a 3D digital model was reconstructed afterwards. A three‐dimensional (3D) resin model was printed out based on the digital model. Before high‐resolution micro‐CT scanning, each meniscus was freeze‐dried. Then, micro‐scale two‐dimensional (2D) CT projection images were obtained. The porosity of the meniscus was calculated according to micro‐CT images. With micro‐CT, multiple 2D projection images were collected. A 3D digital model based on 2D CT pictures was also reconstructed. The 3D digital model was exported as STL format. A 3D resin model was printed by 3D printer based on the 3D digital model. Results As revealed in the HE and Masson images, a meniscus is mostly composed of collagen, with a few cells disseminated between the collagen fiber bundles at the micro‐scale. The SEM image clearly shows the path of highly cross‐linked collagen fibers, and massive pores exist between the fibers. According to the SEM images, the porosity of the meniscus was 34.1% (34.1% ± 0.032%) and the diameters of the collagen fibers were varied. In addition, the cross‐linking pattern of the fibers was irregular. The scanning accuracy of micro‐MRI was 50 μm. The micro‐MRI demonstrated the outline of the meniscus, but the microstructure was obscure. The micro‐CT clearly displayed microfibers in the meniscus with a voxel size of 11.4 μm. The surface layer, lamellar layer, circumferential fibers, and radial fibers could be identified. The mean porosity of the meniscus according to micro‐CT images was 33.92% (33.92% ± 0.03%). Moreover, a 3D model of the microstructure based on the micro‐CT images was built. The microscale fibers could be displayed in the micro‐CT image and the reconstructed 3D digital model. In addition, a 3D resin model was printed out based on the 3D digital model. Conclusion It is extremely difficult to artificially simulate the microstructure of the meniscus because of the irregularity of the diameter and cross‐linking pattern of fibers. The micro‐MRI images failed to demonstrate the meniscus microstructure. Freeze‐drying and micro‐CT scanning are effective methods for 3D microstructure reconstruction of the meniscus, which is an important step towards mechanically functional 3D‐printed meniscus grafts.
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- 2021
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5. Tissue-engineered rhesus monkey nerve grafts for the repair of long ulnar nerve defects: similar outcomes to autologous nerve grafts
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Chang-qing Jiang, Jun Hu, Jian-ping Xiang, Jia-kai Zhu, Xiao-lin Liu, and Peng Luo
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nerve regeneration ,peripheral nerve injury ,tissue engineering ,rhesus monkey ,ulnar nerve ,chemical extraction ,allogenic nerve ,autologous nerve ,transplantation ,Schwann cells ,neural regeneration ,Neurology. Diseases of the nervous system ,RC346-429 - Abstract
Acellular nerve allografts can help preserve normal nerve structure and extracellular matrix composition. These allografts have low immunogenicity and are more readily available than autologous nerves for the repair of long-segment peripheral nerve defects. In this study, we repaired a 40-mm ulnar nerve defect in rhesus monkeys with tissue-engineered peripheral nerve, and compared the outcome with that of autograft. The graft was prepared using a chemical extract from adult rhesus monkeys and seeded with allogeneic Schwann cells. Pathomorphology, electromyogram and immunohistochemistry findings revealed the absence of palmar erosion or ulcers, and that the morphology and elasticity of the hypothenar eminence were normal 5 months postoperatively. There were no significant differences in the mean peak compound muscle action potential, the mean nerve conduction velocity, or the number of neurofilaments between the experimental and control groups. However, outcome was significantly better in the experimental group than in the blank group. These findings suggest that chemically extracted allogeneic nerve seeded with autologous Schwann cells can repair 40-mm ulnar nerve defects in the rhesus monkey. The outcomes are similar to those obtained with autologous nerve graft.
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- 2016
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6. Microstructure Analysis and Reconstruction of a Meniscus
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Shuai Qiu, Zhi Yao, Ge Tong, Xiang Zhou, Lijun Lin, Shuang Zhu, and Jian-ping Xiang
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Male ,Scientific Articles ,business.product_category ,Materials science ,Scanning electron microscope ,Micro‐MRI ,Menisci, Tibial ,3d printer ,03 medical and health sciences ,0302 clinical medicine ,Imaging, Three-Dimensional ,lcsh:Orthopedic surgery ,Microfiber ,Animals ,Humans ,Orthopedics and Sports Medicine ,Lamellar structure ,Scientific Article ,Meniscus ,Porosity ,Micro‐CT ,Microscale chemistry ,030222 orthopedics ,Sheep ,Freeze‐drying ,3D printing ,Middle Aged ,Microstructure ,Magnetic Resonance Imaging ,lcsh:RD701-811 ,Printing, Three-Dimensional ,Microscopy, Electron, Scanning ,Surgery ,Female ,business ,Tomography, X-Ray Computed ,030217 neurology & neurosurgery ,Biomedical engineering - Abstract
Objective To analyze the characteristics of menicus microstructure and to reconstruct a microstructure‐mimicing 3D model of the menicus. Methods Human and sheep meniscus were collected and prepared for this study. Hematoxylin–eosin staining (HE) and Masson staining were conducted for histological analysis of the meniscus. For submicroscopic structure analysis, the meniscus was first freeze‐dried and then scanned by scanning electron microscopy (SEM). The porosity of the meniscus was determined according to SEM images. A micro‐MRI was used to scan each meniscus, immersed in distilled water, and a 3D digital model was reconstructed afterwards. A three‐dimensional (3D) resin model was printed out based on the digital model. Before high‐resolution micro‐CT scanning, each meniscus was freeze‐dried. Then, micro‐scale two‐dimensional (2D) CT projection images were obtained. The porosity of the meniscus was calculated according to micro‐CT images. With micro‐CT, multiple 2D projection images were collected. A 3D digital model based on 2D CT pictures was also reconstructed. The 3D digital model was exported as STL format. A 3D resin model was printed by 3D printer based on the 3D digital model. Results As revealed in the HE and Masson images, a meniscus is mostly composed of collagen, with a few cells disseminated between the collagen fiber bundles at the micro‐scale. The SEM image clearly shows the path of highly cross‐linked collagen fibers, and massive pores exist between the fibers. According to the SEM images, the porosity of the meniscus was 34.1% (34.1% ± 0.032%) and the diameters of the collagen fibers were varied. In addition, the cross‐linking pattern of the fibers was irregular. The scanning accuracy of micro‐MRI was 50 μm. The micro‐MRI demonstrated the outline of the meniscus, but the microstructure was obscure. The micro‐CT clearly displayed microfibers in the meniscus with a voxel size of 11.4 μm. The surface layer, lamellar layer, circumferential fibers, and radial fibers could be identified. The mean porosity of the meniscus according to micro‐CT images was 33.92% (33.92% ± 0.03%). Moreover, a 3D model of the microstructure based on the micro‐CT images was built. The microscale fibers could be displayed in the micro‐CT image and the reconstructed 3D digital model. In addition, a 3D resin model was printed out based on the 3D digital model. Conclusion It is extremely difficult to artificially simulate the microstructure of the meniscus because of the irregularity of the diameter and cross‐linking pattern of fibers. The micro‐MRI images failed to demonstrate the meniscus microstructure. Freeze‐drying and micro‐CT scanning are effective methods for 3D microstructure reconstruction of the meniscus, which is an important step towards mechanically functional 3D‐printed meniscus grafts., Three‐dimensional microstructure reconstruction of the meniscus can be achieved with the method of freeze‐drying and high resolution micro‐CT scanning.
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- 2021
7. Significant association of BDNF rs6265 G>A polymorphism with susceptibility to epilepsy: a meta-analysis
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Jian-Ping Xiang, Yue-Long Xu, Shi-Feng Guo, Su-Jing Zhuang, Bin Wu, Xiu-Xiu Li, Long Wang, and Lan Zhou
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0301 basic medicine ,Brain-derived neurotrophic factor ,Oncology ,medicine.medical_specialty ,business.industry ,Potential risk ,medicine.disease ,03 medical and health sciences ,Epilepsy ,030104 developmental biology ,0302 clinical medicine ,Meta-analysis ,Internal medicine ,Genetic model ,Asian population ,Medicine ,business ,rs6265 ,030217 neurology & neurosurgery - Abstract
Introduction Previously published articles have suggested that BDNF rs6265 G>A polymorphism is a potential risk factor for epilepsy. However, the results were not consistent. Methods We conducted a meta-analysis to explore the association between BDNF rs6265 G>A polymorphism and epilepsy risk. Four online databases were searched, and related studies were reviewed from their inception up to June 20, 2017. ORs and corresponding 95% CIs were used to calculate the associations of each genetic model. Overall, 10 case-control publications involving 9,512 subjects were included in this meta-analysis. Results Significant associations were found between BDNF rs6265 G>A polymorphism and epilepsy (A vs G: OR=0.88, 95% CI=0.83-0.94, P A polymorphism might be involved in epilepsy susceptibility, especially in the Asian population.
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- 2018
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8. Tissue-engineered rhesus monkey nerve grafts for the repair of long ulnar nerve defects: similar outcomes to autologous nerve grafts
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Xiaolin Liu, Jun Hu, Jian-ping Xiang, Jiakai Zhu, Peng Luo, and Chang-qing Jiang
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0301 basic medicine ,medicine.medical_specialty ,Hypothenar eminence ,rhesus monkey ,Nerve conduction velocity ,lcsh:RC346-429 ,03 medical and health sciences ,0302 clinical medicine ,Developmental Neuroscience ,Tissue engineering ,Medicine ,peripheral nerve injury ,Schwann cells ,Ulnar nerve ,nerve regeneration ,tissue engineering ,ulnar nerve ,chemical extraction ,allogenic nerve ,autologous nerve ,transplantation ,neural regeneration ,lcsh:Neurology. Diseases of the nervous system ,business.industry ,Compound muscle action potential ,Surgery ,Transplantation ,030104 developmental biology ,Peripheral nerve injury ,Epineurial repair ,business ,030217 neurology & neurosurgery ,Research Article - Abstract
Acellular nerve allografts can help preserve normal nerve structure and extracellular matrix composition. These allografts have low immunogenicity and are more readily available than autologous nerves for the repair of long-segment peripheral nerve defects. In this study, we repaired a 40-mm ulnar nerve defect in rhesus monkeys with tissue-engineered peripheral nerve, and compared the outcome with that of autograft. The graft was prepared using a chemical extract from adult rhesus monkeys and seeded with allogeneic Schwann cells. Pathomorphology, electromyogram and immunohistochemistry findings revealed the absence of palmar erosion or ulcers, and that the morphology and elasticity of the hypothenar eminence were normal 5 months postoperatively. There were no significant differences in the mean peak compound muscle action potential, the mean nerve conduction velocity, or the number of neurofilaments between the experimental and control groups. However, outcome was significantly better in the experimental group than in the blank group. These findings suggest that chemically extracted allogeneic nerve seeded with autologous Schwann cells can repair 40-mm ulnar nerve defects in the rhesus monkey. The outcomes are similar to those obtained with autologous nerve graft.
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- 2016
9. Expression patterns and role of PTEN in rat peripheral nerve development and injury
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Qingtang Zhu, Xiaolin Liu, Junxia Wu, Canbin Zheng, Hui Chen, Jian-ping Xiang, Tao Lin, and Bo He
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0301 basic medicine ,Myelinated nerve fiber ,Nerve Crush ,Biology ,Nerve conduction velocity ,03 medical and health sciences ,0302 clinical medicine ,Peripheral Nerve Injuries ,Ganglia, Spinal ,medicine ,Tensin ,PTEN ,Animals ,Peripheral Nerves ,PI3K/AKT/mTOR pathway ,General Neuroscience ,PTEN Phosphohydrolase ,Nerve injury ,medicine.disease ,Sciatic Nerve ,Cell biology ,Nerve Regeneration ,Rats ,030104 developmental biology ,nervous system ,Peripheral nerve injury ,biology.protein ,Crush injury ,medicine.symptom ,030217 neurology & neurosurgery - Abstract
Studies have suggested that phosphatase and tensin homolog (PTEN) plays an important role in neuroprotection and neuronal regeneration. To better understand the potential role of PTEN with respect to peripheral nerve development and injury, we investigated the expression pattern of PTEN at different stages of rat peripheral nerve development and injury and subsequently assessed the effect of pharmacological inhibition of PTEN using bpV(pic) on axonal regeneration in a rat sciatic nerve crush injury model. During the early stages of development, PTEN exhibits low expression in neuronal cell bodies and axons. From embryonic day (E) 18.5 and postnatal day (P)5 to adult, PTEN protein becomes more detectable, with high expression in the dorsal root ganglia (DRG) and axons. PTEN expression is inhibited in peripheral nerves, preceding myelination during neuronal development and remyelination after acute nerve injury. Low PTEN expression after nerve injury promotes Akt/mammalian target of rapamycin (mTOR) signaling pathway activity. In vivo pharmacological inhibition of PTEN using bpV(pic) promoted axonal regrowth, increased the number of myelinated nerve fibers, improved locomotive recovery and enhanced the amplitude response and nerve conduction velocity following stimulation in a rat sciatic nerve crush injury model. Thus, we suggest that PTEN may play potential roles in peripheral nerve development and regeneration and that inhibition of PTEN expression is beneficial for nerve regeneration and functional recovery after peripheral nerve injury.
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- 2018
10. Three-dimensional Reconstruction of the Microstructure of Human Acellular Nerve Allograft
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Qingtang Zhu, Liqiang Gu, Jian Qi, Jian Yutao, Shuang Zhu, Yan Liwei, Xiaolin Liu, Yang Weihong, Xiang Zhou, Jian-ping Xiang, Tao Lin, and Bo He
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0301 basic medicine ,X-ray microtomography ,Materials science ,Article ,03 medical and health sciences ,Imaging, Three-Dimensional ,0302 clinical medicine ,Peripheral nerve ,Microscopy ,Humans ,Computer Simulation ,Peripheral Nerves ,Multidisciplinary ,Nerve allograft ,Nerve graft ,Organ Transplantation ,X-Ray Microtomography ,Anatomy ,Allografts ,Microstructure ,030104 developmental biology ,Computed microtomography ,Printing, Three-Dimensional ,Peripheral nerve injury ,Microscopy, Electron, Scanning ,030217 neurology & neurosurgery - Abstract
The exact inner 3D microstructure of the human peripheral nerve has been a mystery for decades. Therefore, it has been difficult to solve several problems regarding peripheral nerve injury and repair. We used high-resolution X-ray computed microtomography (microCT) to scan a freeze-dried human acellular nerve allograft (hANA). The microCT images were then used to reconstruct a 3D digital model, which was used to print a 3D resin model of the nerve graft. The 3D digital model of the hANA allowed visualization of all planes. The magnified 3D resin model clearly showed the nerve bundles and basement membrane tubes of the hANA. Scanning electron microscopy (SEM) was used to analyse the microstructure of the hANA. Compared to the SEM images, the microCT image clearly demonstrated the microstructure of the hANA cross section at a resolution of up to 1.2 μm. The 3D digital model of the hANA facilitates a clear and easy understanding of peripheral nerve microstructure. Furthermore, the enlarged 3D resin model duplicates the unique inner structure of each individual hANA. This is a crucial step towards achieving 3D printing of a hANA or nerve that can be used as a nerve graft.
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- 2016
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11. Calcium intake and hip fracture risk: a meta-analysis of prospective cohort studies
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Dong, Wang, Xiao-Hu, Chen, Guo, Fu, Li-Qiang, Gu, Qing-Tang, Zhu, Xiao-Lin, Liu, Jian, Qi, and Jian-Ping, Xiang
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Review Article - Abstract
It has been suggested that the amount of calcium intake may influence hip fracture incidence. However, the results of the researches in this regard are inconsistent. We performed this meta-analysis to estimate the association between calcium intake and hip fracture risk. Prospective cohort studies on calcium intake and hip fracture risk were identified by searching databases from the period 1960 to 2014. Results from individual studies were synthetically combined using STATA 11 software. The results indicated that a total of 8 prospective cohort studies were included in our meta-analysis, involving 2,435 cases and 267,759 participants. The combined relative risk (RR) of hip fracture for highest compared with lowest amount calcium intake was 0.97 (95% confidence interval [CI]: 0.89-1.07). Little evidence of publication bias was found. In conclusion, this meta-analysis provides evidence of no association between calcium intake and hip fracture risk. However, this finding is based on only a limited number of included studies.
- Published
- 2014
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