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Journal of Antimicrobial ChemotherapyThe Journal of the British Society for Antimicrobial Chemotherapy

A joint enterprise

Journal of Antimicrobial Chemotherapy

Journal

Establishedin 1975

A joint enterprise

Journal of Antimicrobial Chemotherapy

British Society of Antimicrobial Chemotherapy

Journal

OwnerEstablished

in 1975

A joint enterprise

Journal of Antimicrobial Chemotherapy

British Society of Antimicrobial Chemotherapy

Oxford University Press

Journal

Publisher OwnerEstablished

in 1975

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Pre-JIF

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1,0

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2005 2006 2007 2008 2009 2010 2011 2012 2013 2014 2015 2016 2017

JO

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L I

MP

AC

T F

AC

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JAC = 5.217I

CMI = 5.394

AAC = 4.215

IJAA = 4.215

Journal impact factors

Submissions

Journal of Antimicrobial ChemotherapyThe Journal of the British Society for Antimicrobial Chemotherapy

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1988 1990 1992 1994 1996 1998 2000 2002 2004 2006 2008 2010 2012 2014 2016 2018

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1988 1990 1992 1994 1996 1998 2000 2002 2004 2006 2008 2010 2012 2014 2016 2018

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Submissions

~40 per week

Types of articles - 2018

Leading article1%

For debate1%

Letter to the Editor3%

Systematic Review3%

Review3%

Research letter11%

Original research

78%

Downloaded articles - 2018

0

50.000

100.000

150.000

200.000

250.000

Do

wn

load

s

HTML Full-text

PDF

JAC is global

80 countries

Origin of articles submitted - 2018

United States 11%

China 11%

United Kingdom 10%

France 8%

Spain 7%

Italy 5%

Australia 4%

India 4%

Brazil 4%

Netherlands 3%

Germany 3%

South Korea 3%

Taiwan 2%

Japan 2%

Canada 2%

Belgium 2%

Switzerland 1%

South Africa 1%

Iran 1%

Sweden 1%

Turkey 1%

Singapore 1%

Portugal 1%

Thailand 1%

Hong Kong 1%

Greece 1%

others (n= 57)10%

Origin of articles submitted - 2018

United States 11%

China 11%

United Kingdom 10%

France 8%

Spain 7%

Italy 5%

Australia 4%

India 4%

Brazil 4%

Netherlands 3%

Germany 3%

South Korea 3%

Taiwan 2%

Japan 2%

Canada 2%

Belgium 2%

Switzerland 1%

South Africa 1%

Iran 1%

Sweden 1%

Turkey 1%

Singapore 1%

Portugal 1%

Thailand 1%

Hong Kong 1%

Greece 1%

others (n= 57)10%

50% from 6 countries

Authorship

Journal of Antimicrobial ChemotherapyThe Journal of the British Society for Antimicrobial Chemotherapy

Criteria for authorship

The ICMJE recommends that authorship be based on EACH of the following 4 criteria:

http://www.icmje.org

Criteria for authorship

The ICMJE recommends that authorship be based on EACH of the following 4 criteria:

Substantial contributions to the conception or design of the work, or the acquisition, analysis, or interpretation of data for the work

http://www.icmje.org

Criteria for authorship

The ICMJE recommends that authorship be based on EACH of the following 4 criteria:

Substantial contributions to the conception or design of the work, or the acquisition, analysis, or interpretation of data for the work

Drafting the work or revising it critically for important intellectual content

http://www.icmje.org

Criteria for authorship

The ICMJE recommends that authorship be based on EACH of the following 4 criteria:

Substantial contributions to the conception or design of the work, or the acquisition, analysis, or interpretation of data for the work

Drafting the work or revising it critically for important intellectual content

Final approval of the version to be published

http://www.icmje.org

Criteria for authorship

The ICMJE recommends that authorship be based on EACH of the following 4 criteria:

Substantial contributions to the conception or design of the work, or the acquisition, analysis, or interpretation of data for the work

Drafting the work or revising it critically for important intellectual content

Final approval of the version to be published

Agreement to be accountable for all aspects of the work in ensuring that questions related to the accuracy or integrity of any part of the work are appropriately investigated and resolved.

http://www.icmje.org

Instructions for authors

Journal of Antimicrobial ChemotherapyThe Journal of the British Society for Antimicrobial Chemotherapy

JAC homepage

Author guidelines

Author guidelines

Background

The Journal of Antimicrobial Chemotherapy was founded in 1975 by the British

Society for Antimicrobial Chemotherapy (BSAC) as part of its mission to facilitate

the acquisition and dissemination of knowledge in the field of antimicrobial

chemotherapy. Proceeds from the Journal are used by the BSAC to further these

objectives. Articles are published continuously online in JAC Advance Access

and assembled into monthly printed and online issues. The Journal has an

Impact Factor of 5.217 (2017).

Author guidelines

BACKGROUND AND SCOPE OF THE JOURNAL

Aims

The Journal publishes articles that further knowledge and advance the science

and application of antimicrobial chemotherapy with antibiotics and antifungal,

antiviral and antiprotozoal agents. The Journal publishes primarily in human

medicine, and articles in veterinary medicine likely to have an impact on global

health.

Author guidelines

BACKGROUND AND SCOPE OF THE JOURNAL

Scope

The Journal particularly welcomes manuscripts on:

the practice of evidence-based medicine relating to antimicrobials (clinical

trials, systematic reviews and meta-analyses)

antimicrobial treatment (pharmacokinetics, pharmacodynamics and

prescribing practices)

the action of antimicrobial agents and the mechanisms, genetics and

epidemiology of antimicrobial resistance

antimicrobial stewardship

the genetic basis of antimicrobial resistance

Author guidelines

BACKGROUND AND SCOPE OF THE JOURNAL

Scope

In addition, the Journal is very keen to publish articles that:

offer evidence-based synthesis of knowledge and data useful for clinical

practice

analyse, reflect and comment on the current state of the art and practice

consolidate our knowledge of antimicrobial agents and their use

consider the future of antimicrobial chemotherapy

Author guidelines

BACKGROUND AND SCOPE OF THE JOURNAL

Scope

The Journal will consider publishing articles on:

new approaches to improving antimicrobial chemotherapy

new compounds provided evidence is offered of selective antimicrobial activity

and comparative cytotoxicity data

previously unreported antimicrobial activity relating to a marketed drug product

but such studies must take into account the exposure to the drug that can be

safely achieved with clinically acceptable doses

articles reporting the activity of bacteriophages

Author guidelines

BACKGROUND AND SCOPE OF THE JOURNAL

Scope

The Journal will not usually consider publishing material on:

the chemical synthesis or characterization of compounds. These are better

suited to chemistry journals.

the use and activity of biocides or disinfectants. These require specialist

methodology and are generally better suited to more specialist journals.

the process of turning antimicrobials into a medication i.e. pharmaceutics.

These are better suited to a pharmacy journal

drug stability studies

naturally occurring substances or extracts that exhibit antimicrobial activity but

for which no specific active ingredient has been chemically defined

Author guidelines

BACKGROUND AND SCOPE OF THE JOURNAL

The filtering process

The filtering process

The filtering process

aims and scope

The filtering process

aims and scope

editorial review

The filtering process

aims and scope

editorial review

peer review

The filtering process

aims and scope

editorial review

peer review

published

Fate of submissions

Journal of Antimicrobial ChemotherapyThe Journal of the British Society for Antimicrobial Chemotherapy

Fate of submissions

Immediate rejection -

outside scope12%

Immediate rejection -

appeal, merit, quality

25%

Rejection after review

39%

Acceptance24%

Fate of submissions - 2018

Immediate rejection -

outside scope12%

Immediate rejection -

appeal, merit, quality

25%

Rejection after review

39%

Acceptance24%

76% rejection

rate

Origin of articles published

United Kingdom 16%

United States 15%

France 12%

Netherlands 6%

Spain 6%

China 6%

Italy 5%

Australia 5%

Germany 4%

Belgium 3%

Canada 3%

Brazil 3%

Switzerland 2%

Sweden 1%

South Korea 1%

Taiwan 1%

South Africa 1%

India 1%

Hong Kong 1%

Others (n=25)9%

50% from 5 countries

Origin of articles published

United Kingdom 16%

United States 15%

France 12%

Netherlands 6%

Spain 6%

China 6%

Italy 5%

Australia 5%

Germany 4%

Belgium 3%

Canada 3%

Brazil 3%

Switzerland 2%

Sweden 1%

South Korea 1%

Taiwan 1%

South Africa 1%

India 1%

Hong Kong 1%

Others (n=25)9%

31% native English speakers

Editorial management

Journal of Antimicrobial ChemotherapyThe Journal of the British Society for Antimicrobial Chemotherapy

Editorial tree

Senior editors

Editorial tree

Senior editors

Editors

The manuscript

Editorial process

1

Mol ecul ar st r uct ur e of Nucl ei c Aci ds

WATSON, J. D. & CRICK, F. H. C.

Medical Research Council Unit for the Study of Molecular Structure

of Biological Systems, Cavendish Laboratory, Cambridge.

A St r uct ur e f or Deoxyr i bose Nucl ei c Aci d

We wish to suggest a structure for the salt of deoxyribose nucleic

acid (D.N.A.). This structure has novel features which are of

considerable biological interest.

A structure for nucleic acid has already been proposed by Pauling

and Corey1. They kindly made their manuscript available to us in

advance of publication. Their model consists of three intertwined

chains, with the phosphates near the fibre axis, and the bases on

the outside. In our opinion, this structure is unsatisfactory for

two reasons: (1) We believe that the material which gives the X-

ray diagrams is the salt, not the free acid. Without the acidic

hydrogen atoms it is not clear what forces would hold the

structure together, especially as the negatively charged

phosphates near the axis will repel each other. (2) Some of the

van der Waals distances appear to be too small.

Another three-chain structure has also been suggested by Fraser

(in the press). In his model the phosphates are on the outside and

the bases on the inside, linked together by hydrogen bonds. This

structure as described is rather ill-defined, and for this reason

we shall not comment on it.

We wish to put forward a radically different structure for the

salt of deoxyribose nucleic acid. This structure has two helical

chains each coiled round the same axis (see diagram). We have made

the usual chemical assumptions, namely, that each chain consists

of phosphate diester groups joining ß-D-deoxyribofuranose residues

with 3',5' linkages. The two chains (but not their bases) are

related by a dyad perpendicular to the fibre axis. Both chains

follow right- handed helices, but owing to the dyad the sequences

of the atoms in the two chains run in opposite directions. Each

chain loosely resembles Furberg's2 model No. 1; that is, the bases

are on the inside of the helix and the phosphates on the outside.

The configuration of the sugar and the atoms near it is close to

Furberg's 'standard configuration', the sugar being roughly

perpendicular to the attached base. There is a residue on each

every 3.4 A. in the z-direction. We have assumed an angle of 36° between adjacent residues in the same chain, so that the structure

repeats after 10 residues on each chain, that is, after 34 A. The

distance of a phosphorus atom from the fibre axis is 10 A. As the

phosphates are on the outside, cations have easy access to them.

The structure is an open one, and its water content is rather

Editorial process

AdminChecklist

1

Mol ecul ar st r uct ur e of Nucl ei c Aci ds

WATSON, J. D. & CRICK, F. H. C.

Medical Research Council Unit for the Study of Molecular Structure

of Biological Systems, Cavendish Laboratory, Cambridge.

A St r uct ur e f or Deoxyr i bose Nucl ei c Aci d

We wish to suggest a structure for the salt of deoxyribose nucleic

acid (D.N.A.). This structure has novel features which are of

considerable biological interest.

A structure for nucleic acid has already been proposed by Pauling

and Corey1. They kindly made their manuscript available to us in

advance of publication. Their model consists of three intertwined

chains, with the phosphates near the fibre axis, and the bases on

the outside. In our opinion, this structure is unsatisfactory for

two reasons: (1) We believe that the material which gives the X-

ray diagrams is the salt, not the free acid. Without the acidic

hydrogen atoms it is not clear what forces would hold the

structure together, especially as the negatively charged

phosphates near the axis will repel each other. (2) Some of the

van der Waals distances appear to be too small.

Another three-chain structure has also been suggested by Fraser

(in the press). In his model the phosphates are on the outside and

the bases on the inside, linked together by hydrogen bonds. This

structure as described is rather ill-defined, and for this reason

we shall not comment on it.

We wish to put forward a radically different structure for the

salt of deoxyribose nucleic acid. This structure has two helical

chains each coiled round the same axis (see diagram). We have made

the usual chemical assumptions, namely, that each chain consists

of phosphate diester groups joining ß-D-deoxyribofuranose residues

with 3',5' linkages. The two chains (but not their bases) are

related by a dyad perpendicular to the fibre axis. Both chains

follow right- handed helices, but owing to the dyad the sequences

of the atoms in the two chains run in opposite directions. Each

chain loosely resembles Furberg's2 model No. 1; that is, the bases

are on the inside of the helix and the phosphates on the outside.

The configuration of the sugar and the atoms near it is close to

Furberg's 'standard configuration', the sugar being roughly

perpendicular to the attached base. There is a residue on each

every 3.4 A. in the z-direction. We have assumed an angle of 36° between adjacent residues in the same chain, so that the structure

repeats after 10 residues on each chain, that is, after 34 A. The

distance of a phosphorus atom from the fibre axis is 10 A. As the

phosphates are on the outside, cations have easy access to them.

The structure is an open one, and its water content is rather

Editorial process

AdminChecklist

EICAssignment

1

Mol ecul ar st r uct ur e of Nucl ei c Aci ds

WATSON, J. D. & CRICK, F. H. C.

Medical Research Council Unit for the Study of Molecular Structure

of Biological Systems, Cavendish Laboratory, Cambridge.

A St r uct ur e f or Deoxyr i bose Nucl ei c Aci d

We wish to suggest a structure for the salt of deoxyribose nucleic

acid (D.N.A.). This structure has novel features which are of

considerable biological interest.

A structure for nucleic acid has already been proposed by Pauling

and Corey1. They kindly made their manuscript available to us in

advance of publication. Their model consists of three intertwined

chains, with the phosphates near the fibre axis, and the bases on

the outside. In our opinion, this structure is unsatisfactory for

two reasons: (1) We believe that the material which gives the X-

ray diagrams is the salt, not the free acid. Without the acidic

hydrogen atoms it is not clear what forces would hold the

structure together, especially as the negatively charged

phosphates near the axis will repel each other. (2) Some of the

van der Waals distances appear to be too small.

Another three-chain structure has also been suggested by Fraser

(in the press). In his model the phosphates are on the outside and

the bases on the inside, linked together by hydrogen bonds. This

structure as described is rather ill-defined, and for this reason

we shall not comment on it.

We wish to put forward a radically different structure for the

salt of deoxyribose nucleic acid. This structure has two helical

chains each coiled round the same axis (see diagram). We have made

the usual chemical assumptions, namely, that each chain consists

of phosphate diester groups joining ß-D-deoxyribofuranose residues

with 3',5' linkages. The two chains (but not their bases) are

related by a dyad perpendicular to the fibre axis. Both chains

follow right- handed helices, but owing to the dyad the sequences

of the atoms in the two chains run in opposite directions. Each

chain loosely resembles Furberg's2 model No. 1; that is, the bases

are on the inside of the helix and the phosphates on the outside.

The configuration of the sugar and the atoms near it is close to

Furberg's 'standard configuration', the sugar being roughly

perpendicular to the attached base. There is a residue on each

every 3.4 A. in the z-direction. We have assumed an angle of 36° between adjacent residues in the same chain, so that the structure

repeats after 10 residues on each chain, that is, after 34 A. The

distance of a phosphorus atom from the fibre axis is 10 A. As the

phosphates are on the outside, cations have easy access to them.

The structure is an open one, and its water content is rather

Editorial process

AdminChecklist

EICAssignment

Editor Assignment

1

Mol ecul ar st r uct ur e of Nucl ei c Aci ds

WATSON, J. D. & CRICK, F. H. C.

Medical Research Council Unit for the Study of Molecular Structure

of Biological Systems, Cavendish Laboratory, Cambridge.

A St r uct ur e f or Deoxyr i bose Nucl ei c Aci d

We wish to suggest a structure for the salt of deoxyribose nucleic

acid (D.N.A.). This structure has novel features which are of

considerable biological interest.

A structure for nucleic acid has already been proposed by Pauling

and Corey1. They kindly made their manuscript available to us in

advance of publication. Their model consists of three intertwined

chains, with the phosphates near the fibre axis, and the bases on

the outside. In our opinion, this structure is unsatisfactory for

two reasons: (1) We believe that the material which gives the X-

ray diagrams is the salt, not the free acid. Without the acidic

hydrogen atoms it is not clear what forces would hold the

structure together, especially as the negatively charged

phosphates near the axis will repel each other. (2) Some of the

van der Waals distances appear to be too small.

Another three-chain structure has also been suggested by Fraser

(in the press). In his model the phosphates are on the outside and

the bases on the inside, linked together by hydrogen bonds. This

structure as described is rather ill-defined, and for this reason

we shall not comment on it.

We wish to put forward a radically different structure for the

salt of deoxyribose nucleic acid. This structure has two helical

chains each coiled round the same axis (see diagram). We have made

the usual chemical assumptions, namely, that each chain consists

of phosphate diester groups joining ß-D-deoxyribofuranose residues

with 3',5' linkages. The two chains (but not their bases) are

related by a dyad perpendicular to the fibre axis. Both chains

follow right- handed helices, but owing to the dyad the sequences

of the atoms in the two chains run in opposite directions. Each

chain loosely resembles Furberg's2 model No. 1; that is, the bases

are on the inside of the helix and the phosphates on the outside.

The configuration of the sugar and the atoms near it is close to

Furberg's 'standard configuration', the sugar being roughly

perpendicular to the attached base. There is a residue on each

every 3.4 A. in the z-direction. We have assumed an angle of 36° between adjacent residues in the same chain, so that the structure

repeats after 10 residues on each chain, that is, after 34 A. The

distance of a phosphorus atom from the fibre axis is 10 A. As the

phosphates are on the outside, cations have easy access to them.

The structure is an open one, and its water content is rather

Editorial process

AdminChecklist

EICAssignment

Editor Assignment

Referee

Invitation

Selection

Assignment

Scores

1

Mol ecul ar st r uct ur e of Nucl ei c Aci ds

WATSON, J. D. & CRICK, F. H. C.

Medical Research Council Unit for the Study of Molecular Structure

of Biological Systems, Cavendish Laboratory, Cambridge.

A St r uct ur e f or Deoxyr i bose Nucl ei c Aci d

We wish to suggest a structure for the salt of deoxyribose nucleic

acid (D.N.A.). This structure has novel features which are of

considerable biological interest.

A structure for nucleic acid has already been proposed by Pauling

and Corey1. They kindly made their manuscript available to us in

advance of publication. Their model consists of three intertwined

chains, with the phosphates near the fibre axis, and the bases on

the outside. In our opinion, this structure is unsatisfactory for

two reasons: (1) We believe that the material which gives the X-

ray diagrams is the salt, not the free acid. Without the acidic

hydrogen atoms it is not clear what forces would hold the

structure together, especially as the negatively charged

phosphates near the axis will repel each other. (2) Some of the

van der Waals distances appear to be too small.

Another three-chain structure has also been suggested by Fraser

(in the press). In his model the phosphates are on the outside and

the bases on the inside, linked together by hydrogen bonds. This

structure as described is rather ill-defined, and for this reason

we shall not comment on it.

We wish to put forward a radically different structure for the

salt of deoxyribose nucleic acid. This structure has two helical

chains each coiled round the same axis (see diagram). We have made

the usual chemical assumptions, namely, that each chain consists

of phosphate diester groups joining ß-D-deoxyribofuranose residues

with 3',5' linkages. The two chains (but not their bases) are

related by a dyad perpendicular to the fibre axis. Both chains

follow right- handed helices, but owing to the dyad the sequences

of the atoms in the two chains run in opposite directions. Each

chain loosely resembles Furberg's2 model No. 1; that is, the bases

are on the inside of the helix and the phosphates on the outside.

The configuration of the sugar and the atoms near it is close to

Furberg's 'standard configuration', the sugar being roughly

perpendicular to the attached base. There is a residue on each

every 3.4 A. in the z-direction. We have assumed an angle of 36° between adjacent residues in the same chain, so that the structure

repeats after 10 residues on each chain, that is, after 34 A. The

distance of a phosphorus atom from the fibre axis is 10 A. As the

phosphates are on the outside, cations have easy access to them.

The structure is an open one, and its water content is rather

Editorial process

AdminChecklist

EICAssignment

Editor Assignment

Referee

Invitation

Selection

Assignment

Scores

EditorRecommendation

1

Mol ecul ar st r uct ur e of Nucl ei c Aci ds

WATSON, J. D. & CRICK, F. H. C.

Medical Research Council Unit for the Study of Molecular Structure

of Biological Systems, Cavendish Laboratory, Cambridge.

A St r uct ur e f or Deoxyr i bose Nucl ei c Aci d

We wish to suggest a structure for the salt of deoxyribose nucleic

acid (D.N.A.). This structure has novel features which are of

considerable biological interest.

A structure for nucleic acid has already been proposed by Pauling

and Corey1. They kindly made their manuscript available to us in

advance of publication. Their model consists of three intertwined

chains, with the phosphates near the fibre axis, and the bases on

the outside. In our opinion, this structure is unsatisfactory for

two reasons: (1) We believe that the material which gives the X-

ray diagrams is the salt, not the free acid. Without the acidic

hydrogen atoms it is not clear what forces would hold the

structure together, especially as the negatively charged

phosphates near the axis will repel each other. (2) Some of the

van der Waals distances appear to be too small.

Another three-chain structure has also been suggested by Fraser

(in the press). In his model the phosphates are on the outside and

the bases on the inside, linked together by hydrogen bonds. This

structure as described is rather ill-defined, and for this reason

we shall not comment on it.

We wish to put forward a radically different structure for the

salt of deoxyribose nucleic acid. This structure has two helical

chains each coiled round the same axis (see diagram). We have made

the usual chemical assumptions, namely, that each chain consists

of phosphate diester groups joining ß-D-deoxyribofuranose residues

with 3',5' linkages. The two chains (but not their bases) are

related by a dyad perpendicular to the fibre axis. Both chains

follow right- handed helices, but owing to the dyad the sequences

of the atoms in the two chains run in opposite directions. Each

chain loosely resembles Furberg's2 model No. 1; that is, the bases

are on the inside of the helix and the phosphates on the outside.

The configuration of the sugar and the atoms near it is close to

Furberg's 'standard configuration', the sugar being roughly

perpendicular to the attached base. There is a residue on each

every 3.4 A. in the z-direction. We have assumed an angle of 36° between adjacent residues in the same chain, so that the structure

repeats after 10 residues on each chain, that is, after 34 A. The

distance of a phosphorus atom from the fibre axis is 10 A. As the

phosphates are on the outside, cations have easy access to them.

The structure is an open one, and its water content is rather

Editorial process

AdminChecklist

EICAssignment

Editor Assignment

Referee

Invitation

Selection

Assignment

Scores

EditorRecommendation

EIC decision

1

Mol ecul ar st r uct ur e of Nucl ei c Aci ds

WATSON, J. D. & CRICK, F. H. C.

Medical Research Council Unit for the Study of Molecular Structure

of Biological Systems, Cavendish Laboratory, Cambridge.

A St r uct ur e f or Deoxyr i bose Nucl ei c Aci d

We wish to suggest a structure for the salt of deoxyribose nucleic

acid (D.N.A.). This structure has novel features which are of

considerable biological interest.

A structure for nucleic acid has already been proposed by Pauling

and Corey1. They kindly made their manuscript available to us in

advance of publication. Their model consists of three intertwined

chains, with the phosphates near the fibre axis, and the bases on

the outside. In our opinion, this structure is unsatisfactory for

two reasons: (1) We believe that the material which gives the X-

ray diagrams is the salt, not the free acid. Without the acidic

hydrogen atoms it is not clear what forces would hold the

structure together, especially as the negatively charged

phosphates near the axis will repel each other. (2) Some of the

van der Waals distances appear to be too small.

Another three-chain structure has also been suggested by Fraser

(in the press). In his model the phosphates are on the outside and

the bases on the inside, linked together by hydrogen bonds. This

structure as described is rather ill-defined, and for this reason

we shall not comment on it.

We wish to put forward a radically different structure for the

salt of deoxyribose nucleic acid. This structure has two helical

chains each coiled round the same axis (see diagram). We have made

the usual chemical assumptions, namely, that each chain consists

of phosphate diester groups joining ß-D-deoxyribofuranose residues

with 3',5' linkages. The two chains (but not their bases) are

related by a dyad perpendicular to the fibre axis. Both chains

follow right- handed helices, but owing to the dyad the sequences

of the atoms in the two chains run in opposite directions. Each

chain loosely resembles Furberg's2 model No. 1; that is, the bases

are on the inside of the helix and the phosphates on the outside.

The configuration of the sugar and the atoms near it is close to

Furberg's 'standard configuration', the sugar being roughly

perpendicular to the attached base. There is a residue on each

every 3.4 A. in the z-direction. We have assumed an angle of 36° between adjacent residues in the same chain, so that the structure

repeats after 10 residues on each chain, that is, after 34 A. The

distance of a phosphorus atom from the fibre axis is 10 A. As the

phosphates are on the outside, cations have easy access to them.

The structure is an open one, and its water content is rather

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1

Mol ecul ar st r uct ur e of Nucl ei c Aci ds

WATSON, J. D. & CRICK, F. H. C.

Medical Research Council Unit for the Study of Molecular Structure

of Biological Systems, Cavendish Laboratory, Cambridge.

A St r uct ur e f or Deoxyr i bose Nucl ei c Aci d

We wish to suggest a structure for the salt of deoxyribose nucleic

acid (D.N.A.). This structure has novel features which are of

considerable biological interest.

A structure for nucleic acid has already been proposed by Pauling

and Corey1. They kindly made their manuscript available to us in

advance of publication. Their model consists of three intertwined

chains, with the phosphates near the fibre axis, and the bases on

the outside. In our opinion, this structure is unsatisfactory for

two reasons: (1) We believe that the material which gives the X-

ray diagrams is the salt, not the free acid. Without the acidic

hydrogen atoms it is not clear what forces would hold the

structure together, especially as the negatively charged

phosphates near the axis will repel each other. (2) Some of the

van der Waals distances appear to be too small.

Another three-chain structure has also been suggested by Fraser

(in the press). In his model the phosphates are on the outside and

the bases on the inside, linked together by hydrogen bonds. This

structure as described is rather ill-defined, and for this reason

we shall not comment on it.

We wish to put forward a radically different structure for the

salt of deoxyribose nucleic acid. This structure has two helical

chains each coiled round the same axis (see diagram). We have made

the usual chemical assumptions, namely, that each chain consists

of phosphate diester groups joining ß-D-deoxyribofuranose residues

with 3',5' linkages. The two chains (but not their bases) are

related by a dyad perpendicular to the fibre axis. Both chains

follow right- handed helices, but owing to the dyad the sequences

of the atoms in the two chains run in opposite directions. Each

chain loosely resembles Furberg's2 model No. 1; that is, the bases

are on the inside of the helix and the phosphates on the outside.

The configuration of the sugar and the atoms near it is close to

Furberg's 'standard configuration', the sugar being roughly

perpendicular to the attached base. There is a residue on each

every 3.4 A. in the z-direction. We have assumed an angle of 36° between adjacent residues in the same chain, so that the structure

repeats after 10 residues on each chain, that is, after 34 A. The

distance of a phosphorus atom from the fibre axis is 10 A. As the

phosphates are on the outside, cations have easy access to them.

The structure is an open one, and its water content is rather

Editorial process

AdminChecklist

EICAssignment

Editor Assignment

Referee

Invitation

Selection

Assignment

Scores

EditorRecommendation

EIC decision

RejectRevisionAccept

1

Mol ecul ar st r uct ur e of Nucl ei c Aci ds

WATSON, J. D. & CRICK, F. H. C.

Medical Research Council Unit for the Study of Molecular Structure

of Biological Systems, Cavendish Laboratory, Cambridge.

A St r uct ur e f or Deoxyr i bose Nucl ei c Aci d

We wish to suggest a structure for the salt of deoxyribose nucleic

acid (D.N.A.). This structure has novel features which are of

considerable biological interest.

A structure for nucleic acid has already been proposed by Pauling

and Corey1. They kindly made their manuscript available to us in

advance of publication. Their model consists of three intertwined

chains, with the phosphates near the fibre axis, and the bases on

the outside. In our opinion, this structure is unsatisfactory for

two reasons: (1) We believe that the material which gives the X-

ray diagrams is the salt, not the free acid. Without the acidic

hydrogen atoms it is not clear what forces would hold the

structure together, especially as the negatively charged

phosphates near the axis will repel each other. (2) Some of the

van der Waals distances appear to be too small.

Another three-chain structure has also been suggested by Fraser

(in the press). In his model the phosphates are on the outside and

the bases on the inside, linked together by hydrogen bonds. This

structure as described is rather ill-defined, and for this reason

we shall not comment on it.

We wish to put forward a radically different structure for the

salt of deoxyribose nucleic acid. This structure has two helical

chains each coiled round the same axis (see diagram). We have made

the usual chemical assumptions, namely, that each chain consists

of phosphate diester groups joining ß-D-deoxyribofuranose residues

with 3',5' linkages. The two chains (but not their bases) are

related by a dyad perpendicular to the fibre axis. Both chains

follow right- handed helices, but owing to the dyad the sequences

of the atoms in the two chains run in opposite directions. Each

chain loosely resembles Furberg's2 model No. 1; that is, the bases

are on the inside of the helix and the phosphates on the outside.

The configuration of the sugar and the atoms near it is close to

Furberg's 'standard configuration', the sugar being roughly

perpendicular to the attached base. There is a residue on each

every 3.4 A. in the z-direction. We have assumed an angle of 36° between adjacent residues in the same chain, so that the structure

repeats after 10 residues on each chain, that is, after 34 A. The

distance of a phosphorus atom from the fibre axis is 10 A. As the

phosphates are on the outside, cations have easy access to them.

The structure is an open one, and its water content is rather

Editorial process – times taken

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EICAssignment

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Referee

Invitation

Selection

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Scores

EditorRecommendation

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1

Mol ecul ar st r uct ur e of Nucl ei c Aci ds

WATSON, J. D. & CRICK, F. H. C.

Medical Research Council Unit for the Study of Molecular Structure

of Biological Systems, Cavendish Laboratory, Cambridge.

A St r uct ur e f or Deoxyr i bose Nucl ei c Aci d

We wish to suggest a structure for the salt of deoxyribose nucleic

acid (D.N.A.). This structure has novel features which are of

considerable biological interest.

A structure for nucleic acid has already been proposed by Pauling

and Corey1. They kindly made their manuscript available to us in

advance of publication. Their model consists of three intertwined

chains, with the phosphates near the fibre axis, and the bases on

the outside. In our opinion, this structure is unsatisfactory for

two reasons: (1) We believe that the material which gives the X-

ray diagrams is the salt, not the free acid. Without the acidic

hydrogen atoms it is not clear what forces would hold the

structure together, especially as the negatively charged

phosphates near the axis will repel each other. (2) Some of the

van der Waals distances appear to be too small.

Another three-chain structure has also been suggested by Fraser

(in the press). In his model the phosphates are on the outside and

the bases on the inside, linked together by hydrogen bonds. This

structure as described is rather ill-defined, and for this reason

we shall not comment on it.

We wish to put forward a radically different structure for the

salt of deoxyribose nucleic acid. This structure has two helical

chains each coiled round the same axis (see diagram). We have made

the usual chemical assumptions, namely, that each chain consists

of phosphate diester groups joining ß-D-deoxyribofuranose residues

with 3',5' linkages. The two chains (but not their bases) are

related by a dyad perpendicular to the fibre axis. Both chains

follow right- handed helices, but owing to the dyad the sequences

of the atoms in the two chains run in opposite directions. Each

chain loosely resembles Furberg's2 model No. 1; that is, the bases

are on the inside of the helix and the phosphates on the outside.

The configuration of the sugar and the atoms near it is close to

Furberg's 'standard configuration', the sugar being roughly

perpendicular to the attached base. There is a residue on each

every 3.4 A. in the z-direction. We have assumed an angle of 36° between adjacent residues in the same chain, so that the structure

repeats after 10 residues on each chain, that is, after 34 A. The

distance of a phosphorus atom from the fibre axis is 10 A. As the

phosphates are on the outside, cations have easy access to them.

The structure is an open one, and its water content is rather

3 - 4 d

3 - 4 d

3 - 4 d 14 d

≤ 7 d

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1

Mol ecul ar st r uct ur e of Nucl ei c Aci ds

WATSON, J. D. & CRICK, F. H. C.

Medical Research Council Unit for the Study of Molecular Structure

of Biological Systems, Cavendish Laboratory, Cambridge.

A St r uct ur e f or Deoxyr i bose Nucl ei c Aci d

We wish to suggest a structure for the salt of deoxyribose nucleic

acid (D.N.A.). This structure has novel features which are of

considerable biological interest.

A structure for nucleic acid has already been proposed by Pauling

and Corey1. They kindly made their manuscript available to us in

advance of publication. Their model consists of three intertwined

chains, with the phosphates near the fibre axis, and the bases on

the outside. In our opinion, this structure is unsatisfactory for

two reasons: (1) We believe that the material which gives the X-

ray diagrams is the salt, not the free acid. Without the acidic

hydrogen atoms it is not clear what forces would hold the

structure together, especially as the negatively charged

phosphates near the axis will repel each other. (2) Some of the

van der Waals distances appear to be too small.

Another three-chain structure has also been suggested by Fraser

(in the press). In his model the phosphates are on the outside and

the bases on the inside, linked together by hydrogen bonds. This

structure as described is rather ill-defined, and for this reason

we shall not comment on it.

We wish to put forward a radically different structure for the

salt of deoxyribose nucleic acid. This structure has two helical

chains each coiled round the same axis (see diagram). We have made

the usual chemical assumptions, namely, that each chain consists

of phosphate diester groups joining ß-D-deoxyribofuranose residues

with 3',5' linkages. The two chains (but not their bases) are

related by a dyad perpendicular to the fibre axis. Both chains

follow right- handed helices, but owing to the dyad the sequences

of the atoms in the two chains run in opposite directions. Each

chain loosely resembles Furberg's2 model No. 1; that is, the bases

are on the inside of the helix and the phosphates on the outside.

The configuration of the sugar and the atoms near it is close to

Furberg's 'standard configuration', the sugar being roughly

perpendicular to the attached base. There is a residue on each

every 3.4 A. in the z-direction. We have assumed an angle of 36° between adjacent residues in the same chain, so that the structure

repeats after 10 residues on each chain, that is, after 34 A. The

distance of a phosphorus atom from the fibre axis is 10 A. As the

phosphates are on the outside, cations have easy access to them.

The structure is an open one, and its water content is rather

3 - 4 d

3 - 4 d

3 - 4 d

≤ 7 d

Peer reviewers - 2017 (n = 1,671)

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Peer reviewers - 2017 (n = 1,671)

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Overall time to first decision - 2018

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Overall time to first decision - 2018

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Status enquiries - 2018

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1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28 29 30

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Weeks after submission

Status enquiries - 2018

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1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28 29 30

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Weeks after submission

Too eager

Status enquiries - 2018

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5

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1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28 29 30

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Weeks after submission

Quite right

Status enquiries - 2018

0

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1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28 29 30

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Weeks after submission

Too patient

Status enquiries - 2018

0

5

10

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1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28 29 30

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Weeks after submission

Too polite

Status enquiries - 2018

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1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28 29 30

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Weeks after submission

EDITORIAL MANAGER

Colin W. E. Drummond

JAC@BSAC.org.uk

contact

Challenges

Authorship

Journal of Antimicrobial ChemotherapyThe Journal of the British Society for Antimicrobial Chemotherapy

Peer review – author’s perspective

by Nick Kim, Massey University, Wellington http://theconversation.com

Peer review – reviewer’s perspective

Peer review – reviewer’s perspective

Peer review – reviewer’s perspective

Peer review – reviewer’s perspective

Authorship disputes

Challenges

Journal of Antimicrobial ChemotherapyThe Journal of the British Society for Antimicrobial Chemotherapy

Authorship disputes

Who should be first author…..

Obviously

me ‘cos I

need it to

boost my H-

index

Who should be first author…..

Rubbish. It

must be me

‘cos I am the

most senior!

Who should be first author…..

Duh! Didn’t I

do all the

work?

Who should be first author…..

Sigh!

I have so

given up the

will to live!

Personal metrics

Challenges

Journal of Antimicrobial ChemotherapyThe Journal of the British Society for Antimicrobial Chemotherapy

Publish or perish

Impact Factor 2017

citations 2016 + citations 2015

=

Publications 2016 + publications 2015

Journal Impact Factor - 2017

Measuring performance of the journal

Measuring performance of the journal

“While the Impact Factor provides a

useful measure to show JAC’s standing

among other similar journals it should

never be used for measuring a given

authors scientific contribution to the field.”

Plan S

Challenges

Journal of Antimicrobial ChemotherapyThe Journal of the British Society for Antimicrobial Chemotherapy

Plan S

Plan S

The key principle is as follows:

“After 1 January 2020

scientific publications on the

results from research funded

by public grants provided by

national and European

research councils and

funding bodies, must be

published in compliant Open

Access Journals or on

compliant Open Access

Platforms.”

Plan S

Brussels 20th February 2019

PRESS RELEASE

Over 600 individuals and

organisations provided feedback to

cOAlition S on the implementation

guidance of Plan S. Originating from

over 40 countries, respondents

providing feedback include

researchers, librarians and libraries,

publishers and editors, universities,

learned societies, research funders

and performers, and other

interested citizens and

organisations.

Current publishing models

https://www.nature.com/articles/d41586-018-06178-7

Current publishing models

https://www.nature.com/articles/d41586-018-06178-7

Plan S

OUP operates two different open access models:

• An optional open access model (Oxford Open) for the majority of our

journals. Please see the individual journal home pages to find out

whether they offer optional open access.

• OUP also publish fully open access journals

Plan S

Open access publication fees (excluding taxes)

Elsevier

International Journal of Antimicrobial Agents (Hybrid) USD 3000

BSAC

Journal of Antimicrobial Chemotherapy (Hybrid) USD 2800 - 3200

Plan S

Journal of Antimicrobial Cheotherapy

AcknowledgementsEditorial Office Colin Drummond

Clare Jeeves

Suzanne Brockhouse

Sarah Egberger

Roya Khatiblou

Journal team Senior Editors

Editors

Referees

BSAC Phil Howard

Chris Longshaw

Kate Gould

Tracey Guise

OUP Phil Bishop

Emma Welsh

J Peter DonnellyEditor-in-Chief

JAC Editorial Office | Griffin House | 53 Regent Place | Birmingham B1 3NJ | UK

Journal of Antimicrobial

ChemotherapyA Journal of the British Society for Antimicrobial Chemotherapy

JAC

Telephone +31-(0)24-663-5188Mobile +31-(0)64-116-9297e-mail p.donnelly@usa.net