Genre
Pay Attention to MLPs
Transformers [1] have become one of the most important architectural innovations in deep learning and have enabled many breakthroughs over the past few years. Here we propose a simple network architecture, gMLP, based on MLPs with gating, and show that it can perform as well as Transformers in key language and vision applications. Our comparisons show that self-attention is not critical for Vision Transformers, as gMLP can achieve the same accuracy. For BERT, our model achieves parity with Transformers on pretraining perplexity and is better on some downstream NLP tasks. On finetuning tasks where gMLP performs worse, making the gMLP model substantially larger can close the gap with Transformers. In general, our experiments show that gMLP can scale as well as Transformers over increased data and compute.
AttrSeg: Open-Vocabulary Semantic Segmentation via Attribute Decomposition-Aggregation
Open-vocabulary semantic segmentation is a challenging task that requires segmenting novel object categories at inference time. Recent works explore vision-language pre-training to handle this task, but suffer from unrealistic assumptions in practical scenarios, i.e., low-quality textual category names. For example, this paradigm assumes that new textual categories will be accurately and completely provided, and exist in lexicons during pre-training. However, exceptions often happen when meet with ambiguity for brief or incomplete names, new words that are not present in the pre-trained lexicons, and difficult-to-describe categories for users. To address these issues, this work proposes a novel attribute decomposition-aggregation framework, AttrSeg, inspired by human cognition in understanding new concepts.
Appendix Potential Negative Societal Impacts
C.3 Other Differences Besides the above discussion, there are some other differences between Daniely [12] and our work. First, they analyze SGD, and we analyze a constrained optimization problem and projected SGD. This may be the reason why we can get a stronger bound on width. In the experiments in Section 5, we observe that SGD performs badly when the width is small (see the first left column in (b), Figure 4). Therefore, we suspect an algorithmic change is needed to train narrow nets with such width (due to the training difficulty), and we indeed propose a new method to train narrow nets. Second, they consider binary {+1, 1}dataset, while our results apply to arbitrary labels. In addition, their proof seems to be highly dependent on the fact that the labels are {+1, 1}, and seems hard to generalize to general labels.
When Expressivity Meets Trainability: Fewer than n Neurons Can Work
Modern neural networks are often quite wide, causing large memory and computation costs. It is thus of great interest to train a narrower network. However, training narrow neural nets remains a challenging task. We ask two theoretical questions: Can narrow networks have as strong expressivity as wide ones? If so, does the loss function exhibit a benign optimization landscape?
Graph Denoising Diffusion for Inverse Protein Folding
Inverse protein folding is challenging due to its inherent one-to-many mapping characteristic, where numerous possible amino acid sequences can fold into a single, identical protein backbone. This task involves not only identifying viable sequences but also representing the sheer diversity of potential solutions. However, existing discriminative models, such as transformer-based auto-regressive models, struggle to encapsulate the diverse range of plausible solutions. In contrast, diffusion probabilistic models, as an emerging genre of generative approaches, offer the potential to generate a diverse set of sequence candidates for determined protein backbones. We propose a novel graph denoising diffusion model for inverse protein folding, where a given protein backbone guides the diffusion process on the corresponding amino acid residue types. The model infers the joint distribution of amino acids conditioned on the nodes' physiochemical properties and local environment. Moreover, we utilize amino acid replacement matrices for the diffusion forward process, encoding the biologically meaningful prior knowledge of amino acids from their spatial and sequential neighbors as well as themselves, which reduces the sampling space of the generative process. Our model achieves state-of-the-art performance over a set of popular baseline methods in sequence recovery and exhibits great potential in generating diverse protein sequences for a determined protein backbone structure.