ABSTRACT
Echocardiography is an essential examination for cardiac disease diagnosis, from which anatomical structures segmentation is the key to assessing various cardiac functions. However, the obscure boundaries and large shape deformations due to cardiac motion make it challenging to accurately identify the anatomical structures in echocardiography, especially for automatic segmentation. In this study, we propose a dual-branch shape-aware network (DSANet) to segment the left ventricle, left atrium, and myocardium from the echocardiography. Specifically, the elaborate dual-branch architecture integrating shape-aware modules boosts the corresponding feature representation and segmentation performance, which guides the model to explore shape priors and anatomical dependence using an anisotropic strip attention mechanism and cross-branch skip connections. Moreover, we develop a boundary-aware rectification module together with a boundary loss to regulate boundary consistency, adaptively rectifying the estimation errors nearby the ambiguous pixels. We evaluate our proposed method on the publicly available and in-house echocardiography dataset. Comparative experiments with other state-of-the-art methods demonstrate the superiority of DSANet, which suggests its potential in advancing echocardiography segmentation.
ABSTRACT
Overproduction of nitric oxide (NO) can cause neuronal damage, contributing to the pathogenesis of several neurodegenerative diseases and stroke (i.e., focal cerebral ischemia). NO can mediate neurotoxic effects at least in part via protein S-nitrosylation, a reaction that covalently attaches NO to a cysteine thiol (or thiolate anion) to form an S-nitrosothiol. Recently, the tyrosine phosphatase Src homology region 2-containing protein tyrosine phosphatase-2 (SHP-2) and its downstream pathways have emerged as important mediators of cell survival. Here we report that in neurons and brain tissue NO can S-nitrosylate SHP-2 at its active site cysteine, forming S-nitrosylated SHP-2 (SNO-SHP-2). We found that NMDA exposure in vitro and transient focal cerebral ischemia in vivo resulted in increased levels of SNO-SHP-2. S-Nitrosylation of SHP-2 inhibited its phosphatase activity, blocking downstream activation of the neuroprotective physiological ERK1/2 pathway, thus increasing susceptibility to NMDA receptor-mediated excitotoxicity. These findings suggest that formation of SNO-SHP-2 represents a key chemical reaction contributing to excitotoxic damage in stroke and potentially other neurological disorders.
Subject(s)
Brain Ischemia/physiopathology , Nitric Oxide/metabolism , Protein Tyrosine Phosphatase, Non-Receptor Type 11/metabolism , Receptors, N-Methyl-D-Aspartate/physiology , Stroke/physiopathology , Animals , Apoptosis , Immunohistochemistry , MAP Kinase Signaling System , Mice , Neurons/pathologyABSTRACT
Stress proteins located in the cytosol or endoplasmic reticulum (ER) maintain cell homeostasis and afford tolerance to severe insults. In neurodegenerative diseases, several chaperones ameliorate the accumulation of misfolded proteins triggered by oxidative or nitrosative stress, or of mutated gene products. Although severe ER stress can induce apoptosis, the ER withstands relatively mild insults through the expression of stress proteins or chaperones such as glucose-regulated protein (GRP) and protein-disulphide isomerase (PDI), which assist in the maturation and transport of unfolded secretory proteins. PDI catalyses thiol-disulphide exchange, thus facilitating disulphide bond formation and rearrangement reactions. PDI has two domains that function as independent active sites with homology to the small, redox-active protein thioredoxin. During neurodegenerative disorders and cerebral ischaemia, the accumulation of immature and denatured proteins results in ER dysfunction, but the upregulation of PDI represents an adaptive response to protect neuronal cells. Here we show, in brains manifesting sporadic Parkinson's or Alzheimer's disease, that PDI is S-nitrosylated, a reaction transferring a nitric oxide (NO) group to a critical cysteine thiol to affect protein function. NO-induced S-nitrosylation of PDI inhibits its enzymatic activity, leads to the accumulation of polyubiquitinated proteins, and activates the unfolded protein response. S-nitrosylation also abrogates PDI-mediated attenuation of neuronal cell death triggered by ER stress, misfolded proteins or proteasome inhibition. Thus, PDI prevents neurotoxicity associated with ER stress and protein misfolding, but NO blocks this protective effect in neurodegenerative disorders through the S-nitrosylation of PDI.
Subject(s)
Neurodegenerative Diseases/metabolism , Nitric Oxide/metabolism , Protein Disulfide-Isomerases/chemistry , Protein Disulfide-Isomerases/metabolism , Protein Folding , Alzheimer Disease/enzymology , Alzheimer Disease/metabolism , Animals , Binding Sites , Cell Line , Cysteine/metabolism , Endoplasmic Reticulum/metabolism , Humans , Molecular Chaperones/metabolism , N-Methylaspartate/pharmacology , Neurodegenerative Diseases/enzymology , Parkinson Disease/enzymology , Parkinson Disease/metabolism , Proteasome Endopeptidase Complex/metabolism , Proteasome Inhibitors , Protein Disulfide-Isomerases/genetics , Receptors, G-Protein-Coupled/metabolism , Sulfhydryl Compounds/metabolism , Ubiquitin/metabolismABSTRACT
Many hereditary and sporadic neurodegenerative disorders are characterized by the accumulation of aberrant proteins. In sporadic Parkinson's disease, representing the most prevalent movement disorder, oxidative and nitrosative stress are believed to contribute to disease pathogenesis, but the exact molecular basis for protein aggregation remains unclear. In the case of autosomal recessive-juvenile Parkinsonism, mutation in the E3 ubiquitin ligase protein parkin is linked to death of dopaminergic neurons. Here we show both in vitro and in vivo that nitrosative stress leads to S-nitrosylation of wild-type parkin and, initially, to a dramatic increase followed by a decrease in the E3 ligase-ubiquitin-proteasome degradative pathway. The initial increase in parkin's E3 ubiquitin ligase activity leads to autoubiquitination of parkin and subsequent inhibition of its activity, which would impair ubiquitination and clearance of parkin substrates. These findings may thus provide a molecular link between free radical toxicity and protein accumulation in sporadic Parkinson's disease.
