263 research outputs found

    Discord Monitoring for Streaming Time-Series

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    Many applications generate time-series and analyze it. One of the most important time-series analysis tools is anomaly detection, and discord discovery aims at finding an anomaly subsequence in a time-series. Time-series is essentially dynamic, so monitoring the discord of a streaming time-series is an important problem. This paper addresses this problem and proposes SDM (Streaming Discord Monitoring), an algorithm that efficiently updates the discord of a streaming time-series over a sliding window. We show that SDM is approximation-friendly, i.e., the computational efficiency is accelerated by monitoring an approximate discord with theoretical bound. Our experiments on real datasets demonstrate the efficiency of SDM and its approximate version.This version of the contribution has been accepted for publication, after peer review (when applicable) but is not the Version of Record and does not reflect post-acceptance improvements, or any corrections. The Version of Record is available online at: https://doi.org/10.1007/978-3-030-27615-7_6. Use of this Accepted Version is subject to the publisher’s Accepted Manuscript terms of use https://www.springernature.com/gp/open-research/policies/accepted-manuscript-terms.Kato S., Amagata D., Nishio S., et al. Discord Monitoring for Streaming Time-Series. Lecture Notes in Computer Science (including subseries Lecture Notes in Artificial Intelligence and Lecture Notes in Bioinformatics) 11706 LNCS, 79 (2019

    Hyperglycemia raises the threshold of levosimendan- but not milrinone-induced postconditioning in rat hearts

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    <p>Abstract</p> <p>Background</p> <p>The authors examined whether milrinone and levosimendan could exert cardiac postconditioning effects in rats under normoglycemia and hyperglycemia, and whether the effects could be mediated by mitochondrial permeability transition pore (mPTP).</p> <p>Methods</p> <p>Wistar rats underwent 30-min coronary artery occlusion followed by 2-h reperfusion. The rats received milrinone or levosimendan just before reperfusion under normoglycemic or hyperglycemic conditions with or without atractyloside, an mPTP opener.</p> <p>Results</p> <p>Under normoglycemia, both 30 μg/kg milrinone (29 ± 12%) and 10 μg/kg levosimendan (33 ± 13%) reduced infarct size compared with that in the control (58 ± 7%). Under hyperglycemia, milrinone (34 ± 13%) reduced infarct size at the same dose as under normoglycemia. In contrast, neither 10 nor 30 μg/kg levosimendan protected hyperglycemic hearts, and only 100 μg/kg levosimendan (32 ± 9%) reduced infarct size compared with that in the hyperglycemic control (58 ± 13%). All of these cardioprotective effects under normoglycemia and hyperglycemia are abolished by atractyloside.</p> <p>Conclusion</p> <p>Milrinone and levosimendan exert postconditioning effects via inhibition of mPTP opening. Hyperglycemia raises the threshold of levosimendan-induced postconditioning, while milrinone-induced postconditioning is not influenced by hyperglycemia.</p

    Mesenchymal stromal cells in bone marrow express adiponectin and are efficiently targeted by an adiponectin promoter-driven Cre transgene

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    Stromal cells in bone marrow (BM) constitute a specific microenvironment supporting the development and maintenance of hematopoietic cells. Adiponectin is a cytokine secreted by adipocytes. Besides its anti-diabetic and anti-atherogenic roles, adiponectin reportedly regulates the development and function of hematopoietic cells in BM. However, it remains unclear whether mesenchymal stromal cells in BM express adiponectin. Here, we show that PDGFRβ+VCAM-1+ stromal cells express adiponectin. Lineage tracing revealed that a majority of PDGFRβ+VCAM-1+ cells were targeted by an adiponectin promoter-driven Cre (Adipoq-Cre) transgene. Additionally, the Adipoq-Cre transgene targets a minority of osteoblasts at a younger age but larger populations are targeted at an older age. Furthermore, the Adipoq-Cre transgene targets almost all CXCL12-abundant reticular (CAR) cells and most of the stromal cells targeted by the Adipoq-Cre transgene are CAR cells. Finally, deletion of interleukin-7 (IL-7) by the Adipoq-Cre transgene resulted in severe impairment of B lymphopoiesis in BM. These results demonstrate that PDGFRβ+VCAM-1+ stromal cells in BM express adiponectin and are targeted by the Adipoq-Cre transgene, suggesting a broader specificity of the Adipoq-Cre transgene

    Behavioral Partitioning with Exploiting Function-Level Parallelism

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    Abstract-This paper proposes a method to efficiently generate hardware from a large behavioral description by behavioral synthesis. For a program with functions which are executable in parallel, this proposed method determines an optimal behavioral partitioning which fully exploits the function-level parallelism with simultaneously minimizing the area in the datapath and control path. This partitioning problem is formulated as an integer programming problem. Experimental results demonstrate the effectiveness of our proposed method

    Direct effect of mild hypothermia on the coronary vasodilation induced by an ATP-sensitive K channel opener, a nitric oxide donor and isoflurane in isolated rat hearts.

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    PURPOSE: Deliberate mild hypothermia (MHT) is applied for cerebroprotection after cardiopulmonary resuscitation and during cardiac surgery. MHT has been shown to alter both contractility and relaxation of blood vessels in the brain. However, the effects of MHT on drug-induced vasodilation are not fully understood. The aim of this study was to clarify the effects of MHT on the coronary vasodilation induced by cromakalim (an ATP-sensitive K channel opener), S-nitroso acetyl-penicillamine (SNAP; a nitric oxide donor), and isoflurane in isolated rat hearts. METHODS: Male SD rat hearts were isolated and perfused with Krebs-Henseleit buffer. Coronary flow was measured with the coronary perfusion pressure kept at 60 mmHg, and coronary vascular resistance (CVR) was calculated. After cardiac arrest was induced by tetrodotoxin, the hearts were allocated to one of three temperature groups: 37, 34, and 31 degrees C (n = 7 for each). All groups received 0.01, 0.1, and 1.0 muM of either cromakalim or SNAP or were exposed to isoflurane at 1MAC and 2MAC. Finally, 50 mM of adenosine was administered to obtain maximal coronary vasodilation. RESULTS: CVR significantly increased after cardiac arrest, but did not change after the application of each temperature. Cromakalim, SNAP and isoflurane significantly decreased CVR in each temperature group. There were no significant differences in CVR among the three temperature groups with any of the test drugs. CONCLUSION: These results indicate that cromakalim-, SNAP-, and isoflurane-induced coronary vasodilation are not affected by MHT

    Cardiogenic embolism caused hypoglycemia

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    The direct relationship between a hypoglycemic attack and cerebral infarction remains unknown. It has been reported that a hypoglycemic attack can result in takotsubo syndrome, leading to cerebral infarction. We report a case of a cardiogenic cerebral embolism caused by a hypoglycemic attack, with additional literature review. A 71-year-old woman was admitted to our hospital in a semi-comatose state due to a severe hypoglycemic attack ; she developed hemiplegia one day after admission. Magnetic resonance imaging revealed cerebral infarction in the area supplied by the left middle cerebral artery. Takotsubo syndrome was suspected based on echocardiography. We diagnosed cerebral embolism due to takotsubo syndrome, caused by the hypoglycemic attack

    Scalable and template-free production of mesoporous calcium carbonate and its potential to formaldehyde adsorbent

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    Here we report a scalable and template-free production strategy 1 in the synthesis of a mesoporous calcium carbonate, which undergoes self-assembled nanostructure formation through a temperature-induced aggregation and polymorphic transformation of the colloids. The specific surface area and pore size distribution of resulting mesoporous calcium carbonate are clearly different depending on the aging temperature. The specific surface area and average pore size for aging temperature of 293 K are 207.3 ± 9.8 m2/g and 8.8±0.6 nm, respectively, and 65.1 ± 10.1 m2/g and 19.9±2.6 nm at 473 K. Additionally, we apply the mesoporous calcium carbonate powder to formaldehyde vapor adsorbent. We measure the adsorbed amount of gaseous formaldehyde and find that the vaterite-rich powder has larger adsorption per unit area than the calcite-rich one

    The role of astrocytes during repair of cerebral infarction in mdx mice

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    様々な大きさのジストロフィンアイソフォーム(427kDa, 260kDa, 140kDa, 116kDa, 71-75kDa)が広く体内に存在していることはよく知られている.中枢神経系においては71-75kDaのDp71が著明に多く,毛細血管の内皮の基底膜に接しているアストロサイトの細胞質に局在することが報告されている.しかしながらDp71の機能についてはよくわかっていないことが多い.そこで今回,脳組織におけるDp71の役割を調べるために,コントロールマウス(wild-typeマウス)およびデュシャンヌ型筋ジストロフィーモデル動物であるmdxマウスを用いて実験的脳梗塞を作成し,その治癒過程を形態学的に観察した.また,GFAPおよびDp71に関して生化学的に分析をおこなった.HE染色およびGFAP免疫組織学的染色の結果から,形態学的にはmdxマウスとコントロールマウスの脳に違いは認められなかった.しかしながら,mdxマウスの脳において,Dp71の発現量がコントロールマウスよりも少ないことがわかった.またmdxマウスにおいて,脳梗塞の修復過程におけるアストロサイトの反応がコントロールマウスよりも弱いことがわかった.これらの結果から,mdxマウスの脳において,アストロサイトの機能,アストロサイトの血管新生に関わる機能の障害されていることが示唆された.It is now well known that dystrophin isoforms (427kDa, 260kDa, 140kDa, 116kDa, 71-75kDa) are widely distributed throughout our body. In the central nervous system a considerable amount of Dp71 (71-75kDa) is found in the perivascular cytoplasm of the astrocytes. However, the function of this dystrophin is still unknown. To investigate the role of Dp71 in the brain tissue, cerebral infarction was induced in the control (wide-type) mouse and mdx mouse which is known as an animal model of human muscle dystrophy (Duchenne type), and morphological changes of the infarcted area were observed during repair of the infarction. In addition, biochemical analysis of GFAP and Dp71 was carried out in the brain of the control and mdx mouse. In our present study, there were no differences in brain morphology between mdx and control mouse as revealed in H-E stain and GFAP immunohistochemistry. However, the Dp71 were smaller in quantity in the brain of the mdx mouse than that of the control mouse. The reaction of astrocytes during repair of serebral infarction was distinctly delayed in the mdx mouse compared with that of the control mouse. These findings suggest that the astrocytes in the brain of the mdx mouse are functionally impaired including perivascular cytoplasmic processes with relation to neo-vascularization
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