hydroxyethyl starch

  • 文章类型: Journal Article
    肿瘤细胞的适应性抗氧化系统,主要是谷胱甘肽(GSH)和硫氧还蛋白(TRX)网络,严重损害光动力疗法(PDT)的效力和抗肿瘤免疫反应。这里,多级氧化还原稳态纳米破坏剂(Phy@HES-IR),由羟乙基淀粉(HES)-新吲哚菁绿(IR820)缀合物与physcon(Phy)整合,戊糖磷酸途径(PPP)的抑制剂,合理设计以实现PDT引发的癌症免疫疗法。在这个纳米分裂器中,Phy通过抑制6-磷酸葡萄糖酸脱氢酶(6PGD)活性有效地消耗肿瘤细胞的细胞内GSH。同时,首次观察到修饰的IR820-NH2分子不仅发挥PDT作用,而且通过抑制硫氧还蛋白氧化酶(TRXR)活性来干扰TRX抗氧化途径。肿瘤细胞的两种主要抗氧化剂途径的同时弱化有利于最大化由HES-IR缀合物诱导的PDT功效。凭借等离子体膨胀器HES的优异保护能力,Phy@HES-IR可以在血液循环中保持稳定并有效地富集在肿瘤区域。因此,PDT和代谢调节协同诱导免疫原性细胞死亡,它不仅抑制了原发性肿瘤,而且刺激了有效的抗肿瘤免疫力,以抑制4T1荷瘤小鼠中远处肿瘤的生长。
    The adaptive antioxidant systems of tumor cells, predominantly glutathione (GSH) and thioredoxin (TRX) networks, severely impair photodynamic therapy (PDT) potency and anti-tumor immune responses. Here, a multistage redox homeostasis nanodisruptor (Phy@HES-IR), integrated by hydroxyethyl starch (HES)-new indocyanine green (IR820) conjugates with physcion (Phy), an inhibitor of the pentose phosphate pathway (PPP), is rationally designed to achieve PDT primed cancer immunotherapy. In this nanodisruptor, Phy effectively depletes intracellular GSH of tumor cells by inhibiting 6-phosphogluconate dehydrogenase (6PGD) activity. Concurrently, it is observed for the first time that the modified IR820-NH2 molecule not only exerts PDT action but also interferes with TRX antioxidant pathway by inhibiting thioredoxin oxidase (TRXR) activity. The simultaneous weakening of two major antioxidant pathways of tumor cells is favorable to maximize the PDT efficacy induced by HES-IR conjugates. By virtue of the excellent protecting ability of the plasma expander HES, Phy@HES-IR can remain stable in the blood circulation and efficiently enrich in the tumor region. Consequently, PDT and metabolic modulation synergistically induced immunogenic cell death, which not only suppressed primary tumors but also stimulated potent anti-tumor immunity to inhibit the growth of distant tumors in 4T1 tumor-bearing mice.
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  • 文章类型: Journal Article
    尽管类黄酮化合物表现出多种药理活性,它们的临床应用受到低口服生物利用度的限制,因为它们的溶解性差。纳米晶体(NC)代表了提高类黄酮口服生物利用度的极好策略。羟乙基淀粉(HES),一种用作血浆扩张器的生物材料化合物,可能是制备类黄酮NCs的理想稳定剂材料。
    HES用于稳定类黄酮纳米晶体(NC),使用木犀草素(LUT)作为模型药物。经过全面表征,冷冻干燥和储存稳定性,溶解度,肠道吸收,药代动力学,研究了优化的HES稳定的LUTNC(LUT-HESNC)的体内抗高尿酸作用。
    制备的均匀LUT-HESNC的平均粒径为191.1±16.8nm,zeta电位约为-23mV,药物包封率98.52±1.01%,载药量为49.26±0.50%。冻干的LUT-HESNC粉末表现出良好的再分散性和9个月的储存稳定性。值得注意的是,与粗药相比,LUT-HESNC表现出改善的饱和溶解度(7.49倍),增加药物溶出速率,提高Caco-2细胞摄取(2.78倍)和口服生物利用度(Fr=355.7%)。药效学研究表明,LUT-HESNCs可显著降低高尿酸血症小鼠的血尿酸水平69.93%,改善肾脏损害。
    HES是难溶性类黄酮NC的潜在稳定剂,为这些化合物的临床应用提供了有希望的策略。LUT-HESNC可能是高尿酸血症治疗的替代或补充策略。
    UNASSIGNED: Although flavonoid compounds exhibit various pharmacological activities, their clinical applications are restricted by low oral bioavailability owing to their poor solubility. Nanocrystals (NCs) represent an excellent strategy for enhancing the oral bioavailability of flavonoids. Hydroxyethyl starch (HES), a biomaterial compound used as a plasma expander, could be an ideal stabilizer material for preparing flavonoid NCs.
    UNASSIGNED: HES was used to stabilize flavonoid nanocrystals (NCs), using luteolin (LUT) as a model drug. After full characterization, the freeze-drying and storage stability, solubility, intestinal absorption, pharmacokinetics, and in vivo anti-hyperuricemic effect of the optimized HES-stabilized LUT NCs (LUT-HES NCs) were investigated.
    UNASSIGNED: Uniformed LUT-HES NCs were prepared with mean particle size of 191.1±16.8 nm, zeta potential of about -23 mV, drug encapsulation efficiency of 98.52 ± 1.01%, and drug loading of 49.26 ± 0.50%. The freeze-dried LUT-HES NCs powder showed good re-dispersibility and storage stability for 9 months. Notably, compared with the coarse drug, LUT-HES NCs exhibited improved saturation solubility (7.49 times), increased drug dissolution rate, enhanced Caco-2 cellular uptake (2.78 times) and oral bioavailability (Fr=355.7%). Pharmacodynamic studies showed that LUT-HES NCs remarkably lowered serum uric acid levels by 69.93% and ameliorated renal damage in hyperuricemic mice.
    UNASSIGNED: HES is a potential stabilizer for poorly soluble flavonoid NCs and provides a promising strategy for the clinical application of these compounds. LUT-HES NCs may be an alternative or complementary strategy for hyperuricemia treatment.
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  • 文章类型: Journal Article
    有效的EPR和肿瘤渗透是当前纳米医学治疗的瓶颈。利用Comosol软件分析了不同形状的纳米粒子(NPs)的运动过程,从血管到肿瘤组织,来解决这个问题。通过计算,海胆状NP比球形NP承受更高的阻力,促进它们的EPR和肿瘤渗透效应。因此,通过利用ICG响应近红外光(NIR)的不稳定性,制备了类海胆的吲哚菁绿色负载的羟乙基淀粉胆固醇(ICG@HES-CH)NP。在NIR暴露后,ICG降解并部分分解ICG@HES-CHNPs,形态从球形转变为海胆状。长春新碱(VC),作为一种模范药物,装载在海胆样ICG@HES-CHNP中用于治疗淋巴瘤。A20淋巴瘤细胞和3T3-A20肿瘤类器官用于研究形状对NPs细胞摄取的影响,渗透途径,和细胞毒性。这表明海胆样ICG@HES-CHNPs主要通过细胞间途径转运穿过细胞外基质,容易到达深部肿瘤部位并获得较高的细胞毒性。体内VC分布和抗肿瘤结果表明,海胆样NPs增加了VC的EPR和穿透能力,降低VC的神经毒性和优越的抗肿瘤后果。因此,海胆样ICG@HES-CHNPs具有巨大的翻译潜力,可用作抗癌治疗中的化疗纳米载体。
    Effective EPR and tumor penetration are bottlenecks in current nanomedicine therapy. Comosol software was utilized to analyze the motion process of nanoparticles (NPs) with different shapes, from blood vessels to tumor tissue, to address this. By calculation, urchin-like NPs experienced higher drag forces than spherical NPs, facilitating their EPR and tumor penetration effects. Thus, urchin-like indocyanine green-loaded hydroxyethyl starch-cholesterol (ICG@HES-CH) NPs were prepared by leveraging the instability of ICG responding to near-infrared light (NIR). Upon NIR exposure, ICG degraded and partly disintegrated ICG@HES-CH NPs, and its morphology transformed from spherical to urchin-like. Vincristine (VC), as a model drug, was loaded in urchin-like ICG@HES-CH NPs for the treatment of lymphoma. A20 lymphoma cells and 3T3-A20 tumor organoids were employed to investigate the influence of shape on NPs\' cellular uptake, penetration pathway, and cytotoxicity. It demonstrated that urchin-like ICG@HES-CH NPs mainly transport across the extracellular matrix through intercellular pathways, easily reaching the deep tumor sites and achieving higher cytotoxicity. In vivo VC distribution and anti-tumor results indicated that urchin-like NPs increased VC EPR and penetration ability, lowering VC neurotoxicity and superior anti-tumor effect. Therefore, urchin-like ICG@HES-CH NPs have great translational potential to be used as chemotherapeutic nanocarriers in anticancer therapy.
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  • 文章类型: Journal Article
    癌症是世界上最致命的疾病之一。尽管已经开发了许多用于癌症治疗的药物,他们仍然受到各种限制,包括治疗效果差,对正常人细胞的毒性,以及多药耐药性的出现。在这项研究中,使用羟乙基淀粉(HES)和亚油酸作为原料制备两亲性LHES聚合物。分析了LHES聚合物中亚油酸基团的含量和取代度。LHES聚合物用于制造携带亚油酸修饰的小檗碱衍生物(L-BBR)的LHES-B纳米颗粒。LHES-B纳米粒显示出高的载药率(29%),在酸性pH条件下(pH=4.5)能快速释放L-BBR。生物学研究表明,LHES-B纳米颗粒显着抑制HepG2细胞的增殖,并表现出比L-BBR更高的细胞毒性。在转基因Tg(fabp10:rtTA2s-M2;TRE2:EGFP-krasv12)斑马鱼模型中,LHES-B纳米颗粒明显抑制krasv12癌基因的表达。这些结果表明,LHES载体可以提高L-BBR的抗癌活性,合成的LHES-B纳米粒子显示出作为抗癌药物的巨大潜力。
    Cancer is one of the most lethal diseases all over the world. Despite that many drugs have been developed for cancer therapy, they still suffer from various limitations including poor treating efficacy, toxicity to normal human cells, and the emergence of multidrug resistance. In this study, the amphiphilic LHES polymers were prepared using hydroxyethyl starch (HES) and linoleic acid as starting materials. The content and substitution degree of linoleic acid groups in LHES polymers were analyzed. The LHES polymers were used for fabricating LHES-B nanoparticles carrying a linoleic acid modified berberine derivative (L-BBR). The LHES-B nanoparticles showed high drug loading efficiency (29%) and could quickly release L-BBR under acidic pH condition (pH = 4.5). Biological investigations revealed that LHES-B nanoparticles significantly inhibited the proliferation of HepG2 cells and exhibited higher cytotoxicity than L-BBR. In a transgenic Tg(fabp10:rtTA2s-M2; TRE2:EGFP-krasv12) zebrafish model, LHES-B nanoparticles obviously inhibited the expression of krasv12 oncogene. These results indicated that LHES carriers could improve the anticancer activity of L-BBR, and the synthesized LHES-B nanoparticles showed great potential as anticancer drug.
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  • 文章类型: Editorial
    暂无摘要。
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  • 文章类型: Journal Article
    我们的研究旨在开发具有氧化还原敏感性和优异的控释性能的聚合物胶束。3,3'-二硫代二丙酸(DTDPA,合成聚合物的缩写:SS)作为ROS(活性氧)响应键和连接臂引入,以将羟乙基淀粉(HES)与齐墩果酸(OA)偶联,导致合成四种不同接枝率的HES-SS-OA。FTIR(傅立叶变换红外光谱)和1HNMR(1H核磁共振光谱)用于验证HES-SS-OA的成功组合。发现聚合物胶束以无定形形式包封OA,如XRD(X射线衍射)和DSC(差示扫描量热法)的结果所示。当OA在HES上的接枝率从7.72%提高到11.75%时,随着聚合物胶束由于增强的疏水性而变得致密,粒径从297.79nm减小到201.39nm。此外,zeta电位从-16.42mv变为-25.78mv,PDI(多分散指数)从0.3649下降到0.2435,临界胶束浓度(CMC)从0.0955mg/mL下降到0.0123mg/mL。红细胞溶血的结果,细胞毒性和细胞摄取表明HES-SS-OA对AML-12细胞具有优异的生物相容性和最小的细胞毒性。在H2O2和GSH存在下,HES-SS-OA的二硫键断裂证实了HES-SS-OA胶束的氧化还原敏感性及其对OA的优异控释性能。这些发现表明,HES-SS-OA将来可能用作预防或辅助治疗炎症的医疗保健药物和药物。
    Our study aimed at developing polymer micelles that possess redox sensitivity and excellent controlled release properties. 3,3\'-dithiodipropionic acid (DTDPA, Abbreviation in synthetic polymers: SS) was introduced as ROS (Reactive oxygen species)response bond and connecting arm to couple hydroxyethyl starch (HES) with oleanolic acid (OA), resulting in the synthesis of four distinct grafting ratios of HES-SS-OA. FTIR (Fourier Transform infrared spectroscopy) and 1H NMR (1H Nuclear magnetic resonance spectra) were used to verify the triumphant combination of HES-SS-OA. Polymer micelles were found to encapsulate OA in an amorphous form, as indicated by the results of XRD (X-ray diffraction) and DSC (Differential scanning calorimetry). When the OA grafting rate on HES increased from 7.72 % to 11.75 %, the particle size decreased from 297.79 nm to 201.39 nm as the polymer micelles became compact due to enhanced hydrophobicity. In addition, the zeta potential changed from -16.42 mv to -25.78 mv, the PDI (polydispersity index) decreased from 0.3649 to 0.2435, and the critical micelle concentration (CMC) decreased from 0.0955 mg/mL to 0.0123 mg/mL. Results of erythrocyte hemolysis, cytotoxicity and cellular uptake illustrated that HES-SS-OA had excellent biocompatibility and minimal cytotoxicity for AML-12 cells. Disulfide bond breakage of HES-SS-OA in the presence of H2O2 and GSH confirmed the redox sensitivity of the HES-SS-OA micelles and their excellent controlled release properties for OA. These findings suggest that HES-SS-OA can be potentially used in the future as a healthcare drug and medicine for the prevention or adjuvant treatment of inflammation.
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  • 文章类型: Journal Article
    肽类药物的降解限制了肽类药物微球的运用。在聚合物降解过程中,肽在水-油界面的结构变化及其在复杂微环境中空间结构的破坏会影响药物的释放和体内生物活性。这项研究表明,向内部水相(W1)中添加羟乙基淀粉(HES)可显着提高司马鲁肽的稳定性,并优化其在PLGA微球中的释放行为。结果表明,这种改善是由于氢键促进的自发放热反应(ΔH=-132.20kJmol-1)。使用水包油包水(W1/O/W2)乳液法将HES掺入内部水相中,得到PLGA微球,包封率为94.38%。此外,具有HES的微球在44天内表现出良好的药物释放控制,不同于在没有HES的微球中缓慢和不完全的释放。在同一时期内,与无HES微球相比,优化的h-MG2制剂实现了更完全的药物释放(83.23%)并防止了30.65%的药物损失。此外,优化的司马鲁肽微球提供了近3周的血糖控制和足够的安全性.总之,内水相中加入HES,提高了司马鲁肽PLGA微球的原位药物稳定性和释放行为,有效增加多肽药物在PLGA微球中的有效载荷。
    The degradation of peptide drugs limits the application of peptide drug microspheres. Structural changes of peptides at the water-oil interface and the destruction of their spatial structure in the complex microenvironment during polymer degradation can affect drug release and in vivo biological activity. This study demonstrates that adding hydroxyethyl starch (HES) to the internal aqueous phase (W1) significantly enhances the stability of semaglutide and optimizes its release behavior in PLGA microspheres. The results showed that this improvement was due to a spontaneous exothermic reaction (ΔH = -132.20 kJ mol-1) facilitated by hydrogen bonds. Incorporating HES into the internal aqueous phase using the water-in-oil-in-water (W1/O/W2) emulsion method yielded PLGA microspheres with a high encapsulation rate of 94.38 %. Moreover, microspheres with HES demonstrated well-controlled drug release over 44 days, unlike the slower and incomplete release in microspheres without HES. The optimized h-MG2 formulation achieved a more complete drug release (83.23 %) and prevented 30.65 % of drug loss compared to the HES-free microspheres within the same period. Additionally, the optimized semaglutide microspheres provided nearly three weeks of glycemic control with adequate safety. In conclusion, adding HES to the internal aqueous phase improved the in-situ drug stability and release behavior of semaglutide-loaded PLGA microspheres, effectively increasing the peptide drug payload in PLGA microspheres.
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  • 文章类型: Journal Article
    胰岛移植是1型糖尿病最有效的治疗策略。在超低温下的长期储存可用于制备足够的良好质量的胰岛以供移植。为了冷冻胰岛,二甲基亚砜(DMSO)是一种常用的渗透冷冻保护剂(CPA)。然而,DMSO的毒性是细胞冷冻保存的主要障碍。已提出羟乙基淀粉(HES)作为替代CPA。为了研究两种非渗透性CPA的影响,我们比较了4%HES130和HES200与10%DMSO的小鼠胰岛产量,生存能力,和葡萄糖刺激的胰岛素分泌(GSIS)。经过一天的文化,在每种溶液中冷冻保存胰岛。冷冻保存三天后,HES130和HES200组的胰岛恢复率明显高于DMSO组。在第1天和第3天,HES200组的胰岛活力也显着高于DMSO组。在第3天,HES130和200组的GSIS刺激指数高于DMSO组。冷冻保存三天后,HES130和HES200均降低了凋亡和坏死相关蛋白的表达,并促进了胰岛的存活。总之,与使用常规CPA相比,使用HES作为CPA改善了冷冻保存的胰岛的存活率和胰岛素分泌。
    Islet transplantation is the most effective treatment strategy for type 1 diabetes. Long-term storage at ultralow temperatures can be used to prepare sufficient islets of good quality for transplantation. For freezing islets, dimethyl sulfoxide (DMSO) is a commonly used penetrating cryoprotective agent (CPA). However, the toxicity of DMSO is a major obstacle to cell cryopreservation. Hydroxyethyl starch (HES) has been proposed as an alternative CPA. To investigate the effects of two types of nonpermeating CPA, we compared 4 % HES 130 and HES 200 to 10 % DMSO in terms of mouse islet yield, viability, and glucose-stimulated insulin secretion (GSIS). After one day of culture, islets were cryopreserved in each solution. After three days of cryopreservation, islet recovery was significantly higher in the HES 130 and HES 200 groups than in the DMSO group. Islet viability in the HES 200 group was also significantly higher than that in the DMSO group on Day 1 and Day 3. Stimulation indices determined by GSIS were higher in the HES 130 and 200 groups than in the DMSO group on Day 3. After three days of cryopreservation, HES 130 and HES 200 both reduced the expression of apoptosis- and necrosis-associated proteins and promoted the survival of islets. In conclusion, the use of HES as a CPA improved the survival and insulin secretion of cryopreserved islets compared with the use of a conventional CPA.
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  • 文章类型: Journal Article
    目的:将胶体添加到体外循环(CPB)泵的引发液中,以维持胶体渗透压并防止液体超负荷。本研究旨在比较6%羟乙基淀粉(HES)130/0.4和林格氏乳酸盐(RL)灌注溶液对接受CPB离体心脏瓣膜手术患者预后的影响。
    方法:这项随机临床试验包括120名接受心脏瓣膜手术的患者,这些被分为两组。RL组患者接受1500mL的RL,RL+HES组给予HES500mL和RL1000mL。
    结果:RL+HES和RL组患者的中位年龄分别为52岁(IQR42-60)和50岁(IQR40-61),分别(p=0.71)。与RL组相比,RL+HES组的手术室和重症监护病房需要输血的病例数也明显高于RL组(RR2.04,95%CI1.50-2.76;p<.01和RR1.42,95%CI1.01-2.01;p=0.05)。与RL组相比,RL+HES术后肌酐水平和血小板计数下降较高(受试者间效应分别为p=.007和p=.038),而急性肾损伤的发生率在组间具有可比性(RR0.66,95%CI0.13-3.30;p=.55).
    结论:在接受CPB心脏瓣膜手术的患者中,与仅RL相比,在RL中添加6%的HES用于启动,在住院期间增加了需要输血的风险。
    OBJECTIVE: Colloids are added to the priming solution of the cardiopulmonary bypass (CPB) pump to maintain colloid osmotic pressure and prevent fluid overload. This study aimed to compare the effects of 6% hydroxyethyl starch (HES) 130/0.4 and ringer\'s lactate (RL) priming solution on patients\' outcomes undergoing isolated heart valve surgery with CPB.
    METHODS: This randomized clinical trial included one hundred and 20 patients undergoing heart valve surgery, and those were allocated into two groups. Patients in the RL group received 1500 mL of RL, and those in the RL + HES group were given 500 mL of HES and 1000 mL of RL.
    RESULTS: The patients\' median age was 52 (IQR 42-60) and 50 (IQR 40-61) years in the RL + HES and the RL group, respectively (p = .71). The number of cases that required blood product transfusion in both the operating room and intensive care unit was also significantly higher in the RL + HES group compared to the RL group (RR 2.04, 95% CI 1.50-2.76; p < .01 and RR 1.42, 95% CI 1.01-2.01; p = .05, respectively). Declines in postoperative creatinine levels and platelet counts were higher in the RL + HES compared to the RL group (between-subjects effect p = .007 and p = .038, respectively), while the incidence of acute kidney injury was comparable between groups (RR 0.66, 95% CI 0.13-3.30; p = .55).
    CONCLUSIONS: Among patients undergoing heart valve surgery with CPB, 6% HES added to RL for priming compared with only RL increased the risk of the need for blood product transfusion over the hospitalization period.
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  • 文章类型: Journal Article
    目的:粒细胞输注(GTX)是中性粒细胞减少症患者严重感染的一种治疗选择。在以往的研究中,羟乙基淀粉(HES)用于增强红细胞沉降以收集粒细胞(GC)。然而,有关于HES的安全问题,和HES在某些国家并不容易获得。因此,我们比较了两种无HES的单采系统的粒细胞计数和GC效率。
    方法:分析2011年7月至2018年3月在我院进行的所有连续GC手术。使用COBE光谱直到2016年2月5日,之后使用光谱。未使用HES。
    结果:进行了26个GC程序,包括使用COBE光谱进行的18和使用光谱光学进行的8。当使用SpectraOptia时,从八个程序中的七个(88%)收集>1×1010个嗜中性粒细胞。尽管基于COBE光谱和基于光谱的GC程序之间的粒细胞产量没有显着差异,光谱的收集效率明显高于COBE光谱(p=0.021)。此外,与基于COBE光谱的GC相比,基于光谱的GC在单采当天的粒细胞产量与外周血中性粒细胞计数的相关性更强。
    结论:我们的结果表明,光谱光学比COBE光谱具有更大的GC效率,即使没有他。GTX可能是严重中性粒细胞减少症的治疗选择,即使在HES不可用的地方。
    OBJECTIVE: Granulocyte transfusion (GTX) is a treatment option for severe infections in patients with neutropenia. In previous studies, hydroxyethyl starch (HES) was used to enhance red blood cell sedimentation for granulocyte collection (GC). However, there are safety concerns about HES, and HES is not readily available in some countries. Therefore, we compared the granulocyte counts and GC efficiency achieved by two apheresis systems without HES.
    METHODS: All consecutive GC procedures performed between July 2011 and March 2018 at our hospital were analysed. COBE Spectra was used until 5 February 2016, and Spectra Optia was used afterwards. HES was not used.
    RESULTS: Twenty-six GC procedures were performed, including 18 performed using COBE Spectra and 8 using Spectra Optia. When Spectra Optia was used, >1 × 1010 neutrophils were collected from seven of the eight (88%) procedures. Although there was no significant difference in the granulocyte yield between COBE Spectra-based and Spectra Optia-based GC procedures, the collection efficiency of Spectra Optia was significantly higher than that of COBE Spectra (p = 0.021). Furthermore, the granulocyte yields of Spectra Optia-based GC tended to be more strongly correlated with the peripheral blood neutrophil count on the day of apheresis than those of COBE Spectra-based GC.
    CONCLUSIONS: Our results suggest that Spectra Optia achieves greater GC efficiency than COBE Spectra, even without HES. GTX may be a therapeutic option for severe neutropenia, even in places where HES is not available.
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