RESUMO
Curvilinear structures frequently appear in microscopy imaging as the object of interest. Crystallographic defects, i.e dislocations, are one of the curvilinear structures that have been repeatedly investigated under transmission electron microscopy (TEM) and their 3D structural information is of great importance for understanding the properties of materials. 3D information of dislocations is often obtained by tomography which is a cumbersome process since it is required to acquire many images with different tilt angles and similar imaging conditions. Although, alternative stereoscopy methods lower the number of required images to two, they still require human intervention and shape priors for accurate 3D estimation. We propose a fully automated pipeline for both detection and matching of curvilinear structures in stereo pairs by utilizing deep convolutional neural networks (CNNs) without making any prior assumption on 3D shapes. In this work, we mainly focus on 3D reconstruction of dislocations from stereo pairs of TEM images.
RESUMO
We present an Unsupervised Domain Adaptation strategy to compensate for domain shifts on Electron Microscopy volumes. Our method aggregates visual correspondences-motifs that are visually similar across different acquisitions-to infer changes on the parameters of pretrained models, and enable them to operate on new data. In particular, we examine the annotations of an existing acquisition to determine pivot locations that characterize the reference segmentation, and use a patch matching algorithm to find their candidate visual correspondences in a new volume. We aggregate all the candidate correspondences by a voting scheme and we use them to construct a consensus heatmap: a map of how frequently locations on the new volume are matched to relevant locations from the original acquisition. This information allows us to perform model adaptations in two different ways: either by a) optimizing model parameters under a Multiple Instance Learning formulation, so that predictions between reference locations and their sets of correspondences agree, or by b) using high-scoring regions of the heatmap as soft labels to be incorporated in other domain adaptation pipelines, including deep learning ones. We show that these unsupervised techniques allow us to obtain high-quality segmentations on unannotated volumes, qualitatively consistent with results obtained under full supervision, for both mitochondria and synapses, with no need for new annotation effort.