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在肽识别探针中掺入额外的氨基酸以提高基于电化学肽的传感器的特异性和选择性。

Incorporation of extra amino acids in peptide recognition probe to improve specificity and selectivity of an electrochemical peptide-based sensor.

机构信息

University of Nebraska-Lincoln, 651 Hamilton Hall, Lincoln, NE 68588-0304, USA.

University of Nebraska-Lincoln, 651 Hamilton Hall, Lincoln, NE 68588-0304, USA.

出版信息

Anal Chim Acta. 2015 Jul 30;886:157-64. doi: 10.1016/j.aca.2015.05.037. Epub 2015 Jul 7.

Abstract

We investigated the effect of incorporating extra amino acids (AA) at the n-terminus of the thiolated and methylene blue-modified peptide probe on both specificity and selectivity of an electrochemical peptide-based (E-PB) HIV sensor. The addition of a flexible (SG)3 hexapeptide is, in particular, useful in improving sensor selectivity, whereas the addition of a highly hydrophilic (EK)3 hexapeptide has shown to be effective in enhancing sensor specificity. Overall, both E-PB sensors fabricated using peptide probes with the added AA (SG-EAA and EK-EAA) showed better specificity and selectivity, especially when compared to the sensor fabricated using a peptide probe without the extra AA (EAA). For example, the selectivity factor recorded in the 50% saliva was ∼2.5 for the EAA sensor, whereas the selectivity factor was 7.8 for both the SG-EAA and EK-EAA sensors. Other sensor properties such as the limit of detection and dynamic range were minimally affected by the addition of the six AA sequence. The limit of detection was 0.5 nM for the EAA sensor and 1 nM for both SG-EAA and EK-EAA sensors. The saturation target concentration was ∼200 nM for all three sensors. Unlike previously reported E-PB HIV sensors, the peptide probe functions as both the recognition element and antifouling passivating agent; this modification eliminates the need to include an additional antifouling diluent, which simplifies the sensor design and fabrication protocol.

摘要

我们研究了在硫醇化和亚甲蓝修饰的肽探针的 N 端掺入额外氨基酸 (AA) 对基于电化学肽的 (E-PB) HIV 传感器的特异性和选择性的影响。添加柔性 (SG)3 六肽特别有助于提高传感器的选择性,而添加高度亲水的 (EK)3 六肽已被证明可有效提高传感器的特异性。总体而言,使用添加 AA 的肽探针制备的两种 E-PB 传感器 (SG-EAA 和 EK-EAA) 显示出更好的特异性和选择性,尤其是与未添加额外 AA 的肽探针制备的传感器相比 (EAA)。例如,EAA 传感器在 50%唾液中记录的选择性因子约为 2.5,而 SG-EAA 和 EK-EAA 传感器的选择性因子分别为 7.8。添加六个 AA 序列对其他传感器特性(如检测限和动态范围)的影响最小。EAA 传感器的检测限为 0.5 nM,SG-EAA 和 EK-EAA 传感器的检测限均为 1 nM。所有三个传感器的饱和目标浓度约为 200 nM。与之前报道的基于 E-PB 的 HIV 传感器不同,肽探针既作为识别元件又作为抗污钝化剂;这种修饰消除了包含额外抗污稀释剂的需要,简化了传感器设计和制造协议。

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