A biosegmentation benchmark for evaluation of bioimage analysis methods

Background: We present a biosegmentation benchmark that includes infrastructure, datasets with associated ground truth, and validation methods for biological image analysis. The primary motivation for creating this resource comes from the fact that it is very difficult, if not impossible, for an end-user to choose from a wide range of segmentation methods available in the literature for a particular bioimaging problem. No single algorithm is likely to be equally effective on diverse set of images and each method has its own strengths and limitations. We hope that our benchmark resource would be of considerable help to both the bioimaging researchers looking for novel image processing methods and image processing researchers exploring application of their methods to biology. Results: Our benchmark consists of different classes of images and ground truth data, ranging in scale from subcellular, cellular to tissue level, each of which pose their own set of challenges to image analysis. The associated ground truth data can be used to evaluate the effectiveness of different methods, to improve methods and to compare results. Standard evaluation methods and some analysis tools are integrated into a database framework that is available online at http://bioimage.ucsb.edu/biosegmentation/ webcite. Conclusion: This online benchmark will facilitate integration and comparison of image analysis methods for bioimages. While the primary focus is on biological images, we believe that the dataset and infrastructure will be of interest to researchers and developers working with biological image analysis, image segmentation and object tracking in general

Using simulated fluorescence cell micrographs for the evaluation of cell image segmentation algorithms

The zip archive contains real images showing macrophages. (ZIP 28979 kb

A review and comparison of breast tumor cell nuclei segmentation performances using deep convolutional neural networks

Abstract: Breast cancer is currently the second most common cause of cancer-related death in women. Presently, the clinical benchmark in cancer diagnosis is tissue biopsy examination. However, the manual process of histopathological analysis is laborious, time-consuming, and limited by the quality of the specimen and the experience of the pathologist. This study's objective was to determine if deep convolutional neural networks can be trained, with transfer learning, on a set of histopathological images independent of breast tissue to segment tumor nuclei of the breast. Various deep convolutional neural networks were evaluated for the study, including U-Net, Mask R-CNN, and a novel network (GB U-Net). The networks were trained on a set of Hematoxylin and Eosin (H&E)-stained images of eight diverse types of tissues. GB U-Net demonstrated superior performance in segmenting sites of invasive diseases (AJI = 0.53, mAP = 0.39 & AJI = 0.54, mAP = 0.38), validated on two hold-out datasets exclusively containing breast tissue images of approximately 7,582 annotated cells. The results of the networks, trained on images independent of breast tissue, demonstrated that tumor nuclei of the breast could be accurately segmented

Optimal Physical Preprocessing for Example-Based Super-Resolution

In example-based super-resolution, the function relating low-resolution images to their high-resolution counterparts is learned from a given dataset. This data-driven approach to solving the inverse problem of increasing image resolution has been implemented with deep learning algorithms. In this work, we explore modifying the imaging hardware in order to collect more informative low-resolution images for better ultimate high-resolution image reconstruction. We show that this "physical preprocessing" allows for improved image reconstruction with deep learning in Fourier ptychographic microscopy. Fourier ptychographic microscopy is a technique allowing for both high resolution and high field-of-view at the cost of temporal resolution. In Fourier ptychographic microscopy, variable illumination patterns are used to collect multiple low-resolution images. These low-resolution images are then computationally combined to create an image with resolution exceeding that of any single image from the microscope. We use deep learning to jointly optimize the illumination pattern with the post-processing reconstruction algorithm for a given sample type, allowing for single-shot imaging with both high resolution and high field-of-view. We demonstrate, with simulated data, that the joint optimization yields improved image reconstruction as compared with sole optimization of the post-processing reconstruction algorithm

Estimating Appearance Models for Image Segmentation via Tensor Factorization

Image Segmentation is one of the core tasks in Computer Vision and solving it often depends on modeling the image appearance data via the color distributions of each it its constituent regions. Whereas many segmentation algorithms handle the appearance models dependence using alternation or implicit methods, we propose here a new approach to directly estimate them from the image without prior information on the underlying segmentation. Our method uses local high order color statistics from the image as an input to tensor factorization-based estimator for latent variable models. This approach is able to estimate models in multiregion images and automatically output the regions proportions without prior user interaction, overcoming the drawbacks from a prior attempt to this problem. We also demonstrate the performance of our proposed method in many challenging synthetic and real imaging scenarios and show that it leads to an efficient segmentation algorithm

MoNuSAC2020:A Multi-Organ Nuclei Segmentation and Classification Challenge

Detecting various types of cells in and around the tumor matrix holds a special significance in characterizing the tumor micro-environment for cancer prognostication and research. Automating the tasks of detecting, segmenting, and classifying nuclei can free up the pathologists' time for higher value tasks and reduce errors due to fatigue and subjectivity. To encourage the computer vision research community to develop and test algorithms for these tasks, we prepared a large and diverse dataset of nucleus boundary annotations and class labels. The dataset has over 46,000 nuclei from 37 hospitals, 71 patients, four organs, and four nucleus types. We also organized a challenge around this dataset as a satellite event at the International Symposium on Biomedical Imaging (ISBI) in April 2020. The challenge saw a wide participation from across the world, and the top methods were able to match inter-human concordance for the challenge metric. In this paper, we summarize the dataset and the key findings of the challenge, including the commonalities and differences between the methods developed by various participants. We have released the MoNuSAC2020 dataset to the public