Tanić, Nasta

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  • Tanić, Nasta (2)
  • Tanic, Nasta (1)
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Author's Bibliography

Diagnostic testing for SARS-COV-2 by Real-time RT-PCR

Tanić, Nikola; Blagojević, Danijela; Milanović, Ivana; Imširović, Mirela; Lazić, Sandra; Maksimović, Zlatko; Tanić, Nasta

(Belgrade: Institute of Molecular Genetics and Genetic Engineering, University of Belgrade, 2023)

TY  - CONF
AU  - Tanić, Nikola
AU  - Blagojević, Danijela
AU  - Milanović, Ivana
AU  - Imširović, Mirela
AU  - Lazić, Sandra
AU  - Maksimović, Zlatko
AU  - Tanić, Nasta
PY  - 2023
UR  - http://radar.ibiss.bg.ac.rs/handle/123456789/6328
AB  - Introduction: Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) emerged at the end of 2019 and caused COVID-19 pandemic. This coronavirus disease pandemic demonstrated the importance of diagnostic testing in disease outbreak monitoring and control. So, reliable and accurate testing for SARS-CoV-2 was the principal prerequisite for preventing the spread of COVID-19.
Methods: Real Time RT-PCR (RT-qPCR) unquestionably represent the most reliable, rapid and sensitive method for detection of SARS-CoV-2 RNA. However, there are numerous different assays, protocols, reagents, instruments and result analysis methods in use without certified standards, standardized RNA extraction and reporting procedures. Therefore, in practice, the reliability of RT-qPCR results depends on a number of parameters that include sample collection and processing, method of RNA extraction, choice of assay, efficiency of assay, choice of instrument, analysis method as well as operator intervention.
Results: Here we present comparative analyses of the efficiency and sensitivity of 10 different amplification assays, as well as the relevance of manual RNA extractions compared to automatic one. Our results revealed that manual viral RNA extraction should be a method of choice for high sensitivity. In addition, amplification assays targeting three SARS-CoV-2 genes are much more efficient from those targeting one.
Conclusion: Unfortunately, RT-qPCR is almost exclusively used as qualitative diagnostic test for SARSCoV-2. We think that the ideal testing regimen would involve not just qualitative detection of SARS-CoV-2 but reliable and meaningful quantitative reporting of viral load.
PB  - Belgrade: Institute of Molecular Genetics and Genetic Engineering, University of Belgrade
C3  - Abstract Book: CoMBoS2 - the Second Congress of Molecular Biologists of Serbia; 2023 Oct 6-8; Belgrade, Serbia
T1  - Diagnostic testing for SARS-COV-2 by Real-time RT-PCR
IS  - 99
UR  - https://hdl.handle.net/21.15107/rcub_ibiss_6328
ER  - 
@conference{
author = "Tanić, Nikola and Blagojević, Danijela and Milanović, Ivana and Imširović, Mirela and Lazić, Sandra and Maksimović, Zlatko and Tanić, Nasta",
year = "2023",
abstract = "Introduction: Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) emerged at the end of 2019 and caused COVID-19 pandemic. This coronavirus disease pandemic demonstrated the importance of diagnostic testing in disease outbreak monitoring and control. So, reliable and accurate testing for SARS-CoV-2 was the principal prerequisite for preventing the spread of COVID-19.
Methods: Real Time RT-PCR (RT-qPCR) unquestionably represent the most reliable, rapid and sensitive method for detection of SARS-CoV-2 RNA. However, there are numerous different assays, protocols, reagents, instruments and result analysis methods in use without certified standards, standardized RNA extraction and reporting procedures. Therefore, in practice, the reliability of RT-qPCR results depends on a number of parameters that include sample collection and processing, method of RNA extraction, choice of assay, efficiency of assay, choice of instrument, analysis method as well as operator intervention.
Results: Here we present comparative analyses of the efficiency and sensitivity of 10 different amplification assays, as well as the relevance of manual RNA extractions compared to automatic one. Our results revealed that manual viral RNA extraction should be a method of choice for high sensitivity. In addition, amplification assays targeting three SARS-CoV-2 genes are much more efficient from those targeting one.
Conclusion: Unfortunately, RT-qPCR is almost exclusively used as qualitative diagnostic test for SARSCoV-2. We think that the ideal testing regimen would involve not just qualitative detection of SARS-CoV-2 but reliable and meaningful quantitative reporting of viral load.",
publisher = "Belgrade: Institute of Molecular Genetics and Genetic Engineering, University of Belgrade",
journal = "Abstract Book: CoMBoS2 - the Second Congress of Molecular Biologists of Serbia; 2023 Oct 6-8; Belgrade, Serbia",
title = "Diagnostic testing for SARS-COV-2 by Real-time RT-PCR",
number = "99",
url = "https://hdl.handle.net/21.15107/rcub_ibiss_6328"
}
Tanić, N., Blagojević, D., Milanović, I., Imširović, M., Lazić, S., Maksimović, Z.,& Tanić, N.. (2023). Diagnostic testing for SARS-COV-2 by Real-time RT-PCR. in Abstract Book: CoMBoS2 - the Second Congress of Molecular Biologists of Serbia; 2023 Oct 6-8; Belgrade, Serbia
Belgrade: Institute of Molecular Genetics and Genetic Engineering, University of Belgrade.(99).
https://hdl.handle.net/21.15107/rcub_ibiss_6328
Tanić N, Blagojević D, Milanović I, Imširović M, Lazić S, Maksimović Z, Tanić N. Diagnostic testing for SARS-COV-2 by Real-time RT-PCR. in Abstract Book: CoMBoS2 - the Second Congress of Molecular Biologists of Serbia; 2023 Oct 6-8; Belgrade, Serbia. 2023;(99).
https://hdl.handle.net/21.15107/rcub_ibiss_6328 .
Tanić, Nikola, Blagojević, Danijela, Milanović, Ivana, Imširović, Mirela, Lazić, Sandra, Maksimović, Zlatko, Tanić, Nasta, "Diagnostic testing for SARS-COV-2 by Real-time RT-PCR" in Abstract Book: CoMBoS2 - the Second Congress of Molecular Biologists of Serbia; 2023 Oct 6-8; Belgrade, Serbia, no. 99 (2023),
https://hdl.handle.net/21.15107/rcub_ibiss_6328 .

The Role of TP53 and PTEN tumor suppressor genes in response to different breast cancer treatment modalities

Tanić, Nikola; Dramićanin, Tatjana; Milovanović, Zorka; Nedeljković, Milica; Tomić, Tijana; Ademović, Nejla; Murganić, Blagoje; Tanic, Nasta

(Serbian Society for Immunology, Molecular Oncology and Regenerative Medicine, 2022)

TY  - CONF
AU  - Tanić, Nikola
AU  - Dramićanin, Tatjana
AU  - Milovanović, Zorka
AU  - Nedeljković, Milica
AU  - Tomić, Tijana
AU  - Ademović, Nejla
AU  - Murganić, Blagoje
AU  - Tanic, Nasta
PY  - 2022
UR  - http://radar.ibiss.bg.ac.rs/handle/123456789/5773
AB  - Breast cancer (BC) is the most frequent type of malignancy and the leading cause
of cancer related death among women worldwide. More than 70% of all diagnosed invasive
BCs express steroid receptors and, as such, are subjected to endocrine therapy.
BC is exceptionally heterogeneous disease and therefore distinct treatment modalities
are necessary to address these differences. The aim of our study was to investigate
the impact of TP53 and PTEN tumor suppressor genes (TSGs) inactivation on BC
response to different treatment modalities, as well as, their possible cooperation, on
post-operative BC samples. To that end the patients were classified, based on applied
adjuvant therapy, into four distinct groups: those that received hormonal therapy
(HT) only, hormonal therapy combined with chemotherapy (HT/CHT), hormonal
therapy combined with chemo and biological therapy (HT/CHT/H), and other systemic
therapies that exclude HT (for example CHT or H). Functional inactivation of
TP53 and PTEN TSG’s were studied by mutation, loss of heterozygosity (LOH) and
hypermethylatyon analysis. Our results revealed that TP53 gene was altered in 63 out
of 90 specimens (70%), while the frequency of PTEN alterations was slightly lower,
54 out of 90 (60%) patients had inactivated PTEN. Simultaneous inactivation was
detected in 43 tested samples (48%) with significant association between two analyzed
TSGs. Further, we found that TP53 status has significant influence on patients’
therapy response. Patients with wild type TP53 show significantly better therapy response
regardless of the type of therapy, compared to carriers of altered p53 gene. In
support of this we showed that hormonally treated women with intact (wt) TP53 gene
had significantly longer survival rate (p=0.000001) when compared to: (i) hormonally
treated women with aberrant TP53gene, (ii) women with intact (wt) p53 subjected to
any of remaining three therapy combinations, and (iii) women with altered TP53 that
belong to second (HT/CHT), third (HT/CHT/H) or forth (systemic Th that exclude
HT) therapy group. Contrary to this, no significance was found between mutational status of PTEN and various treatment modalities. However, significant association
was found between the type of applied therapy and simultaneous alterations of these
two TSGs (p=0.00001).
AB  - Рак дојке је најчешћи тип малигнитета и водећи узрок смрти од канцера код
жена широм света. Више од 70% свих дијагностикованих инвазивних карцинома
дојке експримира стероидне рецепторе и као такви су подобни за ендокрину терапију. Канцер дојке је изузетно хетерогена болест и стога су неопходни различити модалитети лечења да би се превазишле ове разлике. Циљ нашег истраживања
био је да се испита утицај инактивације ТП53 и ПТЕН тумор супресорских гена
(ТСГ) у одговору на различите модалитете лечења на постоперативним узорцима
карцинома дојке. Са тим циљем пацијенткиње су класификоване, на основу примењене ађувантне терапије, у четири различите групе: оне које су примале само
хормонску терапију (ХТ), хормонску терапију у комбинацији са хемиотерапијом
(ХТ/ЦХТ), хормонску терапију у комбинацији са хемиотерапијом и биолошком
терапијом (ХТ). /ЦХТ/Х) и друге системске терапије које искључују ХТ (на пример ЦХТ или Х). Функционална инактивација ТП53 и ПТЕН тумор супресора
је студирана анализом мутационог статуса, губитка хетерозиготности (ЛОХ) и
анализом метилационог статуса. Наши резултати су показали да је ТП53 ген измењен код 63 од 90 узорака (70%), док је учесталост промена ПТЕН гена била
нешто нижа, 54 од 90 (60%) пацијената је имало инактивиран ПТЕН. Симултана
инактивација је детектована у 43 тестирана узорка (48%) са значајном повезаношћу инактивације два анализирана тумор супресор гена.
Даље, показали смо да статус ТП53 има значајан утицај на одговор пацијената
на терапију. Пацијенти са дивљим типом (wt) ТП53 показују значајно бољи терапијски одговор без обзира на врсту терапије, у поређењу са носиоцима измењеног TП53. У прилог овоме показали смо да су хормонски лечене жене са интактним (wt) ТП53 геном имале значајно већу стопу преживљавања (п=0,000001) у
поређењу са: (1) женама леченим хормонсом теерапијом са аберантним ТП53 геном, (2) женама са интактним (wt) TП53 подвргнутим било којој од преостале три терапијске комбинације, и (3) женама са измењеним ТП53 које припадају другој
(ХТ/ЦХТ), трећој (ХТ/ЦХТ/Х) или четвртој (системска терапија која искључује ХТ) терапијској групи. Супротно овоме, нисмо утврдили значајну асоцијацију
између мутационог статуса ПТЕН-а и различитих модалитета лечења. Међутим,
утврђена је значајна повезаност између врсте примењене терапије и истовремених промена ова два тумор супресор гена (п=0,00001).
PB  - Serbian Society for Immunology, Molecular Oncology and Regenerative Medicine
C3  - Abstract Book: First Serbian molecular medicine congress; 2022 Jun 16-18; Foča, Bosnia and Herzegovina
T1  - The Role of TP53 and PTEN tumor suppressor genes in response to different breast cancer treatment modalities
T1  - Улога ТП53 и ПТЕН тумор супресор гена у одговору на различите модалитете терапије канцера дојке
SP  - 94
EP  - 97
UR  - https://hdl.handle.net/21.15107/rcub_ibiss_5773
ER  - 
@conference{
author = "Tanić, Nikola and Dramićanin, Tatjana and Milovanović, Zorka and Nedeljković, Milica and Tomić, Tijana and Ademović, Nejla and Murganić, Blagoje and Tanic, Nasta",
year = "2022",
abstract = "Breast cancer (BC) is the most frequent type of malignancy and the leading cause
of cancer related death among women worldwide. More than 70% of all diagnosed invasive
BCs express steroid receptors and, as such, are subjected to endocrine therapy.
BC is exceptionally heterogeneous disease and therefore distinct treatment modalities
are necessary to address these differences. The aim of our study was to investigate
the impact of TP53 and PTEN tumor suppressor genes (TSGs) inactivation on BC
response to different treatment modalities, as well as, their possible cooperation, on
post-operative BC samples. To that end the patients were classified, based on applied
adjuvant therapy, into four distinct groups: those that received hormonal therapy
(HT) only, hormonal therapy combined with chemotherapy (HT/CHT), hormonal
therapy combined with chemo and biological therapy (HT/CHT/H), and other systemic
therapies that exclude HT (for example CHT or H). Functional inactivation of
TP53 and PTEN TSG’s were studied by mutation, loss of heterozygosity (LOH) and
hypermethylatyon analysis. Our results revealed that TP53 gene was altered in 63 out
of 90 specimens (70%), while the frequency of PTEN alterations was slightly lower,
54 out of 90 (60%) patients had inactivated PTEN. Simultaneous inactivation was
detected in 43 tested samples (48%) with significant association between two analyzed
TSGs. Further, we found that TP53 status has significant influence on patients’
therapy response. Patients with wild type TP53 show significantly better therapy response
regardless of the type of therapy, compared to carriers of altered p53 gene. In
support of this we showed that hormonally treated women with intact (wt) TP53 gene
had significantly longer survival rate (p=0.000001) when compared to: (i) hormonally
treated women with aberrant TP53gene, (ii) women with intact (wt) p53 subjected to
any of remaining three therapy combinations, and (iii) women with altered TP53 that
belong to second (HT/CHT), third (HT/CHT/H) or forth (systemic Th that exclude
HT) therapy group. Contrary to this, no significance was found between mutational status of PTEN and various treatment modalities. However, significant association
was found between the type of applied therapy and simultaneous alterations of these
two TSGs (p=0.00001)., Рак дојке је најчешћи тип малигнитета и водећи узрок смрти од канцера код
жена широм света. Више од 70% свих дијагностикованих инвазивних карцинома
дојке експримира стероидне рецепторе и као такви су подобни за ендокрину терапију. Канцер дојке је изузетно хетерогена болест и стога су неопходни различити модалитети лечења да би се превазишле ове разлике. Циљ нашег истраживања
био је да се испита утицај инактивације ТП53 и ПТЕН тумор супресорских гена
(ТСГ) у одговору на различите модалитете лечења на постоперативним узорцима
карцинома дојке. Са тим циљем пацијенткиње су класификоване, на основу примењене ађувантне терапије, у четири различите групе: оне које су примале само
хормонску терапију (ХТ), хормонску терапију у комбинацији са хемиотерапијом
(ХТ/ЦХТ), хормонску терапију у комбинацији са хемиотерапијом и биолошком
терапијом (ХТ). /ЦХТ/Х) и друге системске терапије које искључују ХТ (на пример ЦХТ или Х). Функционална инактивација ТП53 и ПТЕН тумор супресора
је студирана анализом мутационог статуса, губитка хетерозиготности (ЛОХ) и
анализом метилационог статуса. Наши резултати су показали да је ТП53 ген измењен код 63 од 90 узорака (70%), док је учесталост промена ПТЕН гена била
нешто нижа, 54 од 90 (60%) пацијената је имало инактивиран ПТЕН. Симултана
инактивација је детектована у 43 тестирана узорка (48%) са значајном повезаношћу инактивације два анализирана тумор супресор гена.
Даље, показали смо да статус ТП53 има значајан утицај на одговор пацијената
на терапију. Пацијенти са дивљим типом (wt) ТП53 показују значајно бољи терапијски одговор без обзира на врсту терапије, у поређењу са носиоцима измењеног TП53. У прилог овоме показали смо да су хормонски лечене жене са интактним (wt) ТП53 геном имале значајно већу стопу преживљавања (п=0,000001) у
поређењу са: (1) женама леченим хормонсом теерапијом са аберантним ТП53 геном, (2) женама са интактним (wt) TП53 подвргнутим било којој од преостале три терапијске комбинације, и (3) женама са измењеним ТП53 које припадају другој
(ХТ/ЦХТ), трећој (ХТ/ЦХТ/Х) или четвртој (системска терапија која искључује ХТ) терапијској групи. Супротно овоме, нисмо утврдили значајну асоцијацију
између мутационог статуса ПТЕН-а и различитих модалитета лечења. Међутим,
утврђена је значајна повезаност између врсте примењене терапије и истовремених промена ова два тумор супресор гена (п=0,00001).",
publisher = "Serbian Society for Immunology, Molecular Oncology and Regenerative Medicine",
journal = "Abstract Book: First Serbian molecular medicine congress; 2022 Jun 16-18; Foča, Bosnia and Herzegovina",
title = "The Role of TP53 and PTEN tumor suppressor genes in response to different breast cancer treatment modalities, Улога ТП53 и ПТЕН тумор супресор гена у одговору на различите модалитете терапије канцера дојке",
pages = "94-97",
url = "https://hdl.handle.net/21.15107/rcub_ibiss_5773"
}
Tanić, N., Dramićanin, T., Milovanović, Z., Nedeljković, M., Tomić, T., Ademović, N., Murganić, B.,& Tanic, N.. (2022). The Role of TP53 and PTEN tumor suppressor genes in response to different breast cancer treatment modalities. in Abstract Book: First Serbian molecular medicine congress; 2022 Jun 16-18; Foča, Bosnia and Herzegovina
Serbian Society for Immunology, Molecular Oncology and Regenerative Medicine., 94-97.
https://hdl.handle.net/21.15107/rcub_ibiss_5773
Tanić N, Dramićanin T, Milovanović Z, Nedeljković M, Tomić T, Ademović N, Murganić B, Tanic N. The Role of TP53 and PTEN tumor suppressor genes in response to different breast cancer treatment modalities. in Abstract Book: First Serbian molecular medicine congress; 2022 Jun 16-18; Foča, Bosnia and Herzegovina. 2022;:94-97.
https://hdl.handle.net/21.15107/rcub_ibiss_5773 .
Tanić, Nikola, Dramićanin, Tatjana, Milovanović, Zorka, Nedeljković, Milica, Tomić, Tijana, Ademović, Nejla, Murganić, Blagoje, Tanic, Nasta, "The Role of TP53 and PTEN tumor suppressor genes in response to different breast cancer treatment modalities" in Abstract Book: First Serbian molecular medicine congress; 2022 Jun 16-18; Foča, Bosnia and Herzegovina (2022):94-97,
https://hdl.handle.net/21.15107/rcub_ibiss_5773 .

Immuno-histomorphometric and -fluorescent characteristics of GH cells after treatment with genistein or daidzein in an animal model of andropause

Ajdžanović, Vladimir; Jarić, Ivana; Živanović, Jasmina; Šošić-Jurjević, Branka ; Trifunović, Svetlana; Tanić, Nasta; Milošević, Verica

(Belgrade: Faculty of Veterinary Medicine, University of Belgrade, 2014)

TY  - JOUR
AU  - Ajdžanović, Vladimir
AU  - Jarić, Ivana
AU  - Živanović, Jasmina
AU  - Šošić-Jurjević, Branka 
AU  - Trifunović, Svetlana
AU  - Tanić, Nasta
AU  - Milošević, Verica
PY  - 2014
UR  - https://radar.ibiss.bg.ac.rs/handle/123456789/2279
AB  - Somatopause, the complex aspect of andropause, is recognizable by
   reduced growth hormone - GH/insulin-like growth factor 1 axis function
   in the ageing male. Soy isoflavones (usually genistein and daidzein),
   which are known for their beneficial effects in the treatment of ageing
   symptoms, are active in the pituitary, as well. The
   iromuno-histomorphometric and fluorescent characteristics of pituitary
   growth hormone secreting cells, in an animal model of andropause, were
   examined after a treatment with genistein or daidzein. Andropausal
   Wistar rats were divided into sham operated, orchidectomized and
   genistein or daidzein treated orchidectomized groups. Genistein or
   daidzein (30 mg/kg/day) were administered subcutaneously for three
   weeks, while sham operated and orchidectomized groups received the
   vehicle alone. Growth hormone secreting cells were identified by the
   percoxidase-antiperoxidase immuno-histochemical, and inmuno-fluorescent
   procedure. The main characteristic of growth hormone secreting cells in
   soy isoflavones treated groups is a weaker immuno-histochemical staining
   and immuno fluorescent signal compared to sham operated and
   orchidectomized groups. The growth hormone secreting cell volume in
   orchidectomized +genistein or +daidzein groups is by 13.8\% and 11.9\%
   (p<0.05) smaller respectively, in comparison with the orchidectomized
   group. In orchidectomized +genistein or +daidzein groups, the growth
   hormone secreting cells relative volume density is by 62.5\% and 61.0\%
   lower (p<0.05) respectively than for the sham operated group, and
   decreased by 65.4\% and 64.0\% (p<0.05) respectively, compared to the
   orchidectomized group. It can be concluded that chronic genistein or
   daidzein treatment, in an animal model of andropause, attenuates
   immuno-histomorphometric and fluorescent characteristics of growth
   hormone secreting cells.
PB  - Belgrade: Faculty of Veterinary Medicine, University of Belgrade
T2  - Acta Veterinaria-Beograd
T1  - Immuno-histomorphometric and -fluorescent characteristics of GH cells after treatment with genistein or daidzein in an animal model of andropause
IS  - 1
VL  - 64
DO  - 10.2478/acve-2014-0010
SP  - 93
EP  - 104
ER  - 
@article{
author = "Ajdžanović, Vladimir and Jarić, Ivana and Živanović, Jasmina and Šošić-Jurjević, Branka  and Trifunović, Svetlana and Tanić, Nasta and Milošević, Verica",
year = "2014",
abstract = "Somatopause, the complex aspect of andropause, is recognizable by
   reduced growth hormone - GH/insulin-like growth factor 1 axis function
   in the ageing male. Soy isoflavones (usually genistein and daidzein),
   which are known for their beneficial effects in the treatment of ageing
   symptoms, are active in the pituitary, as well. The
   iromuno-histomorphometric and fluorescent characteristics of pituitary
   growth hormone secreting cells, in an animal model of andropause, were
   examined after a treatment with genistein or daidzein. Andropausal
   Wistar rats were divided into sham operated, orchidectomized and
   genistein or daidzein treated orchidectomized groups. Genistein or
   daidzein (30 mg/kg/day) were administered subcutaneously for three
   weeks, while sham operated and orchidectomized groups received the
   vehicle alone. Growth hormone secreting cells were identified by the
   percoxidase-antiperoxidase immuno-histochemical, and inmuno-fluorescent
   procedure. The main characteristic of growth hormone secreting cells in
   soy isoflavones treated groups is a weaker immuno-histochemical staining
   and immuno fluorescent signal compared to sham operated and
   orchidectomized groups. The growth hormone secreting cell volume in
   orchidectomized +genistein or +daidzein groups is by 13.8\% and 11.9\%
   (p<0.05) smaller respectively, in comparison with the orchidectomized
   group. In orchidectomized +genistein or +daidzein groups, the growth
   hormone secreting cells relative volume density is by 62.5\% and 61.0\%
   lower (p<0.05) respectively than for the sham operated group, and
   decreased by 65.4\% and 64.0\% (p<0.05) respectively, compared to the
   orchidectomized group. It can be concluded that chronic genistein or
   daidzein treatment, in an animal model of andropause, attenuates
   immuno-histomorphometric and fluorescent characteristics of growth
   hormone secreting cells.",
publisher = "Belgrade: Faculty of Veterinary Medicine, University of Belgrade",
journal = "Acta Veterinaria-Beograd",
title = "Immuno-histomorphometric and -fluorescent characteristics of GH cells after treatment with genistein or daidzein in an animal model of andropause",
number = "1",
volume = "64",
doi = "10.2478/acve-2014-0010",
pages = "93-104"
}
Ajdžanović, V., Jarić, I., Živanović, J., Šošić-Jurjević, B., Trifunović, S., Tanić, N.,& Milošević, V.. (2014). Immuno-histomorphometric and -fluorescent characteristics of GH cells after treatment with genistein or daidzein in an animal model of andropause. in Acta Veterinaria-Beograd
Belgrade: Faculty of Veterinary Medicine, University of Belgrade., 64(1), 93-104.
https://doi.org/10.2478/acve-2014-0010
Ajdžanović V, Jarić I, Živanović J, Šošić-Jurjević B, Trifunović S, Tanić N, Milošević V. Immuno-histomorphometric and -fluorescent characteristics of GH cells after treatment with genistein or daidzein in an animal model of andropause. in Acta Veterinaria-Beograd. 2014;64(1):93-104.
doi:10.2478/acve-2014-0010 .
Ajdžanović, Vladimir, Jarić, Ivana, Živanović, Jasmina, Šošić-Jurjević, Branka , Trifunović, Svetlana, Tanić, Nasta, Milošević, Verica, "Immuno-histomorphometric and -fluorescent characteristics of GH cells after treatment with genistein or daidzein in an animal model of andropause" in Acta Veterinaria-Beograd, 64, no. 1 (2014):93-104,
https://doi.org/10.2478/acve-2014-0010 . .
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