弱对齐的跨光谱人脸检测

跨光谱人脸检测在活体人脸识别、体温筛查等领域有着重要的应用价值.众所周知,可见光人脸易于检测,然而红外人脸难于检测,因此借助可见光图像的人脸检测结果进而完成红外人脸检测是一种有效的解决方案.但是跨光谱图像之间不可避免的存在偏差,导致检测精度不高.为了解决这一问题,提出了一种弱对齐跨光谱图像的人脸检测算法,该方法基于跨光谱图像之间的偏差设计了候选框布置策略,并在此基础上提出了跨光谱特征表示方法用于选取最优候选框.此外,本文还构建了一个跨光谱人脸数据集.最后,在跨光谱人脸数据集和OTCBVS人脸数据集上的实验结果证明,该方法能够较好地完成红外图像人脸检测任务.

双重注意力机制下的跨光谱虹膜识别优化算法

跨光谱虹膜识别任务,通常是指匹配不同光谱下采集的虹膜图像,针对光谱域变化对虹膜识别率影响的问题,提出一种基于双重注意力机制下的跨光谱虹膜识别优化算法。该算法首先通过浅层网络的特征提取,将可见光与近红外光谱域中的浅层特征送入各自的专有外部注意力模块进行优化,以分别存储各自光谱域中虹膜样本数据集的特有信息,随后将优化后的浅层特征送入共享的深度特征提取网络,再将深度特征先后送入改进的空间注意力模块和外部注意力模块,强化虹膜关键特征信息的表达,同时以改进的加性角间距损失函数ArcFace Loss(additive angular margin loss)动态调整对于困难样本的优化力度。该算法在PolyU数据集上进行了实验验证,等错误率EER(equal error rate)达到了0.23%,分离度达到了8.56,该实验结果与跨光谱虹膜识别SOTA(state-of-the-art)算法进行了比较,远高于其他主流算法。

Analysis of the Secondary Structure of the Transmembrane Domain of SARS CoV E Protein Using FTIR Spectroscopy

One of the major obstacles facing the field of structural biology in the post genomic era is the inherent difficulty of analyzing the structure of membrane proteins under native conditions. The method of choice for studying such proteins is FTIR spectroscopy. Following the outbreaking of the severe acute respiratory syndrome （SARS） virus, in 2003, extensive work has been directed at elucidating the structure of the E transmembrane proteins of the SARS coronavirus. In this study, the secondary structure of the transmembrane a-helical bundles was analysised using the biophysical method site specific infrared dichroism （SSID）. Sixteen amino acids were isotopically labeled with （~3C=180） at different positions of the primary structure of the synthesized E protein CoV. The secondary structure was studied using Attenuated Total Internal Reflection （ATR） FTIR spectroscopy. Based on our findings, the presence of two possible H-bonding interactions between the carbonyl oxygen of two residues 26 and 31 （Phe and Leu） respectively with water molecules which may be trapped within the helix structure were postulatesed. These interactions may cause a change in this structure.