trabecular number

骨小梁数
  • 文章类型: Journal Article
    评估骨小梁结构的“金标准”是高分辨率显微CT。在本技术说明中,我们测试了初始扫描分辨率和事后降采样对大猩猩胫骨骨小梁的定量和定性分析的影响。我们分析了一个大猩猩个体的右胫骨远端小梁形态,以研究体素大小变化对测量的小梁变量的影响。对于微CT体积的每个版本,使用医学图像分析方法分割骨小梁。然后使用整体形态计量学分析来分析骨体积(BV/TV),各向异性(DA),小梁厚度(Tb.Th),间距(Tb.Sp),和数量(Tb。N).发现在初始扫描期间增加体素尺寸对DA和Tb具有强烈影响。这些措施,而BV/TV,TB。SP,Tb。发现N对初始扫描分辨率的变化较不敏感。所有测试的参数基本上不受向下采样至90μm分辨率的影响。BV/TV和DA的彩色图也保留了它们的分布直至90μm。这项研究是第一个使用全骨phy方法检查显微CT体素大小变化对小梁结构分析的影响的研究。我们的结果表明,对于大多数小梁参数,对于扫描和下采样分辨率,可以测量高达90μm的体素尺寸的微结构变量。此外,如果只有BV/TV,TB。Sp或Tb。N是测量的,甚至更大的体素尺寸可以被使用,而基本上不影响结果。
    The \"gold standard\" for the assessment of trabecular bone structure is high-resolution micro-CT. In this technical note, we test the influence of initial scan resolution and post hoc downsampling on the quantitative and qualitative analysis of trabecular bone in a Gorilla tibia. We analyzed trabecular morphology in the right distal tibia of one Gorilla gorilla individual to investigate the impact of variation in voxel size on measured trabecular variables. For each version of the micro-CT volume, trabecular bone was segmented using the medical image analysis method. Holistic morphometric analysis was then used to analyze bone volume (BV/TV), anisotropy (DA), trabecular thickness (Tb.Th), spacing (Tb.Sp), and number (Tb.N). Increasing voxel size during initial scanning was found to have a strong impact on DA and Tb.Th measures, while BV/TV, Tb.Sp, and Tb.N were found to be less sensitive to variations in initial scan resolution. All tested parameters were not substantially influenced by downsampling up to 90 μm resolution. Color maps of BV/TV and DA also retained their distribution up to 90 μm. This study is the first to examine the effect of variation in micro-CT voxel size on the analysis of trabecular bone structure using whole epiphysis approaches. Our results indicate that microstructural variables may be measured for most trabecular parameters up to a voxel size of 90 μm for both scan and downsampled resolutions. Moreover, if only BV/TV, Tb.Sp or Tb.N is measured, even larger voxel sizes might be used without substantially affecting the results.
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  • 文章类型: Journal Article
    桡骨头骨折的适当管理是不可或缺的,以防止长期后果,如慢性疼痛和运动丧失。先进的成像系统,像显微计算机断层扫描(μCT),对于理解桡骨头骨折模式很有价值,因为它们利用微米级分辨率来定义骨骼健康的重要参数,如皮质密度和小梁厚度。这项研究的目的是利用μCT识别和描述放射状头的结构形态。将九个新鲜冷冻的尸体人体半径分为四个相等的象限,基于,并标记为后内侧,后外侧,前内侧,和前外侧。用SCANCOMicroCT40扫描象限,以36.0μm的分辨率进行皮质和松质骨密度测量。骨密度,直接骨小梁数,和小梁厚度记录为毫克羟基磷灰石/cm3。进行单向重复测量ANOVA以比较骨密度,小梁数,和四个象限中每个象限的小梁厚度(p<0.05)。后内侧象限比其他象限包含更多的骨骼。与前内侧象限(54.6mgHA/cm3)相比,后内侧象限(148.1mgHA/cm3)的骨密度明显更高,后外侧象限(137.5mgHA/cm3)与前内侧象限(54.6mgHA/cm3)相比,和后外侧象限(137.5mgHA/cm3)与前外侧象限(58.1mgHA/cm3)相比。象限之间的小梁数量没有显着差异。与后内侧(0.1809mgHA/cm3)象限相比,前外侧(0.1417mgHA/cm3)和前内侧(0.1416mgHA/cm3)象限的小梁厚度显着降低。与前半部相比,发现radial头的后半部具有更高的圆柱和拱形密度。桡骨远端骨小梁的微结构形成柱状,struts,和拱门,这允许通过骨骼有效地传递应力。桡骨头的微观结构与桡骨远端具有相似的微观结构,本研究确定了桡骨头中存在柱和拱。这些结构,随着小梁密度,在桡骨头后部可以解释较低的发生率涉及桡骨头后半部的骨折。此外,我们的研究支持以下观点:与其他区域相比,前外侧象限的骨折发生率较高是由于微结构特征和相对缺乏支持结构.从这项研究中获得的新颖见解将有助于开发针对预防措施的先进干预措施,并更好地治疗桡骨头骨折,例如当螺钉指向较密集的后内侧象限时,购买更令人满意的购买。
    Appropriate management of radial head fractures is integral to prevent long-term consequences like chronic pain and loss of motion. Advanced imaging systems, like micro-computed tomography (μCT), are valuable for understanding radial head fracture patterns as they utilize micrometer scale resolution to define important parameters of bone health like cortical density and trabecular thickness. The purpose of this study was to identify and describe the structural morphology of the radial head utilizing μCT. Nine fresh-frozen cadaveric human radii were divided into four equal quadrants, based, and labeled as posteromedial, posterolateral, anteromedial, and anterolateral. Quadrants were scanned with a SCANCO MicroCT40 with both cortical and cancellous bone density measurements at a resolution of 36.0 μm. Bone density, direct trabecular number, and trabecular thickness were recorded as milligrams of hydroxyapatite/cm3. A one-way repeated measures ANOVA was performed to compare the bone densities, trabecular number, and trabecular thickness of each of the four quadrants (p < 0.05). The posteromedial quadrant contained substantially more bone than other quadrants. Significantly greater bone densities were found in the posteromedial quadrant (148.1 mg of HA/cm3) compared to the anteromedial quadrant (54.6 mg of HA/cm3), posterolateral quadrant (137.5 mg of HA/cm3) compared to the anteromedial quadrant (54.6 mg of HA/cm3), and posterolateral quadrant (137.5 mg of HA/cm3) compared to the anterolateral quadrant (58.1 mg of HA/cm3). The trabecular number was not significantly different between quadrants. Trabecular thickness was significantly lower in the anterolateral (0.1417 mg of HA/cm3) and anteromedial (0.1416 mg of HA/cm3) quadrants compared to the posteromedial (0.1809 mg of HA/cm3) quadrant. The posterior half of the radial head was found to have a higher density of columns and arches compared to the anterior half. The microstructure of trabecular bone in the distal radius forms columns, struts, and arches, which allow for efficient transmission of stress through the bone. The microstructure of the radial head has similar microarchitecture to the distal radius with the present study identifying the presence of columns and arches in the radial head. These structures, along with trabecular density, in the posterior radial head may explain the lower incidence of fractures involving the posterior half of the radial head. Furthermore, our study supports the idea that the high incidence of fractures involving the anterolateral quadrant is due to microarchitecture characteristics and the relative lack of supportive structures compared to other areas. The novel insight gained from this study will aid in the development of advanced interventions for preventative measures and better treatment of radial head fractures like more satisfactory purchase when screws are directed towards the denser posteromedial quadrant.
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  • 文章类型: Journal Article
    在评估骨骼健康和疾病的啮齿动物研究中,应分析哪些骨骼部位和参数仍然不确定。在这项使用微型计算机断层扫描(µCT)的横断面小鼠研究中,我们探讨了:(1)哪些微观结构参数可用于区分女性和男性骨骼;(2)评估一个以上的骨骼部位是否有意义。股骨小梁和/或皮质区室的微结构参数,胫骨,胸椎和腰椎体,在10只雌性和10只6个月大的雄性C57BL/6J小鼠中通过µCT评估颅骨和颅骨。骨小梁数(TbN)明显增高,而在所有评估的骨骼部位,雄性小鼠的小梁分离(TbSp)明显低于雌性小鼠。总的来说,骨体积/组织体积(BV/TV)也显著高于男性。雌性老鼠(除了胸椎,没有性别差异)。雄性和雌性小鼠的皮质骨微结构的大多数参数没有差异。BV/TV,TbN,和股骨的TbSp,胫骨和腰椎的TbN和TbSp可以完全(100%)区分女性和男性骨骼。股骨皮质厚度(CtTh)是检测皮质区室性别差异的最佳参数(AUC=0.914)。在6个月大的C57BL/6J小鼠中,BV/TV,TbN,和TbSp可以用来区分男性和女性的骨骼。每当无法评估多个骨骼部位时,我们建议评估股骨的骨微结构以检测潜在的性别差异。
    It remains uncertain which skeletal sites and parameters should be analyzed in rodent studies evaluating bone health and disease. In this cross-sectional mouse study using micro-computed tomography (µCT), we explored: (1) which microstructural parameters can be used to discriminate female from male bones and (2) whether it is meaningful to evaluate more than one bone site. Microstructural parameters of the trabecular and/or cortical compartments of the femur, tibia, thoracic and lumbar vertebral bodies, and skull were evaluated by µCT in 10 female and 10 male six-month-old C57BL/6J mice. The trabecular number (TbN) was significantly higher, while the trabecular separation (TbSp) was significantly lower in male compared to female mice at all skeletal sites assessed. Overall, bone volume/tissue volume (BV/TV) was also significantly higher in male vs. female mice (except for the thoracic spine, which did not differ by sex). Most parameters of the cortical bone microstructure did not differ between male and female mice. BV/TV, TbN, and TbSp at the femur, and TbN and TbSp at the tibia and lumbar spine could fully (100%) discriminate female from male bones. Cortical thickness (CtTh) at the femur was the best parameter to detect sex differences in the cortical compartment (AUC = 0.914). In 6-month-old C57BL/6J mice, BV/TV, TbN, and TbSp can be used to distinguish male from female bones. Whenever it is not possible to assess multiple bone sites, we propose to evaluate the bone microstructure of the femur for detecting potential sex differences.
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  • 文章类型: Journal Article
    背景:肝硬化患者骨丢失的风险增加。最近关于面骨矿物质密度的研究报告了相互矛盾的发现。由于骨微结构的评估是复杂的,对与骨转换的新血清标志物的相关性进行了搜索。关于骨折风险增加患者血清硬化素水平的当前数据是不同的,迄今为止只有一项研究检查了肝硬化患者。因此,这项研究的目的是评估血清硬化素水平,并检验其与微体系结构的相关性。
    方法:本研究在32例最近诊断为肝硬化的患者和32例对照中进行。通过高分辨率外周定量计算机断层扫描评估骨微结构的参数。通过新的ELISA检测硬化蛋白,该ELISA检测硬化蛋白核心区第2环的活性受体相互作用位点。
    结果:硬化素水平轻微,但在患者组中并没有显著降低,与对照组相比。相比之下,酒精性肝硬化患者的水平明显低于对照组.在患者组中观察到与区域骨矿物质密度(BMD)和小梁微结构的显着相关性。然而,在对照组中,硬化蛋白与骨微结构之间几乎没有任何相关性。
    结论:在肝硬化中,硬化蛋白与改变的骨微结构和较低的区域BMD有关。在酒精性肝病中,观察到硬化蛋白浓度低。
    BACKGROUND: Patients with hepatic cirrhosis are at increased risk of bone loss. Recent work on areal bone mineral density has reported contradictory findings. As the assessment of bone microarchitecture is complex, a search was made for correlations with new serum markers of bone turnover. Current data on serum sclerostin levels in patients with increased fracture risk are divergent and to date only one study has examined patients with hepatic cirrhosis. Therefore, the aim of this study was to evaluate serum sclerostin levels and to test for correlations with microarchitecture.
    METHODS: This study was performed in 32 patients with recently diagnosed hepatic cirrhosis and 32 controls. The parameters of bone microarchitecture were assessed by high-resolution peripheral quantitative computed tomography. Sclerostin was detected via a new ELISA that detects the active receptor interaction site at loop 2 of the sclerostin core region.
    RESULTS: Sclerostin levels were slightly, but not significantly lower in the patient group, compared to controls. In contrast, patients with alcoholic liver cirrhosis had significantly lower levels than the controls. A significant correlation with areal bone mineral density (BMD) and trabecular microarchitecture was observed in the patient group. However, there was hardly any correlation between sclerostin and bone microarchitecture in the controls.
    CONCLUSIONS: In hepatic cirrhosis, sclerostin is related to altered bone microarchitecture and lower areal BMD. In alcoholic liver disease, low sclerostin concentrations were seen.
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  • 文章类型: Clinical Trial
    Although the expected skeletal manifestations of testosterone deficiency in Klinefelter\'s syndrome (KS) are osteopenia and osteoporosis, the structural basis for this is unclear. The aim of this study was to assess bone geometry, volumetric bone mineral density (vBMD), microarchitecture, and estimated bone strength using high-resolution peripheral quantitative computed tomography (HR-pQCT) in patients with KS. Thirty-one patients with KS confirmed by lymphocyte chromosome karyotyping aged 35.8 ± 8.2 years were recruited consecutively from a KS outpatient clinic and matched with respect to age and height with 31 healthy subjects aged 35.9 ± 8.2 years. Dual-energy X-ray absorptiometry (DXA) and HR-pQCT were performed in all participants, and blood samples were analyzed for hormonal status and bone biomarkers in KS patients. Twenty-one KS patients were on long-term testosterone-replacement therapy. In weight-adjusted models, HR-pQCT revealed a significantly lower cortical area (p < 0.01), total and trabecular vBMD (p = 0.02 and p = 0.04), trabecular bone volume fraction (p = 0.04), trabecular number (p = 0.05), and estimates of bone strength, whereas trabecular spacing was higher (p = 0.03) at the tibia in KS patients. In addition, cortical thickness was significantly reduced, both at the radius and tibia (both p < 0.01). There were no significant differences in indices of bone structure, estimated bone strength, or bone biomarkers in KS patients with and without testosterone therapy. This study showed that KS patients had lower total vBMD and a compromised trabecular compartment with a reduced trabecular density and bone volume fraction at the tibia. The compromised trabecular network integrity attributable to a lower trabecular number with relative preservation of trabecular thickness is similar to the picture found in women with aging. KS patients also displayed a reduced cortical area and thickness at the tibia, which in combination with the trabecular deficits, compromised estimated bone strength at this site.
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  • 文章类型: Comparative Study
    Optimization of peak bone mass during adolescence is important for osteoporosis prevention. Studies in rodents and humans have demonstrated the harmful effects of sugar intake on bone health. With the high levels of sucrose in the diets of adolescents, it is necessary to understand the influence of glucose and fructose on growing bones. This study compared the effects of dietary glucose and fructose on bone formation, microarchitecture, and strength. Because of the different metabolic effects of glucose and fructose, we hypothesized that their individual effects on bone would be different. Eighteen male Sprague-Dawley rats (age, 60 days) were randomly assigned to high-fructose (n = 9; 40% fructose, 10% glucose) or high-glucose diet (n = 9; 50% glucose) for 12 weeks. Bone measurements included histology and histomorphometry of trabecular bone in the distal femur and a 3-point bending test of the whole tibia. Whole liver mass and postprandial serum glucose, insulin, and triglycerides were used to assess differences in energy metabolism between the diets. There were no differences in food intake, body weight, or visceral adiposity between groups, but fructose consumption led to heavier livers (P = .001) and elevated serum triglycerides (P = .00). The distal femurs of fructose-fed rats had greater bone volume (bone volume/total volume; P = .03), lower bone surface (bone surface/bone volume; P = .02), and thicker trabeculae (trabecular thickness; P = .01). The tibias of the fructose-fed rats also withstood a greater maximum flexure load (P = .032). These results indicate that consumption of the high-fructose diet resulted in stronger bones with enhanced microarchitecture than consumption of the high-glucose diet.
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  • 文章类型: Journal Article
    The effects of obesity and metabolic syndrome (MS) on bone health are controversial. Furthermore, the relationship between body composition and bone quality has not yet been determined in this context. The aim of this study was to investigate the correlations between body composition and bone mineral density (BMD) and bone microstructure in obese individuals with MS. This cross-sectional study assessed 50 obese individuals with MS with respect to their body composition and BMD, both assessed using dual X-ray absorptiometry, and bone microarchitecture, assessed by high-resolution peripheral quantitative computed tomography (HR-pQCT) of the distal tibia and radius. Several HR-pQCT measurements exhibited statistically significant correlations with lean mass. Lean mass was positively correlated with parameters of better bone quality (r: 0.316-0.470) and negatively correlated with parameters of greater bone fragility (r: -0.460 to -0.310). Positive correlations were also observed between lean mass and BMD of the total femur and radius 33%. Fat mass was not significantly correlated with BMD or any HR-pQCT measurements. Our data suggest that lean mass might be a predictor of bone health in obese individuals with MS.
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  • 文章类型: Journal Article
    BACKGROUND: Velvet antlers (VA) have been claimed for centuries to have numerous medical benefits including strengthen bones. To investigate and compare the anti-osteoporotic activities from different sections of VA.
    METHODS: Fresh VA prepared from farmed sika deers (Cervus nippon) was divided into upper (VAU), middle (VAM), and basal (VAB) sections. The chemical constituents and anti-osteoporotic effect of different sections from VA were evaluated using ovariectomized rats.
    RESULTS: Levels of water-soluble extracts, diluted alcoholic extract, amino acids, testosterone, insulin-like growth factor (IGF)-1 and testosterone plus estradiol significantly differed among the different sections. Levels of these constituents were significantly higher in the upper section than in the basal section. Moreover, levels of testosterone and IGF-1 of the VAM were also significantly higher than those of the VAB. Calcium level increased downward from the tip with statistical significance. The strength of vertebrae increased in all VA-treated groups compared to the control, but only treatment with VAU and VAM increased the strength of the femur and the microarchitecure of the trabecular bone. Alkaline phosphatase levels of VAU- and VAM-treated groups significantly decreased, but osteocalcin did not significantly change. Moreover, VAU and VAM dose-dependently increased proliferation and mineralization of MC3T3-E1 cells.
    CONCLUSIONS: Our study provides strong evidence for the regional differences in the effectiveness of velvet antler in treating osteoporosis. However, further studies are needed to elucidate the bioactive chemical constituents associated with the anti-osteoporotic effects of velvet antler.
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  • 文章类型: Journal Article
    普通肝素(UFH)是慢性肾脏病(CKD)患者血液透析中使用最广泛的抗凝剂。许多研究已经证实UFH可以诱导正常骨受试者的骨丢失。但很少有人关注它对肾性骨营养不良的影响。因此,我们在腺嘌呤诱导的CKD大鼠中研究了这个问题。由于CKD也会全身损害矿物质代谢,我们还研究了UFH对CKD-矿物质和骨骼疾病(CKD-MBD)和血管钙化的血清标志物的影响。我们给予低剂量和高剂量的UFH(1U/g和2U/g体重,分别)与CKD大鼠进行比较,并与CKD对照组进行比较。在牺牲时,CKD-MBD的血清标志物在两个UFHCKD组和CKD对照组之间没有显着差异。高剂量UFH(H-UFH)CKD组股骨和由骨小梁和皮质骨构成的感兴趣区域(ROI)的平均骨密度(BMD)低于CKD对照组(分别为P<0.05和P<0.01)。由皮质骨构成的股骨ROI的BMD在H-UFHCKD组和CKD对照组之间没有差异。CKD大鼠的组织形态变化表明继发性甲状旁腺功能亢进,和股骨骨小梁的体积,但不是皮质骨体积,随着UFH剂量的增加而显著降低。在成骨细胞参数中发现了相同的下降趋势,破骨细胞参数呈增加趋势;然而,大多数差异并不显著。此外,CKD对照组和两个UFHCKD组之间的血管钙或磷含量比较无明显统计学差异。因此,结论UFH可引起CKD大鼠继发性甲状旁腺功能亢进的骨丢失,主要通过减少小梁体积,对皮质骨体积影响不大。潜在的机制可能涉及UFH抑制成骨细胞活性和促进破骨细胞活性。我们没有发现UFH对继发性甲状旁腺功能亢进的CKD大鼠血管钙化有任何影响。
    Unfractionated heparin (UFH) is the most widely used anticoagulant in hemodialysis for chronic kidney disease (CKD) patients. Many studies have verified that UFH can induce bone loss in subjects with normal bone, but few have focused on its effect on renal osteodystrophy. We therefore investigated this issue in adenine-induced CKD rats. As CKD also impairs mineral metabolism systemically, we also studied the impacts of UFH on serum markers of CKD-mineral and bone disorder (CKD-MBD) and vascular calcification. We administered low and high doses of UFH (1U/g and 2U/g body weight, respectively) to CKD rats and compared them with CKD controls. At sacrifice, the serum markers of CKD-MBD did not significantly differ among the two UFH CKD groups and the CKD control group. The mean bone mineral densities (BMDs) of the total femur and a region of interest (ROI) constituted of trabecular and cortical bone were lower in the high-dose UFH (H-UFH) CKD group than in the CKD control group (P<0.05 and P<0.01, respectively). The BMD of the femoral ROI constituted of cortical bone did not differ between the H-UFH CKD group and the CKD control group. Histomorphometrical changes in the CKD rats indicated secondary hyperparathyroidism, and the femoral trabecular bone volume, but not cortical bone volume, significantly decreased with increasing UFH dose. The same decreasing trend was found in osteoblast parameters, and an increasing trend was found in osteoclast parameters; however, most differences were not significant. Moreover, no distinct statistical differences were found in the comparison of vascular calcium or phosphorus content among the CKD control group and the two UFH CKD groups. Therefore, we concluded that UFH could induce bone loss in CKD rats with secondary hyperparathyroidism, mainly by reducing the trabecular volume and had little effect on cortical bone volume. The underlying mechanism might involve inhibition of osteoblast activity and promotion of osteoclast activity by UFH. We did not find any effect of UFH on vascular calcification in CKD rats with secondary hyperparathyroidism.
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  • 文章类型: Comparative Study
    Dried plum has been reported to have potent effects on bone in osteopenic animal models, but the mechanisms through which bone metabolism is altered in vivo remain unclear. To address this issue, a study comparing the metabolic response of dried plum to the anabolic agent, parathyroid hormone (PTH), was undertaken. Six month-old female Sprague Dawley rats (n=84) were sham-operated (SHAM) or ovariectomized (OVX) and maintained on a control diet for 6wks until osteopenia was confirmed. Treatments were initiated consisting of a control diet (AIN-93M) supplemented with dried plum (0, 5, 15 or 25%; w/w) or a positive control group receiving PTH. At the end of 6wks of treatment, whole body and femoral bone mineral density (BMD) were restored by the two higher doses of dried plum to the level of the SHAM group. Trabecular bone volume and cortical thickness were also improved with these two doses of dried plum. Dried plum suppressed the OVX-induced increase in bone turnover as indicated by systemic biomarkers of bone metabolism, N-terminal procollagen type 1 (P1NP) and deoxypyridinoline (DPD). Dynamic bone histomorphometric analysis of the tibial metaphysis revealed that dried plum restored the OVX-induced increase in cancellous bone formation rate (BFR) and mineralizing surface (MS/BS) to the SHAM group, but some doses of dried plum increased endocortical mineral apposition rate (MAR). As expected, PTH significantly increased endocortical MAR and BFR, periosteal BFR, and trabecular MAR and BFR beyond that of the OVX and maintained the accelerated rate of bone resorption associated with OVX. Dried plum up-regulated bone morphogenetic protein 4 (Bmp4) and insulin-like growth factor 1 (Igf1) while down-regulating nuclear factor T cell activator 1 (Nfatc1). These findings demonstrate that in the adult osteopenic OVX animal, the effects of dried plum differ from that of PTH in that dried plum primarily suppressed bone turnover with the exception of the indices of bone formation at the endocortical surface.
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