Background: Intracranial dissecting aneurysms (IDAs) are rare but pose significant challenges to treatment. The pipeline embolization device (PED) has been demonstrated to be an effective treatment option with excellent outcomes. Herein, we report our experience with patients treated with the PED for unruptured IDAs. Methods: We retrospectively reviewed our hospital database and identified patients who were treated with PEDs for unruptured IDAs between March 2016 and September 2020. Data including demographics, clinical presentation, aneurysm characteristics, procedural details, intra- or peri-procedural complications, and follow-up details were collected. Results: Eighty patients (61 men, 76.25%) were treated with PED for unruptured IDAs. The most common symptoms were headache (34, 42.5%), dizziness (29, 36.25%), and nausea or vomiting (15, 18.75%). Of these patients, 73 had one aneurysm, and seven harbored two aneurysms. All of them achieved successful PED deployment. Six patients experienced intra- or peri-procedural complications including perforator artery occlusion, thromboembolic, hemorrhagic events, and falling of the stent into the aneurysm sac. Follow-up with digital subtractive angiography was available for 29 patients with a median of 6 months, and 28 (96.56%) patients had aneurysm occlusion. Late thrombosis occurred in four patients, and two of them had unfavorable outcomes. Clinical follow-up showed that a favorable clinical outcome was achieved in 76 (95%) patients, and the mortality rate was 3.75%. Conclusion: Treating unruptured IDAs is safe and effective with long-term favorable clinical and angiographic outcomes. However, the complications of this treatment should be noted. Careful selection of appropriate patients and individualized antiplatelet therapy might be needed.
OBJECTIVE Flow diverters (FDs) have been used in unruptured intracranial vertebral artery dissecting aneurysms (IVADAs) with seemingly more favorable outcomes compared with stent-assisted coiling (SAC). However, the benefits of FDs over SAC in unruptured IVADAs need further evaluation. METHODS This was a propensity score–matched, retrospective cohort study. Consecutive patients with unruptured IVADAs treated with FDs or SAC at the authors’ hospital between January 2016 and December 2020 were reviewed. Propensity score matching at 1:1 was based on age, significant stenosis adjacent to aneurysmal dilatation, maximum diameter, and posterior inferior cerebellar artery involvement. Periprocedural cerebrovascular complications and angiographic and clinical outcomes were compared between the two matched groups. RESULTS A total of 124 unruptured IVADAs in 123 patients (median age 53 [interquartile range 47–59] years; 101 men) were included. The FD and SAC groups included 65 and 59 IVADAs, respectively. Propensity score matching resulted in 47 matched pairs. The rates of immediate complete occlusion were significantly lower in the matched FD group than in the matched SAC group (6.4% vs 68.1%, p < 0.001). The rates of periprocedural cerebrovascular complications were comparable between the two matched groups (6.4% vs 6.4%, p > 0.99). At last follow-up, the rates of complete occlusion (89.4% vs 80.9%, p = 0.39) and favorable clinical outcomes (100.0% vs 97.9%, p > 0.99) were comparable, whereas the rate of recanalization was significantly lower in the matched FD group than in the matched SAC group (0.0% vs 12.8%, p = 0.03). Although the difference between the rates of in-stent stenosis was not statistically significant (17.0% vs 6.4%, p = 0.18), the difference in the effect measures was considerable. CONCLUSIONS In unruptured IVADAs and compared with SAC, FDs provide comparable rates of periprocedural cerebrovascular complications, favorable clinical outcomes, and follow-up complete occlusion, lower rates of immediate complete occlusion and follow-up recanalization, and likely higher rates of in-stent stenosis.
Over the past decade, the research and development (R&D) of anti-tumor drugs in China has undergone a remarkable leap, maintaining a high level of motivation. With respect to pharmaceutical R&D paradigms in China, the domestic market was once dominated by generic drugs. A progressive transition towards the development of innovative pharmaceuticals is emerging, consequent to the reforms in drug evaluation and approval mechanisms and the promotion of novel drug development in China. The introduction of new drugs from other countries to China used to lag behind. Now a progressive approach is being taken towards synchronization in global R&D. The emergence of new players in the pharmaceutical industry and the enhancement of corporate R&D competencies have further facilitated the internationalization of China's drug R&D endeavors. The rapid advancement in pharmaceutical R&D has significantly enhanced China's drug regulatory capabilities. In August 2015, the State Council of the People's Republic of China promulgated the "Opinions on Reforming the Approval Procedures for Drugs and Medical Devices" marking the official commencement of reforms in the drug evaluation and approval system. The Chinese drug regulatory authorities are integrating resources and optimizing drug review processes through the development of a scientifically complete system of Good Review Practice. Innovative drugs, including new drugs, improved new drugs (those improved formulations or dose forms with existing active ingredients), biosimilars, and domestic generic drugs with unimported original drugs, constitute essential assurances for patients in China and offer better accessibility of medications. To better understand the changes since the inception of the drug evaluation and approval reforms in 2015, we have collected data on new drug applications (NDAs) for the aforementioned types of drugs submitted to the Center for Drug Evaluation (CDE) under the National Medical Products Administration (NMPA) in China, spanning from January 2010 to March 2024. A total of 374 NDAs for anti-tumor drugs had been approved from January 1, 2010 to March 31, 2024, including 186 (49.7%) imported drugs and 188 (50.3%) domestic drugs. The domestic drugs included 139 (37.1%) innovative/improved new drugs, 31 (8.3%) generic drugs, and 18 (4.8%) biosimilars, respectively. Before 2018, China's pharmaceutical market mainly relied on domestic generic drugs. However, since 2018, the number of drug authorizations granted to innovative drugs has been on the rise, with a notable increase in domestically developed innovative drugs (Figure 1). The emergence of an upward trend in domestically R&D innovative drugs is due to better regulatory frameworks, faster review processes, and the introduction of technical standards. The Chinese government has implemented policies promoting anti-tumor drug R&D, including priority review, conditional approval, and breakthrough treatment designation. From 2010 to 2015, the CDE approved 45 anti-tumor drugs with an average review time of 580 days. From 2016 to 2024, the average review time for 329 applications dropped to 280.2 days. These measures enhanced review efficiency and transparency, offered a more predictable environment for drug development, and boosted the industry's confidence and interest in R&D. The advent of these domestic drugs has addressed much of the unmet needs of Chinese patients, transformed tumor therapeutics profoundly, and achieved success in the international market, thereby providing additional treatment options for patients worldwide. Bruton's tyrosine kinase inhibitor Zanubrutinib (Brukinsa®), which was granted an accelerated approval by the United States (US) Food and Drug Administration (FDA) in 2019, was tested in a pivotal study—a single-arm trial (SAT) —conducted in Chinese patients after consultation with the CDE to reach consensus. Since 2012, the CDE has issued 61 guidance to support anti-tumor drug R&D and address the technical challenges. This has contributed to the improvement of anti-tumor drug review framework in China. Chidamide (Epidaza®, CS055) represents the first drug to be granted conditional approval based on an SAT [1]. It offers a treatment option for patients suffering from refractory, relapsed peripheral T-cell lymphoma who lack alternative therapies. Subsequently, numerous innovative anti-tumor drugs received conditional approvals. Statistical data show that from May 2014 to May 2021, a total of 19 drugs for 26 indications were granted conditional approvals [2]. SATs inherently carry uncertainties that may pose additional risks to patients. To address this, the CDE has issued three guidance [3-5] which detail the regulatory considerations and technical requirements for the use of SATs in NDAs. SATs, as pivotal studies, must be executed with scientific precision and prudence with a clear and well-articulated drug action mechanism. SATs should be acceptable only in specific scenarios, such as when control studies are infeasible or when the drug exhibits significantly superior efficacy. Moreover, it is advocated to undertake confirmatory studies as early as possible to mitigate the risk of patients being exposed to drugs with uncertain efficacy and safety profiles. On August 25, 2023, the NMPA issued the "Procedures for Review and Approval of Conditional Approval Applications for Marketed Drugs (interim) (Revised Draft for Public Comments)" [6]. It explicitly stipulates that a confirmatory study should be completed within 4 years after the conditional approval. Evidence from the US FDA demonstrates that it is feasible to complete a confirmatory study within 4 years post-marketing if the confirmatory study is to be commenced once an accelerated approval is granted [7]. Biomarkers serve as crucial instruments for achieving precision therapy. From 2010 to 2023, a total of 109 NDAs for 73 distinct anti-tumor drugs incorporated biomarkers to accurately identify the patient demography for therapeutic intervention [8]. As a novel cognitive paradigm for disease identification, the "pan-tumor" classification aggregates diverse tumors into a singular disease category, considering their genesis. This approach is dedicated to the pursuit of universal therapeutic methodologies [9]. As of February 2024, the NMPA has approved 7 drugs for "pan-tumor", including Envafolimab, Tislelizumab, Serplulimab, Larotrectinib, Pucotenlimab, Entrectinib and Pembrolizumab. The approvals of these drugs underscore the ongoing evolution of clinical practice in the field of oncotherapy in China [8]. Patients suffering from various types of tumors exhibit distinct age distributions and organ function. The CDE has issued several guidances (such as the Guidance for the Application of Physiological Pharmacokinetics Models in Drug R&D for Pediatric Populations) [10] to emphasize research among different populations and to enhance the diversity of subjects, thereby providing more reference information for the post-marketing change management of drugs. Recruiting patients at different stages of cancer also reflects the diversity of the population. It is a classic practice to sequential progress from the later-line to the front-line population. However, this R&D strategy results in the front-line patients being deprived of timely access to new drugs. Consequently, we advocate for the initiation of development in the front-line as soon as efficacy is observed in later-line patients. Sometimes, developing drugs in early-stage tumors is of great clinical value. For instance, immunotherapy may have more pronounced therapeutic effects in early-stage patients who have not yet undergone immune function deterioration [11]. It is important that the control group in a clinical trial accurately reflects the most efficacious treatment options currently accessible to the intended patients in real-world clinical settings. Only under these conditions can the findings of the trial truly reveal the clinical value of the new drug. Although some imported drugs received approvals in China, their adoption by the Chinese population did not make much difference to the therapeutics landscape due to economic and other burdens. As such, the urgent issue for patients is to receive drugs that are both efficacious and easily accessible. Accordingly, the CDE does not require a head-to-head comparison with imported drugs. For example, since Trastuzumab was approved in China in 2002, its widespread clinical adoption was constrained by the high price. Consequently, in the clinical trial of Inetetamab, China's first innovative monoclonal antibody targeting human epidermal growth factor receptor 2 (HER2), Vinorelbine was selected as the control drug in the randomized controlled trial (RCT) rather than Trastuzumab. The outcomes of this RCT provided support for the approval of Inetetamab in China [12]. With the emergence of innovative drugs and the increase of imported drugs in China, Chinese clinical practices are gradually improving, and the gap between clinical practices in China and in other countries is gradually narrowing. As clinical practice evolves, regulatory requirements are also changing accordingly. In 2020, the CDE issued the "Guidance for Clinical R&D of Anti-tumor Drugs Oriented by Clinical Value [13]". This document elucidates that innovative drug development should aim highly to provide patients with better (more effective, safer, or more convenient) treatment options. For example, with the approvals of multiple domestic monoclonal antibodies targeting programmed cell death protein 1 (PD-1), the CDE now requests that the combination of anti-PD-1 with chemotherapy, rather than chemotherapy alone, should be employed as a control group in the RCT study for first-line therapy of late-stage non-small cell lung cancer. In China, the new "Provisions for Drug Registration" [14] and the accompanying "Guidance for Conditional Approval of Drugs for Marketing (interim) [15]" stipulate that the selection of surrogate endpoints should be based on their predictive capacity for clinical benefit. For malignant tumors, overall survival (OS) is the gold standard for evaluating the efficacy of drugs. Using appropriate surrogate endpoints can expedite the introduction of drugs into the market, thereby permitting patients to access novel therapies earlier. It is essential that these surrogate endpoints can predict clinical benefit, and their association with OS in the domain of anti-tumor drugs is contingent upon the intrinsic properties of the tumor. The CDE has promulgated guidance for the selection of surrogate endpoints in clinical trials [16, 17]. In instances where the progression of certain tumors is notably rapid, a significant extension of progression-free survival (PFS) is deemed a clinical benefit. Therefore, it is considered appropriate to use PFS as the primary endpoint. A phase III RCT on patients with hormone receptor-positive metastatic breast cancer who had not responded to previous endocrine therapy revealed that the combination of Dalpiciclib, the first domestic cyclin-dependent kinase 4/6 inhibitor, with the elective oestrogen receptor degrader Fulvestrant significantly prolonged the PFS compared to Fulvestrant administered as a monotherapy (15.7 months vs. 7.2 months, hazard ratio of 0.42), with a prolonged OS [18]. Based on the results of this study, the NMPA approved Dalpiciclib for patients with recurrent or metastatic breast cancer in 2021. Both tumor and anti-tumor therapies cause significant pain in patients and severely impact their quality of life. Therefore, it is recommended that patient-reported outcomes (PRO) be adopted as an evaluation metric of clinical benefit. Although PRO has not yet been used as a primary endpoint for anti-tumor drugs, it helps explain clinical data that cannot be revealed by other traditional assessment metrics. Since China started the reforms in the drug review and approval system in 2015, the number of approvals of new drugs has been on the rise, with a steady increase in the number of applications that are globally synchronized. These achievements have reduced the disparity between domestic and international clinical practices, allowing Chinese patients to receive advanced therapeutic drugs and making it easier for pharmaceutical companies to synchronize global R&D strategies. The accelerated R&D and launch of new drugs will ultimately reshape the landscape of tumor therapies, bringing more and diverse treatment options to patients in China. Moving forward, China's drug regulatory authorities are committed to advancing regulatory innovation for anti-tumor drugs to align with the evolving clinical treatment needs and drug R&D demands. We will introduce and integrate advanced international evaluation methods to refine the drug approval process. Regulatory innovation will prioritize the drugs targeting rare and pediatric tumors. We aim to enhance R&D efficiency and facilitate effective treatments through policy support. Additionally, we will promote the convergence of R&D and clinical application of anti-tumor drugs to advance China's anti-tumor drug industry. China's drug regulatory authorities will remain committed to offering a greater number of high-quality, safe, and effective therapeutic drugs for cancer patients. Research concept and design: Jun Ma and Zhimin Yang. Collection and/or assembly of data and policy: Ling Tang, Yuanyuan Song, Analysis and interpretation of data and policy: Ling Tang, Yuanyuan Song, Hong Zhang, Ruimin Hao, Xin Tong, Xing Ai. Article written: Ling Tang. All authors approved the final manuscript. Not applicable. The authors declare that they have no conflicts of interest. Not applicable. Not applicable. The datasets used in the current study are available from the corresponding author upon reasonable request.
Abstract Background Subarachnoid hemorrhage (SAH) is a severe stroke subtype that lacks effective treatment. Exosomes derived from human dental pulp stem cells (DPSCs) are a promising acellular therapeutic strategy for neurological diseases. However, the therapeutic effects of DPSC-derived exosomes (DPSC-Exos) on SAH remain unknown. In this study, we investigated the therapeutic effects and mechanisms of action of DPSC-Exos in SAH. Materials and Methods SAH was established using 120 male Sprague-Dawley rats. One hour after SAH induction, DPSC-Exos were administered via tail vein injection. To investigate the effect of DPSC-Exos, SAH grading, short-term and long-term neurobehavioral assessments, brain water content, western blot (WB), immunofluorescence staining, Nissl staining, and HE staining were performed. The role of miR-197-3p/FOXO3 in regulating pyroptosis was demonstrated through miRNA sequencing, bioinformatics analysis, and rescue experiments. The SAH model in vitro was established by stimulating BV2 cells with hemoglobin (Hb) and the underlying mechanism of DPSC-Exos was investigated through WB and Hoechst/PI staining. Results The expressions of pro-inflammatory cytokines (IL-1β, IL-6, and TNF-α) were increased after SAH. DPSC-Exos alleviated brain edema and neuroinflammation by inhibiting the expression of FOXO3 and reducing NLRP3 inflammasome activation, leading to improved neurobehavioral functions at 24 h after SAH. In vitro, the expression of the NLRP3 inflammasome components (NLRP3 and caspase1-p20), GSDMD-N, and IL-18 was inhibited in BV2 cells pretreated with DPSC-Exos. Importantly, DPSC-Exos overexpressing miR-197-3p had a more obvious protective effect than those from NC-transfected DPSCs, while those from DPSCs transfected with the miR-197-3p inhibitor had a weaker protective effect. Functional studies indicated that miR-197-3p bound to the 3ʹ-untranslated region of FOXO3, inhibiting its transcription. Furthermore, the overexpression of FOXO3 reversed the protective effects of miR-197-3p. Conclusions DPSC-Exos inhibited activation of the NLRP3 inflammasome and related cytokine release via the miR-197-3p/FOXO3 pathway, alleviated neuroinflammation, and inhibited microglial pyroptosis. These findings suggest that using DPSC-Exos is a promising therapeutic strategy for SAH. .
Objective Recently, a randomised controlled trial (DIRECT-MT) demonstrated that mechanical thrombectomy (MT) was non-inferior to MT with intravenous alteplase as to the functional outcomes. This study aims to investigate whether MT alone is cost-effective compared with MT with alteplase in China. Methods A Markov decision analytic model was built from the Chinese healthcare perspective using a lifetime horizon. Probabilities, costs and outcomes data were obtained from the DIRECT-MT trial and other most recent/comprehensive literature. Base case calculation was conducted to compare the costs and effectiveness between MT alone and MT with alteplase. One-way and probabilistic sensitivity analyses were performed to evaluate the robustness of the results. Results MT alone had a lower cost and higher effectiveness compared with MT with alteplase. The probabilistic sensitivity analysis demonstrated that, over a lifetime horizon, MT alone had a 99.5% probability of being cost-effective under the willingness-to-pay threshold of 1× gross domestic product per capita in China based on data obtained from the DIRECT-MT trial. These results remained robust under one-way sensitivity analysis. Conclusions MT alone was cost-effective compared with MT with alteplase in China. However, cautions are needed to extend this conclusion to regions outside of China.
Background:Limited research has been conducted on laparoscopic partial nephrectomy for kidney tuberculosis.This study aimed to evaluate the effectiveness of the skirted continuous suture technique in laparoscopic partial nephrectomy for localized renal tuberculosis. Material/Methods:Five patients with kidney tuberculosis underwent standard retroperitoneal laparoscopic partial nephrectomy after computed tomography evaluation.The skirted continuous suture technique was utilized during the procedure.This retrospective study analyzed the outcomes of these patients who received treatment between January 2011 and December 2020 at Beijing Tsinghua Changgung Hospital and Eighth Medical Center of Chinese People's Liberation Army General Hospital. Results:The surgical success rate was 100%.Renal function was well preserved, with a decrease of glomerular filtration rate by 9.6±9.0ml/min.Only 1 patient experienced postoperative urinous infiltration and lymphatic fistula, while the others did not have any surgical complications.Antituberculous therapy was continued postoperatively, and 1 patient had recurrence during follow-up. Conclusions:The laparoscopic continuous suturing technique offers a reliable and straightforward method for extensively closing incision edges of the renal parenchyma in laparoscopic surgery.It contributes to the improved efficacy and safety of treating localized renal tuberculosis with exceptional application.
To investigate the long-term clinical and angiographic outcomes and their related predictors in endovascular treatment (EVT) of small (<5 mm) ruptured intracranial aneurysms (SRA).The study retrospectively reviewed patients with SRAs who underwent EVT between September 2011 and December 2016 in two Chinese stroke centers. Medical charts and telephone call follow-up were used to identify the overall unfavorable clinical outcomes (OUCO, modified Rankin score ≤2) and any recanalization or retreatment. The independent predictors of OUCO and recanalization were studied using univariate and multivariate analyses. Multivariate Cox proportional hazards models were used to identify the predictors of retreatment.In this study 272 SRAs were included with a median follow-up period of 5.0 years (interquartile range 3.5-6.5 years) and 231 patients with over 1171 aneurysm-years were contacted. Among these, OUCO, recanalization, and retreatment occurred in 20 (7.4%), 24 (12.8%), and 11 (7.1%) patients, respectively. Aneurysms accompanied by parent vessel stenosis (AAPVS), high Hunt-Hess grade, high Fisher grade, and intraoperative thrombogenesis in the parent artery (ITPA) were the independent predictors of OUCO. A wide neck was found to be a predictor of recanalization. The 11 retreatments included 1 case of surgical clipping, 6 cases of coiling, and 4 cases of stent-assisted coiling. A wide neck and AAPVS were the related predictors.The present study demonstrated relatively favorable clinical and angiographic outcomes in EVT of SRAs in long-term follow-up of up to 5 years. THE AAPVS, as a morphological indicator of the parent artery for both OUCO and retreatment, needs further validation.
The heat shock protein 70 gene(hsp70) from penguin pearl oyster Pteria penguin was cloned using techniques of homological cloning and anchored PCR.The full length of cDNA sequence is 2 308 bp,containing a 3'UTR(untranslated region) of 234 bp,a 5'UTR of 118 bp,and an ORF of 1 956 bp which encodes a polypeptide of 651 amino acids with an estimated molecular weight of 70.97 kd.There are two glycosylation sites,NKSI and NVSA.Three signature sequences of heat shock protein 70 family (HSP70 family),IDLGTTYS,DLGGGTFD and IVLVGGSTRIPKIQK,were detected in the deduced amino acid sequence.These results,together with blast analysis,indicate that the cDNA sequence cloned in this study is a member of heat shock protein 70 family.Compared with Hepu pearl oyster Pinctada fucata's hsp70 gene,penguin pearl oyster has an amino acid reduced due to an insertion and two deletions of amino acids.The identities between these two pearl oysters are 92% and 79% for amino acid and nucleotide sequences,respectively.Phylogenetic analysis shows that the two pearl oyster species are most closely related,supporting the traditional classification.It is also indicated that the pearl oysters are closely related with Crassostrea oysters instead of scallops.Cloning and comparison of hsp70 genes from different pearl oyster species could be useful in the studies of anti-stress mechanism,tolerance-improvement breeding and evolution for these animals.
As the exact pathogenesis of inflammatory bowel disease (IBD) is not known, there is increasing evidence of clinical trials and animal models that indicate the beneficial effects of probiotics.
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