Pharmacotherapeutic group: Antineoplastic agents; monoclonal antibodies and antibody drug conjugates.
ATC code: L01FX05.
Pharmacology: Pharmacodynamics: Mechanism of action: Brentuximab vedotin is an antibody drug conjugate (ADC) that delivers an antineoplastic agent that results in apoptotic cell death selectively in CD30-expressing tumour cells. Nonclinical data suggest that the biological activity of brentuximab vedotin results from a multi-step process. Binding of the ADC to CD30 on the cell surface initiates internalisation of the ADC-CD30 complex, which then traffics to the lysosomal compartment. Within the cell, a single defined active species, MMAE, is released via proteolytic cleavage. Binding of MMAE to tubulin disrupts the microtubule network within the cell, induces cell cycle arrest and results in apoptotic death of the CD30-expressing tumour cell.
Classical HL, sALCL and subtypes of CTCL (including MF and pcALCL) express CD30 as an antigen on the surface of their malignant cells. This expression is independent of disease stage, line of therapy or transplant status. These features make CD30 a target for therapeutic intervention. Because of the CD30-targeted mechanism of action brentuximab vedotin is able to overcome chemo-resistance as CD30 is consistently expressed in patients who are refractory to multi-agent chemotherapy, irrespective of prior transplant status. The CD30-targeted mechanism of action of brentuximab vedotin, the consistent expression of CD30 throughout the classical HL, sALCL and CD30+ CTCL disease and therapeutic spectrums and clinical evidence in CD30-positive malignancies following multiple lines of treatment provide a biologic rationale for its use in patients with relapsed and refractory classical HL, sALCL with or without prior ASCT and CD30+ CTCL after at least 1 prior systemic therapy.
Contributions to the mechanism of action by other antibody associated functions have not been excluded.
Pharmacodynamic effects: Cardiac electrophysiology: Forty-six (46) patients with CD30-expressing haematologic malignancies were evaluable of the 52 patients who received 1.8 mg/kg of brentuximab vedotin every 3 weeks as part of a phase 1, single-arm, open-label, multicenter cardiac safety study. The primary objective was to evaluate the effect of brentuximab vedotin on cardiac ventricular re-polarization and the predefined primary analysis was the change in QTc from baseline to multiple time points in Cycle 1.
The upper 90% confidence interval (CI) around the mean effect on QTc was <10 msec at each of the Cycle 1 and Cycle 3 post-baseline time points. These data indicate the absence of clinically relevant QT prolongation due to brentuximab vedotin administered at a dose of 1.8 mg/kg every 3 weeks in patients with CD30-expressing malignancies.
Clinical efficacy and safety: Hodgkin lymphoma: Study C25003: The efficacy and safety of BRENTUXIMAB VEDOTIN (ADCETRIS) were evaluated in a randomised, open-label, 2-arm, multicenter trial in 1334 patients with previously untreated advanced HL in combination with chemotherapy (doxorubicin [A], vinblastine [V] and dacarbazine [D] [AVD]). All patients had a histologically confirmed CD30-expressing disease. Sixty-two percent of patients had extranodal site involvement of the 1334 patients, 664 patients were randomised to the BRENTUXIMAB VEDOTIN (ADCETRIS) + AVD arm and 670 patients were randomised to the ABVD (doxorubicin [A], bleomycin [B], vinblastine [V] and dacarbazine [D]) arm and stratified by number of International Prognostic Factor Project (IPFP) risk factors and region. Patients were treated on days 1 and 15 of each 28-day cycle with 1.2 mg/kg of BRENTUXIMAB VEDOTIN (ADCETRIS) administered as an intravenous infusion over 30 minutes + doxorubicin 25 mg/m
2, vinblastine 6 mg/m
2, and dacarbazine 375 mg/m
2. The median number of cycles received was 6 (range, 1 to 6 cycles). Table 1 provides a summary of the baseline patient and disease characteristics. There were no relevant differences in the patient and disease characteristics between the two arms. (See Table 1.)
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The primary endpoint in Study C25003 was modified PFS (mPFS) per independent review facility (IRF), defined as time from randomisation to disease progression, death, or evidence of non-complete response (non-CR) after completion of first-line therapy per IRF followed by subsequent anticancer therapy. Timing of the modified event was the date of the first PET scan post completion of first-line therapy demonstrating the absence of complete response (CR), defined as Deauville score of ≥3. The median modified PFS by IRF assessment was not reached in either treatment arm. The results in the intent-to-treat (ITT) population showed a statistically significant improvement in modified PFS for BRENTUXIMAB VEDOTIN (ADCETRIS)+ AVD, with a stratified hazard ratio of 0.770 (95% CI, 0.603; 0.983, p=0.035), indicating a 23% reduction in the risk of modified PFS events for BRENTUXIMAB VEDOTIN (ADCETRIS)+ AVD versus ABVD.
A pre-specified subgroup analysis of mPFS by disease stage showed that patients with Stage IV disease had a larger effect compared with the ITT population, with an unstratified hazard ratio of 0.71 (95% CI, 0.53; 0.96), compatible with a 29% reduction in the risk of modified PFS events for BRENTUXIMAB VEDOTIN (ADCETRIS)+ AVD versus ABVD. Of the ITT population, 846 patients (64%) had Stage IV disease.
Table 2 provides the efficacy results for modified PFS and overall survival (OS) in the ITT population and patients with Stage IV disease. (See Table 2 and Figures 1 and 2.)
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Other secondary efficacy endpoints including CR rate and ORR at the end of randomisation regimen, CR rate at the end of first-line therapy, and the rate of PET negativity at the end of Cycle 2, duration of response (DOR), duration of complete remission (DOCR), disease-free survival (DFS,) and event-free survival (EFS) all trended in favour of BRENTUXIMAB VEDOTIN (ADCETRIS) + AVD in both the ITT and Stage IV population.
Pre-specified subgroup analyses of modified PFS per IRF were performed for the ITT population including age, region, cancer stage at baseline, baseline extranodal sites, number of IPFP risk factors, baseline B symptoms, Cycle 2 PET assessment, Cycle 2 PET Deauville score, and receipt of alternative first-line medication (AFM). The analyses showed a consistent trend towards benefit for patients who received BRENTUXIMAB VEDOTIN (ADCETRIS) + AVD compared with patients who received ABVD in most subgroups. The efficacy in elderly patient population (patients ≥60 years of age [n=186] [HR=1.00, 95% CI (0.58, 1.72)] and ≥65 years of age [n=122] [HR=1.01, 95% CI (0.53, 1.94)]) and patients with no extranodal sites (n=445) (HR=1.04, 95% CI [0.67, 1.62]) showed no clinically meaningful difference between the two arms.
Post-hoc subgroup analyses of modified PFS per IRF for patients with Stage IV disease were performed including age, region, baseline extranodal sites, number of IPFP risk factors, baseline B symptoms, baseline ECOG status and gender. The analyses showed a consistent trend towards benefit for patients who received BRENTUXIMAB VEDOTIN (ADCETRIS) + AVD compared with patients who received ABVD in most subgroups. Patients with Stage IV disease for whom extranodal disease was reported ([n=722] [HR=0.69, 95% CI (0.50, 0.94)]) showed an mPFS (per IRF) benefit. In patients with Stage IV disease for whom no extranodal disease was reported, no benefit has been shown at time of analysis ([n=85] [HR=1.49, 95% CI (0.51, 4.31)]). The significance of this finding in stage IV HL patients with no extranodal disease is not established due to small patient numbers and low event rates (14 events). The efficacy in elderly patients with Stage IV disease in the A + AVD arm (patients ≥60 years of age [n=118] [HR=0.80, 95% CI (0.42, 1.53)] and ≥65 years of age [n=78] [HR=0.78, 95% CI (0.36, 1.67)]) showed better benefit compared with elderly patients in ITT population.
In the ITT population, 33% fewer patients treated with BRENTUXIMAB VEDOTIN (ADCETRIS) + AVD in the ITT population received subsequent salvage chemotherapy (n=66) and high-dose chemotherapy and transplant (n=36) compared with those treated with ABVD (n=99 and n=54, respectively). In the Stage IV population, 35% fewer patients treated with BRENTUXIMAB VEDOTIN (ADCETRIS) + AVD received subsequent salvage chemotherapy (n=45) compared with those treated with ABVD (n=69) and 22% fewer patients treated with BRENTUXIMAB VEDOTIN (ADCETRIS) + AVD received high-dose chemotherapy and transplant (n=29) compared with those treated with ABVD (n=37).
The European Organization for Research and Treatment of Cancer Quality of Life 30-Item Questionnaire (EORTC-QLQ-C30) showed no clinically meaningful difference between the two arms in both the ITT and Stage IV population.
Study SGN35-005: The efficacy and safety of BRENTUXIMAB VEDOTIN (ADCETRIS) were evaluated in a randomised, double-blind, placebo-controlled, 2-arm multicenter trial in 329 patients with HL at risk of relapse or progression following ASCT. Patients with known cerebral/meningeal disease, including history of PML were excluded from the study. See Table 3 for patient characteristics. Of the 329 patients, 165 patients were randomised to the treatment arm and 164 patients were randomised to the placebo arm. In the study, patients were to receive their first dose after recovery from ASCT (between days 30-45 following ASCT). Patients were treated with 1.8 mg/kg of BRENTUXIMAB VEDOTIN (ADCETRIS) or matching placebo intravenously over 30 minutes every 3 weeks for up to 16 cycles.
Eligible patients were required to have at least one of the following risk factors: HL that was refractory to frontline treatment; Relapsed or progressive HL that occurred <12 months from the end of frontline treatment; Extranodal involvement at time of pre-ASCT relapse, including extranodal extension of nodal masses into adjacent vital organs. (See Table 3.)
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Efficacy results as of the primary analysis of the primary endpoint are shown in Table 4. The primary endpoint of PFS per IRF was met and showed a difference in median PFS of 18.8 months in favour of the treatment arm. (See Table 4.)
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Pre-specified subgroup analyses of PFS per IRF were performed by patients' best response to pre-ASCT salvage therapy, HL status after frontline therapy, age, gender, baseline weight, baseline ECOG performance status, number of treatments pre-ASCT, geographic region, pre-ASCT PET status, B symptom status after failure of frontline therapy, and pre-ASCT extranodal disease status. The analyses showed a consistent trend towards benefit for patients who received BRENTUXIMAB VEDOTIN (ADCETRIS) compared with patients who received placebo with the exception of patients ≥65 years of age (n=8).
No differences were observed in quality of life between the treatment and placebo arms. Medical resource utilization (MRU) analysis showed that hospitalizations and outpatient visits, as well as working days/other activities missed by patients and caregivers were lower with BRENTUXIMAB VEDOTIN (ADCETRIS) compared with placebo in patients with HL at increased risk of relapse.
An updated analysis conducted after 3 years of follow-up showed a sustained PFS improvement per IRF (HR=0.58 [95% CI (0.41, 0.81)]).
As of study closure, approximately 10 years after enrollment of the first patient, PFS per investigator continued to show a benefit (HR=0.51 [95% CI (0.37, 0.71)]). Overall survival results were consistent with those reported at the time of primary analysis (HR=1.11 [95% CI (0.72, 1.70)]).
Figure 3 shows PFS per investigator in the ITT population as of study closure. (See Figure 3.)
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Post-hoc Risk Factor Analyses: Post-hoc analyses were performed for the primary analysis of the primary endpoint to evaluate the impact of increased risk (number of risk factors) on clinical benefit (Table 5). Representative risk factors for these analyses were: HL that occurred <12 months or HL that was refractory to frontline therapy; Best response of PR or SD to most recent salvage therapy as determined by CT and/or PET scanning; Extranodal disease at pre-ASCT relapse; B symptoms at pre-ASCT relapse; Two or more prior salvage therapies.
The results of these post-hoc analyses suggest increased clinical benefit for patients with two or more risk factors but no difference based on any of the individual risk factors. No benefit in terms of PFS or OS has been observed in patients with one risk factor for relapse or progression. (See Table 5.)
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At the time of the updated analysis (3 years of follow-up) for patients with 2 or more risk factors, the hazard ratio for PFS per IRF was 0.49 (95% CI [0.34, 0.71]) and the hazard ratio for PFS per investigator was 0.41 (95% CI [0.29, 0.58]) (see Figures 4 and 5).
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As of study closure, approximately 10 years after enrollment of the first patient, the hazard ratio for PFS per investigator for patients with 2 or more risk factors was 0.41 (95% CI [0.29, 0.58]). The hazard ratio for PFS per investigator for patients with 3 or more risk factors was 0.38 (95% CI [0.25, 0.59]). Overall survival results remained consistent with those observed as of the primary analysis.
Study SG035-0003: The efficacy and safety of BRENTUXIMAB VEDOTIN (ADCETRIS) as a single agent was evaluated in a pivotal open-label, single-arm, multicenter study in 102 patients with relapsed or refractory HL. See Table 6 as follows for a summary of baseline patient and disease characteristics. (See Table 6.)
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Eighteen (18) patients (18%) received 16 cycles of BRENTUXIMAB VEDOTIN (ADCETRIS); and the median number of cycles received was 9 (ranging from 1 to 16).
Response to treatment with BRENTUXIMAB VEDOTIN (ADCETRIS) was assessed by Independent Review Facility (IRF) using the Revised Response Criteria for Malignant Lymphoma (Cheson, 2007). Treatment response was assessed by spiral CT of chest, neck, abdomen and pelvis; PET scans and clinical data. Response assessments were performed at cycles 2, 4, 7, 10, 13, and 16 with PET at cycles 4 and 7.
The objective response rate (ORR) per IRF assessment was 75% (76 of 102 patients in the intent-to-treat [ITT] set) and tumour reduction was achieved in 94% of patients. Complete remission (CR) was 33% (34 of 102 patients in the ITT set). The median overall survival (OS) is 40.5 months (the median observation time (time to death or last contact) from first dose was 35.1 months (range 1.8 to 72.9+ months). The estimated overall survival rate at 5 years was 41% (95% CI [31%, 51%]). The investigator assessments were generally consistent with the independent review of the scans. Of the patients treated, 8 responding patients went on to receive an allogeneic SCT. For further efficacy results see Table 7. (See Table 7.)
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An exploratory intra-patient analysis showed that approximately 64% of the HL patients treated with BRENTUXIMAB VEDOTIN (ADCETRIS) as part of the SG035-0003 clinical study experienced an improvement in clinical benefit as measured by longer progression free survival (PFS) compared with their most recent prior line of therapy.
Of the 35 patients (33%) who had B symptoms at baseline, 27 patients (77%) experienced resolution of all B symptoms at a median time of 0.7 months from initiation of BRENTUXIMAB VEDOTIN (ADCETRIS).
Data in HL Patients Who Are Not Stem Cell Transplant (SCT) Candidates: Study-C25007: A phase 4 single-arm study was conducted in patients with relapsed or refractory HL (n=60) who had received at least one prior chemotherapeutic regimen and at the time of treatment initiation with BRENTUXIMAB VEDOTIN (ADCETRIS) were not considered candidates for SCT or multiagent chemotherapy. Eligible patients were not to have received a prior SCT. The median number of cycles was 7 (range 1 to 16 cycles). Patients were treated with 1.8 mg/kg of BRENTUXIMAB VEDOTIN (ADCETRIS) every 3 weeks.
At the time of the primary analysis of the primary endpoint, per IRF, the objective response rate (ORR) in the ITT population was 50% (95% CI, 37; 63%). A best overall response of CR was reported for 7 patients (12%); PR was reported for 23 patients (38%). Among these 30 patients, the median time to response, defined as the time from first dose to the soonest of PR or CR, was 6 weeks (range, 5 to 39 weeks). The median time to best overall response, defined as the time from first dose to the clinical best response of CR or PR, was 11 weeks (range, 5 to 60 weeks). Twenty-eight patients (47%) went on to receive SCT after a median of 7 cycles (range, 4 to 16 cycles) of BRENTUXIMAB VEDOTIN (ADCETRIS) treatment. The 32 patients (53%) who did not receive subsequent SCT also received BRENTUXIMAB VEDOTIN (ADCETRIS) for a median of 7 cycles (range, 1 to 16 cycles).
Of the 60 patients in the study, 49 patients (82%) received >1 prior cancer-related treatment and 11 patients (18%) received 1 prior cancer-related treatment. Per IRF, the ORR was 51% (95% CI [36%, 66%]) for the patients who had received >1 prior cancer-related treatment and 45% (95% CI [17%, 77%]) for the patients who had received 1 prior cancer-related treatment. For the patients who received >1 prior cancer-related treatment, a best overall response of CR was reported for 6 patients (12%); PR was reported for 19 patients (39%). For the patients who received 1 prior cancer-related treatment, CR was reported for 1 patient (9%) and PR was reported for 4 patients (36%). Out of the 49 patients receiving >1 line of prior treatment, 22 patients (45%) received subsequent SCT; of the 11 patients who had received 1 prior treatment, 6 patients (55%) received subsequent SCT.
Data were also collected from patients (n=15) in phase 1 dose escalation and clinical pharmacology studies, and from patients (n=26) in a NPP, with relapsed or refractory HL who had not received an ASCT, and who were treated with 1.8 mg/kg of BRENTUXIMAB VEDOTIN (ADCETRIS) every 3 weeks.
Baseline patient characteristics showed failure from multiple prior chemotherapy regimens (median of 3 with a range of 1 to 7) before first administration with BRENTUXIMAB VEDOTIN (ADCETRIS). Fifty nine percent (59%) of patients had advanced stage disease (Stage III or IV) at initial diagnosis.
Results from these phase 1 studies and from the NPP experience showed, that in patients with relapsed or refractory HL without prior ASCT, clinically meaningful responses can be achieved as evidenced by an investigator-assessed, objective response rate of 54% and a complete remission rate of 22% after a median of 5 cycles of BRENTUXIMAB VEDOTIN (ADCETRIS).
Study SGN35-006 (Retreatment Study): The efficacy of retreatment in patients who had previously responded (CR or PR) to treatment with BRENTUXIMAB VEDOTIN (ADCETRIS) was evaluated in a phase 2, open-label, multicenter trial. Twenty patients with relapsed or refractory HL received a starting dose of 1.8 mg/kg and one patient received a starting dose of 1.2 mg/kg of BRENTUXIMAB VEDOTIN (ADCETRIS) administered intravenously over 30 minutes every 3 weeks. The median number of cycles was 7 (range, 2 to 37 cycles). Of the 20 evaluable patients with HL, 6 patients (30%) achieved a CR and 6 patients (30%) achieved a PR with BRENTUXIMAB VEDOTIN (ADCETRIS) retreatment, for an ORR of 60%. The median duration of response was 9.2 and 9.4 months in patients who achieved OR (CR+PR) and CR, respectively.
Previously untreated systemic anaplastic large cell lymphoma (sALCL) or other CD30-expressing peripheral T-cell lymphomas (PTCL), in combination with chemotherapy: Study SGN35-014: The efficacy of BRENTUXIMAB VEDOTIN (ADCETRIS) in combination with chemotherapy for the treatment of adult patients with previously untreated, CD30-expressing PTCL was evaluated in a multicenter, randomized, double-blind, double-dummy, actively controlled trial. For enrollment, the trial required CD30 expression ≥10% per immunohistochemistry. The trial excluded patients with primary cutaneous CD30-positive T-cell lymphoproliferative disorders and lymphomas. The trial required hepatic transaminases ≤3 times ULN, total bilirubin ≤1.5 times ULN, and serum creatinine ≤2 times ULN.
Of the 452 total patients, 226 patients were randomized to the BRENTUXIMAB VEDOTIN (ADCETRIS) + CHP arm and 226 patients were randomized to the CHOP arm. Patients in both treatment arms were treated intravenously on Day 1 of each 21-day cycle for 6 to 8 cycles; prednisone was administered orally on Days 1-5. Dosing in each treatment arm was administered according to the following: BRENTUXIMAB VEDOTIN (ADCETRIS) + CHP arm: BRENTUXIMAB VEDOTIN (ADCETRIS) 1.8 mg/kg over 30 minutes, cyclophosphamide 750 mg/m
2, doxorubicin 50 mg/m
2, and prednisone 100 mg orally; CHOP arm: cyclophosphamide 750 mg/m
2, doxorubicin 50 mg/m
2, vincristine 1.4 mg/m
2, and prednisone 100 mg orally.
The median age was 58 years (range: 18 to 85), 63% were male, 62% were White, 22% were Asian, and 78% had an ECOG performance status of 0-1. Of the 452 patients enrolled, the disease subtypes included patients with systemic ALCL [70%; 48% anaplastic lymphoma kinase (ALK) negative and 22% ALK positive], PTCL not otherwise specified (16%), angioimmunoblastic T-cell lymphoma (12%), adult T-cell leukemia/lymphoma (2%), and enteropathy-associated T-cell lymphoma (<1%).
Most patients had Stage III or IV disease (81%) and a baseline international prognostic index of 2 or 3 (63%).
During randomized treatment, on the BRENTUXIMAB VEDOTIN (ADCETRIS) + CHP arm, 70% of patients received 6 cycles and 18% of patients received 8 cycles. On the CHOP arm, 62% of patients received 6 cycles and 19% received 8 cycles.
Efficacy was based on IRF-assessed PFS, which was defined as time from randomization to progression, death due to any cause, or receipt of subsequent anticancer chemotherapy to treat residual or progressive disease. Other efficacy endpoints included PFS in patients with systemic ALCL, overall survival, complete response rate, and overall response rate. Efficacy results are summarized in Table 8: Kaplan-Meier curves for PFS and overall survival are presented in Figure 6 and Figure 7, respectively. (See Table 8 and Figures 6 and 7.)
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Median overall survival was not reached in either treatment arm.
Systemic anaplastic large cell lymphoma: Study SGN35-014: The efficacy and safety of BRENTUXIMAB VEDOTIN (ADCETRIS) were evaluated in a randomised, double-blind, double-dummy, active-controlled, multicenter trial of 452 patients with previously untreated CD30+ PTCL in combination with cyclophosphamide [C], doxorubicin [H] and prednisone [P] (CHP). For enrollment, the trial required CD30 expression ≥10% per immunohistochemistry. Only patients with CD30+ PTCLs who were eligible for a cyclophosphamide [C], doxorubicin [H], vincristine [O] and prednisone [P] (CHOP)-based regimen were included. The combination of BRENTUXIMAB VEDOTIN (ADCETRIS) + CHP has not been studied in all PTCL subtypes. See Table 8 for enrolled PTCL subtypes. Of the 452 patients, 226 were randomised to treatment with BRENTUXIMAB VEDOTIN (ADCETRIS) + CHP and 226 patients were randomised to treatment with CHOP. Randomisation was stratified by ALK-positive sALCL versus all other subtypes and by the International Prognostic Index (IPI) score. Patients were treated with 1.8 mg/kg of BRENTUXIMAB VEDOTIN (ADCETRIS) administered as an intravenous infusion over 30 minutes on day 1 of each 21-day cycle + CHP (cyclophosphamide 750 mg/m
2 every 3 weeks by IV infusion; doxorubicin 50 mg/m
2 every 3 weeks by IV infusion; and prednisone 100 mg on Days 1 to 5 of each 3-week cycle, orally) for 6 to 8 cycles. The median number of cycles received was 6 (range, 1 to 8 cycles); 70% of patients received 6 cycles of treatment, and 18% received 8 cycles of treatment. Table 9 provides a summary of baseline patient and disease characteristics. (See Table 9.)
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The primary endpoint in SGN35-014 was PFS per IRF, defined as the time from the date of randomisation to the date of first documentation of progressive disease, death due to any cause, or receipt of subsequent anticancer chemotherapy to treat residual or progressive disease, whichever occurs first. Receipt of post-treatment consolidative radiotherapy, post-treatment chemotherapy for the purpose of mobilising peripheral blood stem cells, or consolidative autologous or allogeneic stem cell transplant were not considered as disease progression or as having started new anticancer therapy.
Key secondary endpoints included PFS per IRF for patients with centrally-confirmed sALCL, CR rate per IRF following the completion of study treatment, OS and ORR per IRF following the completion of study treatment which were tested by a fixed sequence testing procedure following the statistical significance of PFS per IRF.
The primary endpoint and alpha-protected, key secondary endpoints, which were evaluated hierarchically, were met. The median PFS per IRF for the ITT population was 48.2 months on the BRENTUXIMAB VEDOTIN (ADCETRIS) + CHP arm versus 20.8 months on the CHOP arm. The stratified hazard ratio was 0.71 (95% CI: 0.54; 0.93, p=0.011), indicating a 29% reduction in the risk of PFS events for BRENTUXIMAB VEDOTIN (ADCETRIS) + CHP versus CHOP. For overall survival, the stratified hazard ratio was 0.66 (95% CI: 0.46; 0.95, p=0.024), a 34% reduction in the risk of OS events for BRENTUXIMAB VEDOTIN (ADCETRIS) + CHP versus CHOP.
PFS per IRF for patients with centrally-confirmed sALCL was a pre-specified key secondary endpoint. The median PFS per IRF was 55.7 months on the BRENTUXIMAB VEDOTIN (ADCETRIS) + CHP arm versus 54.2 months on the CHOP arm. The stratified hazard ratio was 0.59 (95% CI: 0.42; 0.84), compatible with a statistically significant 41% reduction in the risk of PFS events for BRENTUXIMAB VEDOTIN (ADCETRIS) + CHP versus CHOP (p-value=0.003), see Figure 6 and Table 9.
Subgroup analyses were performed for patients with locally-diagnosed sALCL. For overall survival, the stratified hazard ratio was 0.54 (95% CI: 0.34; 0.87), a 46% reduction in the risk of OS events for BRENTUXIMAB VEDOTIN (ADCETRIS) + CHP versus CHOP, see Figure 7. At the end of treatment, the CR rate by IRF assessment was 71.0% for patients on the BRENTUXIMAB VEDOTIN (ADCETRIS) + CHP arm compared with 53.2% for patients on the CHOP arm with a difference of 17.7% (95% CI: 7.2%; 28.3%). At the end of treatment, the ORR rate by IRF assessment was 87.7% for patients on the BRENTUXIMAB VEDOTIN (ADCETRIS) + CHP arm compared with 70.8% for patients on the CHOP arm with a difference of 16.9% (95% CI: 8.1%; 25.7%). In the subgroup of patients with ALK+ sALCL and ALK-sALCL the stratified hazard ratio for PFS per IRF was 0.29 (95% CI: 0.11; 0.79) and 0.65 (95% CI: 0.44; 0.95), respectively. (See Table 10 and Figures 8 and 9.)
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As of study closure more than 7 years after enrollment of the first patient, PFS per investigator results in the ITT population indicated a 30% reduction in the risk of a PFS event in the BRENTUXIMAB VEDOTIN (ADCETRIS)+CHP arm compared with patients treated with CHOP (HR=0.70 [95% CI (0.53, 0.91)]). PFS per investigator results in the sALCL population indicated a 45% reduction in the risk of a PFS event in the BRENTUXIMAB VEDOTIN (ADCETRIS)+CHP arm compared with patients treated with CHOP (HR=0.55 [95% CI (0.39, 0.79)]).
As of study closure, overall survival results continued to show a benefit and were consistent with those reported at the time of the primary analysis. Overall survival results in the ITT population indicated a 28% reduction in the risk of death in the BRENTUXIMAB VEDOTIN (ADCETRIS)+CHP arm compared with patients treated with CHOP (HR=0.72 [95% CI (0.53 to 0.99)]). Overall survival results in the sALCL population indicated a 34% reduction in the risk of death in the BRENTUXIMAB VEDOTIN (ADCETRIS)+CHP arm compared with patients treated with CHOP (HR=0.66 [95% CI (0.43, 1.01)]), see Figure 10. (See Figure 10.)
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Study SG035-0004: The efficacy and safety of BRENTUXIMAB VEDOTIN (ADCETRIS) as a single agent was evaluated in an open-label, single-arm, multicenter study in 58 patients with relapsed or refractory sALCL. See Table 11 as follows for a summary of baseline patient and disease characteristics. (See Table 11.)
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The median time from initial sALCL diagnosis to first dose with BRENTUXIMAB VEDOTIN (ADCETRIS) was 16.8 months.
Ten (10) patients (17%) received 16 cycles of BRENTUXIMAB VEDOTIN (ADCETRIS); the median number of cycles received was 7 (range, 1 to 16).
Response to treatment with BRENTUXIMAB VEDOTIN (ADCETRIS) was assessed by Independent Review Facility (IRF) using the Revised Response Criteria for Malignant Lymphoma (Cheson, 2007). Treatment response was assessed by spiral CT of chest, neck, abdomen and pelvis; PET scans and clinical data. Response assessments were performed at cycles 2, 4, 7, 10, 13 and 16 with PET at cycles 4 and 7.
The ORR per IRF assessment was 86% (50 of 58 patients in the ITT set). CR was 59% (34 of 58 patients in the ITT set) and tumour reduction (of any degree) was achieved in 97% of patients. The estimated overall survival at 5 years was 60% (95% CI [47%,73%]). The median observation time (time to death or last contact) from first dose was 71.4 months. The investigator assessments were generally consistent with the independent review of the scans. Of the patients treated, 9 responding patients went on to receive an allogeneic stem cell transplant (SCT) and 9 responding patients went on to autologous SCT. For further efficacy results, see Table 12 and Figure 11. (See Table 12 and Figure 11.)
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An exploratory intra-patient analysis showed that approximately 69% of the sALCL patients treated with BRENTUXIMAB VEDOTIN (ADCETRIS) as part of the SG035-0004 clinical study experienced an improvement in clinical benefit as measured by longer progression free survival (PFS) compared with their most recent prior line of therapy.
Of the 17 patients (29%) who had B symptoms at baseline, 14 patients (82%) experienced resolution of all B symptoms in a median time from initiation of BRENTUXIMAB VEDOTIN (ADCETRIS) of 0.7 months.
Study C25006: The efficacy and safety of BRENTUXIMAB VEDOTIN (ADCETRIS) as a single agent were also evaluated in a phase 4 open-label, single-arm multicenter study in 50 patients with relapsed or refractory sALCL. The ORR per IRF assessment was 64% (32 of 50 patients in the ITT set). The median DOR per IRF was not reached (95% CI 19.71 months, NE). The CR rate was 30% (15 of 50 patients in the ITT set), and tumour reduction (of any degree) was achieved in 93% of evaluable patients. The median DOCR per IRF was not reached (95% CI 10.61 months, NE). Response assessments were generally consistent between IRF and investigator. Of the patients treated, 13 patients went on to receive a haematopoietic stem cell transplant.
Pooled data from studies C25006 and SG035-0004 (N=108) show an ORR per IRF of 76% (82 of 108 patients in the ITT set). The median DOR per IRF was 17.0 months (95% CI 12.62, 32.46). CR was 45% (49 of 108 patients in the ITT set) and tumour reduction (of any degree) was achieved in 96% of evaluable patients. The median DOCR per IRF was 26.3 months (95% CI 16.16, NE). Response assessments per IRF and investigator were generally consistent.
Study SGN35-006 (Retreatment study): The efficacy of retreatment in patients who had previously responded (CR or PR) to treatment with BRENTUXIMAB VEDOTIN (ADCETRIS) was evaluated in a phase 2, open-label, multicenter trial. Seven patients with relapsed sALCL received a starting dose of 1.8 mg/kg and one patient received a starting dose of 1.2 mg/kg of BRENTUXIMAB VEDOTIN (ADCETRIS) administered intravenously over 30 minutes every 3 weeks. The median number of cycles was 8.5 (range, 2 to 30 cycles). Of the 8 sALCL patients, 3 were retreated twice for a total of 11 retreatment experiences. Retreatment with BRENTUXIMAB VEDOTIN (ADCETRIS) resulted in 6 CRs (55%) and 4 PRs (36%), for an ORR of 91%. The median duration of response was 8.8 and 12.3 months in patients who achieved OR (CR+PR) and CR, respectively.
Cutaneous T-cell lymphoma: Study C25001: The efficacy and safety of BRENTUXIMAB VEDOTIN (ADCETRIS) as a single agent was evaluated in a pivotal phase 3, open-label, randomised, multicentre study in 128 patients with histologically confirmed CD30+ CTCL. CD30 positivity was defined as ≥10% target lymphoid cells demonstrating membrane, cytoplasmic, and/or Golgi staining pattern based on an immunohistochemistry assay (Ventana anti-CD30 [Ber-H2]). Patients with a diagnosis of mycosis fungoides [MF] or primary cutaneous anaplastic large cell lymphoma [pcALCL] were considered eligible for the study. Patients were stratified by these disease types and randomised 1:1 to receive either BRENTUXIMAB VEDOTIN (ADCETRIS) or the physician's choice of either methotrexate or bexarotene. Patients with pcALCL received either prior radiation therapy or at least 1 prior systemic therapy and patients with MF received at least 1 prior systemic therapy. Patients with a concurrent diagnosis of systemic ALCL, Sezary syndrome and other non-Hodgkin lymphoma (except for lymphomatoid papulosis [LyP]) were excluded from this study. Patients were treated with 1.8 mg/kg of BRENTUXIMAB VEDOTIN (ADCETRIS) intravenously over 30 minutes every 3 weeks for up to 16 cycles or physician's choice for up to 48 weeks. The median number of cycles was approximately 12 cycles in the BRENTUXIMAB VEDOTIN (ADCETRIS) arm. In the physician's choice arm, the median duration of treatment (number of cycles) for patients receiving bexarotene was approximately 16 weeks (5.5 cycles) and 11 weeks (3 cycles) for patients receiving methotrexate. Table 13 provides a summary of the baseline patient and disease characteristics. (See Table 13.)
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The most common prior skin directed therapies in the ITT population were radiotherapy (64%), phototherapy (48%) and topical steroids (17%). The most common prior systemic therapies in the ITT population were chemotherapy (71%), immunotherapy (43%) and bexarotene (38%).
The primary endpoint was objective response rate that lasts at least 4 months (ORR4) (duration from first response to last response ≥4 months), as determined by an independent review of the Global Response Score (GRS) consisting of skin evaluations (modified severity weighted assessment tool [mSWAT] as assessed per investigator), nodal and visceral radiographic assessment, and detection of circulating Sézary cells (Olsen 2011). Table 14 includes the results for ORR4 and other key secondary endpoints. (See Table 14.)
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Pre-specified subgroup analyses of ORR4 per IRF were performed by patients' CTCL subtype, physicians' choice of treatment, baseline ECOG status, age, gender, and geographic region. The analyses showed a consistent trend towards benefit for patients who received BRENTUXIMAB VEDOTIN (ADCETRIS) compared with patients who received physician's choice. ORR4 was 50% and 75% in the BRENTUXIMAB VEDOTIN (ADCETRIS) arm versus 10.2% and 20% in the physician's choice arm for MF and pcALCL, respectively.
No meaningful differences in quality of life (assessed by the EuroQol five dimensions questionnaire [EQ-5D] and Functional Assessment of Cancer Therapy-General [FACT-G]) were observed between the treatment arms.
The efficacy and safety of BRENTUXIMAB VEDOTIN (ADCETRIS) were evaluated in two additional open-label studies in 108 patients with relapsed CD30+ CTCL (including MF and pcALCL as well as SS, LyP and mixed CTCL histology), regardless of CD30 expression level. Patients were treated with BRENTUXIMAB VEDOTIN (ADCETRIS) 1.8 mg/kg intravenously over 30 minutes every 3 weeks for up to 16 cycles. The safety and efficacy results in these studies were consistent with results in Study C25001. Overall response rates for MF were 54-66%; pcALCL, 67%; SS, 50%; LyP, 92%; and mixed CTCL histology, 82-85%.
Paediatric Population: Combination therapy: C25004: The safety and anti-tumour activity of BRENTUXIMAB VEDOTIN (ADCETRIS) were evaluated in an open-label, multicenter trial in 59 paediatric patients (6-17 years of age) with previously untreated advanced-stage classical CD30+ HL in combination with chemotherapy (doxorubicin [A], vinblastine [V] and dacarbazine [D] [AVD]). All patients had a histologically confirmed CD30-expressing disease. Fifty-nine percent of patients (n=35) had extranodal site involvement. All 59 paediatric patients were treated on days 1 and 15 of each 28-day cycle with 48 mg/m
2 of BRENTUXIMAB VEDOTIN (ADCETRIS) administered as an intravenous infusion over 30 minutes + doxorubicin 25 mg/m
2, vinblastine 6 mg/m
2, and dacarbazine 375 mg/m
2. The BSA-based dose of BRENTUXIMAB VEDOTIN (ADCETRIS) was chosen to match the observed PK exposures in adults in Study C25003. The paediatric maximum tolerated dose (MTD) was not reached. The majority of patients (88%) achieved an objective response by IRF assessment at the EOT, with 76% achieving a CR. No patient died. A total of 13 patients (22%) in the safety population were reported to have received irradiation after Cycle 6.
Monotherapy: C25002: The safety, pharmacokinetics and anti-tumour activity of BRENTUXIMAB VEDOTIN (ADCETRIS) in 36 paediatric patients (7-17 years of age) with r/r HL and sALCL (children aged 7-11 years, n=12 and adolescents aged 12 to 17 years, n=24) were evaluated in a phase 1/2 open-label, single-agent, multicentre dose-escalation study (C25002). Phase 1 of the study assessed the safety profile (see Adverse Reactions), determined the paediatric maximum tolerated dose (MTD) and/or recommended phase 2 dose (RP2D), and assessed the pharmacokinetics of BRENTUXIMAB VEDOTIN (ADCETRIS) (see Pharmacology: Pharmacokinetics as follows). Phase 1 included 3 r/r HL patients treated at 1.4 mg/kg and 9 patients (7 r/r HL and 2 sALCL) treated at 1.8 mg/kg. The MTD was not reached. The RP2D was determined to be 1.8 mg/kg. Across the study, a total of 16 patients with r/r HL and 17 patients with r/r sALCL, of whom 10 were in first relapse, were treated with 1.8 mg/kg of BRENTUXIMAB VEDOTIN (ADCETRIS). The overall response rate (ORR) per independent review facility (IRF) was analysed across both study phases at the RP2D. Of these 33 patients who received the RP2D, 32 were evaluable for response. The ORR was 47% in response-evaluable patients with r/r HL, 53% in patients with r/r sALCL and 60% in sALCL patients in first relapse. Eight HL patients and 9 sALCL patients went on to receive SCT following treatment with BRENTUXIMAB VEDOTIN (ADCETRIS).
Pharmacokinetics: Monotherapy: The pharmacokinetics of brentuximab vedotin were evaluated in phase 1 studies and in a population pharmacokinetic analysis of data from 314 patients. In all clinical trials, brentuximab vedotin was administered as an intravenous infusion.
Maximum concentrations of brentuximab vedotin ADC were typically observed at the end of infusion or the sampling timepoint closest to the end of infusion. A multiexponential decline in ADC serum concentrations was observed with a terminal half-life of approximately 4 to 6 days. Exposures were approximately dose proportional. Minimal to no accumulation of ADC was observed with multiple doses at the every 3-week schedule, consistent with the terminal half-life estimate. Typical C
max and AUC of ADC after a single 1.8 mg/kg in a phase 1 study was approximately 31.98 μg/mL and 79.41 μg/mL x day respectively.
MMAE is the major metabolite of brentuximab vedotin. Median C
max, AUC and T
max of MMAE after a single 1.8 mg/kg of the ADC in a phase 1 study was approximately 4.97 ng/mL, 37.03 ng/mL x day and 2.09 days respectively. MMAE exposures decreased after multiple doses of brentuximab vedotin with approximately 50% to 80% of the exposure of the first dose being observed at subsequent doses. MMAE is further metabolised mainly to an equally potent metabolite; however, its exposure is an order of magnitude lower than that of MMAE. Thus, it is not likely to have any substantial contribution to the systemic effects of MMAE.
In the first cycle, higher MMAE exposure was associated with an absolute decrease in neutrophil count.
Combination therapy: The pharmacokinetics of BRENTUXIMAB VEDOTIN (ADCETRIS) in combination with AVD were evaluated in a single phase 3 study in 661 patients. Population pharmacokinetic analysis indicated that the pharmacokinetics of BRENTUXIMAB VEDOTIN (ADCETRIS) in combination with AVD were consistent to that in monotherapy.
After multiple-dose, IV infusion of 1.2 mg/kg brentuximab vedotin every two weeks, maximal serum concentrations of ADC were observed near the end of the infusion and elimination exhibited a multi-exponential decline with a t
1/2z of approximately 4 to 5 days. Maximal plasma concentrations of MMAE were observed approximately 2 days after the end of infusion, and exhibited a mono-exponential decline with a t
1/2z of approximately 3 to 4 days.
After multiple-dose, IV infusion of 1.2 mg/kg brentuximab vedotin every two weeks, steady-state trough concentrations of ADC and MMAE were achieved by Cycle 3. Once steady-state was achieved, the PK of ADC did not appear to change with time. ADC accumulation (as assessed by AUC
14D between Cycle 1 and Cycle 3) was 1.27-fold. The exposure of MMAE (as assessed by AUC
14D between Cycle 1 and Cycle 3) appeared to decrease with time by approximately 50%.
The pharmacokinetics of ADCETRIS in combination with CHP were evaluated in a single phase 3 study in 223 patients (SGN35-014). After multiple-dose IV infusion of 1.8 mg/kg BRENTUXIMAB VEDOTIN (ADCETRIS) every 3 weeks, the pharmacokinetics of ADC and MMAE were similar to those of monotherapy.
Distribution: In vitro, the binding of MMAE to human serum plasma proteins ranged from 68-82%. MMAE is not likely to displace or to be displaced by highly protein-bound medicines.
In vitro, MMAE was a substrate of P-gp and was not an inhibitor of P-gp at clinical concentrations.
In humans, the mean steady state volume of distribution was approximately 6-10 L for ADC. Based on population PK estimation the typical apparent central volume of distribution of MMAE was 35.5 L.
Metabolism: The ADC is expected to be catabolised as a protein with component amino acids recycled or eliminated.
In vivo data in animals and humans suggest that only a small fraction of MMAE released from brentuximab vedotin is metabolised. The levels of MMAE metabolites have not been measured in human plasma. At least one metabolite of MMAE has been shown to be active
in vitro.
MMAE is a substrate of CYP3A4 and possibly CYP2D6.
In vitro data indicate that the MMAE metabolism that occurs is primarily via oxidation by CYP3A4/5.
In vitro studies using human liver microsomes indicate that MMAE inhibits only CYP3A4/5 at concentrations much higher than was achieved during clinical application. MMAE does not inhibit other isoforms.
MMAE did not induce any major CYP450 enzymes in primary cultures of human hepatocytes.
Elimination: The ADC is eliminated by catabolism with a typical estimated CL and half life of 1.5 L/day and 4-6 days respectively.
The elimination of MMAE was limited by its rate of release from ADC, typical apparent CL and half life of MMAE was 19.99 L/day and 3-4 days respectively.
An excretion study was undertaken in patients who received a dose of 1.8 mg/kg of brentuximab vedotin. Approximately 24% of the total MMAE administered as part of the ADC during a brentuximab vedotin infusion was recovered in both urine and faeces over a 1-week period. Of the recovered MMAE, approximately 72% was recovered in the faeces. A lesser amount of MMAE (28%) was excreted in the urine.
Pharmacokinetics in special populations: Population PK analysis showed that baseline serum albumin concentration was a significant covariate of MMAE clearance. The analysis indicated that MMAE clearance was 2-fold lower in patients with low serum albumin concentrations <3.0 g/dL compared with patients with serum albumin concentrations within the normal range.
Hepatic impairment: A study evaluated the PK of brentuximab vedotin and MMAE after the administration of 1.2 mg/kg of BRENTUXIMAB VEDOTIN (ADCETRIS) to patients with mild (Child-Pugh A; n=1), moderate (Child-Pugh B; n=5) and severe (Child-Pugh C; n=1) hepatic impairment. Compared to patients with normal hepatic function, MMAE exposure increased approximately 2.3-fold (90% CI 1.27-4.12-fold) in patients with hepatic impairment.
Renal impairment: A study evaluated the PK of brentuximab vedotin and MMAE after the administration of 1.2 mg/kg of BRENTUXIMAB VEDOTIN (ADCETRIS) to patients with mild (n=4), moderate (n=3) and severe (n=3) renal impairment. Compared to patients with normal renal function, MMAE exposure increased approximately 1.9-fold (90% CI 0.85-4.21-fold) in patients with severe renal impairment (creatinine clearance <30 mL/min). No effect was observed in patients with mild or moderate renal impairment.
Elderly: The population pharmacokinetics of brentuximab vedotin were examined from several studies, including data from 380 patients up to 87 years old (34 patients ≥65-<75 and 17 patients ≥75 years of age). Additionally, the population pharmacokinetics of brentuximab vedotin in combination with AVD were examined, including data from 661 patients up to 82 years old (42 patients ≥65-<75 and 17 patients ≥75 years of age). The influence of age on pharmacokinetics was investigated in each analysis and it was not a significant covariate.
Paediatric population: Monotherapy C25002: The pharmacokinetics of brentuximab vedotin ADC and MMAE following a 30-minute intravenous infusion of BV administered at 1.4 mg/kg or 1.8 mg/kg given every 3 weeks were evaluated in a phase 1/2 clinical trial of 36 paediatric patients (7-17 years of age) with r/r HL and sALCL (children aged 7-11 years, n=12 and adolescents aged 12 to 17 years, n=24) (see Pharmacodynamics as previously mentioned). The C
max of ADC was typically observed at the end of infusion or the sampling closest to the end of infusion. A multi-exponential decline in ADC serum concentrations was observed with a terminal half-life of approximately 4 to 5 days. Exposures were approximately dose proportional with a trend observed for lower ADC exposures at lower ages/body weights in the study population. Median ADC AUC in children and adolescents from this study was approx. 14% and 3% lower than in adult patients, respectively, while MMAE exposures were 53% lower and 13% higher, respectively, than in adult patients. Median C
max and AUC of ADC after a single 1.8 mg/kg dose were 29.8 μg/mL and 67.9 μg*day/mL, respectively, in patients <12 years of age and 34.4 μg/mL and 77.8 μg*day/mL, respectively, in patients ≥12 years of age. Median C
max, AUC, and T
max of MMAE after a single 1.8 mg/kg dose were 3.73 ng/mL, 17.3 ng*day/mL, and 1.92 days, respectively, in patients <12 years of age and 6.33 ng/mL, 42.3 ng*day/mL, and 1.82 days, respectively, in patients ≥12 years of age. There was a trend of increased clearance of brentuximab vedotin in paediatric patients confirmed positive for ADAs. No patients aged <12 years (0 of 11) and 2 patients aged ≥12 years (2 of 23) became persistently ADA positive.
Combination therapy: C25004: The pharmacokinetics of brentuximab vedotin ADC and MMAE following a 30-minute intravenous infusion of BV administered at 48 mg/m
2 every 2 weeks in combination with doxorubicin, vinblastine, and dacarbazine (AVD) were evaluated in a phase 1/2 clinical trial of 59 paediatric patients (6-17 years of age) with advanced-stage newly diagnosed CD30+ classical Hodgkin lymphoma (children aged 6-11 years, n=11 and adolescents aged 12 to 17 years, n=48). The C
max of ADC occurred in serum approximately at the end of infusion and declined in a multiexponential manner with a terminal half-life of approximately 4 days. The C
max of MMAE occurred in plasma approximately 2 days following BV administration with a half-life of approximately 2 days. Geometric mean C
max and AUC of ADC following a single 48 mg/m
2 dose were 22.5 μg/mL and 46.7 μg*day/mL, respectively. Geometric mean C
max and AUC of MMAE following a single 48 mg/m
2 dose were 4.9 ng/mL and 27.2 ng*day/mL, respectively. Similar ADC exposures were achieved following body surface area-based dosing of BV at 48 mg/m
2 in combination with AVD among paediatric age groups (<12 years, 12-16 years and >16 years).
Toxicology: Preclinical safety data: MMAE has been shown to have aneugenic properties in an
in vivo rat bone marrow micronucleus study. These results were consistent with the pharmacological effect of MMAE on the mitotic apparatus (disruption of the microtubule network) in cells.
The effects of brentuximab vedotin on human male and female fertility have not been studied. However, results of repeat-dose toxicity studies in rats indicate the potential for brentuximab vedotin to impair male reproductive function and fertility. Testicular atrophy and degeneration were partially reversible following a 16-week treatment-free period.
Brentuximab vedotin caused embryo-foetal lethality in pregnant female rats.
In nonclinical studies, lymphoid depletion and reduced thymic weight were observed, consistent with the pharmacologic disruption of microtubules caused by MMAE derived from brentuximab vedotin.
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