Detection of C. trachomatis in the Serum of the Patients with Urogenital Chlamydiosis
Extragenital chlamydial complications may be associated with systemic spread of infection, but haematogenous route for C. trachomatis dissemination has not been clearly demonstrated. Here we report that serum specimens obtained from patients with chlamydiosis contain elementary bodies of C. trachoma...
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| Published in | BioMed research international Vol. 2013; no. 2013; pp. 1 - 7 |
|---|---|
| Main Authors | , , , , , , , , |
| Format | Journal Article |
| Language | English |
| Published |
Cairo, Egypt
Hindawi Publishing Corporation
01.01.2013
John Wiley & Sons, Inc |
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| Abstract | Extragenital chlamydial complications may be associated with systemic spread of infection, but haematogenous route for C. trachomatis dissemination has not been clearly demonstrated. Here we report that serum specimens obtained from patients with chlamydiosis contain elementary bodies of C. trachomatis shown by culture and immunogold electron microscopy. We have found that 31 of the 52 patients had serum precipitates which were infective to McCoy cells. Immunostaining revealed very small inclusions resembling those reported during persistent C. trachomatis infection in vitro. DNA specimens from 49 (out of 52) patients with chlamydiosis gave positive PCR readings. The viability of the pathogen present in the sera was confirmed by chlamydial RNA detection in the cell monolayer inoculated by the serum precipitates. By using DNA isolation protocol from 1 mL of serum and quantitative TaqMan PCR, it was estimated that bacterial load in patients’ sera was 2×102–103 GE/mL. These findings for the first time demonstrated that C. trachomatis can be disseminated directly by the plasma, independently from blood cell, which may represent a new possible pathway of the chronic infection development. Therefore, new methodological approaches for detection of C. trachomatis in the serum of patients with complicated and chronic chlamydiosis could be important in the diagnosis of the infection regardless of its anatomical localization. |
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| AbstractList | Extragenital chlamydial complications may be associated with systemic spread of infection, but haematogenous route for
C. trachomatis
dissemination has not been clearly demonstrated. Here we report that serum specimens obtained from patients with chlamydiosis contain elementary bodies of
C. trachomatis
shown by culture and immunogold electron microscopy. We have found that 31 of the 52 patients had serum precipitates which were infective to McCoy cells. Immunostaining revealed very small inclusions resembling those reported during persistent
C. trachomatis
infection
in vitro
. DNA specimens from 49 (out of 52) patients with chlamydiosis gave positive PCR readings. The viability of the pathogen present in the sera was confirmed by chlamydial RNA detection in the cell monolayer inoculated by the serum precipitates. By using DNA isolation protocol from 1 mL of serum and quantitative TaqMan PCR, it was estimated that bacterial load in patients’ sera was
2
×
10
2
–
10
3
GE/mL. These findings for the first time demonstrated that
C. trachomatis
can be disseminated directly by the plasma, independently from blood cell, which may represent a new possible pathway of the chronic infection development. Therefore, new methodological approaches for detection of
C. trachomatis
in the serum of patients with complicated and chronic chlamydiosis could be important in the diagnosis of the infection regardless of its anatomical localization. Extragenital chlamydial complications may be associated with systemic spread of infection, but haematogenous route for C. trachomatis dissemination has not been clearly demonstrated. Here we report that serum specimens obtained from patients with chlamydiosis contain elementary bodies of C. trachomatis shown by culture and immunogold electron microscopy. We have found that 31 of the 52 patients had serum precipitates which were infective to McCoy cells. Immunostaining revealed very small inclusions resembling those reported during persistent C. trachomatis infection in vitro. DNA specimens from 49 (out of 52) patients with chlamydiosis gave positive PCR readings. The viability of the pathogen present in the sera was confirmed by chlamydial RNA detection in the cell monolayer inoculated by the serum precipitates. By using DNA isolation protocol from 1 mL of serum and quantitative TaqMan PCR, it was estimated that bacterial load in patients’ sera was 2×102–103 GE/mL. These findings for the first time demonstrated that C. trachomatis can be disseminated directly by the plasma, independently from blood cell, which may represent a new possible pathway of the chronic infection development. Therefore, new methodological approaches for detection of C. trachomatis in the serum of patients with complicated and chronic chlamydiosis could be important in the diagnosis of the infection regardless of its anatomical localization. Extragenital chlamydial complications may be associated with systemic spread of infection, but haematogenous route for C. trachomatis dissemination has not been clearly demonstrated. Here we report that serum specimens obtained from patients with chlamydiosis contain elementary bodies of C. trachomatis shown by culture and immunogold electron microscopy. We have found that 31 of the 52 patients had serum precipitates which were infective to McCoy cells. Immunostaining revealed very small inclusions resembling those reported during persistent C. trachomatis infection in vitro . DNA specimens from 49 (out of 52) patients with chlamydiosis gave positive PCR readings. The viability of the pathogen present in the sera was confirmed by chlamydial RNA detection in the cell monolayer inoculated by the serum precipitates. By using DNA isolation protocol from 1 mL of serum and quantitative TaqMan PCR, it was estimated that bacterial load in patients' sera was 2 × 10 2 –10 3 GE/mL. These findings for the first time demonstrated that C. trachomatis can be disseminated directly by the plasma, independently from blood cell, which may represent a new possible pathway of the chronic infection development. Therefore, new methodological approaches for detection of C. trachomatis in the serum of patients with complicated and chronic chlamydiosis could be important in the diagnosis of the infection regardless of its anatomical localization. Extragenital chlamydial complications may be associated with systemic spread of infection, but haematogenous route for C. trachomatis dissemination has not been clearly demonstrated. Here we report that serum specimens obtained from patients with chlamydiosis contain elementary bodies of C. trachomatis shown by culture and immunogold electron microscopy. We have found that 31 of the 52 patients had serum precipitates which were infective to McCoy cells. Immunostaining revealed very small inclusions resembling those reported during persistent C. trachomatis infection in vitro . DNA specimens from 49 (out of 52) patients with chlamydiosis gave positive PCR readings. The viability of the pathogen present in the sera was confirmed by chlamydial RNA detection in the cell monolayer inoculated by the serum precipitates. By using DNA isolation protocol from 1 mL of serum and quantitative TaqMan PCR, it was estimated that bacterial load in patients' sera was 2 super(102) - super(103) GE/mL. These findings for the first time demonstrated that C. trachomatis can be disseminated directly by the plasma, independently from blood cell, which may represent a new possible pathway of the chronic infection development. Therefore, new methodological approaches for detection of C. trachomatis in the serum of patients with complicated and chronic chlamydiosis could be important in the diagnosis of the infection regardless of its anatomical localization. Extragenital chlamydial complications may be associated with systemic spread of infection, but haematogenous route for C. trachomatis dissemination has not been clearly demonstrated. Here we report that serum specimens obtained from patients with chlamydiosis contain elementary bodies of C. trachomatis shown by culture and immunogold electron microscopy. We have found that 31 of the 52 patients had serum precipitates which were infective to McCoy cells. Immunostaining revealed very small inclusions resembling those reported during persistent C. trachomatis infection in vitro. DNA specimens from 49 (out of 52) patients with chlamydiosis gave positive PCR readings. The viability of the pathogen present in the sera was confirmed by chlamydial RNA detection in the cell monolayer inoculated by the serum precipitates. By using DNA isolation protocol from 1 mL of serum and quantitative TaqMan PCR, it was estimated that bacterial load in patients' sera was 2 × 10(2)-10(3) GE/mL. These findings for the first time demonstrated that C. trachomatis can be disseminated directly by the plasma, independently from blood cell, which may represent a new possible pathway of the chronic infection development. Therefore, new methodological approaches for detection of C. trachomatis in the serum of patients with complicated and chronic chlamydiosis could be important in the diagnosis of the infection regardless of its anatomical localization.Extragenital chlamydial complications may be associated with systemic spread of infection, but haematogenous route for C. trachomatis dissemination has not been clearly demonstrated. Here we report that serum specimens obtained from patients with chlamydiosis contain elementary bodies of C. trachomatis shown by culture and immunogold electron microscopy. We have found that 31 of the 52 patients had serum precipitates which were infective to McCoy cells. Immunostaining revealed very small inclusions resembling those reported during persistent C. trachomatis infection in vitro. DNA specimens from 49 (out of 52) patients with chlamydiosis gave positive PCR readings. The viability of the pathogen present in the sera was confirmed by chlamydial RNA detection in the cell monolayer inoculated by the serum precipitates. By using DNA isolation protocol from 1 mL of serum and quantitative TaqMan PCR, it was estimated that bacterial load in patients' sera was 2 × 10(2)-10(3) GE/mL. These findings for the first time demonstrated that C. trachomatis can be disseminated directly by the plasma, independently from blood cell, which may represent a new possible pathway of the chronic infection development. Therefore, new methodological approaches for detection of C. trachomatis in the serum of patients with complicated and chronic chlamydiosis could be important in the diagnosis of the infection regardless of its anatomical localization. Extragenital chlamydial complications may be associated with systemic spread of infection, but haematogenous route for C. trachomatis dissemination has not been clearly demonstrated. Here we report that serum specimens obtained from patients with chlamydiosis contain elementary bodies of C. trachomatis shown by culture and immunogold electron microscopy. We have found that 31 of the 52 patients had serum precipitates which were infective to McCoy cells. Immunostaining revealed very small inclusions resembling those reported during persistent C. trachomatis infection in vitro. DNA specimens from 49 (out of 52) patients with chlamydiosis gave positive PCR readings. The viability of the pathogen present in the sera was confirmed by chlamydial RNA detection in the cell monolayer inoculated by the serum precipitates. By using DNA isolation protocol from 1 mL of serum and quantitative TaqMan PCR, it was estimated that bacterial load in patients' sera was 2 × 10(2)-10(3) GE/mL. These findings for the first time demonstrated that C. trachomatis can be disseminated directly by the plasma, independently from blood cell, which may represent a new possible pathway of the chronic infection development. Therefore, new methodological approaches for detection of C. trachomatis in the serum of patients with complicated and chronic chlamydiosis could be important in the diagnosis of the infection regardless of its anatomical localization. |
| Audience | Academic |
| Author | Didenko, Lubov V. Kapotina, Lidia N. Koroleva, Ekaterina A. Morgunova, Elena Y. Petyaev, Ivan M. Rumyantseva, Yulia P. Zigangirova, Naylia A. Bashmakov, Yuriy K. Kost, Elena A. |
| AuthorAffiliation | 1 Department of Medical Microbiology, Gamaleya Institute of Epidemiology and Microbiology, Ministry of Health of the Russian Federation, Gamaleya Street 18, Moscow 123098, Russia 2 Lycotec Ltd., St John's Innovation Park, Cowley Road, Cambridge CB4 0WS, UK |
| AuthorAffiliation_xml | – name: 2 Lycotec Ltd., St John's Innovation Park, Cowley Road, Cambridge CB4 0WS, UK – name: 1 Department of Medical Microbiology, Gamaleya Institute of Epidemiology and Microbiology, Ministry of Health of the Russian Federation, Gamaleya Street 18, Moscow 123098, Russia |
| Author_xml | – sequence: 1 fullname: Petyaev, Ivan M. – sequence: 2 fullname: Bashmakov, Yuriy K. – sequence: 3 fullname: Kost, Elena A. – sequence: 4 fullname: Didenko, Lubov V. – sequence: 5 fullname: Kapotina, Lidia N. – sequence: 6 fullname: Morgunova, Elena Y. – sequence: 7 fullname: Rumyantseva, Yulia P. – sequence: 8 fullname: Zigangirova, Naylia A. – sequence: 9 fullname: Koroleva, Ekaterina A. |
| BackLink | https://www.ncbi.nlm.nih.gov/pubmed/23509729$$D View this record in MEDLINE/PubMed |
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| CitedBy_id | crossref_primary_10_17116_molgen201836041177 crossref_primary_10_1016_j_micres_2015_11_005 crossref_primary_10_3389_fmed_2017_00194 crossref_primary_10_15789_2220_7619_2018_3_316_324 crossref_primary_10_1155_2014_154627 crossref_primary_10_17116_patol20248605168 crossref_primary_10_3103_S089141681804002X |
| Cites_doi | 10.1128/JCM.40.12.4652-4658.2002 10.1086/652398 10.1128/IAI.54.1.90-95.1986 10.7861/clinmedicine.3-3-206 10.1111/j.1574-695X.2008.00526.x 10.1136/ard.2005.044966 10.1172/JCI119136 10.1111/j.1462-5822.2005.00627.x 10.1086/652397 10.1128/IAI.72.4.1843-1855.2004 10.1136/gut.28.11.1514 10.1016/S0966-842X(02)00011-2 10.1111/j.1600-0897.2009.00705.x 10.1128/JCM.38.6.2062-2064.2000 10.1002/hep.1840090328 10.2214/ajr.182.3.1820822 |
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| Copyright | Copyright © 2013 Naylia A. Zigangirova et al. COPYRIGHT 2013 John Wiley & Sons, Inc. Copyright © 2013 Naylia A. Zigangirova et al. 2013 |
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| Snippet | Extragenital chlamydial complications may be associated with systemic spread of infection, but haematogenous route for C. trachomatis dissemination has not... Extragenital chlamydial complications may be associated with systemic spread of infection, but haematogenous route for C. trachomatis dissemination has not... |
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| SubjectTerms | Adult Blood cells Chlamydia infections Chlamydia Infections - blood Chlamydia Infections - microbiology Chlamydia trachomatis - isolation & purification Development and progression Diagnosis DNA, Bacterial - analysis Electron microscopy Female Health aspects Humans Immunohistochemistry Male Microscopy, Fluorescence Middle Aged Plasma - microbiology Polymerase Chain Reaction Reproducibility of Results RNA, Ribosomal, 16S - analysis Urogenital System - microbiology Young Adult |
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| Title | Detection of C. trachomatis in the Serum of the Patients with Urogenital Chlamydiosis |
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