TY  - JOUR
AU  - Maksić, Jasmina
AU  - Maksimović, Nela
AU  - Rasulić, Lukas
AU  - Milankov, Olgica
AU  - Marjanović, Ana
AU  - Cvetković, Dragana
AU  - Rakočević, Vidosava
AU  - Rakočević  Stojanović, Vidosava
AU  - Novaković, Ivana
PY  - 2023
UR  - http://rfasper.fasper.bg.ac.rs/handle/123456789/4756
AB  - Duchenne muscular dystrophy (DMD) and Becker muscular
dystrophy (BMD) are caused by mutations in the dystrophin gene. They are X-linked
recessive diseases, where males are affected and females are mostly healthy carriers of the
mutation. It is estimated that 2/3 mothers of DMD probands are carriers, while 1/3 of
patients have de novo mutations. The aim was to confirm the carrier status of females in the
families of DMD/BMD probands, using direct genetic methods. Methods. We tested 38
females from 31 families of DMD/BMD probands with deletion/duplication in the
dystrophin gene. Also, 4 cases of prenatal diagnosis of DMD/BMD were included. We
preformed the polymerase chain reaction (PCR) and the multiplex ligation-dependent
method (MLPA) for deletion detection, i.e. deletion/duplication in the dystrophin gene.
Results. In 31 DMD/BMD probands, we identified 87.1% deletions and 12.9%
duplications of one or more exons. Of the 29 tested mothers, mutations were found in 17
(14 deletions and 3 duplications). Mutations were found in 57.9% (11/19) mothers of DMD
and in 60% (6/10) mothers of BMD, respectively. Also, in probands with deletions 56%
(14/25) of mothers were carries and in probands with duplications 3 mothers of 4 (75%).
Of the 9 other female relatives, mutations were found in 4. In prenatal diagnosis, we
identified deletion in one male and one female foetus of one mother. Conclusion. The
study showed that mothers were carriers in almost 60% of sporadic cases of DMD/BMD
with deletions and duplication. Also, the carrier frequency tended to be higher in mothers
of the probands with duplication (75%) then in probands with deletions (56%). In the case
of a mother who was confirmed as a carrier, deletion was detected in 2 of 3 foetuses.
AB  - Dišenova mišićna distrofija (DMD) i Bekerova mišićna distrofija (BMD) su
uzrokovane mutacijama u genu za distrofin. To su X-vezane recesivne bolesti, gde
oboljevaju muškarci a žene su uglavnom zdravi prenosioci mutacije. Procenjeno je da su
kod DMD probanada 2/3 majki nosioci, dok 1/3 pacijenata ima novu mutaciju. Cilj rada je
bio da se utvrdi status prenosioca kod žena u porodicama obolelih od DMD/BMD,
primenom direktne genetičke metode. Metode. Testirali smo 38 žena iz 31 porodice
DMD/BMD probanada sa delecijama i duplikacijama u genu za distrofin. Takođe, u studiju
su bila uključena i 4 slučaja prenatalne DMD/BMD dijagnoze. Primenjene su metoda
lančane reakcije polimerizacije (PCR) i metoda višestrukog umnožavanja vezanih proba
(MLPA) za detekciju delecija, odnosno delecija i duplikacija u genu za distrofin. Rezultati.
Kod 31-og DMD/BMD probanda utvrđeno je 87,1% delecija i 12,9% duplikacija jednog ili
više egzona. Od 29 testiranih majki probanada, mutacije su nađene kod njih 17 (14 delecija
i 3 duplikacije). Mutacije su nađene kod 57,9% (11/19) majki probanada sa DMD
fenotipom i kod 60% majki probanada sa BMD. Takođe, kod probanada sa delecijom 56%
(14/25) majki su potvrđene kao nosioci, a kod probanada sa duplikacijom 3 od 4 majke
(75%). Od preostalih 9 ženskih srodnika, mutacije su nađene kod nijh 4. Prenatalnom
dijagnostikom utvrđene su delecije kod jednog muškog i jednog ženskog ploda iste majke.
Zaključak. Istraživanje je pokazalo da su majke bile nosioci u skoro 60% izolovanih
DMD/BMD slučajeva sa delecijama i duplikacijama. Takođe, učestalost majki nosioca kod
probanada sa duplikaciom (75%) se pokazala većom nego kod majki probanada sa
delecijom (56%). U slučaju majke koja je bila potvrđena kao nosilac, delecija je otkrivena
kod njena 2 ploda od 3 ispitana.
PB  - Vojnomedicinska akademija
T2  - Vojnosanitetski pregled
T1  - The importance of direct genetic testing to determine female carriers in dystrophinopathies
T1  - Značaj direktnog genetičkog testiranja za utvrđivanje žena prenosioca kod distrofinopatija
EP  - 207
IS  - 3
SP  - 201
VL  - 80
DO  - 10.2298/VSP190208030SM
ER  - 

@article{
author = "Maksić, Jasmina and Maksimović, Nela and Rasulić, Lukas and Milankov, Olgica and Marjanović, Ana and Cvetković, Dragana and Rakočević, Vidosava and Rakočević  Stojanović, Vidosava and Novaković, Ivana",
year = "2023",
abstract = "Duchenne muscular dystrophy (DMD) and Becker muscular
dystrophy (BMD) are caused by mutations in the dystrophin gene. They are X-linked
recessive diseases, where males are affected and females are mostly healthy carriers of the
mutation. It is estimated that 2/3 mothers of DMD probands are carriers, while 1/3 of
patients have de novo mutations. The aim was to confirm the carrier status of females in the
families of DMD/BMD probands, using direct genetic methods. Methods. We tested 38
females from 31 families of DMD/BMD probands with deletion/duplication in the
dystrophin gene. Also, 4 cases of prenatal diagnosis of DMD/BMD were included. We
preformed the polymerase chain reaction (PCR) and the multiplex ligation-dependent
method (MLPA) for deletion detection, i.e. deletion/duplication in the dystrophin gene.
Results. In 31 DMD/BMD probands, we identified 87.1% deletions and 12.9%
duplications of one or more exons. Of the 29 tested mothers, mutations were found in 17
(14 deletions and 3 duplications). Mutations were found in 57.9% (11/19) mothers of DMD
and in 60% (6/10) mothers of BMD, respectively. Also, in probands with deletions 56%
(14/25) of mothers were carries and in probands with duplications 3 mothers of 4 (75%).
Of the 9 other female relatives, mutations were found in 4. In prenatal diagnosis, we
identified deletion in one male and one female foetus of one mother. Conclusion. The
study showed that mothers were carriers in almost 60% of sporadic cases of DMD/BMD
with deletions and duplication. Also, the carrier frequency tended to be higher in mothers
of the probands with duplication (75%) then in probands with deletions (56%). In the case
of a mother who was confirmed as a carrier, deletion was detected in 2 of 3 foetuses., Dišenova mišićna distrofija (DMD) i Bekerova mišićna distrofija (BMD) su
uzrokovane mutacijama u genu za distrofin. To su X-vezane recesivne bolesti, gde
oboljevaju muškarci a žene su uglavnom zdravi prenosioci mutacije. Procenjeno je da su
kod DMD probanada 2/3 majki nosioci, dok 1/3 pacijenata ima novu mutaciju. Cilj rada je
bio da se utvrdi status prenosioca kod žena u porodicama obolelih od DMD/BMD,
primenom direktne genetičke metode. Metode. Testirali smo 38 žena iz 31 porodice
DMD/BMD probanada sa delecijama i duplikacijama u genu za distrofin. Takođe, u studiju
su bila uključena i 4 slučaja prenatalne DMD/BMD dijagnoze. Primenjene su metoda
lančane reakcije polimerizacije (PCR) i metoda višestrukog umnožavanja vezanih proba
(MLPA) za detekciju delecija, odnosno delecija i duplikacija u genu za distrofin. Rezultati.
Kod 31-og DMD/BMD probanda utvrđeno je 87,1% delecija i 12,9% duplikacija jednog ili
više egzona. Od 29 testiranih majki probanada, mutacije su nađene kod njih 17 (14 delecija
i 3 duplikacije). Mutacije su nađene kod 57,9% (11/19) majki probanada sa DMD
fenotipom i kod 60% majki probanada sa BMD. Takođe, kod probanada sa delecijom 56%
(14/25) majki su potvrđene kao nosioci, a kod probanada sa duplikacijom 3 od 4 majke
(75%). Od preostalih 9 ženskih srodnika, mutacije su nađene kod nijh 4. Prenatalnom
dijagnostikom utvrđene su delecije kod jednog muškog i jednog ženskog ploda iste majke.
Zaključak. Istraživanje je pokazalo da su majke bile nosioci u skoro 60% izolovanih
DMD/BMD slučajeva sa delecijama i duplikacijama. Takođe, učestalost majki nosioca kod
probanada sa duplikaciom (75%) se pokazala većom nego kod majki probanada sa
delecijom (56%). U slučaju majke koja je bila potvrđena kao nosilac, delecija je otkrivena
kod njena 2 ploda od 3 ispitana.",
publisher = "Vojnomedicinska akademija",
journal = "Vojnosanitetski pregled",
title = "The importance of direct genetic testing to determine female carriers in dystrophinopathies, Značaj direktnog genetičkog testiranja za utvrđivanje žena prenosioca kod distrofinopatija",
pages = "207-201",
number = "3",
volume = "80",
doi = "10.2298/VSP190208030SM"
}

Maksić, J., Maksimović, N., Rasulić, L., Milankov, O., Marjanović, A., Cvetković, D., Rakočević, V., Rakočević  Stojanović, V.,& Novaković, I.. (2023). The importance of direct genetic testing to determine female carriers in dystrophinopathies. in Vojnosanitetski pregled
Vojnomedicinska akademija., 80(3), 201-207.
https://doi.org/10.2298/VSP190208030SM

Maksić J, Maksimović N, Rasulić L, Milankov O, Marjanović A, Cvetković D, Rakočević V, Rakočević  Stojanović V, Novaković I. The importance of direct genetic testing to determine female carriers in dystrophinopathies. in Vojnosanitetski pregled. 2023;80(3):201-207.
doi:10.2298/VSP190208030SM .

Maksić, Jasmina, Maksimović, Nela, Rasulić, Lukas, Milankov, Olgica, Marjanović, Ana, Cvetković, Dragana, Rakočević, Vidosava, Rakočević  Stojanović, Vidosava, Novaković, Ivana, "The importance of direct genetic testing to determine female carriers in dystrophinopathies" in Vojnosanitetski pregled, 80, no. 3 (2023):201-207,
https://doi.org/10.2298/VSP190208030SM . .

TY  - BOOK
AU  - Kostić, Vladimir
AU  - Apostolski, Slobodan
AU  - Bulat, Petar
AU  - Bumbaširević, ljiljana
AU  - Cerovac, Nataša
AU  - Dragašević, Nataša
AU  - Jančić, Jasna
AU  - Jovanović, Dejana
AU  - Jovanović, Zagorka
AU  - Jović, Nebojša
AU  - Kozić, Dušan
AU  - Lavrnić, Dragana
AU  - Martinović, Žarko
AU  - Milić, Vedrana
AU  - Drulović, Jelena
AU  - Ocić, Gordana
AU  - Pavlović, Dragan
AU  - Rakočević, Vidosava
PY  - 2016
UR  - http://rfasper.fasper.bg.ac.rs/handle/123456789/2515
PB  - Medicinski fakultet u Beogradu
T1  - Neurologija za studente medicine
SP  - 397
UR  - https://hdl.handle.net/21.15107/rcub_rfasper_2515
ER  - 

@book{
author = "Kostić, Vladimir and Apostolski, Slobodan and Bulat, Petar and Bumbaširević, ljiljana and Cerovac, Nataša and Dragašević, Nataša and Jančić, Jasna and Jovanović, Dejana and Jovanović, Zagorka and Jović, Nebojša and Kozić, Dušan and Lavrnić, Dragana and Martinović, Žarko and Milić, Vedrana and Drulović, Jelena and Ocić, Gordana and Pavlović, Dragan and Rakočević, Vidosava",
year = "2016",
publisher = "Medicinski fakultet u Beogradu",
title = "Neurologija za studente medicine",
pages = "397",
url = "https://hdl.handle.net/21.15107/rcub_rfasper_2515"
}

Kostić, V., Apostolski, S., Bulat, P., Bumbaširević, l., Cerovac, N., Dragašević, N., Jančić, J., Jovanović, D., Jovanović, Z., Jović, N., Kozić, D., Lavrnić, D., Martinović, Ž., Milić, V., Drulović, J., Ocić, G., Pavlović, D.,& Rakočević, V.. (2016). Neurologija za studente medicine. 
Medicinski fakultet u Beogradu., 397.
https://hdl.handle.net/21.15107/rcub_rfasper_2515

Kostić V, Apostolski S, Bulat P, Bumbaširević L, Cerovac N, Dragašević N, Jančić J, Jovanović D, Jovanović Z, Jović N, Kozić D, Lavrnić D, Martinović Ž, Milić V, Drulović J, Ocić G, Pavlović D, Rakočević V. Neurologija za studente medicine. 2016;:397.
https://hdl.handle.net/21.15107/rcub_rfasper_2515 .

Kostić, Vladimir, Apostolski, Slobodan, Bulat, Petar, Bumbaširević, ljiljana, Cerovac, Nataša, Dragašević, Nataša, Jančić, Jasna, Jovanović, Dejana, Jovanović, Zagorka, Jović, Nebojša, Kozić, Dušan, Lavrnić, Dragana, Martinović, Žarko, Milić, Vedrana, Drulović, Jelena, Ocić, Gordana, Pavlović, Dragan, Rakočević, Vidosava, "Neurologija za studente medicine" (2016):397,
https://hdl.handle.net/21.15107/rcub_rfasper_2515 .

TY  - JOUR
AU  - Marinković, Dragan
AU  - Milenković, Sanja
AU  - Rakočević, Vidosava
AU  - Marinković, Tatjana
PY  - 2009
UR  - http://rfasper.fasper.bg.ac.rs/handle/123456789/256
AB  - Over the last decade, fluorescence in situ hybridization (FISH) has become a firmly established clinical and research tool for the recognition of chromosome imbalances within interphase nuclei. Detectable alterations involve aneusomies, deletions, amplifications and translocations, with huge advantage in preserved morphology of the specimen, similarity with immunohistochemistry and applicability to formalinfixed paraffin-embedded material. However, this technique is not widely used in the routine diagnostics evaluations due to perception that is technically demanding, especially if paraffin-embedded tissues are used. The relevance of FISH method greatly enhanced recently with technical advances such as improved hybridization protocols, expanded probe and fluorochrome availability, multicolor analysis and advent of assays like tissue microarrays. In this review, we discussed main FISH principles and improvements, highlighted main advantages and disadvantages of FISH and familiarize the reader with current applications in diagnostics and research. We hope that these suggestions will make FISH technology more accessible to routine diagnostic and investigative laboratories.
AB  - Tokom poslednje decenije, fluorescentna in situ hibridizacija (FISH) postala je standardna klinička i istraživačka metoda za utvrđivanje hromozomskih aberacija u interfaznom jedru ćelije. Hromozomske alteracije koje se mogu detektovati uključuju aneuzomije, delecije, amplifikacije i translokacije, sa velikom prednošću u očuvanoj morfologiji uzorka, sličnosti sa imunohistohemijom i primenljivosti na formalin-fiksiran parafinom obložen materijal. Međutim, ova se tehnika ne koristi dovoljno u rutinskim dijagnostičkim analizama verovatno zbog sklonosti mišljenju da je tehnički zahtevna, posebno u slučaju kada se koriste uzorci iz parafinskih blokova. Značaj FISH metode je porastao u poslednje vreme sa unapređenjem tehničkih mogućnosti kao što su poboljšani hibridizacioni protokoli, povećana dostupnost proba i fluorohroma, multikolorna analiza i uključivanjem eseja kao što je tissue microarray. U ovom revijskom radu, diskutovali smo osnovne principe FISH tehnike, ukazali smo na glavne prednosti i nedostatke i upoznali smo čitaoca sa trenutnim aplikacijama u dijagnostici i istraživačkom radu. Nadamo se da će ove sugestije učiniti FISH dostupnijim rutinskoj dijagnostici i istraživačkim laboratorijama.
PB  - Kliničko-bolnički centar Zemun, Beograd
T2  - Materia medica
T1  - FISH method in theory and practice
T1  - FISH metoda u teoriji i praksi
EP  - 33
IS  - 1
SP  - 19
VL  - 25
UR  - https://hdl.handle.net/21.15107/rcub_rfasper_256
ER  - 

@article{
author = "Marinković, Dragan and Milenković, Sanja and Rakočević, Vidosava and Marinković, Tatjana",
year = "2009",
abstract = "Over the last decade, fluorescence in situ hybridization (FISH) has become a firmly established clinical and research tool for the recognition of chromosome imbalances within interphase nuclei. Detectable alterations involve aneusomies, deletions, amplifications and translocations, with huge advantage in preserved morphology of the specimen, similarity with immunohistochemistry and applicability to formalinfixed paraffin-embedded material. However, this technique is not widely used in the routine diagnostics evaluations due to perception that is technically demanding, especially if paraffin-embedded tissues are used. The relevance of FISH method greatly enhanced recently with technical advances such as improved hybridization protocols, expanded probe and fluorochrome availability, multicolor analysis and advent of assays like tissue microarrays. In this review, we discussed main FISH principles and improvements, highlighted main advantages and disadvantages of FISH and familiarize the reader with current applications in diagnostics and research. We hope that these suggestions will make FISH technology more accessible to routine diagnostic and investigative laboratories., Tokom poslednje decenije, fluorescentna in situ hibridizacija (FISH) postala je standardna klinička i istraživačka metoda za utvrđivanje hromozomskih aberacija u interfaznom jedru ćelije. Hromozomske alteracije koje se mogu detektovati uključuju aneuzomije, delecije, amplifikacije i translokacije, sa velikom prednošću u očuvanoj morfologiji uzorka, sličnosti sa imunohistohemijom i primenljivosti na formalin-fiksiran parafinom obložen materijal. Međutim, ova se tehnika ne koristi dovoljno u rutinskim dijagnostičkim analizama verovatno zbog sklonosti mišljenju da je tehnički zahtevna, posebno u slučaju kada se koriste uzorci iz parafinskih blokova. Značaj FISH metode je porastao u poslednje vreme sa unapređenjem tehničkih mogućnosti kao što su poboljšani hibridizacioni protokoli, povećana dostupnost proba i fluorohroma, multikolorna analiza i uključivanjem eseja kao što je tissue microarray. U ovom revijskom radu, diskutovali smo osnovne principe FISH tehnike, ukazali smo na glavne prednosti i nedostatke i upoznali smo čitaoca sa trenutnim aplikacijama u dijagnostici i istraživačkom radu. Nadamo se da će ove sugestije učiniti FISH dostupnijim rutinskoj dijagnostici i istraživačkim laboratorijama.",
publisher = "Kliničko-bolnički centar Zemun, Beograd",
journal = "Materia medica",
title = "FISH method in theory and practice, FISH metoda u teoriji i praksi",
pages = "33-19",
number = "1",
volume = "25",
url = "https://hdl.handle.net/21.15107/rcub_rfasper_256"
}

Marinković, D., Milenković, S., Rakočević, V.,& Marinković, T.. (2009). FISH method in theory and practice. in Materia medica
Kliničko-bolnički centar Zemun, Beograd., 25(1), 19-33.
https://hdl.handle.net/21.15107/rcub_rfasper_256

Marinković D, Milenković S, Rakočević V, Marinković T. FISH method in theory and practice. in Materia medica. 2009;25(1):19-33.
https://hdl.handle.net/21.15107/rcub_rfasper_256 .

Marinković, Dragan, Milenković, Sanja, Rakočević, Vidosava, Marinković, Tatjana, "FISH method in theory and practice" in Materia medica, 25, no. 1 (2009):19-33,
https://hdl.handle.net/21.15107/rcub_rfasper_256 .