LF拓扑空间的D_α-导集

在L-fuzzy拓扑空间中,利用Dα-闭集定义了Dα-导集,系统地讨论它的基本性质。

L-fuzzy拓扑空间的可数强F紧性理论研究

利用α-远域族的工具,在L-fuzzy拓扑空间中引进可数强F紧性,研究了可数强F紧性的刻划问题.证明了可数强F紧性是"L-好的推广"、对闭子集遗传以及是F完备映射的逆不变量,同时,系统地研究了可数强F紧性的一些特征性质.

L-fuzzy几乎良紧性的若干性质

进一步研究L-fuzzy几乎良紧性的特征及其与良紧性、近似良紧性、几乎F紧性、可数良紧性和NS闭性等概念之间的关系。证明了L-fuzzy几乎良紧性是L-fuzzy θ-闭遗传的和拓扑不变的等重要性质。

L-模糊集的可数starplus-紧性(英文)

本文研究了在L-拓扑空间中,利用L-拓扑的水平拓扑引入可数starplus-紧性的概念,获得了可数starplus-紧性的性质,并且对一般拓扑中可数starplus-紧性的推广.

可数强F紧集的刻画与性质

借助 α- ω聚点与 α-聚点概念给出可数强 F紧集的两个刻画定理 ,进而讨论可数强 F紧集在 L值 Zadeh型函数下的逆不变性 ,证明了可数强 F紧集与强 F紧集的乘积是可数强 F紧的。

Tuning the molecular size of site-specific interferon-polymer conjugate for optimized antitumor efficacy

The covalent attachment of protein-resistant polymers to therapeutic proteins is a widely used method for extending their in vivo half-lives; however, the effect of molecular weight of polymer on the in vitro and in vivo functions of protein-polymer conjugates has not been well elucidated. Herein we report the effect of molecular weight of poly（oligo（ethylene glycol） methyl ether methacrylate） （POEGMA） on the in vitro and in vivo properties of C-termi- nal interferon-alpha （IFN）-POEGMA conjugates. Increasing the molecular weight of POEGMA decreased the in vitro activity of IFN-ct but increased its thermal stability and in vivo pharmacokinetics. Intriguingly, the in vivo antitumor efficacy of IFN-a was increased by increasing the POEGMA molecular weight from ca. 20 to 60 kDa, but was not further increased by increasing the molecular weight of POEGMA from ca. 60 to 100 kDa due to the neutralization of the improved pharmacokinetics and the reduced in vitro activity. This finding offers a new viewpoint on the molecular size rationale for designing next-generation protein-polymer conjugates, which may benefit patients by reducing admin- istration frequency and adverse reactions, and improving therapeutic efficacy.