VLC Media Player (64-bit)

最新版本 SnapGene Viewer 5.2.0

SnapGene Viewer 5.2.0

SnapGene Viewer 5.2.0
VLC 媒體播放器 64 位(以前稱為 VideoLAN 客戶端)是一種高度便攜的免費多媒體播放器,適用於各種音頻和視頻格式,包括 MPEG-1,MPEG-2,MPEG-4,DivX,MP3 和 OGG,以及 DVD ,VCD 和各種流媒體協議。它也可以用作高帶寬網絡中 IPv4 或 IPv6 的單播或組播流的服務器。下載適用於 Windows 的 VLC Offline Installer 安裝程序。2.1.2 是 VLC 64 位的主要升級版本,它具有全新的音頻核心,硬件解碼和編碼,移動平台端口,Ultra-HD 視頻準備和特殊照顧等功能。

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VLC 新特性:
重寫的視頻輸出核心和模塊,允許混合使用 GPU。 Shader 支持 OpenGL 輸出,用於轉換,包括 10bits。 Windows 8 和 7,Android,iOS 和 OS / 2 的視頻輸出。去粒,紋理,去噪和防閃爍濾波器。去隔行濾鏡,包括反轉電視電影算法。重新採樣更高質量的音頻。動態範圍壓縮機和卡拉 OK 過濾器。簡化音頻核心,加快處理速度。適用於 iOS,Android 和 OS / 2 的音頻輸出。針對 H.264,MPEG-4 / Xvid 和 WebM 的多線程解碼。支持 10 位編解碼器,WMV 圖像和一些其他編解碼器。重寫了對圖像的支持,包括 jpeg,png,xcf,bmp 等。支持 RealVideo 和 Real Format 的重要更改。 CrystalHD 卡和 Android OpenMAX 支持硬件解碼。和更多的功能... 也可用:下載 VLC 媒體播放器為 Mac

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軟體資訊
檔案版本 SnapGene Viewer 5.2.0

檔案名稱 snapgene_viewer_5.2.0_win.exe
檔案大小
系統 Windows XP64 / Vista64 / Windows 7 64 / Windows 8 64 / Windows 10 64
軟體類型 開源軟體
作者 VideoLAN team
官網 http://www.videolan.org/vlc/
更新日期 2020-10-14
更新日誌

What's new in this version:

New Functionality:
- Enabled visualization of GC content as a color plot in Map view or base colors in Sequence view
- Added support for finding similar DNA sequences with mismatches or indels compared to the search query
- Added support for simulating the migration of supercoiled DNA molecules in agarose gels using TBE, TAE or SB buffer
- Added support for single-stranded DNA (ssDNA) sequences
- Enabled import of Sequencher project files (*.spf)
- Enabled "Undo" for edits in large sequences
- Added DNA ladders from DyneBio
- Added supercoiled MW markers from ELPIS BIOTECH and New England Biolabs
- Added BsmBI-v2 to the list of enzymes available from New England BioLabs
- Added fields for username and email address in the license registration dialog

Enhancements:
- Optimized storage of history for the following operations: Change Methylation, Change Transformation Strain, Set Origin, Flip, Insert/Delete/Replace, Linearize, Circularize
- Updated the supported protein feature types by adding new types (NonStdRes, Protein, Precursor, SecStr, Het, CDS, gene, misc_feature, unsure, variation), promoting Region subtypes to types, and adding new Site and Bond subtypes
- Added a note in Features view to indicate the presence of internal stop codons in a translated feature
- Enhanced the Preferences tools to allow more flexible default options for displaying ORFs
- Enabled carrying over feature qualifiers when creating a protein sequence using "Make Protein" or "Reverse Translate"
- Added the option to merge segments when using "Make Protein" on a multi-segment DNA feature
- Added a "Hide noncutters" check box in the Choose Enzymes dialog
- Enabled importing features from any supported file type when using "Import Features from a SnapGene File"
- Enabled more flexible batch conversion of chromatogram traces to other formats
- Improved search performance for large DNA sequences
- Configured the minimap to show both scrolled areas when two copies of Sequence view are visible
- Updated the format of the Preferences dialog, and added an "Agarose Gels" tab
- Added the option to designate a new collection as the Main Collection
- Enabled saving imported online sequences directly to a collection
- Added shortcuts in a collection Overview for navigating to the DNA Files, Protein Files, or Miscellaneous Files sections
- Enabled symbols to be entered in search queries when searching SnapGene Online Sequences
- Increased the size of the length indicator in the map label at the "Small" font size
- Consolidated all Fisher MW Markers for agarose gels in the Fisher Scientific set
- Configured the Nonredundant Commercial enzyme set to include similar enzymes that differ by methylation sensitivity
- Configured SnapGene to show the Launch dialog on macOS when the SnapGene icon in the Dock is clicked, if no SnapGene windows are open
- Changed the icon for enabling interrupted circle format for a linear DNA sequence in Map view
- Configured the "Export Map" and "Export History" options to be always enabled
- Improved the wording of various menu options and dialogs to provide greater clarity and consistency
- Added a message informing the user that files can be dragged into the list when using Align Multiple Sequences

Fixed:
- Fixed an issue that prevented cloning dialogs from allowing the use of hidden enzymes
- Corrected an issue in "Protein Search" whereby terminal stop codons were not included in the search query
- Ensured that edits in an alignment window do not cause inappropriate scrolling
- Corrected an issue that could prevent alignment of a high-quality sequence trace
- Ensured that the "Find" control in the Enzymes view chooser always shows a message to indicate if the enzyme is not in the chosen set
- Corrected an issue in which U's in overhangs resulting from linearizing were not preserved
- Configured "Select All" in the trace viewer context menu to actually select all
- Ensured that History view reflects changes after editing DNA ends
- Ensured that case changes in the "Find" entry field are preserved when the search is executed
- Ensured that imported RNA alignments are converted to DNA rather than protein alignments
- Corrected the license inactivity countdown to displays seconds rather than milliseconds
- Ensured that the "Accession Number:" label remains next to its entry field in the collection Search dialog
- Ensured that a "Sequence Name" search in the Protein Files area of a collection also searches the map labels and aliases
- Corrected an issue that resulted in alignment and collection windows not showing unsaved changes in the title bar on Windows and Linux
- Ensured more consistent sorting of enzymes in the Choose Enzymes dialog
- Streamlined the substitution matrix options presented when computing pairwise alignments
- Ensured that open alignments can be used as profiles when computing new alignments
- Corrected an issue that could result in the "Kind" column disappearing when viewing a collection
- Ensured that crisp screenshots are shown when detecting updates
- Improved import of the full publication date from PubMed
- Made various stability fixes

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