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Unsymmetric vesicles with a different design on each side for near-infrared fluorescence imaging of tumor tissues

机译:两侧各具不同设计的不对称囊泡,用于肿瘤组织的近红外荧光成像

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摘要

Spherical vesicular assemblies with unsymmetric membranes are prepared from A{3}B-type and AB′-type peptides with different helix senses in the hydrophobic B and B′ blocks under the control of three associated factors: stereo-complex formation, dipole–dipole interactions, and steric effects. [(Sar){26}]{3}-b-(L-Leu-Aib){6} (A{3}BL), (Sar){27}-b-(L-Leu-Aib){6} (ABL), (Sar){28}-b-(D-Leu-Aib){6} (ABD), lipoic-acid terminated ABL (lipoABL), and lipoic-acid terminated ABD (lipoABD) are mixed while keeping equimolar ratios of the total amounts of the right- and the left-handed helices. When A{3}BL exceeds more than 60% of all the right-handed helices of the mixture, the unsymmetric vesicles are formed, as indicated by the selective adsorption of gold nanoparticles on the vesicle surface observed by TEM. The unsymmetric vesicles are also prepared using ICGABL and ICGABD with a near-infrared fluorophore, indocyanine green (ICG), at the terminals of ABL and ABD. The unsymmetric vesicle formation is verified by fluorescence quenching with the addition of In ions to the solution. When these vesicles are injected into tumor-bearing mice, the vesicles are effectively accumulated into tumor tissues via the EPR effect. The unsymmetric vesicle containing ICG at the inward surface induces less IgM production than that with ICG at the outward surface. More stealth vesicles in the blood stream are therefore obtainable by concealing the imaging fluorophores in the vesicle.
机译:在三个相关因素的控制下,由疏水性B和B'嵌段中具有不同螺旋感的A {3} B型和AB'型肽制备具有不对称膜的球形囊泡组件相互作用和空间效应。 [(Sar){26}] {3} -b-(L-Leu-Aib){6}(A {3} BL),(Sar){27} -b-(L-Leu-Aib){6 }(ABL),(Sar){28} -b-(D-Leu-Aib){6}(ABD),硫辛酸终止的ABL(lipoABL)和硫辛酸终止的ABD(lipoABD)混合在一起右旋和左旋螺旋的总量的等摩尔比。当A {3} BL超过混合物的所有右手螺旋的60%以上时,形成不对称的囊泡,如通过TEM观察到的金纳米颗粒在囊泡表面上的选择性吸附所表明的。还使用ICGABL和ICGABD在ABL和ABD的末端使用带有近红外荧光团的吲哚菁绿(ICG)制备不对称囊泡。通过向溶液中添加In离子进行荧光猝灭来验证不对称囊泡的形成。当将这些囊泡注射到荷瘤小鼠中时,这些囊泡通过EPR作用有效地积累在肿瘤组织中。与在外表面上具有ICG的相比,在内表面上包含ICG的非对称囊泡诱导的IgM产生更少。因此,通过隐藏囊泡中的成像荧光团,可以获得血流中更多的隐形囊泡。

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