JavaScript is NOT enabled !

Article

FT
Medvik - BMC

Something wrong with this record ?

Mapping the genes for susceptibility and response to Leishmania tropica in mouse

Y. Sohrabi, H. Havelková, T. Kobets, M. Šíma, V. Volkova, I. Grekov, T. Jarošíková, I. Kurey, J. Vojtíšková, M. Svobodová, P. Demant, M. Lipoldová,

PLoS neglected tropical diseases. 2013 ; 7 (7) : e2282.

PLoS negl. trop. dis.
ISSN 1935-2735
Medvik
Source

Language English Country United States

Document type Journal Article, Research Support, Non-U.S. Gov't

Persistent link https://www.medvik.cz/link/bmc14050900

Online Full text

NLK Directory of Open Access Journals from 2007
Free Medical Journals from 2007
Public Library of Science (PLoS) from 2007
PubMed Central from 2007
Europe PubMed Central from 2007
ProQuest Central from 2007-10-01
Open Access Digital Library from 2007-01-01
Open Access Digital Library from 2007-01-01
Open Access Digital Library from 2007-08-30
Medline Complete (EBSCOhost) from 2009-04-01
Health & Medicine (ProQuest) from 2007-10-01
Public Health Database (ProQuest) from 2007-10-01
ROAD: Directory of Open Access Scholarly Resources from 2007

PubMed 23875032
DOI 10.1371/journal.pntd.0002282
Knihovny.cz E-resources

BACKGROUND: L. tropica can cause both cutaneous and visceral leishmaniasis in humans. Although the L. tropica-induced cutaneous disease has been long known, its potential to visceralize in humans was recognized only recently. As nothing is known about the genetics of host responses to this infection and their clinical impact, we developed an informative animal model. We described previously that the recombinant congenic strain CcS-16 carrying 12.5% genes from the resistant parental strain STS/A and 87.5% genes from the susceptible strain BALB/c is more susceptible to L. tropica than BALB/c. We used these strains to map and functionally characterize the gene-loci regulating the immune responses and pathology. METHODS: We analyzed genetics of response to L. tropica in infected F2 hybrids between BALB/c×CcS-16. CcS-16 strain carries STS-derived segments on nine chromosomes. We genotyped these segments in the F2 hybrid mice and tested their linkage with pathological changes and systemic immune responses. PRINCIPAL FINDINGS: We mapped 8 Ltr (Leishmania tropica response) loci. Four loci (Ltr2, Ltr3, Ltr6 and Ltr8) exhibit independent responses to L. tropica, while Ltr1, Ltr4, Ltr5 and Ltr7 were detected only in gene-gene interactions with other Ltr loci. Ltr3 exhibits the recently discovered phenomenon of transgenerational parental effect on parasite numbers in spleen. The most precise mapping (4.07 Mb) was achieved for Ltr1 (chr.2), which controls parasite numbers in lymph nodes. Five Ltr loci co-localize with loci controlling susceptibility to L. major, three are likely L. tropica specific. Individual Ltr loci affect different subsets of responses, exhibit organ specific effects and a separate control of parasite load and organ pathology. CONCLUSION: We present the first identification of genetic loci controlling susceptibility to L. tropica. The different combinations of alleles controlling various symptoms of the disease likely co-determine different manifestations of disease induced by the same pathogen in individual mice.

References provided by Crossref.org

000: 00000naa a2200000 a 4500

001: bmc14050900

003: CZ-PrNML

005: 20140411094157.0

007: ta

008: 140401s2013 xxu f 000 0|eng||

009: AR

024 7_: $a 10.1371/journal.pntd.0002282 $2 doi

035 __: $a (PubMed)23875032

040 __: $a ABA008 $b cze $d ABA008 $e AACR2

041 0_: $a eng

044 __: $a xxu

100 1_: $a Sohrabi, Yahya

245 10: $a Mapping the genes for susceptibility and response to Leishmania tropica in mouse / $c Y. Sohrabi, H. Havelková, T. Kobets, M. Šíma, V. Volkova, I. Grekov, T. Jarošíková, I. Kurey, J. Vojtíšková, M. Svobodová, P. Demant, M. Lipoldová,

520 9_: $a BACKGROUND: L. tropica can cause both cutaneous and visceral leishmaniasis in humans. Although the L. tropica-induced cutaneous disease has been long known, its potential to visceralize in humans was recognized only recently. As nothing is known about the genetics of host responses to this infection and their clinical impact, we developed an informative animal model. We described previously that the recombinant congenic strain CcS-16 carrying 12.5% genes from the resistant parental strain STS/A and 87.5% genes from the susceptible strain BALB/c is more susceptible to L. tropica than BALB/c. We used these strains to map and functionally characterize the gene-loci regulating the immune responses and pathology. METHODS: We analyzed genetics of response to L. tropica in infected F2 hybrids between BALB/c×CcS-16. CcS-16 strain carries STS-derived segments on nine chromosomes. We genotyped these segments in the F2 hybrid mice and tested their linkage with pathological changes and systemic immune responses. PRINCIPAL FINDINGS: We mapped 8 Ltr (Leishmania tropica response) loci. Four loci (Ltr2, Ltr3, Ltr6 and Ltr8) exhibit independent responses to L. tropica, while Ltr1, Ltr4, Ltr5 and Ltr7 were detected only in gene-gene interactions with other Ltr loci. Ltr3 exhibits the recently discovered phenomenon of transgenerational parental effect on parasite numbers in spleen. The most precise mapping (4.07 Mb) was achieved for Ltr1 (chr.2), which controls parasite numbers in lymph nodes. Five Ltr loci co-localize with loci controlling susceptibility to L. major, three are likely L. tropica specific. Individual Ltr loci affect different subsets of responses, exhibit organ specific effects and a separate control of parasite load and organ pathology. CONCLUSION: We present the first identification of genetic loci controlling susceptibility to L. tropica. The different combinations of alleles controlling various symptoms of the disease likely co-determine different manifestations of disease induced by the same pathogen in individual mice.

650 _2: $a zvířata $7 D000818

650 12: $a mapování chromozomů $7 D002874

650 _2: $a modely nemocí na zvířatech $7 D004195

650 12: $a náchylnost k nemoci $7 D004198

650 _2: $a ženské pohlaví $7 D005260

650 _2: $a genetické lokusy $7 D056426

650 12: $a interakce hostitele a patogenu $7 D054884

650 _2: $a leishmanióza kožní $x genetika $7 D016773

650 _2: $a myši $7 D051379

655 _2: $a časopisecké články $7 D016428

655 _2: $a práce podpořená grantem $7 D013485

700 1_: $a Havelková, Helena $u -

700 1_: $a Kobets, Tetyana $u -

700 1_: $a Šíma, Matyáš $u -

700 1_: $a Volkova, Valeriya $u -

700 1_: $a Grekov, Igor $u -

700 1_: $a Jarošíková, Taťána $u -

700 1_: $a Kurey, Iryna $u -

700 1_: $a Vojtíšková, Jarmila $u -

700 1_: $a Svobodová, Milena $u -

700 1_: $a Demant, Peter $u -

700 1_: $a Lipoldová, Marie $u -

773 0_: $w MED00165375 $t PLoS neglected tropical diseases $x 1935-2735 $g Roč. 7, č. 7 (2013), s. e2282

856 41: $u https://pubmed.ncbi.nlm.nih.gov/23875032 $y Pubmed

910 __: $a ABA008 $b sig $c sign $y a $z 0

990 __: $a 20140401 $b ABA008

991 __: $a 20140411094247 $b ABA008

999 __: $a ok $b bmc $g 1018036 $s 849480

BAS __: $a 3

BAS __: $a PreBMC

BMC __: $a 2013 $b 7 $c 7 $d e2282 $i 1935-2735 $m PLoS neglected tropical diseases $n PLoS negl. trop. dis. $x MED00165375

LZP __: $a Pubmed-20140401

Back

Borrow
RIS

Find record

In PubMed

Mapping the genes for susceptibility and response to Leishmania tropica in mouse

Find record

Citation metrics

Archiving options