Ontology type: schema:ScholarlyArticle
1965-02
AUTHORSAUDREY FJELDE, J. L. TURK
ABSTRACTAFTER a period during which intensive investigation of carcinogenesis continued along classical lines, there has recently developed a major shift in emphasis as it is becoming more apparent that certain carcinogens, even when applied locally, are capable of initiating significant changes in the genetic apparatus of the host cells. Some of the present developments have, to a large extent, been the outgrowth of investigations showing that some carcinogens arrest the synthesis of DNA dependent RNA, in a manner similar to actinomycin-D. Structurally related non-carcinogens, on the other hand, exert no such action. These results indicate the possibility that the initial event in carcinogenesis might be an impairment in the expression of genetic (DNA dependent RNA) information, as has been suggested recently by De Maeyer and De Maeyer-Guignard1. Gelboin and Klein2 have, moreover, shown that tumour formation by 7,12-dimethyl-benz(a)anthracene can be markedly inhibited by the topical application of actinomycin-D before and after treatment. This would also support classical models for carcinogenesis such as that suggested by the work of Monod and Jacob on genetic systems in micro-organisms3. More... »
PAGES813-815
http://scigraph.springernature.com/pub.10.1038/205813b0
DOIhttp://dx.doi.org/10.1038/205813b0
DIMENSIONShttps://app.dimensions.ai/details/publication/pub.1033541328
JSON-LD is the canonical representation for SciGraph data.
TIP: You can open this SciGraph record using an external JSON-LD service: JSON-LD Playground Google SDTT
[
{
"@context": "https://springernature.github.io/scigraph/jsonld/sgcontext.json",
"about": [
{
"id": "http://purl.org/au-research/vocabulary/anzsrc-for/2008/06",
"inDefinedTermSet": "http://purl.org/au-research/vocabulary/anzsrc-for/2008/",
"name": "Biological Sciences",
"type": "DefinedTerm"
},
{
"id": "http://purl.org/au-research/vocabulary/anzsrc-for/2008/0604",
"inDefinedTermSet": "http://purl.org/au-research/vocabulary/anzsrc-for/2008/",
"name": "Genetics",
"type": "DefinedTerm"
}
],
"author": [
{
"affiliation": {
"alternateName": "Schweizerisches Forschungsinstitut Medizinische Abteilung, Davos-Platz, Switzerland",
"id": "http://www.grid.ac/institutes/None",
"name": [
"Schweizerisches Forschungsinstitut Medizinische Abteilung, Davos-Platz, Switzerland"
],
"type": "Organization"
},
"familyName": "FJELDE",
"givenName": "AUDREY",
"id": "sg:person.0112547152.38",
"sameAs": [
"https://app.dimensions.ai/discover/publication?and_facet_researcher=ur.0112547152.38"
],
"type": "Person"
},
{
"affiliation": {
"alternateName": "Department of Immunology, Institute of Dermatology, St. John's Hospital for Diseases of the Skin, Homerton Grove, E.9, London",
"id": "http://www.grid.ac/institutes/None",
"name": [
"Department of Immunology, Institute of Dermatology, St. John's Hospital for Diseases of the Skin, Homerton Grove, E.9, London"
],
"type": "Organization"
},
"familyName": "TURK",
"givenName": "J. L.",
"type": "Person"
}
],
"citation": [
{
"id": "sg:pub.10.1038/1981215a0",
"sameAs": [
"https://app.dimensions.ai/details/publication/pub.1016658435",
"https://doi.org/10.1038/1981215a0"
],
"type": "CreativeWork"
}
],
"datePublished": "1965-02",
"datePublishedReg": "1965-02-01",
"description": "AFTER a period during which intensive investigation of carcinogenesis continued along classical lines, there has recently developed a major shift in emphasis as it is becoming more apparent that certain carcinogens, even when applied locally, are capable of initiating significant changes in the genetic apparatus of the host cells. Some of the present developments have, to a large extent, been the outgrowth of investigations showing that some carcinogens arrest the synthesis of DNA dependent RNA, in a manner similar to actinomycin-D. Structurally related non-carcinogens, on the other hand, exert no such action. These results indicate the possibility that the initial event in carcinogenesis might be an impairment in the expression of genetic (DNA dependent RNA) information, as has been suggested recently by De Maeyer and De Maeyer-Guignard1. Gelboin and Klein2 have, moreover, shown that tumour formation by 7,12-dimethyl-benz(a)anthracene can be markedly inhibited by the topical application of actinomycin-D before and after treatment. This would also support classical models for carcinogenesis such as that suggested by the work of Monod and Jacob on genetic systems in micro-organisms3.",
"genre": "article",
"id": "sg:pub.10.1038/205813b0",
"inLanguage": "en",
"isAccessibleForFree": false,
"isPartOf": [
{
"id": "sg:journal.1018957",
"issn": [
"0028-0836",
"1476-4687"
],
"name": "Nature",
"publisher": "Springer Nature",
"type": "Periodical"
},
{
"issueNumber": "4973",
"type": "PublicationIssue"
},
{
"type": "PublicationVolume",
"volumeNumber": "205"
}
],
"keywords": [
"local lymph nodes",
"lymph nodes",
"immunological response",
"topical application",
"certain carcinogens",
"tumor formation",
"chemical carcinogens",
"carcinogenesis",
"carcinogens",
"initial event",
"host cells",
"significant changes",
"actinomycin",
"intensive investigation",
"impairment",
"treatment",
"induction",
"DNA-dependent RNA",
"cells",
"outgrowth",
"expression",
"response",
"RNA",
"period",
"genetic apparatus",
"action",
"investigation",
"events",
"such actions",
"changes",
"manner",
"genetic information",
"extent",
"development",
"lines",
"dependent RNA",
"hand",
"large extent",
"genetic system",
"nodes",
"major shift",
"results",
"possibility",
"emphasis",
"information",
"synthesis",
"formation",
"model",
"apparatus",
"system",
"shift",
"classical lines",
"dimethyl",
"micro",
"work",
"applications",
"classical model",
"Jacobs",
"present development",
"Monod",
"de Maeyer"
],
"name": "Induction of an Immunological Response in Local Lymph Nodes by Chemical Carcinogens",
"pagination": "813-815",
"productId": [
{
"name": "dimensions_id",
"type": "PropertyValue",
"value": [
"pub.1033541328"
]
},
{
"name": "doi",
"type": "PropertyValue",
"value": [
"10.1038/205813b0"
]
}
],
"sameAs": [
"https://doi.org/10.1038/205813b0",
"https://app.dimensions.ai/details/publication/pub.1033541328"
],
"sdDataset": "articles",
"sdDatePublished": "2022-05-20T07:40",
"sdLicense": "https://scigraph.springernature.com/explorer/license/",
"sdPublisher": {
"name": "Springer Nature - SN SciGraph project",
"type": "Organization"
},
"sdSource": "s3://com-springernature-scigraph/baseset/20220519/entities/gbq_results/article/article_98.jsonl",
"type": "ScholarlyArticle",
"url": "https://doi.org/10.1038/205813b0"
}
]Download the RDF metadata as: json-ld nt turtle xml License info
JSON-LD is a popular format for linked data which is fully compatible with JSON.
curl -H 'Accept: application/ld+json' 'https://scigraph.springernature.com/pub.10.1038/205813b0'
N-Triples is a line-based linked data format ideal for batch operations.
curl -H 'Accept: application/n-triples' 'https://scigraph.springernature.com/pub.10.1038/205813b0'
Turtle is a human-readable linked data format.
curl -H 'Accept: text/turtle' 'https://scigraph.springernature.com/pub.10.1038/205813b0'
RDF/XML is a standard XML format for linked data.
curl -H 'Accept: application/rdf+xml' 'https://scigraph.springernature.com/pub.10.1038/205813b0'
This table displays all metadata directly associated to this object as RDF triples.
131 TRIPLES
22 PREDICATES
88 URIs
79 LITERALS
6 BLANK NODES
| Subject | Predicate | Object | |
|---|---|---|---|
| 1 | sg:pub.10.1038/205813b0 | schema:about | anzsrc-for:06 |
| 2 | ″ | ″ | anzsrc-for:0604 |
| 3 | ″ | schema:author | N60f9d40f36214f688d4061215f3f9d3a |
| 4 | ″ | schema:citation | sg:pub.10.1038/1981215a0 |
| 5 | ″ | schema:datePublished | 1965-02 |
| 6 | ″ | schema:datePublishedReg | 1965-02-01 |
| 7 | ″ | schema:description | AFTER a period during which intensive investigation of carcinogenesis continued along classical lines, there has recently developed a major shift in emphasis as it is becoming more apparent that certain carcinogens, even when applied locally, are capable of initiating significant changes in the genetic apparatus of the host cells. Some of the present developments have, to a large extent, been the outgrowth of investigations showing that some carcinogens arrest the synthesis of DNA dependent RNA, in a manner similar to actinomycin-D. Structurally related non-carcinogens, on the other hand, exert no such action. These results indicate the possibility that the initial event in carcinogenesis might be an impairment in the expression of genetic (DNA dependent RNA) information, as has been suggested recently by De Maeyer and De Maeyer-Guignard1. Gelboin and Klein2 have, moreover, shown that tumour formation by 7,12-dimethyl-benz(a)anthracene can be markedly inhibited by the topical application of actinomycin-D before and after treatment. This would also support classical models for carcinogenesis such as that suggested by the work of Monod and Jacob on genetic systems in micro-organisms3. |
| 8 | ″ | schema:genre | article |
| 9 | ″ | schema:inLanguage | en |
| 10 | ″ | schema:isAccessibleForFree | false |
| 11 | ″ | schema:isPartOf | N6f786b2430d649ae8c18c299dd3e0f56 |
| 12 | ″ | ″ | Ne92e932e4712492e9b6b9fdaaca89052 |
| 13 | ″ | ″ | sg:journal.1018957 |
| 14 | ″ | schema:keywords | DNA-dependent RNA |
| 15 | ″ | ″ | Jacobs |
| 16 | ″ | ″ | Monod |
| 17 | ″ | ″ | RNA |
| 18 | ″ | ″ | actinomycin |
| 19 | ″ | ″ | action |
| 20 | ″ | ″ | apparatus |
| 21 | ″ | ″ | applications |
| 22 | ″ | ″ | carcinogenesis |
| 23 | ″ | ″ | carcinogens |
| 24 | ″ | ″ | cells |
| 25 | ″ | ″ | certain carcinogens |
| 26 | ″ | ″ | changes |
| 27 | ″ | ″ | chemical carcinogens |
| 28 | ″ | ″ | classical lines |
| 29 | ″ | ″ | classical model |
| 30 | ″ | ″ | de Maeyer |
| 31 | ″ | ″ | dependent RNA |
| 32 | ″ | ″ | development |
| 33 | ″ | ″ | dimethyl |
| 34 | ″ | ″ | emphasis |
| 35 | ″ | ″ | events |
| 36 | ″ | ″ | expression |
| 37 | ″ | ″ | extent |
| 38 | ″ | ″ | formation |
| 39 | ″ | ″ | genetic apparatus |
| 40 | ″ | ″ | genetic information |
| 41 | ″ | ″ | genetic system |
| 42 | ″ | ″ | hand |
| 43 | ″ | ″ | host cells |
| 44 | ″ | ″ | immunological response |
| 45 | ″ | ″ | impairment |
| 46 | ″ | ″ | induction |
| 47 | ″ | ″ | information |
| 48 | ″ | ″ | initial event |
| 49 | ″ | ″ | intensive investigation |
| 50 | ″ | ″ | investigation |
| 51 | ″ | ″ | large extent |
| 52 | ″ | ″ | lines |
| 53 | ″ | ″ | local lymph nodes |
| 54 | ″ | ″ | lymph nodes |
| 55 | ″ | ″ | major shift |
| 56 | ″ | ″ | manner |
| 57 | ″ | ″ | micro |
| 58 | ″ | ″ | model |
| 59 | ″ | ″ | nodes |
| 60 | ″ | ″ | outgrowth |
| 61 | ″ | ″ | period |
| 62 | ″ | ″ | possibility |
| 63 | ″ | ″ | present development |
| 64 | ″ | ″ | response |
| 65 | ″ | ″ | results |
| 66 | ″ | ″ | shift |
| 67 | ″ | ″ | significant changes |
| 68 | ″ | ″ | such actions |
| 69 | ″ | ″ | synthesis |
| 70 | ″ | ″ | system |
| 71 | ″ | ″ | topical application |
| 72 | ″ | ″ | treatment |
| 73 | ″ | ″ | tumor formation |
| 74 | ″ | ″ | work |
| 75 | ″ | schema:name | Induction of an Immunological Response in Local Lymph Nodes by Chemical Carcinogens |
| 76 | ″ | schema:pagination | 813-815 |
| 77 | ″ | schema:productId | N9951311f7a1f406eaa1bc68334aa7588 |
| 78 | ″ | ″ | Na9d2db7d86384831b0fc7d05e07390d8 |
| 79 | ″ | schema:sameAs | https://app.dimensions.ai/details/publication/pub.1033541328 |
| 80 | ″ | ″ | https://doi.org/10.1038/205813b0 |
| 81 | ″ | schema:sdDatePublished | 2022-05-20T07:40 |
| 82 | ″ | schema:sdLicense | https://scigraph.springernature.com/explorer/license/ |
| 83 | ″ | schema:sdPublisher | N397d5ccc670545459a9d5b025202702a |
| 84 | ″ | schema:url | https://doi.org/10.1038/205813b0 |
| 85 | ″ | sgo:license | sg:explorer/license/ |
| 86 | ″ | sgo:sdDataset | articles |
| 87 | ″ | rdf:type | schema:ScholarlyArticle |
| 88 | N217db5d95186452dba777ae224dcaa6f | rdf:first | Ne1814aad3c544dd99eb26173b1ade699 |
| 89 | ″ | rdf:rest | rdf:nil |
| 90 | N397d5ccc670545459a9d5b025202702a | schema:name | Springer Nature - SN SciGraph project |
| 91 | ″ | rdf:type | schema:Organization |
| 92 | N60f9d40f36214f688d4061215f3f9d3a | rdf:first | sg:person.0112547152.38 |
| 93 | ″ | rdf:rest | N217db5d95186452dba777ae224dcaa6f |
| 94 | N6f786b2430d649ae8c18c299dd3e0f56 | schema:volumeNumber | 205 |
| 95 | ″ | rdf:type | schema:PublicationVolume |
| 96 | N9951311f7a1f406eaa1bc68334aa7588 | schema:name | dimensions_id |
| 97 | ″ | schema:value | pub.1033541328 |
| 98 | ″ | rdf:type | schema:PropertyValue |
| 99 | Na9d2db7d86384831b0fc7d05e07390d8 | schema:name | doi |
| 100 | ″ | schema:value | 10.1038/205813b0 |
| 101 | ″ | rdf:type | schema:PropertyValue |
| 102 | Ne1814aad3c544dd99eb26173b1ade699 | schema:affiliation | grid-institutes:None |
| 103 | ″ | schema:familyName | TURK |
| 104 | ″ | schema:givenName | J. L. |
| 105 | ″ | rdf:type | schema:Person |
| 106 | Ne92e932e4712492e9b6b9fdaaca89052 | schema:issueNumber | 4973 |
| 107 | ″ | rdf:type | schema:PublicationIssue |
| 108 | anzsrc-for:06 | schema:inDefinedTermSet | anzsrc-for: |
| 109 | ″ | schema:name | Biological Sciences |
| 110 | ″ | rdf:type | schema:DefinedTerm |
| 111 | anzsrc-for:0604 | schema:inDefinedTermSet | anzsrc-for: |
| 112 | ″ | schema:name | Genetics |
| 113 | ″ | rdf:type | schema:DefinedTerm |
| 114 | sg:journal.1018957 | schema:issn | 0028-0836 |
| 115 | ″ | ″ | 1476-4687 |
| 116 | ″ | schema:name | Nature |
| 117 | ″ | schema:publisher | Springer Nature |
| 118 | ″ | rdf:type | schema:Periodical |
| 119 | sg:person.0112547152.38 | schema:affiliation | grid-institutes:None |
| 120 | ″ | schema:familyName | FJELDE |
| 121 | ″ | schema:givenName | AUDREY |
| 122 | ″ | schema:sameAs | https://app.dimensions.ai/discover/publication?and_facet_researcher=ur.0112547152.38 |
| 123 | ″ | rdf:type | schema:Person |
| 124 | sg:pub.10.1038/1981215a0 | schema:sameAs | https://app.dimensions.ai/details/publication/pub.1016658435 |
| 125 | ″ | ″ | https://doi.org/10.1038/1981215a0 |
| 126 | ″ | rdf:type | schema:CreativeWork |
| 127 | grid-institutes:None | schema:alternateName | Department of Immunology, Institute of Dermatology, St. John's Hospital for Diseases of the Skin, Homerton Grove, E.9, London |
| 128 | ″ | ″ | Schweizerisches Forschungsinstitut Medizinische Abteilung, Davos-Platz, Switzerland |
| 129 | ″ | schema:name | Department of Immunology, Institute of Dermatology, St. John's Hospital for Diseases of the Skin, Homerton Grove, E.9, London |
| 130 | ″ | ″ | Schweizerisches Forschungsinstitut Medizinische Abteilung, Davos-Platz, Switzerland |
| 131 | ″ | rdf:type | schema:Organization |