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Načrtovanje in sinteza novih protimikrobno delujočih zaviralcev DNA-giraze in Hsp90 : doktorska disertacija
ID Lamut, Andraž (Avtor), ID Tomašič, Tihomir (Mentor) Več o mentorju... Povezava se odpre v novem oknu, ID Kikelj, Danijel (Komentor)

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Izvleček
Infekcijske bolezni zaradi naraščajoče odpornosti mikroorganizmov na obstoječe načine zdravljenja predstavljajo velik izziv svetovnemu javnemu zdravstvu. Identifikacija ustreznih tarč in razvoj novih protimikrobnih učinkovin z alternativnim mehanizmom delovanja je ena od strategij za zmanjševanje in preprečevanje pojava rezistentnih sevov. DNA-giraza je klinično validirana tarča za razvoj novih protibakterijskih učinkovin, medtem ko Hsp90 predstavlja obetavno tarčo za razvoj protivirusnih učinkovin. Odkrivanje zaviralcev teh dveh tarč je aktivno področje raziskovanja, o čemer govorijo številne znanstvene publikacije ter veliko število sintetiziranih spojin in objavljene patentne prijave. Še posebno velik izziv predstavlja rezistenca po Gramu negativnih bakterij, ki z zmanjšano propustnostjo zunanje membrane in kompleksnimi sistemi za efluks strukturno raznovrstnih spojin iz bakterijske celice zmanjšuje učinkovitost trenutnega nabora protibakterijskih učinkovin. Možno rešitev, da zaobidemo ta dva mehanizma rezistence, predstavljata strategija z inhibitorji efluks črpalk in strategija olajšanja prehoda spojin preko bakterijskih membran po principu trojanskega konja, pri kateri bioaktivne spojine konjugiramo s siderofori ali mimetiki sideroforov ter tako dobimo protibakterijsko delujoče molekule, imenovane sideromicini. Validacija koncepta trojanskega konja v kliničnem okolju je bila nedavno potrjena z registracijo cefiderokola kot prvega predstavnika iz tega razreda učinkovin, in sicer za zdravljenje trdovratnih infekcij, povzročenih z rezistentnimi po Gramu negativnimi patogeni, kot so Escherichia coli, Pseudomonas aeruginosa in Klebsiella pneumoniae. V okviru predstavljene doktorske disertacije smo uspešno načrtovali in sintetizirali nove pirolamidne zaviralce DNA-giraze B (GyrB) s (S)-4,5,6,7-tetrahidrobenzo[1,2-d]tiazol-2,6-diaminskim osnovnim skeletom, pri čemer so izhodišče za naše delo predstavljali analogi prve generacije teh spojin. Pri delu smo se oprli na že poznane kristalne strukture kompleksov strukturno sorodnih pirolamidnih spojin v ATP-vezavnem mestu GyrB, kar je vodilo načrtovanje naših analogov in pripravo sintezne strategije. Najprej smo pripravili serijo spojin, ki imajo na mestu 6 osnovnega skeleta vezane različno substituirane pirole z namenom raziskati kemijski prostor, ki je na voljo znotraj vezavnega mesta GyrB. Nato smo z vezavo različnih substituentov na mesto 2 osnovnega skeleta poskušali povečati jakost interakcij tudi v tem delu molekule. Z namenom izboljšanja protibakterijske aktivnosti naših zaviralcev smo uspešno načrtovali in pripravili konjugate med zaviralci GyrB in različnimi mimetiki sideroforov. Mimetike sideroforov smo pripeli na mesto, za katerega smo glede na omenjene kristalne strukture sklepali, da ne bo poslabšalo vezave zaviralcev ali pa bo vezavo celo izboljšalo. Z uporabo koncepta trojanskega konja smo Andraž Lamut: Načrtovanje in sinteza novih protimikrobno delujočih zaviralcev DNA-giraze in Hsp90 2 želeli povečati koncentracijo zaviralcev GyrB v bakterijskih celicah, kar bi predvidoma vodilo v izboljšanje in vitro protibakterijske aktivnosti ter zmanjšanje učinka efluksa, kar je bila glavna pomanjkljivost prve generacije spojin s 4,5,6,7-tetrahidrobenzo[1,2-d]tiazol-2,6-diaminskim skeletom. Rezultati encimskih testiranj so pokazali, da druga generacija spojin izkazuje večjo jakost zaviranja encimske reakcije DNA-giraze od prve generacije, saj so najmočnejši analogi imeli vrednosti IC50 med 0.016 [mikro]M in 0.044 [mikro][mikro]M proti E. coli DNA-girazi in med 0.43 [mikro]M in 0.71 [mikro]M proti Staphylococcus aureus DNA-girazi. Druga generacija spojin je prav tako izkazala izboljšano in vitro protibakterijsko aktivnost proti po Gramu pozitivnim bakterijam, saj sta najučinkovitejša analoga imela vrednosti MIC med 8.2 [mikro]M in 30 [mikro]M na proti vankomicinu in proti meticilinu odpornih sevih S. aureus. Najmočnejši konjugati zaviralcev DNA-giraze B z mimetiki sideroforov so izkazali nanomolarne zaviralne aktivnosti proti E. coli DNA-girazi z vrednostmi IC50 med 0.058 [mikro]M in 0.11 [mikro]M, kar je dokaz, da sideroforna komponenta ni motila vezave zaviralca v tarčno mesto. Testiranje na mutantu E. coli [delta]tolC z onemogočeno funkcijo efluks črpalke je razkrilo, da so tako spojine druge generacije kot tudi pripravljeni konjugati podvrženi aktivnemu efluksu iz bakterijskih celic, kar je eden izmed omejitvenih dejavnikov za doseganje protibakterijskega učinka proti po Gramu negativnim bakterijam. Večina spojin, ki je bila testirana proti E. coli [delta]tolC, je sicer izkazala izboljšano učinkovitost tudi proti temu sevu in najučinkovitejši derivati so imeli vrednosti MIC med 3.13 [mikro]M in 6.25 [mikro]M. Nadalje so konjugati izkazali le minimalno izboljšanje vrednosti MIC proti divjemu sevu E. coli v testnem sistemu z nizko koncentracijo železovih ionov, ki posnema pogoje infekcije, in zato so potrebne dodatne študije za ovrednotenje uspešnosti koncepta trojanskega konja v primeru sideromicinov s 4,5,6,7-tetrahidrobenzo[1,2-d]tiazol-2,6-diaminskim osnovnim skeletom. Z ozirom na dejstvo, da nekateri dobro znani zaviralci GyrB izkazujejo protivirusne učinke in zaviralno delovanje tudi na Hsp90, smo izbranim zaviralcem GyrB s 4,5,6,7-tetrahidrobenzo[1,2-d]tiazol-2,6-diaminskim jedrom ovrednotili njihovo protivirusno delovanje. Spojine so bile aktivne proti virusom influence A (H1N1, H3N2) in influence B z vrednostmi EC50 v nizkem mikromolarnem območju in so prav tako izkazale afiniteto vezave do Hsp90. Ugotovitve nakazujejo, da je protivirusni učinek spojin najverjetneje posledica zaviranja Hsp90. Sintetizirani zaviralci DNA-giraze in Hsp90 v sklopu te doktorske disertacije predstavljajo izvirni prispevek k znanosti na področju odkrivanja novih protimikrobnih učinkovin, saj gre za inovativne spojine z alternativnim mehanizmom delovanja glede na obstoječo terapijo in ponujajo možnost za soočenje z izzivom virusne in bakterijske rezistence v prihodnje.

Jezik:Slovenski jezik
Ključne besede:protibakterijske učinkovine, DNA giraza, zaviralci GyrA, zaviralci GyrB, protivirusne učinkovine, HSP90
Vrsta gradiva:Doktorska disertacija
Tipologija:2.08 - Doktorska disertacija
Organizacija:FFA - Fakulteta za farmacijo
Kraj izida:Ljubljana
Založnik:[A. Lemut]
Leto izida:2020
Št. strani:355 str.
PID:20.500.12556/RUL-137109 Povezava se odpre v novem oknu
UDK:615.015.8:616.9(043.3)
COBISS.SI-ID:32135427 Povezava se odpre v novem oknu
Datum objave v RUL:01.06.2022
Število ogledov:755
Število prenosov:49
Metapodatki:XML DC-XML DC-RDF
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Sekundarni jezik

Jezik:Angleški jezik
Naslov:Design and synthesis of novel antimicrobial DNA gyrase and Hsp90 inhibitors
Izvleček:
Infectious diseases represent a global public health concern due to increasing microbial resistance to currently available therapies. Identification of suitable targets and development of novel antimicrobial agents with alternative mechanisms of action are among the strategies to prevent and to lower the outburst of resistant strains. DNA gyrase is a clinically validated target for development of novel antibacterial drugs, while Hsp90 represents a promising target for development of novel antiviral drugs. Numerous scientific publications and patent applications and the large number of such compounds synthesized bear witness to the active research for novel inhibitors of these two targets. The especially large challenge is the resistance mechanisms of Gram-negative bacteria, among which the most important are low outer membrane permeability and complex efflux systems that expel structurally diverse compounds from the bacterial cell, thus lowering the effectiveness of many of the available antibacterial drugs. The possible strategies to circumvent these two resistance barriers are the use of efflux pump inhibitors and increased drug penetration across the bacterial cell wall through what is termed a Trojan horse strategy, in which bioactive compounds are conjugated with siderophores or siderophore mimics to yield antibacterial molecules known as sideromycins. Validation of this Trojan horse concept in the clinical setting was recently confirmed with the registration of cefiderocol as a first-in-class agent for the treatment of serious infections caused by resistant Gram-negative pathogens, such as Escherichia coli, Pseudomonas aeruginosa, and Klebsiella pneumoniae. In the present doctoral dissertation, we have successfully designed and synthesized novel pyrrolamide-based inhibitors of DNA gyrase B (GyrB) with an (S)-4,5,6,7-tetrahydrobenzo[1,2-d]thiazole-2,6-diamine scaffold, based on their previously reported first generation. The design of these inhibitors and their synthetic strategy was guided by the known crystal structures of structurally similar pyrrolamides in complex with the ATP-binding site of GyrB. First, we prepared a series of compounds with differently substituted pyrroles attached at position 6 of the core scaffold, to explore the available chemical space in the binding site of GyrB. Secondly, we attached various substituents at position 2 of the core scaffold, to increase the strength of the interactions at this site of the molecule also. To further improve the antibacterial activities of these GyrB inhibitors, we successfully designed and prepared their conjugates with different siderophore mimics. Based on the above-mentioned crystal structures, the siderophore mimics were attached at the inhibitor region, for which we predicted that this would not decrease the binding affinity of the inhibitors, or will even contribute to their binding. Using the Trojan Andraž Lamut: Načrtovanje in sinteza novih protimikrobno delujočih zaviralcev DNA-giraze in Hsp90 4 horse concept, the aim here was to increase the concentrations of these GyrB inhibitors inside the bacterial cells, to potentially improve their in vitro antibacterial activities and diminish the effects of the bacterial efflux pumps, as the main drawbacks of the first generation 4,5,6,7-tetrahydrobenzo[1,2-d]thiazole-2,6-diamines. Enzyme inhibition assays showed that these second-generation compounds were indeed more potent than those of the first generation, with IC50 values of the most potent analogs from 0.016 [micro]M to 0.044 [micro]M against E. coli DNA gyrase and from 0.43 [micro]M to 0.71 [micro]M against Staphylococcus aureus DNA gyrase. These second-generation compounds were also more efficient in in vitro antibacterial assays against Gram-positive bacteria, with MICs of the most efficient compounds from 8.2 [micro]M to 30 [micro]M against vancomycin-resistant and methicillin-resistant S. aureus strains. The most potent GyrB inhibitor-siderophore mimic conjugates had IC50 values from 0.058 [micro]M to 0.11 [micro]M against E. coli DNA gyrase and thus the siderophore component of the conjugates did not disturb the binding of the inhibitors to the target site of GyrB. Antibacterial testing against E. coli [delta]tolC, which has a defective efflux pump, showed that both the second-generation compounds as well as prepared conjugates are good substrates for the efflux pumps, which is one of the limiting factors for sufficient efficiency against Gram-negative bacteria. Nevertheless, most of the compounds, which were tested against E. coli [delta]tolC, showed improved activity over the first generation, with the most efficient ones with MICs from 3.13 [micro]M to 6.25 [micro]M. However, the conjugates showed only minor improvements to their MICs against wild-type E. coli in a test system with low iron concentrations, which mimics the conditions present in the host during infection. Therefore, further studies are needed to evaluate the success of the Trojan horse concept for these 4,5,6,7-tetrahydrobenzo[1,2-d]thiazole-2,6-diamine-based sideromycins. Selected GyrB inhibitors with this 4,5,6,7-tetrahydrobenzo[1,2-d]thiazole-2,6-diamine core were also tested for antiviral activities, as some of the other well-known GyrB inhibitors have antiviral properties as well as Hsp90 inhibitory activities. Some of these compounds were active against influenza A (H1N1, H3N2) and influenza B viruses, with EC50 values in the low micromolar range. They also showed binding to Hsp90, which suggests that Hsp90 inhibition might be the mechanism that underlies their antiviral activities. DNA gyrase and Hsp90 inhibitors that were synthesized in the scope of the presented doctoral dissertation represent an original contribution to science in this field of research, as these are innovative compounds with an alternative mechanism of action when compared to the currently available therapies. Thus, they offer the opportunity to cope with the challenge of bacterial and viral resistance in the future.


Projekti

Financer:ARRS - Agencija za raziskovalno dejavnost Republike Slovenije
Številka projekta:P1-0208
Naslov:Farmacevtska kemija: načrtovanje, sinteza in vrednotenje učinkovin

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