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Biochemical Journal — Template for authors

Publisher: Portland Press

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Guideline source

Categories	Rank	Trend in last 3 yrs
Biochemistry	#99 of 415	down by 19 ranks
Molecular Biology	#121 of 382	down by 20 ranks
Cell Biology	#94 of 279	down by 12 ranks

Journal quality:

High

Last 4 years overview: 1030 Published Papers | 6922 Citations

Indexed in: Scopus

Last updated: 29/06/2020

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Insights

General info

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Journal Performance & Insights

Impact Factor

CiteRatio

Determines the importance of a journal by taking a measure of frequency with which the average article in a journal has been cited in a particular year.

A measure of average citations received per peer-reviewed paper published in the journal.

4.097

5% from 2018

Impact factor for Biochemical Journal from 2016 - 2019
Year	Value
2019	4.097
2018	4.331
2017	3.857
2016	3.797

Graph view

6.7

12% from 2019

CiteRatio for Biochemical Journal from 2016 - 2020
Year	Value
2020	6.7
2019	7.6
2018	7.4
2017	7.0
2016	7.1

Graph view

Insights

Impact factor of this journal has decreased by 5% in last year.
This journal’s impact factor is in the top 10 percentile category.

Insights

CiteRatio of this journal has decreased by 12% in last years.
This journal’s CiteRatio is in the top 10 percentile category.

SCImago Journal Rank (SJR)

Source Normalized Impact per Paper (SNIP)

Measures weighted citations received by the journal. Citation weighting depends on the categories and prestige of the citing journal.

Measures actual citations received relative to citations expected for the journal's category.

1.706

13% from 2019

SJR for Biochemical Journal from 2016 - 2020
Year	Value
2020	1.706
2019	1.954
2018	2.142
2017	2.224
2016	2.402

Graph view

1.117

Year	Value
2020	1.117
2019	1.117
2018	1.107
2017	0.973
2016	0.992

Graph view

Insights

SJR of this journal has decreased by 13% in last years.
This journal’s SJR is in the top 10 percentile category.

Insights

This journal’s SNIP is in the top 10 percentile category.

Guideline source: View

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Portland Press

Biochemical Journal

The Biochemical Journal publishes papers in English in all fields of biochemistry and cellular and molecular biology, provided that they make a sufficient contribution to knowledge in these fields. Papers may include new results obtained experimentally, descriptions of new experimental methods of biochemical importance, or new interpretations of existing results. Novel theoretical contributions will be considered, although these papers should also contain some experimental testing of the theory. All work presented should have as its aim the development of biochemical concepts rather than the mere recording of facts. Preliminary, confirmatory or inconclusive work will not be published. International contributions are welcome. Read Less

Biochemistry

Molecular Biology

Cell Biology

Biochemistry, Genetics and Molecular Biology

Last updated on	28 Jun 2020
ISSN	0264-6021
Impact Factor	High - 1.325
Acceptance Rate	20%
Open Access	Yes
Sherpa RoMEO Archiving Policy	White
Plagiarism Check	Available via Turnitin
Endnote Style	Download Available
Bibliography Name	unsrt
Citation Type	Numbered [25]
Bibliography Example	C. W. J. Beenakker. Specular andreev reflection in graphene. Phys. Rev. Lett., 97(6):067007, 2006.

Top papers written in this journal

Open access • Journal Article • DOI: 10.1042/BJ0620315 •

A study of the conditions and mechanism of the diphenylamine reaction for the colorimetric estimation of deoxyribonucleic acid

K. Burton¹ •

01 Feb 1956 - Biochemical Journal

Abstract:

Of the colour reactions available for the determination and identification of deoxyribonucleic acid (DNA), the reaction with diphenylamine in a mixture of acetic and sulphuric acids at 1000 (Dische, 1930) has been perhaps the most widely used. The present study arose from the observation that a more intense colour was sometim... Of the colour reactions available for the determination and identification of deoxyribonucleic acid (DNA), the reaction with diphenylamine in a mixture of acetic and sulphuric acids at 1000 (Dische, 1930) has been perhaps the most widely used. The present study arose from the observation that a more intense colour was sometimes produced if, instead of being heated at 1000 for 10 min., the reaction mixture was allowed to stand overnight at room temperature. As a result of this observation the procedure has been modified, principally by adding acetaldehyde to the reagents and by allowing the solution to stand for about 17 hr. at 30° instead of heating it at 1000. The modified method is 3-5 times as sensitive as Dische's original procedure, and several substances which interfere in the original method do not do so in the modified procedure. Some observations on the mechanism of the reaction have been made; in particular it was discovered that there is a liberation of inorganic orthophosphate from DNA during the early stages of the reaction. This finding has a bearing on the structure of DNA. The modified method has already been used in an investigation of nucleic acid metabolism during bacteriophage multiplication (Burton, 1955). read more

Topics:

Diphenylamine (57%)57% related to the paper

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13,649 Citations

Open access • Journal Article • DOI: 10.1042/BJ0890114 •

The preparation of 131i-labelled human growth hormone of high specific radioactivity

F C Greenwood, W M Hunter,

01 Oct 1963 - Biochemical Journal

Abstract:

A simple and rapid method is presented for the preparation of I/sup 131/- labeled human growth hormone of high specific radioactivity (240-300 mu C/ mu g). Low amounts of carrierfree I/sup 131/ iodide (2 mC) are allowed to react, without prior treatment, with small quantities of protein (5 mu g) in a highyield reaction (appro... A simple and rapid method is presented for the preparation of I/sup 131/- labeled human growth hormone of high specific radioactivity (240-300 mu C/ mu g). Low amounts of carrierfree I/sup 131/ iodide (2 mC) are allowed to react, without prior treatment, with small quantities of protein (5 mu g) in a highyield reaction (approx. 70% transfer of I/sup 131/ to protein). The degree of chemical substitution is minimized (0.5- 1.0 atom of iodine/molecule of protein) by the use of carrier-free I/sup 131/ iodide. The I/sup 131/-labeled hormone (up to 300 mu C/ mu g) contains no detectable degradation products and is immunologically identical with the unlabeled hormone. The loss of immunological reactivity at high specific radioactivities or at high levels of chemical substitution with STAI/sup 127/!iodine is demonstrated. (auth) read more

Topics:

Somatostatin binding (51%)51% related to the paper

10,047 Citations

Open access • Journal Article • DOI: 10.1042/BJ20081386 •

How mitochondria produce reactive oxygen species.

Michael P. Murphy

01 Jan 2009 - Biochemical Journal

Abstract:

The production of ROS (reactive oxygen species) by mammalian mitochondria is important because it underlies oxidative damage in many pathologies and contributes to retrograde redox signalling from the organelle to the cytosol and nucleus. Superoxide (O2•−) is the proximal mitochondrial ROS, and in the present review I outline... The production of ROS (reactive oxygen species) by mammalian mitochondria is important because it underlies oxidative damage in many pathologies and contributes to retrograde redox signalling from the organelle to the cytosol and nucleus. Superoxide (O2•−) is the proximal mitochondrial ROS, and in the present review I outline the principles that govern O2•− production within the matrix of mammalian mitochondria. The flux of O2•− is related to the concentration of potential electron donors, the local concentration of O2 and the second-order rate constants for the reactions between them. Two modes of operation by isolated mitochondria result in significant O2•− production, predominantly from complex I: (i) when the mitochondria are not making ATP and consequently have a high Δp (protonmotive force) and a reduced CoQ (coenzyme Q) pool; and (ii) when there is a high NADH/NAD+ ratio in the mitochondrial matrix. For mitochondria that are actively making ATP, and consequently have a lower Δp and NADH/NAD+ ratio, the extent of O2•− production is far lower. The generation of O2•− within the mitochondrial matrix depends critically on Δp, the NADH/NAD+ and CoQH2/CoQ ratios and the local O2 concentration, which are all highly variable and difficult to measure in vivo. Consequently, it is not possible to estimate O2•− generation by mitochondria in vivo from O2•−-production rates by isolated mitochondria, and such extrapolations in the literature are misleading. Even so, the description outlined here facilitates the understanding of factors that favour mitochondrial ROS production. There is a clear need to develop better methods to measure mitochondrial O2•− and H2O2 formation in vivo, as uncertainty about these values hampers studies on the role of mitochondrial ROS in pathological oxidative damage and redox signalling. read more

Topics:

Mitochondrial ROS (65%)65% related to the paper, MitoQ (61%)61% related to the paper, Mitochondrion (56%)56% related to the paper,

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6,371 Citations

Open access • Journal Article • DOI: 10.1042/BJ2190001 •

Oxygen toxicity, oxygen radicals, transition metals and disease

Barry Halliwell, John M.C. Gutteridge

01 Apr 1984 - Biochemical Journal

Topics:

Oxygen toxicity (58%)58% related to the paper, Oxygen (58%)58% related to the paper, Radical (51%)51% related to the paper

5,223 Citations

Open access • Journal Article • DOI: 10.1042/BJ3260001 •

Caspases: the executioners of apoptosis

Gerald M. Cohen¹ •

15 Aug 1997 - Biochemical Journal

Abstract:

Apoptosis is a major form of cell death, characterized initially by a series of stereotypic morphological changes. In the nematode Caenorhabditis elegans, the gene ced-3 encodes a protein required for developmental cell death. Since the recognition that CED-3 has sequence identity with the mammalian cysteine protease interleu... Apoptosis is a major form of cell death, characterized initially by a series of stereotypic morphological changes. In the nematode Caenorhabditis elegans, the gene ced-3 encodes a protein required for developmental cell death. Since the recognition that CED-3 has sequence identity with the mammalian cysteine protease interleukin-1 beta-converting enzyme (ICE), a family of at least 10 related cysteine proteases has been identified. These proteins are characterized by almost absolute specificity for aspartic acid in the P1 position. All the caspases (ICE-like proteases) contain a conserved QACXG (where X is R, Q or G) pentapeptide active-site motif. Capases are synthesized as inactive proenzymes comprising an N-terminal peptide (prodomain) together with one large and one small subunit. The crystal structures of both caspase-1 and caspase-3 show that the active enzyme is a heterotetramer, containing two small and two large subunits. Activation of caspases during apoptosis results in the cleavage of critical cellular substrates, including poly(ADP-ribose) polymerase and lamins, so precipitating the dramatic morphological changes of apoptosis. Apoptosis induced by CD95 (Fas/APO-1) and tumour necrosis factor activates caspase-8 (MACH/FLICE/Mch5), which contains an N-terminus with FADD (Fas-associating protein with death domain)-like death effector domains, so providing a direct link between cell death receptors and the caspases. The importance of caspase prodomains in the regulation of apoptosis is further highlighted by the recognition of adapter molecules, such as RAIDD [receptor-interacting protein (RIP)-associated ICH-1/CED-3-homologous protein with a death domain]/CRADD (caspase and RIP adapter with death domain), which binds to the prodomain of caspase-2 and recruits it to the signalling complex. Cells undergoing apoptosis following triggering of death receptors execute the death programme by activating a hierarchy of caspases, with caspase-8 and possibly caspase-10 being at or near the apex of this apoptotic cascade. read more

Topics:

Intrinsic apoptosis (68%)68% related to the paper, Death domain (64%)64% related to the paper, Caspase (63%)63% related to the paper,

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4,699 Citations

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Biochemical Journal format uses unsrt citation style.

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Frequently asked questions

1. Can I write Biochemical Journal in LaTeX?

Absolutely not! Our tool has been designed to help you focus on writing. You can write your entire paper as per the Biochemical Journal guidelines and auto format it.

2. Do you follow the Biochemical Journal guidelines?

Yes, the template is compliant with the Biochemical Journal guidelines. Our experts at SciSpace ensure that. If there are any changes to the journal's guidelines, we'll change our algorithm accordingly.

3. Can I cite my article in multiple styles in Biochemical Journal?

Of course! We support all the top citation styles, such as APA style, MLA style, Vancouver style, Harvard style, and Chicago style. For example, when you write your paper and hit autoformat, our system will automatically update your article as per the Biochemical Journal citation style.

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Sign up for our free trial, and you'll be able to use all our features for seven days. You'll see how helpful they are and how inexpensive they are compared to other options, Especially for Biochemical Journal.

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Yes. You can choose the right template, copy-paste the contents from the word document, and click on auto-format. Once you're done, you'll have a publish-ready paper Biochemical Journal that you can download at the end.

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It only takes a matter of seconds to edit your manuscript. Besides that, our intuitive editor saves you from writing and formatting it in Biochemical Journal.

7. Where can I find the template for the Biochemical Journal?

It is possible to find the Word template for any journal on Google. However, why use a template when you can write your entire manuscript on SciSpace , auto format it as per Biochemical Journal's guidelines and download the same in Word, PDF and LaTeX formats? Give us a try!.

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Of course! You can do this using our intuitive editor. It's very easy. If you need help, our support team is always ready to assist you.

9. Biochemical Journal an online tool or is there a desktop version?

SciSpace's Biochemical Journal is currently available as an online tool. We're developing a desktop version, too. You can request (or upvote) any features that you think would be helpful for you and other researchers in the "feature request" section of your account once you've signed up with us.

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11. What is the output that I would get after using Biochemical Journal?

After writing your paper autoformatting in Biochemical Journal, you can download it in multiple formats, viz., PDF, Docx, and LaTeX.

12. Is Biochemical Journal's impact factor high enough that I should try publishing my article there?

To be honest, the answer is no. The impact factor is one of the many elements that determine the quality of a journal. Few of these factors include review board, rejection rates, frequency of inclusion in indexes, and Eigenfactor. You need to assess all these factors before you make your final call.

13. What is Sherpa RoMEO Archiving Policy for Biochemical Journal?

We extracted this data from Sherpa Romeo to help researchers understand the access level of this journal in accordance with the Sherpa Romeo Archiving Policy for Biochemical Journal. The table below indicates the level of access a journal has as per Sherpa Romeo's archiving policy.

RoMEO Colour	Archiving policy
Green	Can archive pre-print and post-print or publisher's version/PDF
Blue	Can archive post-print (ie final draft post-refereeing) or publisher's version/PDF
Yellow	Can archive pre-print (ie pre-refereeing)
White	Archiving not formally supported

FYI:

Pre-prints as being the version of the paper before peer review and
Post-prints as being the version of the paper after peer-review, with revisions having been made.

14. What are the most common citation types In Biochemical Journal?

The 5 most common citation types in order of usage for Biochemical Journal are:.

S. No.	Citation Style Type
1.	Author Year
2.	Numbered
3.	Numbered (Superscripted)
4.	Author Year (Cited Pages)
5.	Footnote

15. How do I submit my article to the Biochemical Journal?

16. Can I download Biochemical Journal in Endnote format?

Yes, SciSpace provides this functionality. After signing up, you would need to import your existing references from Word or Bib file to SciSpace. Then SciSpace would allow you to download your references in Biochemical Journal Endnote style according to Elsevier guidelines.

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Biochemical Journal — Template for authors

Related Journals

Journal Performance & Insights

Impact Factor

CiteRatio

4.097

6.7

Insights

Insights

SCImago Journal Rank (SJR)

Source Normalized Impact per Paper (SNIP)

1.706

1.117

Insights

Insights

Biochemical Journal

Top papers written in this journal

Abstract:

Topics:

Abstract:

Topics:

Abstract:

Topics:

Topics:

Abstract:

Topics:

What to expect from SciSpace?

Speed and accuracy over MS Word

Plagiarism Reports via Turnitin

Freedom from formatting guidelines

Easy support from all your favorite tools

Frequently asked questions

Fast and reliable, built for complaince.

No word template required

Verifed journal formats

Trusted by academicians

Fast and reliable,
built for complaince.