gnu: Add python-scdamandtools.
* gnu/packages/bioinformatics.scm (python-scdamandtools): New variable. Signed-off-by: Ricardo Wurmus <rekado@elephly.net>
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@ -2154,6 +2154,41 @@ Python.")
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;; licensed lgpl2.1+
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;; licensed lgpl2.1+
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(license (list license:expat license:lgpl2.1+))))
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(license (list license:expat license:lgpl2.1+))))
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(define-public python-scdamandtools
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(package
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(name "python-scdamandtools")
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(version "1.0")
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(source (origin
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(method git-fetch)
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(uri (git-reference
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(url "https://github.com/KindLab/scDamAndTools")
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(commit (string-append "v" version))))
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(file-name (git-file-name name version))
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(sha256
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(base32
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"1mblw6cn5jqik6ky8cv7ry99z6jm1i4r71pzdfl398vrwbda65gd"))))
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(build-system pyproject-build-system)
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(arguments
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(list #:tests? #f)) ;there are none
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(propagated-inputs (list python-h5py
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python-numpy
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python-sortedcontainers
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python-pandas
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python-pysam
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python-tqdm))
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(native-inputs (list python-cython python-pytest))
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(home-page "https://github.com/KindLab/scDamAndTools")
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(synopsis "Functions for processing raw scDam&T-seq data")
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(description
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"This is a set of functions for processing raw scDam&T-seq data.
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scDam&T-seq is a method to simultaneously measure protein-DNA interactions and
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transcription from single cells (Rooijers et al., 2019). It combines a
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DamID-based method to measure protein-DNA interactions and an adaptation of
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CEL-Seq to measure transcription. The starting point of the workflow is raw
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sequencing data and the end result are tables of UMI-unique DamID and CEL-Seq
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counts.")
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(license license:expat)))
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(define-public python-bioframe
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(define-public python-bioframe
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(package
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(package
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(name "python-bioframe")
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(name "python-bioframe")
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