寡聚T细胞受体能否用作检测感染细胞上病毒肽表位的工具?
Can oligomeric T-cell receptor be used as a tool to detect viral peptide epitopes on infected cells?
作者信息
Anikeeva Nadia, Mareeva Tatiana, Liu Wei, Sykulev Yuri
机构信息
Department of Microbiology and Immunology and Kimmel Cancer Center, BLSB 650, Thomas Jefferson University, Philadelphia, PA 19107, USA.
出版信息
Clin Immunol. 2009 Jan;130(1):98-109. doi: 10.1016/j.clim.2008.08.025. Epub 2008 Oct 8.
Abstract
We have utilized soluble HIV Gag-specific T-cell receptor (TCR) D3 with low affinity and TCR-like antibody 25-D1.16 recognizing its natural peptide-MHC (pMHC) ligand with high affinity to determine how affinity and off-rate of the receptor-pMHC interactions affect the sensitivity of pMHC detection on the cell surface. We found that with soluble TCR cognate pMHCs can be detected only at relatively high cell surface densities when the TCR was oligomerized using either Streptavidin or quantum dot (QD) scaffolds. While the higher affinity probe led to a greater sensitivity of pMHC detection, monomers and oligomers of the probe showed essentially the same detection limit, which is restricted by the sensitivity of standard flow cytometry technique. We have also shown that imaging of QD/TCR specifically bound to cognate pMHC on the cell surface yielded a very bright fluorescent signal that can enhance the sensitivity of viral peptide detection on infected cells.
摘要
我们利用了低亲和力的可溶性HIV Gag特异性T细胞受体(TCR)D3和高亲和力识别其天然肽-主要组织相容性复合体(pMHC)配体的类TCR抗体25-D1.16,以确定受体-pMHC相互作用的亲和力和解离速率如何影响细胞表面pMHC检测的灵敏度。我们发现,当使用链霉亲和素或量子点(QD)支架使TCR寡聚化时,只有在相对较高的细胞表面密度下才能检测到可溶性TCR同源pMHC。虽然较高亲和力的探针导致pMHC检测具有更高的灵敏度,但探针的单体和寡聚体显示出基本相同的检测限,这受到标准流式细胞术技术灵敏度的限制。我们还表明,对细胞表面与同源pMHC特异性结合的QD/TCR进行成像产生了非常明亮的荧光信号,这可以提高对感染细胞上病毒肽检测的灵敏度。
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