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Stabilnost različnih oblik železovih intravenskih preparatov in njihov privzem v makrofage in vitro
ID Kuhanec, Danaja (Author), ID Marc, Janja (Mentor) More about this mentor... This link opens in a new window, ID Kristan, Katja (Comentor)

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Abstract
Železo je esencialni element in pomembna sestavina vsakega živega organizma. Ob pomanjkanju železa pri ljudeh lahko pride do pojava pogoste hematološke bolezni, anemije zaradi pomanjkanja železa. V državah tretjega sveta je vzrok za to anemijo običajno podhranjenost, medtem ko so v razvitih državah vzroki ponavadi prekomerna izguba krvi, posledica malabsorpcije in kroničnih bolezni. Zdravljenje anemije zaradi pomanjkanja železa je cenovno ugodno in preprosto z uporabo peroralnih pripravkov Fe2+ soli. Tovrstno zdravljenje pa ima lahko neželene učinke na gastrointestinalni trakt, prav tako pa se nekateri bolniki ne odzivajo na zdravljenje s peroralnimi pripravki. Tako je prišlo do razvoja parenteralnih železovih pripravkov, ki bi omogočali hitro, učinkovito in varno nadomestitev pomanjkanja železa. Namen naše magistrske naloge je bila primerjava stabilnosti parenteralnih železovih pripravkov druge in tretje generacije, ki so dostopni na trgu, ter in vitro ovrednotenje njihove varnosti. V študiji smo uporabili šest različnih formulacij parenteralnih železovih pripravkov. Železov glukonat, železov saharat in železov dekstran z nizko molekulsko maso (en intravenski in en intramuskularni pripravek) spadajo v drugo generacijo parenteralnih železovih pripravkov. Železova karboksimaltoza, ferumoksitol in železov (III) izomaltozid 1000 spadajo v tretjo generacijo parenteralnih železovih pripravkov. V študiji smo ovrednotili stabilnost in hitrost razgradnje železovih pripravkov pri različnih temperaturnih in časovnih pogojih s pomočjo reducenta in s kislinsko hidrolizo. Prav tako smo določili nivo labilnega železa pripravkov v serumu in ocenili obseg privzema železovih kompleksov iz različnih pripravkov v celice retikuloendotelnega sistema s študijo fagocitoze monocitov/makrofagov. S kombinacijo metod smo poskušali ponazoriti obnašanje železovih pripravkov po aplikaciji in oceniti, ali je predpisan način njihovega doziranja učinkovit ter varen. Ugotovili smo, da izbira ogljikovega hidrata v posameznem železovem kompleksu vpliva na stabilnost formulacije zdravila, količino labilnega železa in s tem povezano toksičnostjo. Na relativno stabilnost železovega kompleksa pa vplivata tudi njegova velikost in molekulska masa. Pripravki druge generacije so po velikosti in molekulski masi med manjšimi na trgu. Rezultati so pokazali nižjo relativno stabilnost kompleksov (nizka termostabilnost pripravkov, najhitrejši profili sproščanja), največ labilnega železa, največjo stopnjo hidrolize v kislini ter manjši obseg fagocitoze pri pripravkih druge generacije. Med železovimi pripravki druge generacije je železov dekstran z nizko molekulsko maso povezan z večjo relativno stabilnostjo. Po velikosti in molekulski masi nato železovemu dekstranu z nizko molekulsko maso sledijo pripravki tretje generacije. Ti kažejo visoko relativno stabilnost (večja termostabilnost pripravkov, počasnejši profili sproščanja), manjšo stopnjo hidrolize v kislini in najmanjši odsotek labilnega železa. Poleg tega smo ugotovili, da je v največji meri fagocitiran ferumoksitol, ki ima največjo molekulsko maso. Če povzamemo bi lahko razvrstili železove pripravke glede na njihovo relativno stabilnost formulacije sledeče: železov glukonat < železov saharat << železov dekstran z nizko molekulsko maso ⡈ železova karboksimaltoza ⡈ železov (III) izomaltozid ⡈ ferumoksitol. Iz rezultatov lahko sklepamo, da pridobljeni in vitro podatki o železovih pripravkih druge in tretje generacije potrjujejo rezulate kilničnih študij, ki so dokazale, da so izdelki klinično varni. Iz pridobljenih rezultatov je razvidno, da je upoštevanje lastnosti pripravkov zelo pomembno pri odločitvah tekom terapije v kliniki. Železovi pripravki druge generacije so primerni za dlje trajajočo aplikacijo zdravila (med 30 in 60 minut) in v nižjih enkratnih odmerkih. Posledično so bolj primerni za bolnike, ki večkrat obiščejo zdravstvene ustanove. Zdravstveni sistem pa si prizadeva, da zraven varnosti in zadovoljstva pacientov upoštevamo tudi stroškovno učinkovitost storitev. S tem namenom v ospredje prihajajo parenteralni železovi pripravki tretje generacije, saj so primerni za klinično varno, hitro in enkratno nadomestitev večjih potreb po železu.

Language:Slovenian
Keywords:Železovi intravenski pripravki, labilno železo, stabilnost, fagocitoza, anemija.
Work type:Master's thesis/paper
Organization:FFA - Faculty of Pharmacy
Year:2020
PID:20.500.12556/RUL-121253 This link opens in a new window
Publication date in RUL:02.10.2020
Views:2387
Downloads:270
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Secondary language

Language:English
Title:Stability of various intravenous iron formulations and their in vitro uptake into macrophages
Abstract:
Iron is an essential element and an important component of every living organism. When people suffer from iron deficiency, a common haematological problem can occur - iron deficiency anemia (IDA). In third world countries, IDA is frequently linked to malnutrition, in developed countries the most common causes are excessive blood loss, malabsorption and chronic diseases. The treatment of iron deficiency anemia is oral iron replacement therapy, which is affordable and simple. However, this type of treatment can be limited by gastrointestinal side effects and some patients do not respond to treatment. Therefore, parenteral iron preparations have been developed enabling rapid, effective and safe iron substitution. During our master´s thesis we have compared the stability of second and third generation intravenous iron preparations that are available on the market, and evaluated their safety in vitro. Six different types of parenteral iron formulations have been used in the study. Iron gluconate, iron sucrose and low molecular weight iron dextran belong to the second generation of parenteral iron preparations. Iron carboxymaltose, ferumoxytol and iron (III) isomaltoside 1000 belong to the third generation of parenteral iron preparations. During the study, the stability and degradation rate of iron preparations were analyzed using a reducing agent buffer and acid hydrolysis. We have determined the relative labile iron release in the serum. Furthermore, we have assessed the uptake of iron complexes into mouse monocytes/macrophages. By using a combination of methods, we have tried to illustrate the behavior of iron preparations after their administration. We have also tried to assess whether the prescribed dosing technique is effective and safe. We found that the choice of carbohydrate ligand in an individual iron complex affects the formulation´s stability, the amount of labile iron and consequently, its toxicity. The relative stability of the iron complex is also affected by the size and molecular weight of the iron complex. Second generation preparations are among the smallest on the market in terms of their size and molecular weight. Our study results coincide with their physicochemical properties – they have lower relative stability of complexes (low thermal stability, fast release profiles), the highest amounts of labile iron, the highest degree of hydrolysis in acid and they show low to moderate uptake into the monocytes/macrophages. Among the iron preparations of the second generation, the iron dextran with low molecular weight is associated with greater relative stability. In terms of size and molecular weight, the iron dextran with low molecular weight is followed by third generation preparations. During the study we have come to the conclusions that indicate their high relative stability (higher thermal stability, slow release profiles), low amounts of labile iron and low degree of hydrolysis in acid. Moreover, ferumoxytol, which has the highest molecular weight, is readily uptaken into monocytes/macrophages. In summary, iron preparations could be classified according to their relative stability of formulation as follows: iron gluconate < iron sucrose << low molecular wieght iron dextran ⡈ iron carboxymaltose ⡈ iron isomaltoside 1000 ⡈ ferumoxytol. From the results, we can conclude that the obtained in vitro data on iron preparations of the second and third generation confrim the results of clinical studies, that have proven that the products are clinically safe. The obtained results show that taking into acocount the properties of the preparations is very important, when making decisions during therapy. Second generation iron preparations are suitable for longer administration times (between 30 and 60 minutes) in lower single doses, and are therefore more suitable for patients who often visit medical institutions. However, in addition to patient safety and satisfaction, the healthcare system also strives to make these services cost-effective. Consequently, third generation parenteral iron preparations are coming to the fore as they are clinically safe, fast and can replace major iron needs in a single administration.

Keywords:Iron intravenous formulations, labile iron, stability, phagocytosis, anemia.

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