COMPUTATIONAL BIOLOGY AND CHEMISTRY

ISSN:

1476-9271

eISSN:

1476-928X

Disciplines
(Field of Science):

information and communication technology (Engineering and Technology)
biomedical engineering (Engineering and Technology)
medical biology (Medical and Health Sciences )
pharmacology and pharmacy (Medical and Health Sciences )
health sciences (Medical and Health Sciences )
agriculture and horticulture (Agricultural sciences)
biotechnology (Natural sciences)
computer and information sciences (Natural sciences)
biological sciences (Natural sciences)
chemical sciences (Natural sciences)

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Ministry points: Help

Ministry points - current year
Year	Points	List
Year 2024	70	Ministry scored journals list 2024

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Ministry points - previous years
Year	Points	List
2024	70	Ministry scored journals list 2024
2023	70	Ministry Scored Journals List
2022	70	Ministry Scored Journals List 2019-2022
2021	70	Ministry Scored Journals List 2019-2022
2020	70	Ministry Scored Journals List 2019-2022
2019	70	Ministry Scored Journals List 2019-2022
2018	25	A
2017	25	A
2016	20	A
2015	20	A
2014	25	A
2013	25	A
2012	25	A
2011	25	A
2010	32	A

Model:

Hybrid

Points CiteScore:

Points CiteScore - current year
Year	Points
Year 2023	6.1

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Points CiteScore - previous years
Year	Points
2023	6.1
2022	6.4
2021	5.1
2020	3.5
2019	2.8
2018	2.3
2017	2.3
2016	2
2015	1.7
2014	2
2013	2.8
2012	3.4
2011	3

Impact Factor:

Sherpa Romeo:

https://v2.sherpa.ac.uk/id/publication/11156

Papers published in journal

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total: 2

Year 2019

Kinetic flux vector splitting scheme for solving non-reactive multi-component flows
Publication
- M. Saqib
- A. Rabbani
- U. Nisar
- W. Ashraf
- S. Qamar
- COMPUTATIONAL BIOLOGY AND CHEMISTRY - Year 2019
Full text to download in external service

Year 2016

Structure-based design and evaluation of novel N-phenyl-1H-indol-2-amine derivatives for fat mass and obesity-associated (FTO) protein inhibition
Publication
- M. Padariya
- U. Kalathiya
- COMPUTATIONAL BIOLOGY AND CHEMISTRY - Year 2016
Fat mass and obesity-associated (FTO) protein contributes to non-syndromic human obesity which refers to excessive fat accumulation in human body and results in health risk. FTO protein has become a promising target for anti-obesity medicines as there is an immense need for the rational design of potent inhibitors to treat obesity. In our study, a new scaffold N-phenyl-1H-indol-2-amine was selected as a base for FTO protein inhibitors...

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COMPUTATIONAL BIOLOGY AND CHEMISTRY

ISSN:

eISSN:

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Ministry points: Help

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Papers published in journal

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Year 2019

Kinetic flux vector splitting scheme for solving non-reactive multi-component flows

Year 2016

Structure-based design and evaluation of novel N-phenyl-1H-indol-2-amine derivatives for fat mass and obesity-associated (FTO) protein inhibition

Disciplines
(Field of Science):