CAN MYCOPLASMA INFECTION AFFECT THE PATHOGENESIS OF PROSTATE CANCER?

CAN MYCOPLASMA INFECTION AFFECT THE PATHOGENESIS OF PROSTATE CANCER?

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<span>Objective: to define a possible correlation between Mycoplasma infection persistence and prostate cancer (PC). Subjects and methods. Two hundred and fifty males aged 45 to 83 years (mean age 65.50.71 years) with suspected PC were examined. In all the patients, polyfocal prostate biopsy f...

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Main Authors: Yu. G. Alyaev, A. Z. Vinarov, D. N. Fiyev, Yu. A. Barykova, N. A. Vinarova, D. Yu. Logunov, M. M. Shmarov, B. S. Naroditsky, A. V. Gudkov, A. L. Gintsburg
Format: Article
Language:Russian
Published: ABV-press 2014-07-01
Series:Onkourologiâ
Subjects:
prostate cancer
viral and infectious diseases
correlation
Mycoplasma
Online Access:http://oncourology.abvpress.ru/index.php/oncur/article/view/13
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spelling doaj-fa7de256f5df4fc99c7190f436e4029f2020-11-24T20:57:48ZrusABV-pressOnkourologiâ 1726-97761996-18122014-07-0161283228CAN MYCOPLASMA INFECTION AFFECT THE PATHOGENESIS OF PROSTATE CANCER?Yu. G. Alyaev0A. Z. Vinarov1D. N. Fiyev2Yu. A. Barykova3N. A. Vinarova4D. Yu. Logunov5M. M. Shmarov6B. S. Naroditsky7A. V. Gudkov8A. L. Gintsburg9I.M. Sechenov Moscow Medical AcademyI.M. Sechenov Moscow Medical AcademyI.M. Sechenov Moscow Medical AcademyN.F. Gamaleya Research Institute of Experimental MedicineI.M. Sechenov Moscow Medical AcademyN.F. Gamaleya Research Institute of Experimental MedicineN.F. Gamaleya Research Institute of Experimental MedicineN.F. Gamaleya Research Institute of Experimental MedicineInstitute of Cancer, Roswell Park, USAN.F. Gamaleya Research Institute of Experimental Medicine<span>Objective: to define a possible correlation between Mycoplasma infection persistence and prostate cancer (PC). Subjects and methods. Two hundred and fifty males aged 45 to 83 years (mean age 65.50.71 years) with suspected PC were examined. In all the patients, polyfocal prostate biopsy from 12 points was carried out, by additionally taking 2 tissue columns from the peripheral area of both lobes. The basic material was referred for morphological study; the two additional columns were tested for Mycoplasma DNA by a polymerase chain reaction (PCR) and real-time PCR. The study was blind. According to the morphological findings, the patients were divided into 2 groups: 1) those with chronic prostatitis, prostate adenoma, low-grade prostatic interstitial neoplasia (PIN); 2) those with high-grade PIN (HG-PIN), PC. There were no age differences between the groups (p = 0.05). Results. The standard procedure for PCR was applied to 127 subjects. Twenty-six (20.5%) of the 127 subjects with suspected PC were found to have Mycoplasma infection, Mycoplasma being detected in 21 (26.2%) of the 81 patients with verified HG-PIN and PC. Mycoplasma hominis was encountered in 19 (15%) patients of the 127 subjects with suspected PC and this infection was present in 16 (20%) of the 81 patients with verified HG-PIN and PC. Comparison of the frequency of HG-PIN and PC in the patients of general group (60%) and in those with Mycoplasma infection (80.8%) revealed significant differences (p = 0.031). HG-PIN and PC were also significantly more frequently seen in the patients with Mycoplasma hominis (84.2%) that in the general patient group (60%) (p = 0.033). There were no significant differences in the frequency of HG-PIN and PC between the patients from the general group (60%) and those with Mycoplasma genitalium (71.4%) (p = 0.05). The patients with verified PC and HG-PIN were more frequently found to have Mycoplasma hominis (20%) than Mycoplasma genitalium (6.2%), which further drew our closer attention to just this pathogen. The real-time PCR was used in 123 subjects to detect Mycoplasma. HG-PIN and prostate adenocarcinoma were revealed in 63 of the 123 patients with suspected PC, Mycoplasma hominis was seen in 46 (37%). The frequency (n=46) was 73.9%. The frequency of HG-PIN and PC was significantly higher in the patients with isolated Mycoplasma hominis DNA that in those without this pathogen (p &lt; 0.001). Conclusion. Thus, the investigation showed a significantly higher correlation in the frequency of HG-PIN and PC in the patients with Mycoplasma infection that in the general study patients with suspected PC. This was supported by the use of both the standard procedure for Mycoplasma DNA determination and real-time PCR diagnosis.</span>http://oncourology.abvpress.ru/index.php/oncur/article/view/13prostate cancerviral and infectious diseasescorrelationMycoplasma
collection DOAJ
language Russian
format Article
sources DOAJ
author Yu. G. Alyaev
A. Z. Vinarov
D. N. Fiyev
Yu. A. Barykova
N. A. Vinarova
D. Yu. Logunov
M. M. Shmarov
B. S. Naroditsky
A. V. Gudkov
A. L. Gintsburg
spellingShingle Yu. G. Alyaev
A. Z. Vinarov
D. N. Fiyev
Yu. A. Barykova
N. A. Vinarova
D. Yu. Logunov
M. M. Shmarov
B. S. Naroditsky
A. V. Gudkov
A. L. Gintsburg
CAN MYCOPLASMA INFECTION AFFECT THE PATHOGENESIS OF PROSTATE CANCER?
Onkourologiâ
prostate cancer
viral and infectious diseases
correlation
Mycoplasma
author_facet Yu. G. Alyaev
A. Z. Vinarov
D. N. Fiyev
Yu. A. Barykova
N. A. Vinarova
D. Yu. Logunov
M. M. Shmarov
B. S. Naroditsky
A. V. Gudkov
A. L. Gintsburg
author_sort Yu. G. Alyaev
title CAN MYCOPLASMA INFECTION AFFECT THE PATHOGENESIS OF PROSTATE CANCER?
title_short CAN MYCOPLASMA INFECTION AFFECT THE PATHOGENESIS OF PROSTATE CANCER?
title_full CAN MYCOPLASMA INFECTION AFFECT THE PATHOGENESIS OF PROSTATE CANCER?
title_fullStr CAN MYCOPLASMA INFECTION AFFECT THE PATHOGENESIS OF PROSTATE CANCER?
title_full_unstemmed CAN MYCOPLASMA INFECTION AFFECT THE PATHOGENESIS OF PROSTATE CANCER?
title_sort can mycoplasma infection affect the pathogenesis of prostate cancer?
publisher ABV-press
series Onkourologiâ
issn 1726-9776
1996-1812
publishDate 2014-07-01
description <span>Objective: to define a possible correlation between Mycoplasma infection persistence and prostate cancer (PC). Subjects and methods. Two hundred and fifty males aged 45 to 83 years (mean age 65.50.71 years) with suspected PC were examined. In all the patients, polyfocal prostate biopsy from 12 points was carried out, by additionally taking 2 tissue columns from the peripheral area of both lobes. The basic material was referred for morphological study; the two additional columns were tested for Mycoplasma DNA by a polymerase chain reaction (PCR) and real-time PCR. The study was blind. According to the morphological findings, the patients were divided into 2 groups: 1) those with chronic prostatitis, prostate adenoma, low-grade prostatic interstitial neoplasia (PIN); 2) those with high-grade PIN (HG-PIN), PC. There were no age differences between the groups (p = 0.05). Results. The standard procedure for PCR was applied to 127 subjects. Twenty-six (20.5%) of the 127 subjects with suspected PC were found to have Mycoplasma infection, Mycoplasma being detected in 21 (26.2%) of the 81 patients with verified HG-PIN and PC. Mycoplasma hominis was encountered in 19 (15%) patients of the 127 subjects with suspected PC and this infection was present in 16 (20%) of the 81 patients with verified HG-PIN and PC. Comparison of the frequency of HG-PIN and PC in the patients of general group (60%) and in those with Mycoplasma infection (80.8%) revealed significant differences (p = 0.031). HG-PIN and PC were also significantly more frequently seen in the patients with Mycoplasma hominis (84.2%) that in the general patient group (60%) (p = 0.033). There were no significant differences in the frequency of HG-PIN and PC between the patients from the general group (60%) and those with Mycoplasma genitalium (71.4%) (p = 0.05). The patients with verified PC and HG-PIN were more frequently found to have Mycoplasma hominis (20%) than Mycoplasma genitalium (6.2%), which further drew our closer attention to just this pathogen. The real-time PCR was used in 123 subjects to detect Mycoplasma. HG-PIN and prostate adenocarcinoma were revealed in 63 of the 123 patients with suspected PC, Mycoplasma hominis was seen in 46 (37%). The frequency (n=46) was 73.9%. The frequency of HG-PIN and PC was significantly higher in the patients with isolated Mycoplasma hominis DNA that in those without this pathogen (p &lt; 0.001). Conclusion. Thus, the investigation showed a significantly higher correlation in the frequency of HG-PIN and PC in the patients with Mycoplasma infection that in the general study patients with suspected PC. This was supported by the use of both the standard procedure for Mycoplasma DNA determination and real-time PCR diagnosis.</span>
topic prostate cancer
viral and infectious diseases
correlation
Mycoplasma
url http://oncourology.abvpress.ru/index.php/oncur/article/view/13
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