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4. DPYD haplotype structure for variants *2A, *13, c.2846A>T, c.1236G>A/HapB3, c.496A>G (rs2297595), *6 (rs1801160) and *9A (rs1801265) in the Croatian population

Author

Ganoci, L., Lešnjaković, L., Šimičević, L., Palić, J., Mucalo, I., and Božina, N.

Subjects
DPYD, haplotype, genes
Abstract

Background: Dihydropyrimidine dehydrogenase, coded by the DPYDgene, isarate-limitingenzyme in the metabolism of fluoropyrimidines.Data on the frequency of DPYD haplo type sand impact of common DPYD variants on fluoropyrimidine-related toxicityis limited.We analysed genotype and haplotype frequencies off our DPYD variants from pharmacogenomics guideline sand three additional common DPYD polymorphisms in the Croatian population. Methods: In this study, we analysed data DPYD genotyping from routine pharmacogenetic testing in cancer patients treated with fluoropyrimidine therapy. A total of 998 subjects of Caucasian an cestry were genotyped for DPYD*2A (c.1905+1G>A), *13 (c.1679T>G), c.2846A>T, c.1236G>A/HapB3, c.496A>G (rs2297595), *6(c.2194G>A, rs1801160) and *9A(c.85T>C, rs1801265)by TaqMan real-time PCR. Genotyping data were analysed to estimate allele frequencies, common haplotypes and haplotype frequencies. Results: The DPYD variants allele frequency were*2A q=0.01653, *13q=0.0005, c.2846A>T q=0.00401, c.1236G>A q=0.02555, *6q=0.05962, *9Aq=0.23447 andc.496A>Gq=0.13176.439subjects (44.0%) were carriers of wt alleles, 141(14.1%) were carriers ofc.496G/*9A genotype, 134 (13.4%) of *1/*9A genotype, 67 (6.7%) of *1/*6 genotype, 36(3.6%) of *1/c.496G genotype, 29(2.9%) ofc.1236A/*9A genotype, 6(0.6%) of *1/c.1236Agenotype.Analysing the combination of DPYD variants revealed that263subjects(26.4%)were carriers of one variant allele, while271(27.2%)were carriers of two or more different (compound) variant alleles. Conclusions: This study provides information on DPYD haplotype frequencies in the Caucasian population, which is essential for the design of pharmacogenetic studies investigating the impact of common DPYD variants and haplotypes on fluoropyrimidine-related toxicity.

Published
2023

5. DPYD polymorphism c.496A>G and risk of severe adverse drug reactions in cancer patients treated with fluoropyrimidine-based protocols

Author

Ganoci, L., Bilić, I., Trkulja, V., Lešnjaković, L., Šimićević, L., Mucalo, I., pleština, S., and Božina, N.

Subjects
drugs reaction, cancer, fluoropyrimidine
Abstract

Patients with reduced dihydropyrimidine dehydrogenase (DPD) activity are at increased risk of severe fluoropyrimidine (FP)- related adverse events (AE). Several guidelines recommend FP dosing based on genotyping of four clinically relevant DPYD variants to predict DPD activity. We investigated the relationship between three further DPYD polymorphisms and the risk of severe FP-related AES. Study involved FP-treated cancer patients, genotyped for recommended DPYD variants 2A. *13 (c.1679T G). c.2846A T. c.1236G>A/HapB3. as well for c.496A G. c.2194G>A and c.85T>C (TaqMan real-time PCR) and for UGT1A1*28 (LightSNIP) if irinotecan was included. Patients were monitored for occurrence of grade 23 (National Cancer Institute Common Terminology Criteria) vs. grade 0-2 AES. For each tested polymorphisms, variant allele carriers were matched to respective wild type controls. Of 503 included patients (82.3% colorectal cancer), 283 (56.3%) developed grade 23 AES. Odds of grade 23 AEs were higher in c.496A G variant allele carriers (n=127) than in controls (n-376) [OR-5.20 (95%CI 1.88-14.3). Bayesian OR-5, 24 (95% Cri 3.06- 9.12)]. Odds tended to be higher in c.2194G>A variant allele carries (n=58) than in controls (n=432) (OR=1.88 (0.95-3.73), Bayesian OR=1.90 (1.03.3.56), c.8ST-G variant did not appear associated with grade 23 AES. DRYD C496ADG variant might need to be considered for inclusion in the DPYD genotyping pariel.

Published
2021

6. UGT2B7 c.-161C>T polymorphism frequency in Croatian population

Author

Božina Tamara, Karačić Ena, Ganoci Lana, Čuković-Čavka Silvija, Palić Jozefina, Božina Nada, and Šimičević Livija

Subjects
allelic variants, genotyping, glucuronidation, pharmacogenetics, uridine diphosphate glucuronosyltransferase-2b7, hrvatsko stanovništvo, glukuronidacija, farmakogenetika, polimorfizmi, ugt2b7, Toxicology. Poisons, RA1190-1270
Abstract

Uridine diphosphate glucuronosyltransferase-2B7 (UGT2B7), enzyme responsible for the elimination of a number of xenobiotics through glucuronidation, is expressed in the gut, kidneys, intestines, and brain. However, data on the frequency of UGT2B7 polymorphisms in the Croatian population are limited. The aim of this study was to assess the frequency of the UGT2B7 c.-161C>T (rs7668258) polymorphism in the Croatian population and to compare it with reported frequencies in other populations. This polymorphism is in complete linkage disequilibrium with the UGT2B7 c.802C>T (UGT2B7*2, rs7439366) variant, which is important in clinical medicine. The study reports data of 501 participants from University Hospital Centre Zagreb. All data were collected and analysed retrospectively. Genotyping was performed by real-time polymerase chain reaction (PCR) using the TaqMan® Drug Metabolism Genotyping Assay for UGT2B7 c.-161C>T (rs7668258). We found that 120 (23.95 %) participants were carriers of the UGT2B7 c.-161CC genotype and 255 (50.9 %) were heterozygous carriers (UGT2B7 c.-161CT), while 126 (25.15 %) were homozygous carriers of the variant allele (UGT2B7 c.-161TT). The frequency of the variant UGT2B7 c.-161C>T allele in this study was T=0.506. The frequency of the UGT2B7 c.-161C>T allelic variants and genotypes in the Croatian population is similar to other European populations.

Published
2022
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10. Drug-drug-gene interactions as mediators of adverse drug reactions to diclofenac and statins: a case report and literature review

Author

Božina Nada, Ganoci Lana, Simičević Livija, Gvozdanović Katarina, Domjanović Iva Klarica, Fistrek Prlić Margareta, Križ Tena, Borić Bilušić Ana, Laganović Mario, and Božina Tamara

Subjects
drug interactions, hepatotoxicity, myotoxicity, nephrotoxicity, pharmacogenetics, farmakogenetika, hepatotoksičnost, interakcije lijekova, miotoksičnost, nefrotoksičnost, Toxicology. Poisons, RA1190-1270
Abstract

Concomitant treatment with drugs that inhibit drug metabolising enzymes and/or transporters, such as commonly prescribed statins and nonsteroidal anti-inflammatory drugs (NSAIDs), has been associated with prolonged drug exposure and increased risk of adverse drug reactions (ADRs) due to drug-drug interactions. The risk is further increased in patients with chronic diseases/comorbidities who are more susceptible because of their genetic setup or external factors. In that light, we present a case of a 46-year-old woman who had been experiencing acute renal and hepatic injury and myalgia over two years of concomitant treatment with diclofenac, atorvastatin, simvastatin/fenofibrate, and several other drugs, including pantoprazole and furosemide. Our pharmacogenomic findings supported the suspicion that ADRs, most notably the multi-organ toxicity experienced by our patient, may be owed to drug-drug-gene interactions and increased bioavailability of the prescribed drugs due to slower detoxification capacity and decreased hepatic and renal elimination. We also discuss the importance of CYP polymorphisms in the biotransformation of endogenous substrates such as arachidonic acid and their modulating role in pathophysiological processes. Yet even though the risks of ADRs related to the above mentioned drugs are substantially evidenced in literature, pre-emptive pharmacogenetic analysis has not yet found its way into common clinical practice.

Published
2021
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14. The Loss-of-Function ATP Binding Cassette Subfamily G Member 2 Polymorphism ABCG2 c.421C>A Reduces Lamotrigine Trough Concentrations in Adults with Epilepsy.

Author

Božina N, Domjanović IK, Sporiš IŠ, Ganoci L, Lovrić M, and Trkulja V

Subjects
Humans, Adult, Male, Female, Middle Aged, Young Adult, Lamotrigine pharmacokinetics, Epilepsy drug therapy, Epilepsy genetics, Anticonvulsants pharmacokinetics, Anticonvulsants administration & dosage, ATP Binding Cassette Transporter, Subfamily G, Member 2 genetics, Polymorphism, Single Nucleotide, Neoplasm Proteins genetics
Abstract

Background and Objectives: The commonly used antiseizure medication lamotrigine is a substrate to ATP binding cassette subfamily G member 2 (ABCG2) transporter. The objective of this study was to evaluate the effect of the common loss-of-function polymorphism ABCG2 c.421C>A (rs2231142) on the lamotrigine trough concentrations at steady state in adults with epilepsy., Methods: In two consecutive studies (Study 1, Study 2) in patients on lamotrigine monotherapy, carriers of the variant ABCG2 c.421C>A allele (CA/AA) were considered exposed, and wild-type homozygotes (CC) were considered controls. They were mutually balanced on covariates (age, sex, body weight, several polymorphisms in genes encoding other transporter proteins and lamotrigine-metabolizing enzymes that have been suggested to affect exposure to lamotrigine) to estimate the exposure effect (geometric means ratios, GMRs) in each study separately and overall (individual patient data meta-analysis). The overall estimate was evaluated for sensitivity to residual confounding., Results: In both studies (exposed n = 28 vs. controls n = 103; exposed n = 44 vs. controls n = 153, in Study 1 and Study 2, respectively) and overall (exposed n = 72 vs. controls n = 256), dose-corrected lamotrigine trough concentrations were moderately lower in the exposed patients: frequentist GMR [95% CI] = 0.82 [0.63-1.08]; GMR = 0.69 [0.60-0.81] and GMR = 0.72 [0.63-0.83] in Study 1, Study 2 and overall, respectively; Bayes GMR [95% CrI] = 0.83 [0.68-1.00]; GMR = 0.69 [0.58-0.83] and GMR = 0.75 [0.65-0.86] in Study 1, Study 2 and overall, respectively. Estimates appeared resistant to unmeasured confounding-the E-values for the pooled point estimates were high, and estimates corrected for a strong hypothetical bias were GMR = 0.78 [0.68-0.90] frequentist and GMR = 0.81 [0.70-0.93] Bayes., Conclusion: Polymorphism ABCG2 c.421C>A moderately reduces lamotrigine concentrations in adults with epilepsy., Competing Interests: Declarations. Funding: The studies presented in this report received no funding. Conflict of Interest: None of the authors have any conflict of interest to declare. The authors declare no support from any organization for the submitted work, no other financial relationships with any organizations that might have an interest in the submitted work, and no other relationships or activities that could appear to have influenced the submitted work. Author Contributions: The studies were conceived and designed by Nada Božina, Iva Klarica Domjanović, Ivana Šušak Sporiš and Vladimir Trkulja. Ivana Šušak Sporiš executed and supervised recruitment and management of most of the included patients. Lana Ganoci performed genetic analysis, Mila Lovrić pefromed lamotrigine measurements, and both were supervised by Nada Božina. Data were collected and assembled by Iva Klarica Domjanović, Ivana Šušak Sporiš, Lana Ganoci and Mila Lovrić. The present analysis was performed by Vladimir Trkulja who drafted the manuscript. Data were interpreted by Nada Božina and Vladimir Trkulja. All co-authors provided final approval of the manuscript. Ethics Approval: Both studies presented in this report were approved by the Institutional Ethics Committee (Study 1 – approval class: 8.1.-14/78-2, registration number: 02/21/JG, issued October 7, 2015; Study 2 – approval class: 8.1.-19/12-2, registration number: 02/21 AG, issued November 29, 2018). Consent to Participate: Only patients who signed a written informed consent for (1) genotyping for the pharmacogenes of interest and (2) publication of (anonymized) data for scientific purposes were included in the studies. Consent for Publication: Not applicable. Data Availability Statement: All data/datasets generated for the present analysis are available from the corresponding author upon a reasonable request. Code Availability: Codes used to generate frequentist (SAS for Windows 9.4) and Bayes estimates (R package rstanarm) are available from the corresponding author upon request., (© 2024. The Author(s), under exclusive licence to Springer Nature Switzerland AG.)

Published
2025
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15. Challenging pharmacotherapy management of a psychotic disorder due to a delicate pharmacogenetic profile and drug-drug interactions: a case report and literature review.

Author

Belančić A, Pavešić Radonja A, Ganoci L, Vitezić D, and Božina N

Subjects
Humans, Adult, Female, Psychotic Disorders drug therapy, Psychotic Disorders genetics, Aripiprazole administration & dosage, Aripiprazole therapeutic use, Schizophrenia drug therapy, Schizophrenia genetics, Cytochrome P-450 CYP1A2 genetics, Pharmacogenomic Testing, Pharmacogenetics, Cytochrome P-450 CYP3A genetics, Cytochrome P-450 CYP2D6 genetics, Drug Interactions, Antipsychotic Agents administration & dosage, Antipsychotic Agents therapeutic use
Abstract

This report presents challenging psychopharmacotherapy management of a psychotic disorder in a patient with a delicate pharmacogenetic profile and drug-drug interactions. A 31-year old woman diagnosed with schizophrenia in 2017 was referred by her psychiatrist to a clinical pharmacologist for interpretation of a pharmacogenetic test and advice regarding optimal psychopharmacotherapy. In spite of adherence to aripiprazole, olanzapine, risperidone, and levomepromazine, and rational anxiolytic therapy, she still experienced anxiety, anhedonia, loss of appetite, sleeping problems, and auditory hallucinations with commands to harm herself. Due to a lack of alternative therapeutic steps, low aripiprazole serum concentrations, and a lack of explanation for pharmacotherapy unresponsiveness, pharmacogenetic testing was performed. The patient was defined as CYP2D6 *1/*1, CYP1A2 *1F/*1F, CYP3A4 *1/*1B, CYP3A5 *1/*3, and having increased activity of the enzymes UGT1A4 and UGT2B7, intermediate activity of ABCB1 transporter, and low activity of COMT. Carbamazepine was discontinued, aripiprazole was increased to a maximum of 30 mg/day orally with long-acting injection (400 mg monthly), and olanzapine was increased to a daily dose of 35 mg orally. These changes led to an optimal therapeutic drug concentration and improved clinical status. At the last follow-up, the patient was without severe auditory hallucinations, became more engaged in daily life, had more interaction with others, had found a job, and even had started an emotional relationship. In psychiatry, pharmacogenetic testing is an important tool for guiding pharmacological therapy, particularly in patients with an unsatisfactory clinical response and a lack of alternative therapeutic steps for pharmacotherapy unresponsiveness.

Published
2024

16. Common P-glycoprotein ( ABCB1 ) polymorphisms do not seem to be associated with the risk of rivaroxaban-related bleeding events: Preliminary data.

Author

Slišković AM, Palić J, Božina T, Ganoci L, Vrkić Kirhmajer M, Trkulja V, Bulum J, and Šimičević L

Subjects
Humans, Male, Female, Case-Control Studies, Aged, Middle Aged, Factor Xa Inhibitors adverse effects, Factor Xa Inhibitors therapeutic use, Risk Factors, Rivaroxaban adverse effects, Rivaroxaban therapeutic use, ATP Binding Cassette Transporter, Subfamily B genetics, Hemorrhage chemically induced, Hemorrhage genetics, Polymorphism, Single Nucleotide
Abstract

Introduction: Considering conflicting previous reports, we aimed to evaluate whether the common ABCB1 polymorphisms (rs1128503, rs2032582, rs1045642, rs4148738) affected the risk of bleeding in rivaroxaban-treated patients., Materials and Methods: We report preliminary data from a larger nested case-control study. Consecutive adults started on rivaroxaban for any indication requiring > 6 months of treatment were followed-up to one year. Patients who experienced major or non-major clinically relevant bleeding during the initial 6 months were considered cases, whereas subjects free of bleeding over > 6 months were controls. The polymorphisms of interest (rs1128503, rs2032582, rs1045642, rs4148738) were in a strong linkage disequilibrium, hence patients were classified regarding the "load" of variant alleles: 0-2, 3-5 or 6-8. The three subsets were balanced regarding a range of demographic, comorbidity, comedication and genetic characteristics. A logistic model was fitted to probability of bleeding., Results: There were 60 cases and 220 controls. Raw proportions of cases were similar across the subsets with increasing number of ABCB1 variant alleles (0-2, N = 85; 3-6, N = 133; 6-8, N = 62): 22.4%, 21.8%, and 19.4%, respectively. Fully adjusted probabilities of bleeding were also similar across the subsets: 22.9%, 27.5% and 17.7%, respectively. No trend was observed (linear, t = -0.63, df = 273, P = 0.529; quadratic, t = -1.10, df = 273, P = 0.272). Of the 15 identified haplotypes, the completely variant (c.1236T_c.2677T(A)_c.3435T_c.2482-2236A) (40.7%) and completely wild-type (C_G_C_G) (39.5%) haplotypes prevailed, and had a closely similar prevalence of cases: 21.1% vs . 23.1%, respectively., Conclusions: The evaluated common ABCB1 polymorphisms do not seem to affect the risk of early bleeding in patients started on rivaroxaban., Competing Interests: Potential conflict of interest None declared., (Copyright Croatian Society of Medical Biochemistry and Laboratory Medicine.)

Published
2024
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17. Inosine monophosphate dehydrogenase type 2 polymorphism IMPDH2 3757T>C (rs11706052) and 12-month evolution of the graft function in renal transplant recipients on mycophenolate-based immunosuppression.

Author

Penezić L, Nađ-Škegro S, Hadžavdić A, Ganoci L, Kaštelan Ž, Trkulja V, and Božina N

Subjects
Humans, Male, Female, Middle Aged, Adult, Aged, Immunosuppression Therapy methods, Immunosuppression Therapy adverse effects, Kidney Transplantation adverse effects, IMP Dehydrogenase genetics, Mycophenolic Acid therapeutic use, Mycophenolic Acid adverse effects, Immunosuppressive Agents therapeutic use, Immunosuppressive Agents adverse effects, Glomerular Filtration Rate drug effects, Graft Rejection genetics, Graft Rejection prevention & control, Graft Rejection immunology, Polymorphism, Single Nucleotide genetics
Abstract

Variant allele at the inosine monophosphate dehydrogenase type 2 polymorphism IMPDH2 3757T>C has been associated with increased enzyme activity and reduced susceptibility to mycophenolic acid (MPA) in vitro. It has been suggested associated with an increased risk of acute rejection in renal transplant recipients on MPA-based immunosuppression, but not unambiguously. We assessed one-year evolution of the estimated glomerular filtration rate (eGFR) in transplanted variant allele carriers and wild-type subjects, while controlling for a number of demographic, pharmacogenetic, (co)morbidity, and treatment baseline and time-varying covariates. The eGFR slopes to day 28 (GMR = 1.01, 95% CI 0.93-1.09), and between days 28 and 365 (GMR = 1.01, 95% CI 0.99-1.02) were practically identical in 52 variant carriers and 202 wild-type controls. The estimates (95%CIs) remained within the limits of ±20% difference even after adjustment for a strong hypothetical effect of unmeasured confounders. Polymorphism IMPDH2 3757T>C does not affect the renal graft function over the 1st year after transplantation., (© 2024. The Author(s), under exclusive licence to Springer Nature Limited.)

Published
2024
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18. Is CYP2C Haplotype Relevant for Efficacy and Bleeding Risk in Clopidogrel-Treated Patients?

Author

Ganoci L, Palić J, Trkulja V, Starčević K, Šimičević L, Božina N, Lovrić-Benčić M, Poljaković Z, and Božina T

Subjects
Humans, Male, Female, Aged, Middle Aged, Genotype, Ticlopidine analogs & derivatives, Ticlopidine adverse effects, Ticlopidine therapeutic use, Clopidogrel adverse effects, Clopidogrel therapeutic use, Haplotypes, Cytochrome P-450 CYP2C19 genetics, Hemorrhage chemically induced, Hemorrhage genetics, Platelet Aggregation Inhibitors adverse effects, Platelet Aggregation Inhibitors therapeutic use
Abstract

A recently discovered haplotype- CYP2C:TG -determines the ultrarapid metabolism of several CYP2C19 substrates. The platelet inhibitor clopidogrel requires CYP2C19-mediated activation: the risk of ischemic events is increased in patients with a poor (PM) or intermediate (IM) CYP2C19 metabolizer phenotype (vs. normal, NM; rapid, RM; or ultrarapid, UM). We investigated whether the CYP2C:TG haplotype affected efficacy/bleeding risk in clopidogrel-treated patients. Adults ( n = 283) treated with clopidogrel over 3-6 months were classified by CYP2C19 phenotype based on the CYP2C19*2*17 genotype, and based on the CYP2C19/CYP2C cluster genotype, and regarding carriage of the CYP2:TG haplotype, and were balanced on a number of covariates across the levels of phenotypes/haplotype carriage. Overall, 45 (15.9%) patients experienced ischemic events, and 49 (17.3%) experienced bleedings. By either classification, the incidence of ischemic events was similarly numerically higher in PM/IM patients (21.6%, 21.8%, respectively) than in mutually similar NM, RM, and UM patients (13.2-14.8%), whereas the incidence of bleeding events was numerically lower (13.1% vs. 16.6-20.5%). The incidence of ischemic events was similar in CYP2C:TG carries and non-carries (14.1% vs. 16.1%), whereas the incidence of bleedings appeared mildly lower in the former (14.9% vs. 20.1%). We observed no signal to suggest a major effect of the CYP2C19/CYP2C cluster genotype or CYP2C:TG haplotype on the clinical efficacy/safety of clopidogrel.

Published
2024
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19. Breast cancer resistance protein polymorphism ABCG2 c.421C>A (rs2231142) moderates the effect of valproate on lamotrigine trough concentrations in adults with epilepsy.

Author

Šušak Sporiš I, Božina N, Klarica Domjanović I, Sporiš D, Bašić S, Bašić I, Lovrić M, Ganoci L, and Trkulja V

Subjects
Adult, Humans, Female, Valproic Acid therapeutic use, Valproic Acid pharmacology, Lamotrigine therapeutic use, Bayes Theorem, ATP Binding Cassette Transporter, Subfamily G, Member 2 genetics, Neoplasm Proteins genetics, Neoplasm Proteins metabolism, Neoplasm Proteins therapeutic use, Anticonvulsants adverse effects, Polymorphism, Single Nucleotide, Epilepsy drug therapy, Epilepsy genetics, Breast Neoplasms drug therapy
Abstract

Background: Valproate inhibits clearance of lamotrigine and greatly increases its concentrations. We assessed whether this effect was moderated by a polymorphism (ABCG2 c.421C>A) of the breast cancer resistance protein., Methods: In two consecutive independent studies in adults with epilepsy on lamotrigine monotherapy or cotreated with valproate: (i) Exposure to valproate was considered treatment, (ii) dose-adjusted lamotrigine troughs at steady state were the outcome, and (iii) ABCG2 c.421C>A genotype (wild-type [wt] homozygosity or variant carriage) was the tested moderator. We used entropy balancing (primary analysis) and exact/optimal full matching (secondary analysis) to control for confounding, including polymorphisms (and linked polymorphisms) suggested to affect exposure to lamotrigine (UGT1A4*3 c.142T>G, rs2011425; UGT2B7-161C>T, rs7668258; ABCB1 1236C>T, rs1128503) to generate frequentist and Bayesian estimates of valproate effects (geometric means ratios [GMR])., Results: The two studies yielded consistent results (replicated); hence, we analyzed combined data (total N = 471, 140 treated, 331 controls, 378 ABCG2 c.421C>A wt subjects, 93 variant carriers). Primary analysis: in variant carriers, valproate effect (GMR) on lamotrigine (treated, n = 21 vs. controls, n = 72) was around 60% higher than in wt subjects (treated, n = 119 vs. controls, n = 259)-ratio of GMRs 1.61 (95%CI 1.23-2.11) (frequentist) and 1.63 (95%CrI 1.26-2.10) (Bayes). Similar differences in valproate effects between variant carriers and wt subjects were found in the secondary analysis (valproate troughs up to 364 μmol/L vs. no valproate; or valproate ≥364 μmol/L vs. no valproate). Susceptibility of the estimates to unmeasured confounding was low., Conclusion: Data suggest that polymorphism rs2231142 moderates the effect of valproate on exposure to lamotrigine., (© 2023 Société Française de Pharmacologie et de Thérapeutique. Published by John Wiley & Sons Ltd.)

Published
2024
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20. Plasma Brain-Derived Neurotrophic Factor Levels in First-Episode and Recurrent Major Depression and before and after Bright Light Therapy in Treatment-Resistant Depression.

Author

Kosanovic Rajacic B, Sagud M, Begic D, Nikolac Perkovic M, Dvojkovic A, Ganoci L, and Pivac N

Subjects
Female, Humans, Cross-Sectional Studies, Depression, Phototherapy, Brain-Derived Neurotrophic Factor blood, Brain-Derived Neurotrophic Factor chemistry, Depressive Disorder, Major therapy
Abstract

Brain-derived neurotrophic factor (BDNF) is implicated in the etiology and treatment response in major depressive disorder (MDD). However, peripheral BDNF concentrations have not been compared across different MDD stages. Bright light therapy (BLT) offers some potential in treatment-resistant depression (TRD), but its effects on BDNF levels are unknown. This study included a cross-sectional analysis of plasma BDNF concentration in females with TRD, unmedicated MDD patients, and healthy controls (HC), and measurements of longitudinal BLT effects on plasma BDNF levels in TRD patients. The present study included 55 drug-naïve, first-episode patients, 25 drug-free recurrent-episode MDD patients, 71 HC participants, and 54 TRD patients. Patients were rated by Hamilton Depression Rating Scale (HAMD)-17 and the Montgomery-Åsberg Depression Rating Scale (MADRS). Patients with TRD received BLT during 4 weeks. The total HAMD-17 and MADRS scores decreased following BLT. All patient groups had lower plasma BDNF than HC, but BDNF levels did not differ between first- and recurrent-episode BDNF patients and TRD patients before or after BLT. However, responders and remitters to BLT had higher post-treatment plasma BDNF concentrations than patients who did not achieve response or remission. The changes in plasma BDNF levels may be candidates for biomarkers of treatment response to BLT in TRD patients.

Published
2023
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21. Lack of guidelines and translational knowledge is hindering the implementation of psychiatric genetic counseling and testing within Europe - A multi-professional survey study.

Author

Koido K, Malmgren CI, Pojskic L, Almos PZ, Bergen SE, Borg I, Božina N, Coviello DA, Degenhardt F, Ganoci L, Jensen UB, Durand-Lennad L, Laurent-Levinson C, McQuillin A, Navickas A, Pace NP, Paneque M, Rietschel M, Grigoroiu-Serbanescu M, Soller MJ, Suvisaari J, Utkus A, Van Assche E, Vissouze L, Zuckerman S, Chaumette B, and Tammimies K

Subjects
Humans, Surveys and Questionnaires, Europe, European Union, Genetic Counseling methods, Genetic Testing methods
Abstract

Genetic research has identified a large number of genetic variants, both rare and common, underlying neurodevelopmental disorders (NDD) and major psychiatric disorders. Currently, these findings are being translated into clinical practice. However, there is a lack of knowledge and guidelines for psychiatric genetic testing (PsychGT) and genetic counseling (PsychGC). The European Union-funded COST action EnGagE (CA17130) network was started to investigate the current implementation status of PsychGT and PsychGC across 35 participating European countries. Here, we present the results of a pan-European online survey in which we gathered the opinions, knowledge, and practices of a self-selected sample of professionals involved/interested in the field. We received answers from 181 respondents. The three main occupational categories were genetic counselor (21.0%), clinical geneticist (24.9%), and researcher (25.4%). Of all 181 respondents, 106 provide GC for any psychiatric disorder or NDD, corresponding to 58.6% of the whole group ranging from 43.2% in Central Eastern Europe to 66.1% in Western Europe. Overall, 65.2% of the respondents reported that genetic testing is offered to individuals with NDD, and 26.5% indicated the same for individuals with major psychiatric disorders. Only 22.1% of the respondents indicated that they have guidelines for PsychGT. Pharmacogenetic testing actionable for psychiatric disorders was offered by 15%. Interestingly, when genetic tests are fully covered by national health insurance, more genetic testing is provided for individuals with NDD but not those with major psychiatric disorders. Our qualitative analyses of responses highlight the lack of guidelines and knowledge on utilizing and using genetic tests and education and training as the major obstacles to implementation. Indeed, the existence of psychiatric genetic training courses was confirmed by only 11.6% of respondents. The question on the relevance of up-to-date education and training in psychiatric genetics on everyday related practice was highly relevant. We provide evidence that PsychGC and PsychGT are already in use across European countries, but there is a lack of guidelines and education. Harmonization of practice and development of guidelines for genetic counseling, testing, and training professionals would improve equality and access to quality care for individuals with psychiatric disorders within Europe., (Copyright © 2023 The Authors. Published by Elsevier Masson SAS.. All rights reserved.)

Published
2023
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22. Bearing variant alleles at uridine glucuronosyltransferase polymorphisms UGT2B7 -161C > T (rs7668258) or UGT1A4*3 c.142 T > G (rs2011425) has no relevant consequences for lamotrigine troughs in adults with epilepsy.

Author

Božina N, Sporiš IŠ, Domjanović IK, Ganoci L, Šimičević L, Lovrić M, Romić ZČ, Gadže ŽP, and Trkulja V

Subjects
Humans, Adult, Lamotrigine therapeutic use, Alleles, Bayes Theorem, Polymorphism, Single Nucleotide, Anticonvulsants therapeutic use, Glucuronosyltransferase genetics, Glucuronosyltransferase metabolism, Genotype, UDP-Glucuronosyltransferase 1A9, Valproic Acid therapeutic use, Epilepsy drug therapy, Epilepsy genetics
Abstract

Purpose: To estimate whether epilepsy patients with variant UGT2B7 -161C > T (rs7668258) or UGT1A4*3 c.142 T > G (rs2011425) alleles differ from their wild-type (wt) peers in exposure to lamotrigine., Methods: Consecutive adults on lamotrigine monotherapy or lamotrigine + valproate co-treatment undergoing routine therapeutic drug monitoring, otherwise generally healthy and free of interacting drugs, were genotyped for UGT2B7 -161C > T and UGT1A4*3 c.142 T > G. Heterozygous, variant homozygous, or combined heterozygous/variant homozygous subjects were compared to their wt controls for dose-adjusted lamotrigine troughs with adjustment for age, sex, body weight, rs7668258/rs2011425, polymorphisms of efflux transporter proteins ABCG2 c.421C > A (rs2231142) and ABCB1 1236C > T (rs1128503), and level of exposure to valproate using covariate entropy balancing., Results: Of the 471 included patients, 328 (69.6%) were on monotherapy and 143 were co-treated with valproate. Dose-adjusted lamotrigine troughs in UGT2B7 -161C > T heterozygous (CT, n = 237) or variant homozygous (TT, n = 115) subjects were closely similar to those in their wt controls (CC, n = 119): geometric means ratios (GMRs) (frequentist and Bayes) 1.00 (95%CI 0.86-1.16) and 1.00 (95%CrI 0.83-1.22) for CT vs. CC; and 0.97 (0.81-1.17) and 0.97 (0.80-1.20) for TT vs. CC subjects. Lamotrigine troughs were also closely similar in UGT1A4*3 c.142 T > G variant carriers (n = 106: 102 TG + 4 GG subjects) and wt controls (TT, n = 365): GMR = 0.95 (0.81-1.12) frequentist, 0.96 (0.80-1.16) Bayes. GMRs for variant carriers vs. wt controls were around unity also at different levels of exposure to valproate., Conclusion: Dose-adjusted lamotrigine troughs in epilepsy patients with variant UGT2B7 -161C > T or UGT1A4*3 c.142 T > G alleles are equivalent to those in their respective wt peers., (© 2023. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published
2023
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23. Risk Factors for Rivaroxaban-Related Bleeding Events-Possible Role of Pharmacogenetics: Case Series.

Author

Šimičević L, Slišković AM, Kirhmajer MV, Ganoci L, Holik H, Palić J, Samardžić J, and Božina T

Abstract

Non-vitamin K antagonist oral anticoagulants' interindividual trough concentration variability affects efficacy and safety, especially in bleeding events. Rivaroxaban is metabolised via CYP3A4/5-, CYP2J2-, and CYP-independent mechanisms and is a substrate of two transporter proteins: ABCB1 (MDR1, P-glycoprotein) and ABCG2 (BCRP; breast-cancer-resistance protein). The polymorphisms of these genes may possibly affect the pharmacokinetics of rivaroxaban and, consequently, its safety profile. Rivaroxaban variability may be associated with age, liver and kidney function, concomitant illness and therapy, and pharmacogenetic predisposition. This case series is the first, to our knowledge, that presents multiple risk factors for rivaroxaban-related bleeding (RRB) including age, renal function, concomitant diseases, concomitant treatment, and pharmacogenetic data. It presents patients with RRB, along with their complete clinical and pharmacogenetic data, as well as an evaluation of possible risk factors for RRB. Thirteen patients were carriers of ABCB1 , ABCG2 , CYP2J2 , and/or CYP3A4 /5 gene polymorphisms. Possible drug-drug interactions with increased bleeding risk were identified in nine patients. Six patients had eGFR <60 mL/min/1.73 m 2 . Our data suggest a possible role of multiple factors and their interactions in predicting RRB; however, they also indicate the need for further comprehensive multidisciplinary research to enable safer use of this product based on a personalised approach.

Published
2023
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24. DPYD genotyping and predicting fluoropyrimidine toxicity: where do we stand?

Author

Lešnjaković L, Ganoci L, Bilić I, Šimičević L, Mucalo I, Pleština S, and Božina N

Subjects
Humans, Capecitabine adverse effects, Genotype, Antimetabolites, Antineoplastic adverse effects, Antimetabolites, Antineoplastic toxicity, Dihydropyrimidine Dehydrogenase Deficiency genetics, Dihydrouracil Dehydrogenase (NADP) genetics, Fluorouracil adverse effects, Fluorouracil toxicity, Pharmacogenomic Variants
Abstract

Fluoropyrimidines (FPs) are antineoplastic drugs widely used in the treatment of various solid tumors. Nearly 30% of patients treated with FP chemotherapy experience severe FP-related toxicity, and in some cases, toxicity can be fatal. Patients with reduced activity of DPD, the main enzyme responsible for the breakdown of FP, are at an increased risk of experiencing severe FP-related toxicity. While European regulatory agencies and clinical societies recommend pre-treatment DPD deficiency screening for patients starting treatment with FPs, this is not the case with American ones. Pharmacogenomic guidelines issued by several pharmacogenetic organizations worldwide recommend testing four DPD gene ( DPYD ) risk variants, but these can predict only a proportion of toxicity cases. New evidence on additional common DPYD polymorphisms, as well as identification and functional characterization of rare DPYD variants, could partially address the missing heritability of DPD deficiency and FP-related toxicity.

Published
2023
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25. ABCG2 and SLCO1B1 gene polymorphisms in the Croatian population.

Author

Božina T, Ganoci L, Karačić E, Šimičević L, Vrkić-Kirhmajer M, Klarica-Domjanović I, Križ T, Sertić Z, and Božina N

Subjects
Female, Humans, Alleles, Croatia, Gene Frequency, Genotype, Real-Time Polymerase Chain Reaction, ATP Binding Cassette Transporter, Subfamily G, Member 2 genetics, Liver-Specific Organic Anion Transporter 1 genetics, Neoplasm Proteins genetics, Polymorphism, Single Nucleotide
Abstract

Background: Organic anion-transporting polypeptide 1B1 (OATP1B1) and the ATP-binding cassette subfamily G member 2, ABCG2, are important transporters involved in the transport of endogenous substrates and xenobiotics, including drugs. Genetic polymorphisms of these transporters have effect on transporter activity. There is significant interethnic variability in the frequency of allele variants., Aim: To determined allele and genotype frequencies of ABCG2 and SLCO1B1 genes in Croatian populations of European descent., Subjects and Methods: A total of 905 subjects (482 women) were included. Genotyping for ABCG2 c.421C > A (rs2231142) and for SLCO1B1 c.521T > C (rs4149056), was performed by real-time polymerase chain reaction (PCR) using TaqMan ® DME Genotyping Assays., Results: For ABCG2 c.421C > A, the frequency of CC, CA and AA genotypes was 81.4%, 17.8% and 0.8% respectively. The frequency of variant ABCG2 421 A allele was 9.7%. For SLCO1B1 c.521T > C, the frequency of TT, TC and CC genotypes was 61.7%, 34.8% and 3.5% respectively. The frequency of variant SLCO1B1 521 C allele was 20.9%., Conclusion: The frequency of the ABCG2 and SLCO1B1 allelic variants and genotypes in the Croatian population is in accordance with other European populations. Pharmacogenetic analysis can serve to individualise drug therapy and minimise the risk of developing adverse drug reactions.

Published
2022
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26. Rapid clearance of tacrolimus blood concentration triggered by variant pharmacogenes.

Author

Šimičević L, Canjuga I, Zibar L, Borić-Bilušić A, Ganoci L, and Božina N

Subjects
Cytochrome P-450 CYP3A genetics, Genotype, Graft Rejection genetics, Graft Rejection prevention & control, Humans, Immunosuppressive Agents, Kidney Transplantation, Tacrolimus
Abstract

What Is Known and Objective: Tacrolimus (TAC) is an immunosuppressant with large interpatient pharmacokinetic variability and a narrow therapeutic index. We report a case of acute cellular rejection (ACR) type IB with insufficient TAC blood concentrations (TAC C 0 )., Case Summary: ACR developed on the eighth postoperative day of kidney transplantation. During this period, TAC C 0 were insufficient. This referred pharmacogenetic assessment disclosed the patient as a CYP3A5 expresser and CYP3A4*1B carrier. According to the genotype, higher doses of TAC, 15 mg twice daily, were administered and targeted TAC C 0 were achieved., What Is New and Conclusion: Our case presents an association of TAC rapid clearance and two alleles modifying greater CYP3A enzyme activity., (© 2022 John Wiley & Sons Ltd.)

Published
2022
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27. DPYD polymorphisms c.496A>G, c.2194G>A and c.85T>C and risk of severe adverse drug reactions in patients treated with fluoropyrimidine-based protocols.

Author

Božina N, Bilić I, Ganoci L, Šimičević L, Pleština S, Lešnjaković L, and Trkulja V

Subjects
Adult, Antimetabolites, Bayes Theorem, Dihydrouracil Dehydrogenase (NADP) genetics, Fluorouracil adverse effects, Genotype, Humans, Irinotecan adverse effects, Polymorphism, Single Nucleotide, Drug-Related Side Effects and Adverse Reactions genetics, Neoplasms chemically induced, Neoplasms drug therapy, Neoplasms genetics
Abstract

Aims: Cancer patients with reduced dihydropyrimidine dehydrogenase (DPD) activity are at increased risk of severe fluoropyrimidine (FP)-related adverse events (AE). Guidelines recommend FP dosing adjusted to genotype-predicted DPD activity based on four DPYD variants (rs3918290, rs55886062, rs67376798 and rs56038477). We evaluated the relationship between three further DPYD polymorphisms: c.496A>G (rs2297595), *6 c.2194G>A (rs1801160) and *9A c.85T>C (rs1801265) and the risk of severe AEs., Methods: Consecutive FP-treated adult patients were genotyped for "standard" and tested DPYD variants, and for UGT1A1*28 if irinotecan was included, and were monitored for the occurrence of grade ≥3 (National Cancer Institute Common Terminology Criteria) vs. grade 0-2 AEs. For each of the tested polymorphisms, variant allele carriers were matched to respective wild type controls (optimal full matching combined with exact matching, in respect to: age, sex, type of cancer, type of FP, DPYD activity score, use of irinotecan/UGT1A1, adjuvant therapy, radiotherapy, biological therapy and genotype on the remaining two tested polymorphisms)., Results: Of the 503 included patients (82.3% colorectal cancer), 283 (56.3%) developed grade ≥3 AEs, mostly diarrhoea and neutropenia. Odds of grade ≥3 AEs were higher in c.496A>G variant carriers (n = 127) than in controls (n = 376) [OR = 5.20 (95% CI 1.88-14.3), Bayesian OR = 5.24 (95% CrI 3.06-9.12)]. Odds tended to be higher in c.2194G>A variant carriers (n = 58) than in controls (n = 432) [OR = 1.88 (0.95-3.73), Bayesian OR = 1.90 (1.03-3.56)]. c.85T>C did not appear associated with grade ≥3 AEs (206 variant carriers vs. 284 controls)., Conclusion: DPYD c.496A>G and possibly c.2194G>A variants might need to be considered for inclusion in the DPYD genotyping panel., (© 2021 British Pharmacological Society.)

Published
2022
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28. Loss of function polymorphisms in SLCO1B1 (c.521T>C, rs4149056) and ABCG2 (c.421C>A, rs2231142) genes are associated with adverse events of rosuvastatin: a case-control study.

Author

Merćep I, Radman I, Trkulja V, Božina T, Šimičević L, Budimir E, Ganoci L, and Božina N

Subjects
Age Factors, Aged, Bayes Theorem, Case-Control Studies, Chemical and Drug Induced Liver Injury genetics, Comorbidity, Cytochrome P-450 CYP2C19 genetics, Cytochrome P-450 CYP2C9 genetics, Dose-Response Relationship, Drug, Female, Genotype, Humans, Male, Middle Aged, Myotoxicity genetics, Phenotype, Polymorphism, Single Nucleotide, Sex Factors, ATP Binding Cassette Transporter, Subfamily G, Member 2 genetics, Hydroxymethylglutaryl-CoA Reductase Inhibitors adverse effects, Liver-Specific Organic Anion Transporter 1 genetics, Neoplasm Proteins genetics, Rosuvastatin Calcium adverse effects
Abstract

Purpose: The study aims to evaluate relationship between polymorphisms associated with a reduced function of two transporter proteins resulting in increased exposure to rosuvastatin - organic anion transporter 1B1 (OATP1B1) (SLCO1B1 c.521T>C) and ATP binding cassette subfamily G member 2 (ABCG2) (ABCG2 c.421C>A) and occurrence of rosuvastatin related myotoxicity/hepatotoxicity., Methods: In a case-control study, cases (rosuvastatin treated patients developing myotoxicity or hepatotoxicity) and controls (concurrent rosuvastatin treated patients free of adverse events) were prospectively recruited over a 2 year period in a single tertiary center specialized in treatment of metabolic disorders. Subjects were evaluated for clinical, comorbidity, and comedication characteristics and for genotype predicted metabolizing phenotypes regarding cytochrome P450 enzymes CYP2C9 and CYP2C19. Standard regression analysis and analysis in matched sets of cases and controls (optimal full matching) were undertaken by fitting frequentist and Bayesian models (covariates/matching variables: age, sex, diabetes, liver/renal disease, hypertension, CYP2C9 and C19 phenotype, use of CYP or transporter inhibitors, non evaluated transporter genotype)., Results: A total of 88 cases (81 with myotoxicity, 6 with hepatotoxicity, 1 with both) and 129 controls were recruited. Odds of variant SLCO1B1 c.521T>C allele were 2.2-2.5 times higher in cases than in controls (OR = 2.45, 95% CI 1.34-4.48; Bayesian OR = 2.59, 95% CrI 1.42-4.90 in regression analysis; OR = 2.20, 1.10-4.42; Bayesian OR = 2.26, 1.28-4.41 in matched analysis). Odds of variant ABCG2 c.421C>A allele were 2.1-2.3 times higher in cases than in controls (OR = 2.24, 1.04-4.83; Bayesian OR = 2.35, 1.09-4.31 in regression analysis; OR = 2.10, 0.83-5.31; Bayesian OR = 2.17, 1.07-4.35 in matched analysis)., Conclusion: Loss of function polymorphisms in SLCO1B1 c.521T>C and ABCG2 c.421C>A genes are associated with the presence of rosuvastatin related myotoxicity and/or hepatotoxicity., (© 2021. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published
2022
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29. ABCB1, ABCG2 and CYP2D6 polymorphism effects on disposition and response to long-acting risperidone.

Author

Ganoci L, Trkulja V, Živković M, Božina T, Šagud M, Lovrić M, and Božina N

Subjects
Adult, Aged, Alleles, Female, Genotype, Humans, Male, Middle Aged, Pharmacogenetics, Polymorphism, Single Nucleotide, Schizophrenia genetics, Treatment Outcome, Young Adult, ATP Binding Cassette Transporter, Subfamily B, Member 1 genetics, ATP Binding Cassette Transporter, Subfamily G, Member 2 genetics, Antipsychotic Agents therapeutic use, Cytochrome P-450 CYP2D6 genetics, Risperidone therapeutic use, Schizophrenia drug therapy
Abstract

The relevance of the multidrug resistance (ABCB1) and breast cancer resistance (ABCG2) protein transporter polymorphisms for treatment with long-acting intramuscular (LAI) risperidone is largely unknown. We explored the relationship between these polymorphisms and cytochrome P450 (CYP) 2D6 genotype-predicted phenotype in their effects on drug disposition and clinical outcomes in adults with schizophrenia. In a 24-week observational study, patients initiated on LAI-risperidone (n=101) were genotyped [enzymes (CYP2D6 dupl,*3,*4,*5,*6,*41; CYP3A4*22, CYP3A5*3), transporters (ABCG2 421C>A; ABCB1 1236C>T, 2677G>T/A, 3435C>T)] and evaluated for steady-state (weeks 6-8) serum levels of dose-corrected risperidone, 9-OH-risperidone, risperidone+9-OH-risperidone (active moiety), and for response to treatment (PANSS, reduction vs. baseline ≥30% at week 12 and ≥45% at week 24). CYP2D6 normal/ultrarapid metabolizers (NM/UM) (vs. other) had lower risperidone (29%) and active moiety levels (24%) (9-OH-risperidone not affected). The effect on the three analytes was mild (0 to 23% reduction) in ABCG2 wild-type homozygotes and pronounced (44-55% reduction) in ABCG2 variant allele carriers. ABCG2 variant had no effect on disposition in CYP2D6 "other" phenotypes, while the effect was pronounced in CYP2D6 NM/UM subjects (31-37% reduction). ABCB1 polymorphisms had no effect on exposure to risperidone. CYP2D6 NM/UM phenotype tended to lower odds of PANSS response, ABCG2 variant was associated with 4-fold higher odds and ABCB1 (1236C>T, 2677G>T/A, 3435C>T) overall mainly wild-type genotype was associated with around 4--fold lower odds of response. In patients treated with LAI-risperidone, CYP2D6 phenotype effect on systemic exposure is conditional on the ABCG2 421C>A polymorphism. ABCG2 and ABCB1 polymorphisms affect clinical response independently of systemic risperidone disposition., Competing Interests: Declaration of Competing Interest None., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published
2021
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30. Association of HSPA1B genotypes with psychopathology and neurocognition in patients with the first episode of psychosis: a longitudinal 18-month follow-up study.

Author

Bosnjak Kuharic D, Bozina N, Ganoci L, Makaric P, Kekin I, Prpic N, Bozina T, and Rojnic Kuzman M

Subjects
Adult, Antipsychotic Agents adverse effects, Croatia, Female, Follow-Up Studies, Genotype, Humans, Longitudinal Studies, Male, Pharmacogenetics, Phenotype, Psychotic Disorders diagnosis, Psychotic Disorders psychology, Time Factors, Treatment Outcome, Young Adult, Antipsychotic Agents therapeutic use, Cognition drug effects, HSP70 Heat-Shock Proteins genetics, Pharmacogenomic Variants, Polymorphism, Single Nucleotide, Psychotic Disorders drug therapy, Psychotic Disorders genetics
Abstract

Our aim was to analyze the association of HSPA1B genotypes and treatment response measured by the changes of psychopathology and neurocognitive symptoms in patients with first-episode psychosis (FEP) after 18 months of treatment. A sample of 159 patients with FEP admitted at two Croatian psychiatric hospitals in the period between year 2014 and year 2017 was assessed at baseline and after 18 months of follow-up with Positive and Negative Syndrome Scale (PANSS), Calgary Depression Scale for Schizophrenia (CDSS) and a battery of neurocognitive tests. Associations of scale and test results with HSPA1B polymorphic locus rs1061581 were analyzed using the general linear model. The carriers of the AA genotype showed the highest improvement in CDSS and RAVLT A test after the 18-month follow-up. Concordantly, we found significantly higher improvement assessed with the CDSS, RAVLT A, RAVLT A 30' and positive PANSS scales in the not-GG (AA/AG) group compared with the GG group. Our study suggests that HSPA1B rs1061581variants may moderate treatment response in FEP measured with changes of psychopathology and neurocognitive test results.

Published
2020
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31. Use of pharmacogenomics in elderly patients treated for cardiovascular diseases.

Author

Božina N, Vrkić Kirhmajer M, Šimičević L, Ganoci L, Mirošević Skvrce N, Klarica Domjanović I, and Merćep I

Subjects
Aged, Cardiovascular Agents adverse effects, Cardiovascular Agents therapeutic use, Humans, Precision Medicine, Cardiovascular Diseases drug therapy, Cardiovascular Diseases genetics, Drug-Related Side Effects and Adverse Reactions prevention & control, Pharmacogenetics
Abstract

Older people are increasingly susceptible to adverse drug reactions (ADRs) or therapeutic failure. This could be mediated by considerable polypharmacy, which increases the possibility of drug-drug and drug-gene interactions. Precision medicine, based on individual genetic variations, enables the screening of patients at risk for ADRs and the implementation of personalized treatment regimens. It combines genetic and genomic data with environmental and clinical factors in order to tailor prevention and disease-management strategies, including pharmacotherapy. The identification of genetic factors that influence drug absorption, distribution, metabolism, excretion, and action at the drug target level allows individualized therapy. Positive pharmacogenomic findings have been reported for the majority of cardiovascular drugs (CVD), suggesting that pre-emptive testing can improve efficacy and minimize the toxicity risk. Gene variants related to drug metabolism and transport variability or pharmacodynamics of major CVD have been translated into dosing recommendations. Pharmacogenetics consortia have issued guidelines for oral anticoagulants, antiplatelet agents, statins, and some beta-blockers. Since the majority of pharmacogenetics recommendations are based on the assessment of single drug-gene interactions, it is imperative to develop tools for the prediction of multiple drug-drug-gene interactions, which are common in the elderly with comorbidity. The availability of genomic testing has grown, but its clinical application is still insufficient.

Published
2020

32. Remission Is not Associated with DRD2 rs1800497 and DAT1 rs28363170 Genetic Variants in Male Schizophrenic Patients after 6-months Monotherapy with Olanzapine.

Author

Zivkovic M, Mihaljevic-Peles A, Muck-Seler D, Sagud M, Ganoci L, Vlatkovic S, Tudor L, Pivac N, and Bozina N

Subjects
Adult, Antipsychotic Agents administration & dosage, Humans, Male, Middle Aged, Time Factors, Treatment Outcome, White People genetics, Antipsychotic Agents therapeutic use, Dopamine Plasma Membrane Transport Proteins genetics, Mutation, Olanzapine administration & dosage, Olanzapine therapeutic use, Receptors, Dopamine D2 genetics, Schizophrenia drug therapy, Schizophrenia genetics
Abstract

Background: Symptomatic remission is an achievable goal in the treatment of schizophrenia. The type of antipsychotic medication and particular genetic variants of the dopaminergic system might be associated with remission. Potential pharmacogenetic markers of the treatment response to antipsychotic medication are missing. This study assessed the possible association between dopamine receptor type 2 (DRD2 rs1800497) and dopamine transporter (DAT1 rs28363170) gene variants with symptomatic remission in schizophrenia., Subjects and Methods: Olanzapine (5-20 mg/d) monotherapy was administered for 6 months to 150 male Caucasian subjects with schizophrenia. Remission was evaluated according to "Remission in Schizophrenia Working Group" criteria. Genotyping was performed by PCR-RFLP., Results: Symptomatic remission was found in 31% of patients. DRD2 rs1800497 and DAT1 rs28363170 gene variants were not significantly associated with symptomatic remission. The limitations are a relatively small sample size of patients with schizophrenia (N=150), especially of group with symptomatic remission (N=45). However, the study had moderate but adequate sample sizes for most of the comparisons. Only two dopaminergic polymorphisms were analyzed, and plasma concentration of olanzapine was not determined., Conclusion: These results revealed a lack of association between DRD2 rs1800497 and DAT1 rs28363170 genetic variants and symptomatic remission in male patients treated with olanzapine, suggesting that these genetic variants could not be used to predict symptomatic remission to olanzapine monotherapy. Negative results should be further confirmed or rejected in the larger samples, including haplotype analyses, to detect clinically useful and easy obtainable pharmacogenetic markers that might predict therapeutic response or remission in schizophrenia.

Published
2020
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33. Impact of Continuous P2Y12 Inhibition Tailoring in Acute Coronary Syndrome and Genetically Impaired Clopidogrel Absorption.

Author

Samardzic J, Bozina N, Skoric B, Ganoci L, Krpan M, Petricevic M, Pasalic M, Bozina T, Pavasovic S, Cikes M, and Milicic D

Subjects
ATP Binding Cassette Transporter, Subfamily B genetics, ATP Binding Cassette Transporter, Subfamily B metabolism, Acute Coronary Syndrome blood, Acute Coronary Syndrome diagnosis, Aged, Blood Platelets metabolism, Clopidogrel metabolism, Drug Monitoring, Female, Humans, Male, Middle Aged, Platelet Aggregation Inhibitors metabolism, Purinergic P2Y Receptor Antagonists metabolism, Randomized Controlled Trials as Topic, Receptors, Purinergic P2Y12 blood, Treatment Outcome, Acute Coronary Syndrome drug therapy, Blood Platelets drug effects, Clopidogrel administration & dosage, Gastrointestinal Absorption genetics, Pharmacogenomic Variants, Platelet Aggregation drug effects, Platelet Aggregation Inhibitors administration & dosage, Purinergic P2Y Receptor Antagonists administration & dosage, Receptors, Purinergic P2Y12 drug effects
Abstract

Clopidogrel is still widely used in acute coronary syndrome despite the development of more potent P2Y12 inhibitors. Previously, we conducted a trial that evaluated serial clopidogrel dose adjustment based on platelet function testing in acute coronary syndrome patients with initial high on-treatment platelet reactivity (HTPR). In this substudy, we performed post hoc analysis of the effect of ABCB1 genetic variants C3435T and G2677T/A on platelet inhibition and outcomes. There were no differences in the proportion of HTPR patients among C3435T carriers and noncarriers in both interventional and control group. G2677T carriers expressed significantly higher proportion of HTPR pattern throughout 12-month follow-up in the control group with no difference in the interventional group. There was no difference in ischemic outcomes between C3435T and G2677T carriers and noncarriers in both groups of patients. The results indicate that ABCB1 genotyping is not useful to guide clopidogrel therapy tailoring to improve high-risk patient management.

Published
2020
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34. Association of CNR1 genotypes with changes in neurocognitive performance after eighteen-month treatment in patients with first-episode psychosis.

Author

Rojnic Kuzman M, Bosnjak Kuharic D, Ganoci L, Makaric P, Kekin I, Rossini Gajsak L, Prpic N, Bozina T, Bajic Z, and Bozina N

Subjects
Adult, Attention, Case-Control Studies, Female, Genotype, Humans, Male, Neuropsychological Tests, Psychotic Disorders drug therapy, Psychotic Disorders psychology, Young Adult, Executive Function, Psychotic Disorders genetics, Receptor, Cannabinoid, CB1 genetics
Abstract

Introduction: We analyzed the association of cannabinoid receptor CNR1 genotypes with changes in neurocognitive performance in patients with first-episode psychosis (FEP) after 18 months of treatment. Our secondary aim was to analyze the association of CNR1 genotypes with changes of perceived levels of stress., Methods: We enrolled a sample of 159 patients with FEP from two Croatian psychiatric hospitals between 2014 and 2017. Patients were assessed at baseline and after 18 months. We analyzed the associations of changes in neurocognitive test results and the perceived levels of stress with CNR1 polymorphic loci (rs7766029 and rs12720071) in 121 patients., Results: In the analysis adjusted only for baseline neurocognitive test scores, carriers of rs7766029 CC genotype had significantly (with false discovery rate, FDR < 15%) higher improvement in verbal memory (Wechsler, Wechsler 30') and attention (Digit span F) compared with other participants. In such analysis, rs12720071 carriers of AG genotype had significantly (FDR < 15%) higher improvement in executive functions (Block design), but lower improvement in language functions than AA carriers. In the fully adjusted analysis for age, sex, cannabis use and negative symptoms, only the association of rs7766029 genotypes with the change in the Weschler 30' score was significant (FDR < 15%). In the analysis adjusted only for the baseline neurocognitive tests' scores, both rs7766029 and rs12720071 genotypes were significantly associated with the change in perceived levels of stress (FDR < 15%). In the fully adjusted analysis, only the association with rs7766029 genotype remained significant., Conclusions: The rs7766029 CNR1 variants may moderate changes in neurocognitive performance as well as in perceived levels of stress of patients with FEP over time., (Copyright © 2019 Elsevier Masson SAS. All rights reserved.)

Published
2019
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36. Integration of complementary biomarkers in patients with first episode psychosis: research protocol of a prospective follow up study.

Author

Rojnic Kuzman M, Makaric P, Bosnjak Kuharic D, Kekin I, Rossini Gajsak L, Boban M, Bozina N, Bozina T, Celic Ruzic M, Darmopil S, Filipcic I, Ganoci L, Hladnik A, Madzarac Z, Malojcic B, Mihaljevic Peles A, Mueller DJ, Ostojic D, Petanjek Z, Petrovic R, Vogrinc Z, Savic A, Silic A, Sagud M, Zivkovic M, and Bajic Z

Subjects
Female, Follow-Up Studies, Genome-Wide Association Study, Humans, Hydrocortisone analysis, Male, Pharmacogenetics, Prospective Studies, Psychotic Disorders complications, Psychotic Disorders diagnosis, Psychotic Disorders drug therapy, Saliva chemistry, Schizophrenia complications, Biomarkers analysis, Psychotic Disorders genetics
Abstract

In this project, we recruited a sample of 150 patients with first episode of psychosis with schizophrenia features (FEP) and 100 healthy controls. We assessed the differences between these two groups, as well as the changes between the acute phase of illness and subsequent remission among patients over 18-month longitudinal follow-up. The assessments were divided into four work packages (WP): WP1- psychopathological status, neurocognitive functioning and emotional recognition; WP2- stress response measured by saliva cortisol during a stress paradigm; cerebral blood perfusion in the resting state (with single photon emission computed tomography (SPECT) and during activation paradigm (with Transcranial Ultrasonography Doppler (TCD); WP3-post mortem analysis in histologically prepared human cortical tissue of post mortem samples of subjects with schizophrenia in the region that synaptic alteration was suggested by WP1 and WP2; WP4- pharmacogenetic analysis (single gene polymorphisms and genome wide association study (GWAS). We expect that the analysis of these data will identify a set of markers that differentiate healthy controls from patients with FEP, and serve as an additional diagnostic tool in the first episode of psychosis, and prediction tool which can be then used to help tailoring individualized treatment options. In this paper, we describe the project protocol including aims and methods and provide a brief description of planned post mortem studies and pharmacogenetic analysis.

Published
2019
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37. Interaction between ABCG2 421C>A polymorphism and valproate in their effects on steady-state disposition of lamotrigine in adults with epilepsy.

Author

Klarica Domjanović I, Lovrić M, Trkulja V, Petelin-Gadže Ž, Ganoci L, Čajić I, and Božina N

Subjects
ATP Binding Cassette Transporter, Subfamily B genetics, ATP Binding Cassette Transporter, Subfamily B metabolism, ATP Binding Cassette Transporter, Subfamily G, Member 2 metabolism, Adolescent, Adult, Aged, Alleles, Anticonvulsants therapeutic use, Dose-Response Relationship, Drug, Drug Interactions, Drug Therapy, Combination methods, Epilepsy genetics, Female, Glucuronosyltransferase genetics, Glucuronosyltransferase metabolism, Humans, Lamotrigine therapeutic use, Male, Middle Aged, Neoplasm Proteins metabolism, Polymorphism, Single Nucleotide, Prospective Studies, Valproic Acid therapeutic use, Young Adult, ATP Binding Cassette Transporter, Subfamily G, Member 2 genetics, Anticonvulsants pharmacology, Epilepsy drug therapy, Lamotrigine pharmacology, Neoplasm Proteins genetics, Valproic Acid pharmacology
Abstract

Aims: To investigate the impact of glucuronidation enzyme (UGT1A4*3 142T>G, UGT1A4*2 70C>A, UGT2B7 -161C>T) and transporter (MDR1/ABCB1 1236C>T, ABCG2 421C>A) polymorphisms on steady-state disposition of lamotrigine and on the lamotrigine-valproate interaction., Methods: Adults with epilepsy on lamotrigine monotherapy (n = 131) or lamotrigine + valproate treatment (n = 74) were genotyped and steady-state lamotrigine and valproate morning troughs were determined as a part of routine therapeutic drug monitoring., Results: No effect of UGT and MDR1/ABCB1 polymorphisms was observed. In the entire cohort, ABCG2 421A allele had no effect however an interaction between the variant allele and valproate was observed: (i) in lamotrigine-only patients, variant allele (vs. wild type homozygosity) was independently (adjustments: age, sex, body mass index, lamotrigine dose, other polymorphisms) associated with mildly lower lamotrigine troughs [geometric means ratio (GMR) = 0.76, 95% confidence interval (CI) 0.59-0.98], whereas in lamotrigine + valproate patients it was associated with higher troughs (GMR = 1.72, 95%CI 1.14-2.62); (ii) valproate cotreatment was overall associated with markedly higher troughs vs. lamotrigine monotherapy (GMR = 3.49, 95%CI 2.73-4.44), but more so in variant allele carriers (GMR = 5.24, 95%CI 3.38-8.15) than in wild type homozygotes (GMR = 2.32, 95%CI 1.89-2.83); (iii) variant allele effects in two treatment subsets and valproate effects in two genotype subsets differed by 2.36-fold (95%CI 1.39-3.67); (iv) increase in lamotrigine troughs associated with increasing valproate troughs was greater in variant allele carriers than in wild type homozygotes, i.e. variant allele effect increased with increasing valproate troughs., Conclusion: This study is first to indicate a potentially relevant interaction between ABCG2 421C>A polymorphism and valproate in their effects on lamotrigine disposition., (© 2018 The British Pharmacological Society.)

Published
2018
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38. Brain-derived neurotrophic factor serum and plasma levels in the treatment of acute schizophrenia with olanzapine or risperidone: 6-week prospective study.

Author

Kudlek Mikulic S, Mihaljevic-Peles A, Sagud M, Bajs Janovic M, Ganoci L, Grubisin J, Kuzman Rojnic M, Vuksan Cusa B, Bradaš Z, and Božina N

Subjects
Acute Disease, Adult, Age Factors, Female, Humans, Male, Middle Aged, Olanzapine, Prospective Studies, Sex Factors, Young Adult, Antipsychotic Agents therapeutic use, Benzodiazepines therapeutic use, Brain-Derived Neurotrophic Factor blood, Risperidone therapeutic use, Schizophrenia blood, Schizophrenia drug therapy
Abstract

Antipsychotics have been the mainstay of the treatment of schizophrenia, and their potential role in neuroprotection could be related to brain-derived neurotrophic factor (BDNF). So far different effects on both serum and plasma levels of BDNF were reported related to the various antipsychotic treatments. Aim of this study was to investigate the influence of olanzapine or risperidone on both plasma and serum levels of BDNF in patients with acute schizophrenia. For 50 participants with acute episode of schizophrenia both plasma and serum BDNF, along with the Positive and Negative Syndrome Scale (PANSS) and the Clinical Global Impression scale, were assessed pretreatment and post treatment - after 6 weeks of either risperidone or olanzapine. Results show that a weak correlation between pretreatment plasma and serum levels of BNDF was found no longer significant after 6 weeks of treatment. Antipsychotics, olanzapine and risperidone showed no significant effect on post treatment plasma and serum levels of BDNF. Pretreatment plasma level of BDNF and PANSS positive subscale were positively correlated. Post treatment serum level of BDNF and Clinical Global Impression were negatively correlated. In conclusion, plasma and serum BDNF levels could be different markers to some extent with regard to clinical symptoms, response to therapy and outcome. The interrelation between serum and plasma BDNF should be established in further studies.

Published
2017
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39. Dapsone-induced agranulocytosis-possible involvement of low-activity N-acetyltransferase 2.

Author

Potočnjak I, Likić R, Šimić I, Juričić Nahal D, Čegec I, Ganoci L, and Božina N

Subjects
Agranulocytosis diagnosis, Enzyme Activation drug effects, Enzyme Activation physiology, Humans, Male, Middle Aged, Agranulocytosis chemically induced, Agranulocytosis enzymology, Anti-Infective Agents adverse effects, Arylamine N-Acetyltransferase metabolism, Dapsone adverse effects
Abstract

Dapsone-induced agranulocytosis is a rare but potentially fatal adverse drug reaction (ADR). A 45-year-old male Caucasian patient developed agranulocytosis caused by dapsone (diamino-diphenyl sulfone), which he was prescribed for leukocytoclastic vasculitis. Patient's treatment consisted of termination of dapsone, antibiotic therapy, and granulocyte colony-stimulating factor leading to prompt improvement of symptoms and normalization of laboratory blood values. Diagnostic evaluation revealed methemoglobinemia and excluded glucose-6-phosphate dehydrogenase deficiency. Pharmacogenetics testing showed that he was a carrier of NAT2 *5/*6 genotype, predisposing to low activity of the N-acetyltransferase 2 enzyme. This was the first and only ADR to dapsone reported in Croatia. In total, there have been 73 ADR to dapsone recorded worldwide, including only four cases of agranulocytosis., (© 2017 Société Française de Pharmacologie et de Thérapeutique.)

Published
2017
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40. Genetic polymorphisms of cytochrome P450 enzymes: CYP2C9, CYP2C19, CYP2D6, CYP3A4, and CYP3A5 in the Croatian population.

Author

Ganoci L, Božina T, Mirošević Skvrce N, Lovrić M, Mas P, and Božina N

Subjects
Adult, Aged, Aged, 80 and over, Alleles, Croatia, Cytochrome P-450 Enzyme System metabolism, Female, Genotype, Humans, Male, Middle Aged, Young Adult, Cytochrome P-450 Enzyme System genetics, Polymorphism, Genetic genetics
Abstract

Background: Data on the frequency of pharmacogenetic polymorphisms in the Croatian population are limited. We determined and analyzed frequencies for the most important CYP2C9, CYP2C19, CYP2D6, CYP3A4, and CYP3A5 genetic variants in the Croatian population., Methods: 2637 subjects were included. Genotyping was performed by real-time polymerase chain reaction (PCR) using TaqMan® DME or TaqMan® SNP Genotyping Assays, and by PCR, and PCR-RFLP analysis., Results: For CYP2C9, allele frequencies of *2 and *3 variant were 14.5% and 7.6%, respectively. Among them, 3.98% of subjects were predicted to be poor metabolizers. For CYP2C19, the most frequent variant alleles were *2 (14.8%), and *17 (23.7%), while 2.4% of subjects were predicted to be poor metabolizers, and 5.39% were homozygous carriers of *17 predicted to be ultrarapid metabolizers (UM). For CYP2D6, the frequencies of tested variant alleles were *3 (2.2%), *4 (17.4%), *5 (1%), *6 (1.1%), and *41 (10.8%). Out of these, 5.59% were predicted to be poor metabolizers, 3.19% were classified as UM while 1.0% were carriers of variant alleles duplications (undefined phenotype). For CYP3A4 allele frequencies of *1B and *22 variants were 1.4% and 2.7%, respectively. Allele frequency of CYP3A5*3 was 95.5%. Analyzing CYP3A cluster according to the combination of CYP3A4*22 and CYP3A5*3 revealed 5.34% of subjects to be poor metabolizers, while 8.66% were classified as extensive metabolizers., Conclusions: The frequency of the CYP allelic variants, genotypes, and predicted phenotypes in the Croatian population is in accordance with the other European populations, between the values of published data for Middle European and Mediterranean populations.

Published
2017
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41. CYP2D6 *6/*6 genotype and drug interactions as cause of haloperidol-induced extrapyramidal symptoms.

Author

Šimić I, Potočnjak I, Kraljičković I, Stanić Benić M, Čegec I, Juričić Nahal D, Ganoci L, and Božina N

Subjects
Aged, Antipsychotic Agents therapeutic use, Drug Interactions, Genetic Variation genetics, Genotype, Glucuronosyltransferase genetics, Haloperidol therapeutic use, Humans, Male, Mental Disorders complications, Mental Disorders drug therapy, Antipsychotic Agents adverse effects, Basal Ganglia Diseases chemically induced, Basal Ganglia Diseases genetics, Cytochrome P-450 CYP2D6 genetics, Haloperidol adverse effects
Abstract

A 66-year-old male Caucasian, received 1 mg of haloperidol orally and rapidly developed severe iatrogenic extrapyramidal symptoms. Treatment was immediately discontinued, and the side effects resolved. Haloperidol is mainly metabolized by Phase I CYP2D6 and to the lesser extent by CYP3A4 and by Phase II UGT2B7 enzymes. Genotyping was performed revealing CYP2D6*6/*6, CYP3A4*1/*1, and UGT2B7 -161 C/T genotypes, implicating poor, extensive and intermediate metabolism, respectively. Of the CYPs, haloperidol is metabolized by CYP2D6 and CYP3A4 primarily. It was the introduction of ciprofloxacin which was a trigger for the development of adverse drug reaction due to inhibition of CYP3A4, which was in presented patient main metabolic pathway for haloperidol since he was CYP2D6 poor metabolizer. Presented case report highlights the importance of genotyping. Pharmacogenetics testing should be considered when drug toxicity is suspected, polymorphic metabolic pathways used and drugs concomitantly applied.

Published
2016
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42. ABCG2 gene polymorphisms as risk factors for atorvastatin adverse reactions: a case-control study.

Author

Mirošević Skvrce N, Macolić Šarinić V, Šimić I, Ganoci L, Muačević Katanec D, and Božina N

Subjects
ATP Binding Cassette Transporter, Subfamily G, Member 2, Adult, Asian People, Cytochrome P-450 CYP3A genetics, Female, Genotype, Humans, Liver-Specific Organic Anion Transporter 1, Male, Middle Aged, Organic Anion Transporters genetics, Polymorphism, Single Nucleotide, Risk Factors, ATP-Binding Cassette Transporters genetics, Atorvastatin adverse effects, Drug-Related Side Effects and Adverse Reactions genetics, Genetic Association Studies, Neoplasm Proteins genetics
Abstract

Aim: To explore the association between dose-related adverse drug reactions (ADRs) of atorvastatin and polymorphisms of ABCG2, taking into account the influence of CYP3A4 and SLCO1B1 genes., Materials & Methods: Sixty patients who experienced atorvastatin dose-related ADRs and 90 matched patients without ADRs were enrolled in the study. Genotyping for ABCG2 421C > A, CYP3A4*22, SLCO1B1 388A > G, SLCO1B1 521T > C variants was performed by real-time PCR., Results: Patients with ABCG2 421CA or AA genotypes had 2.9 times greater odds of developing atorvastatin dose-dependent ADRs (OR: 2.91; 95% CI: 1.22-6.95; p = 0.016) than those with ABCG2 421CC genotype. After adjustments for clinical and genetic risk factors, ABCG2 remained a statistically significant predictor of adverse drug reactions (OR: 2.75; 95% CI: 1.1-6.87; p = 0.03;). Also, carriers of SLCO1B1 521 TC or CC genotypes had 2.3 greater odds (OR: 1.03-4.98; 95% CI: 1.03-4.98; p = 0.043) of experiencing ADRs caused by atorvastatin in comparison with carriers of SLCO1B1 521 TT genotype., Conclusion: Our study demonstrated an association between atorvastatin-induced ADRs and genetic variants in the ABCG2 gene.

Published
2015
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43. CYP2C19*2 genotype influence in acute coronary syndrome patients undergoing serial clopidogrel dose tailoring based on platelet function testing: Analysis from randomized controlled trial NCT02096419.

Author

Samardzic J, Bozina N, Skoric B, Ganoci L, Petricevic M, Krpan M, Pasalic M, and Milicic D

Subjects
Acute Coronary Syndrome blood, Acute Coronary Syndrome drug therapy, Aged, Clopidogrel, Cytochrome P-450 CYP2C19 metabolism, Dose-Response Relationship, Drug, Electrocardiography, Female, Follow-Up Studies, Genotype, Humans, Male, Middle Aged, Platelet Aggregation Inhibitors administration & dosage, Platelet Function Tests, Randomized Controlled Trials as Topic, Ticlopidine administration & dosage, Treatment Outcome, Acute Coronary Syndrome genetics, Blood Platelets physiology, Cytochrome P-450 CYP2C19 genetics, Ticlopidine analogs & derivatives
Published
2015
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