Gradient-Guided Dynamic Efficient Adversarial Training

Adversarial training is arguably an effective but time-consuming way to train robust deep neural networks that can withstand strong adversarial attacks. As a response to the inefficiency, we propose the Dynamic Efficient Adversarial Training (DEAT), which gradually increases the adversarial iteration during training. Moreover, we theoretically reveal that the connection of the lower bound of Lipschitz constant of a given network and the magnitude of its partial derivative towards adversarial examples. Supported by this theoretical finding, we utilize the gradient's magnitude to quantify the effectiveness of adversarial training and determine the timing to adjust the training procedure. This magnitude based strategy is computational friendly and easy to implement. It is especially suited for DEAT and can also be transplanted into a wide range of adversarial training methods. Our post-investigation suggests that maintaining the quality of the training adversarial examples at a certain level is essential to achieve efficient adversarial training, which may shed some light on future studies.Comment: 14 pages, 8 figure

dbAPIS: a database of anti-prokaryotic immune system genes

Anti-prokary otic immune sy stem (APIS) proteins, typically encoded b y phages, prophages, and plasmids, inhibit prokaryotic immune systems (e.g. restriction modification, to xin-antito xin, CRISPR-Cas). A gro wing number of APIS genes ha v e been characterized and dispersed in the literature. Here w e de v eloped dbAPIS ( https:// bcb.unl.edu/ dbAPIS ), as the first literature curated data repository for experimentally verified APIS genes and their associated protein f amilies. T he k e y features of dbAPIS include: (i) e xperimentally v erified APIS genes with their protein sequences, functional annotation, PDB or AlphaFold predicted str uct ures, genomic context, sequence and str uct ural homologs from different microbiome / virome databases; (ii) classification of APIS proteins into sequence-based families and construction of hidden Mark o v models (HMMs); (iii) user-friendly web interface for data browsing by the inhibited immune system types or by the hosts, and functions for searching and batch downloading of pre-computed data; (iv) Inclusion of all types of APIS proteins (e x cept f or anti-CRISPRs) that inhibit a v ariety of prokary otic defense systems (e.g. RM, TA, CB A SS , Thoeris, Gabija). The current release of dbAPIS contains 41 verified APIS proteins and ∼4400 sequence homologs of 92 families and 38 clans. dbAPIS will facilitate the discovery of novel anti-defense genes and genomic islands in phages, by providing a user-friendly data repository and a web resource for an easy homology search against known APIS proteins

Genome mining for anti-CRISPR operons using machine learning

Motivation: Encoded by (pro-)viruses, anti-CRISPR (Acr) proteins inhibit the CRISPR-Cas immune system of their prokaryotic hosts. As a result, Acr proteins can be employed to develop more controllable CRISPR-Cas genome editing tools. Recent studies revealed that known acr genes often coexist with other acr genes and with phage structural genes within the same operon. For example, we found that 47 of 98 known acr genes (or their homologs) co-exist in the same operons. None of the current Acr prediction tools have considered this important genomic context feature. We have developed a new software tool AOminer to facilitate the improved discovery of new Acrs by fully exploiting the genomic context of known acr genes and their homologs. Results: AOminer is the first machine learning based tool focused on the discovery of Acr operons (AOs). A two-state HMM (hidden Markov model) was trained to learn the conserved genomic context of operons that contain known acr genes or their homologs, and the learnt features could distinguish AOs and non-AOs. AOminer allows automated mining for potential AOs from query genomes or operons. AOminer outperformed all existing Acr prediction tools with an accuracy¼0.85. AOminer will facilitate the discovery of novel anti-CRISPR operons

Different Random Distributions Research on Logistic-Based Sample Assumption

Logistic-based sample assumption is proposed in this paper, with a research on different random distributions through this system. It provides an assumption system of logistic-based sample, including its sample space structure. Moreover, the influence of different random distributions for inputs has been studied through this logistic-based sample assumption system. In this paper, three different random distributions (normal distribution, uniform distribution, and beta distribution) are used for test. The experimental simulations illustrate the relationship between inputs and outputs under different random distributions. Thereafter, numerical analysis infers that the distribution of outputs depends on that of inputs to some extent, and this assumption system is not independent increment process, but it is quasistationary