端到端模型在自动语音识别中快速更换传统的混合模型。变压器,基于机器翻译任务的自我关注的序列到序列模型,在用于自动语音识别时已经给出了有希望的结果。本文探讨了在培训基于变压器的模型的同时在编码器输入时结合扬声器信息的不同方式,以提高其语音识别性能。我们以每个扬声器的扬声器嵌入形式呈现扬声器信息。我们使用两种类型的扬声器嵌入进行实验:在我们以前的工作中提出的X-Vectors和新颖的S-Vectors。我们向两个数据集报告结果a)肉kel讲座数据库和b)librispeech 500小时分割。NPTEL是一个开源电子学习门户,提供来自印度顶级大学的讲座。通过我们将扬声器嵌入的方法集成到模型中,我们通过基线获得了基线的错误率的改进。
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While the brain connectivity network can inform the understanding and diagnosis of developmental dyslexia, its cause-effect relationships have not yet enough been examined. Employing electroencephalography signals and band-limited white noise stimulus at 4.8 Hz (prosodic-syllabic frequency), we measure the phase Granger causalities among channels to identify differences between dyslexic learners and controls, thereby proposing a method to calculate directional connectivity. As causal relationships run in both directions, we explore three scenarios, namely channels' activity as sources, as sinks, and in total. Our proposed method can be used for both classification and exploratory analysis. In all scenarios, we find confirmation of the established right-lateralized Theta sampling network anomaly, in line with the temporal sampling framework's assumption of oscillatory differences in the Theta and Gamma bands. Further, we show that this anomaly primarily occurs in the causal relationships of channels acting as sinks, where it is significantly more pronounced than when only total activity is observed. In the sink scenario, our classifier obtains 0.84 and 0.88 accuracy and 0.87 and 0.93 AUC for the Theta and Gamma bands, respectively.
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Previous work has shown the potential of deep learning to predict renal obstruction using kidney ultrasound images. However, these image-based classifiers have been trained with the goal of single-visit inference in mind. We compare methods from video action recognition (i.e. convolutional pooling, LSTM, TSM) to adapt single-visit convolutional models to handle multiple visit inference. We demonstrate that incorporating images from a patient's past hospital visits provides only a small benefit for the prediction of obstructive hydronephrosis. Therefore, inclusion of prior ultrasounds is beneficial, but prediction based on the latest ultrasound is sufficient for patient risk stratification.
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Artificial intelligence methods including deep neural networks (DNN) can provide rapid molecular classification of tumors from routine histology with accuracy that matches or exceeds human pathologists. Discerning how neural networks make their predictions remains a significant challenge, but explainability tools help provide insights into what models have learned when corresponding histologic features are poorly defined. Here, we present a method for improving explainability of DNN models using synthetic histology generated by a conditional generative adversarial network (cGAN). We show that cGANs generate high-quality synthetic histology images that can be leveraged for explaining DNN models trained to classify molecularly-subtyped tumors, exposing histologic features associated with molecular state. Fine-tuning synthetic histology through class and layer blending illustrates nuanced morphologic differences between tumor subtypes. Finally, we demonstrate the use of synthetic histology for augmenting pathologist-in-training education, showing that these intuitive visualizations can reinforce and improve understanding of histologic manifestations of tumor biology.
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We consider the problem of data classification where the training set consists of just a few data points. We explore this phenomenon mathematically and reveal key relationships between the geometry of an AI model's feature space, the structure of the underlying data distributions, and the model's generalisation capabilities. The main thrust of our analysis is to reveal the influence on the model's generalisation capabilities of nonlinear feature transformations mapping the original data into high, and possibly infinite, dimensional spaces.
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Partially observable Markov decision processes (POMDPs) provide a flexible representation for real-world decision and control problems. However, POMDPs are notoriously difficult to solve, especially when the state and observation spaces are continuous or hybrid, which is often the case for physical systems. While recent online sampling-based POMDP algorithms that plan with observation likelihood weighting have shown practical effectiveness, a general theory characterizing the approximation error of the particle filtering techniques that these algorithms use has not previously been proposed. Our main contribution is bounding the error between any POMDP and its corresponding finite sample particle belief MDP (PB-MDP) approximation. This fundamental bridge between PB-MDPs and POMDPs allows us to adapt any sampling-based MDP algorithm to a POMDP by solving the corresponding particle belief MDP, thereby extending the convergence guarantees of the MDP algorithm to the POMDP. Practically, this is implemented by using the particle filter belief transition model as the generative model for the MDP solver. While this requires access to the observation density model from the POMDP, it only increases the transition sampling complexity of the MDP solver by a factor of $\mathcal{O}(C)$, where $C$ is the number of particles. Thus, when combined with sparse sampling MDP algorithms, this approach can yield algorithms for POMDPs that have no direct theoretical dependence on the size of the state and observation spaces. In addition to our theoretical contribution, we perform five numerical experiments on benchmark POMDPs to demonstrate that a simple MDP algorithm adapted using PB-MDP approximation, Sparse-PFT, achieves performance competitive with other leading continuous observation POMDP solvers.
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当植物天然产物与药物共容纳时,就会发生药代动力学天然产物 - 药物相互作用(NPDIS)。了解NPDI的机制是防止不良事件的关键。我们构建了一个知识图框架NP-KG,作为迈向药代动力学NPDIS的计算发现的一步。 NP-KG是一个具有生物医学本体论,链接数据和科学文献的全文,由表型知识翻译框架和语义关系提取系统,SEMREP和集成网络和动态推理组成的构建的科学文献的全文。通过路径搜索和元路径发现对药代动力学绿茶和kratom-prug相互作用的案例研究评估NP-KG,以确定与地面真实数据相比的一致性和矛盾信息。完全集成的NP-KG由745,512个节点和7,249,576个边缘组成。 NP-KG的评估导致了一致(绿茶的38.98%,kratom的50%),矛盾(绿茶的15.25%,21.43%,Kratom的21.43%),同等和矛盾的(15.25%)(21.43%,21.43%,21.43% kratom)信息。几种声称的NPDI的潜在药代动力学机制,包括绿茶 - 茶氧化烯,绿茶 - 纳多洛尔,Kratom-Midazolam,Kratom-Quetiapine和Kratom-Venlafaxine相互作用,与已出版的文献一致。 NP-KG是第一个将生物医学本体论与专注于天然产品的科学文献的全文相结合的公斤。我们证明了NP-KG在鉴定涉及酶,转运蛋白和药物的药代动力学相互作用的应用。我们设想NP-KG将有助于改善人机合作,以指导研究人员将来对药代动力学NPDIS进行研究。 NP-KG框架可在https://doi.org/10.5281/zenodo.6814507和https://github.com/sanyabt/np-kg上公开获得。
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通用数据模型解决了标准化电子健康记录(EHR)数据的许多挑战,但无法将其集成深度表型所需的资源。开放的生物学和生物医学本体论(OBO)铸造本体论提供了可用于生物学知识的语义计算表示,并能够整合多种生物医学数据。但是,将EHR数据映射到OBO Foundry本体论需要大量的手动策展和域专业知识。我们介绍了一个框架,用于将观察性医学成果合作伙伴关系(OMOP)标准词汇介绍给OBO铸造本体。使用此框架,我们制作了92,367条条件,8,615种药物成分和10,673个测量结果的映射。域专家验证了映射准确性,并且在24家医院进行检查时,映射覆盖了99%的条件和药物成分和68%的测量结果。最后,我们证明OMOP2OBO映射可以帮助系统地识别可能受益于基因检测的未诊断罕见病患者。
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成像表明临床前和人类肿瘤是异质性的,即单个肿瘤可以表现出多个区域,在正常发育过程中均表现出不同的行为,也可以反应治疗。在对照组肿瘤中观察到的大变化可能会掩盖由于归因于变化原因的歧义而导致的显着治疗作用的检测。由于实验设计的局限性,而不是由于治疗衰竭,这可能会阻碍有效疗法的发展。描述了对成像信号中生物变异和异质性进行建模的改进方法。具体而言,线性泊松建模(LPM)在放疗前和72小时之前评估了两种结直肠癌的异种移植模型,在放疗前和72小时后评估了明显的扩散效率(ADC)的变化。使用基本ADC分布参数的常规t检验分析将测量变化的统计显着性与可实现的变化的统计显着性进行了比较。当LPM应用于治疗的肿瘤时,LPM检测到了高度显着的变化。与常规方法相比,所有肿瘤的分析对于所有肿瘤都很重要,相当于4倍的增益(即等同于样本量大16倍)。相比之下,只有使用t检验在队列水平上检测到极大的变化,从而限制了其在个性化医学中的潜在用途,并增加了测试过程中所需的动物数量。此外,LPM使每个异种移植模型估计响应和非反应组织的相对体积。对处理过的异种移植物的剩余分析提供了质量控制并确定了潜在的异常值,从而提高了对临床相关样本量的LPM数据的信心。
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ICECUBE是一种用于检测1 GEV和1 PEV之间大气和天体中微子的光学传感器的立方公斤阵列,该阵列已部署1.45 km至2.45 km的南极的冰盖表面以下1.45 km至2.45 km。来自ICE探测器的事件的分类和重建在ICeCube数据分析中起着核心作用。重建和分类事件是一个挑战,这是由于探测器的几何形状,不均匀的散射和冰中光的吸收,并且低于100 GEV的光,每个事件产生的信号光子数量相对较少。为了应对这一挑战,可以将ICECUBE事件表示为点云图形,并将图形神经网络(GNN)作为分类和重建方法。 GNN能够将中微子事件与宇宙射线背景区分开,对不同的中微子事件类型进行分类,并重建沉积的能量,方向和相互作用顶点。基于仿真,我们提供了1-100 GEV能量范围的比较与当前ICECUBE分析中使用的当前最新最大似然技术,包括已知系统不确定性的影响。对于中微子事件分类,与当前的IceCube方法相比,GNN以固定的假阳性速率(FPR)提高了信号效率的18%。另外,GNN在固定信号效率下将FPR的降低超过8(低于半百分比)。对于能源,方向和相互作用顶点的重建,与当前最大似然技术相比,分辨率平均提高了13%-20%。当在GPU上运行时,GNN能够以几乎是2.7 kHz的中位数ICECUBE触发速率的速率处理ICECUBE事件,这打开了在在线搜索瞬态事件中使用低能量中微子的可能性。
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