Protocol for treatment of lupus nephritis
11622991 · 2023-04-11
Assignee
Inventors
Cpc classification
A61B5/4848
HUMAN NECESSITIES
A61K31/5377
HUMAN NECESSITIES
A61K31/343
HUMAN NECESSITIES
A61K31/573
HUMAN NECESSITIES
International classification
A61K31/343
HUMAN NECESSITIES
A61K31/5377
HUMAN NECESSITIES
A61K31/573
HUMAN NECESSITIES
Abstract
By employing a pharmacodynamic dosing regimen, the effectiveness of a protocol for treatment of a proteinuric kidney disease with voclosporin can be maximized while minimizing undesirable side effects.
Claims
1. A method of treating lupus nephritis (LN) in a subject, the method comprising: a) selecting for treatment a subject having LN, the selecting comprising determining the subject's estimated Glomerular Filtration Rate (eGFR) at a first time point prior to initiating administering step b); b) administering to the subject voclosporin, mycophenolate mofetil (MMF), and corticosteroids, wherein the administering comprises administering the voclosporin at a starting dose of 23.7 mg administered orally twice daily (BID); c) assessing the subject's eGFR at a second time point after initiating the administering step b); and d) administering to the subject a reduced dose of 15.8 mg BID or 7.9 mg BID voclosporin to treat LN in the subject if, between the first and the second time points, the subject's eGFR decreases in the range of >20% to <30% below the subject's eGFR at the first time point to below 60 ml/min/1.73 m.sup.2.
2. The method of claim 1, comprising continuing the administering step b) for a period of at least 16 weeks and wherein the corticosteroids dose is not more than 2.5 mg/day by week 16.
3. The method of claim 1, wherein the reduced dose is 15.8 mg BID.
4. The method of claim 1, wherein the voclosporin is a mixture of at least 90% E isomer and not more than 10% Z isomer.
5. The method of claim 1, wherein the corticosteroids are methylprednisolone and/or prednisone.
6. The method of claim 1, comprising continuing the administering step b) for a period of at least 16 weeks.
7. The method of claim 1, comprising continuing the administering step b) for a period of at least 24 weeks.
8. The method of claim 1, comprising continuing the administering step b) for a period of at least 48 weeks.
9. The method of claim 1, comprising continuing the administering step b) for a period of at least 52 weeks.
10. The method of claim 1, wherein the selecting step a) further comprises determining the subject's UPCR prior to initiating the administering step b), and selecting a subject having LN that has a urine protein to creatinine ratio (UPCR) of ≥1.5 mg/mg.
11. The method of claim 1, wherein the selecting step a) comprises selecting a subject that has an eGFR of ≥45 mL/min/1.73 m.sup.2 at the first time point.
12. The method of claim 1, further comprising assessing the subject's eGFR at a third time point after initiating step d), and administering to the subject a reduced dose of 15.8 mg BID or 7.9 mg BID voclosporin if, between the first and the third time points, the eGFR of the subject decreases in the range of >20% to <30% below the subject's eGFR at the first time point to below 60 ml/min/1.73 m.sup.2.
13. The method of claim 1, comprising continuing to administer to the subject the dose of 23.7 mg BID voclosporin to treat LN in the subject if, between the first and the second time points, the subject's eGFR decreases by ≤20% below the subject's eGFR at the first time point.
14. A method of treating lupus nephritis (LN) in a subject, the method comprising: a) selecting for treatment a subject having LN, the selecting comprising determining the subject's estimated Glomerular Filtration Rate (eGFR) at a first time point prior to initiating administering step b); b) administering to the subject voclosporin, mycophenolate mofetil (MMF), and corticosteroids, wherein the administering comprises administering the voclosporin at a starting dose of 23.7 mg administered orally twice daily (BID); c) assessing the subjects eGFR at a second time point after initiating the administering step b); and d) administering to the subject a reduced dose of 15.8 mg BID or 7.9 mg BID voclosporin to treat LN in the subject if, between the first and the second time points, the subjects eGFR decreases in the range of >20% to <30% below the subject's eGFR at the first time point to below 60 ml/min/1.73 m.sup.2, and wherein the administering of d) achieves a urine protein creatinine ratio (UPCR) of <0.5 mg/mg.
15. The method of claim 1, wherein the reduced dose is 7.9 mg BID.
16. The method of claim 14, comprising continuing to administer to the subject the dose of 23.7 mg BID voclosporin to treat LN in the subject if, between the first and the second time points, the subject's eGFR decreases by ≤20% below the subject's eGFR at the first time point.
17. The method of claim 14, comprising continuing the administering step b) for a period of at least 16 weeks and wherein the corticosteroids dose is not more than 2.5 mg/day by week 16.
18. The method of claim 14, wherein the reduced dose is 15.8 mg BID.
19. The method of claim 14, wherein the voclosporin is a mixture of at least 90% E isomer and not more than 10% Z isomer.
20. The method of claim 14, wherein the corticosteroids are methylprednisolone and/or prednisone.
21. The method of claim 14, comprising continuing the administering step b) for a period of at least 16 weeks.
22. The method of claim 14, comprising continuing the administering step b) for a period of at least 24 weeks.
23. The method of claim 14, comprising continuing the administering step b) for a period of at least 48 weeks.
24. The method of claim 14, comprising continuing the administering step b) for a period of at least 52 weeks.
25. The method of claim 14, wherein the selecting step a) further comprises determining the subject's UPCR prior to initiating the administering step b), and selecting a subject having LN that has a urine protein to creatinine ratio (UPCR) of ≥1.5 mg/mg.
26. The method of claim 14, wherein the selecting step a) comprises selecting a subject that has an eGFR of ≥45 mL/min/1.73 m.sup.2 at the first time point.
27. The method of claim 14, wherein the reduced dose is 7.9 mg BID.
Description
BRIEF DESCRIPTION OF THE DRAWINGS
(1)
(2)
MODES OF CARRYING OUT THE INVENTION
(3) As noted above, the pharmacodynamic protocol of the invention relates to adjustment of administration of voclosporin depending on certain physiological indicators of the subjects. As further noted, the voclosporin administration is preferably conducted with a background of administration of MMF and of corticosteroids.
(4) In general, the treatment protocols on which the invention is based show dramatically better results than the current standard of care—the rate of complete remission is almost 50% as compared to much lower levels achieved using the current standard of care treatment and the rate of partial remission after 48 weeks is even higher, wherein this rate (PR) includes the subjects with complete remission (CR). As shown below, a lower dosage of voclosporin is more effective than a higher dose in a comparable protocol wherein complete remission was obtained in 40% of the subjects at the higher dosage as opposed to 49% of the subjects in the lower dose group.
(5) Critical to the present invention is pharmacodynamic administration of the voclosporin component. This pharmacodynamic administration is essential as the effects of this drug may be too intense and/or have undesirable side effects or the results may indicate lack of effectiveness and thus the dosage is reduced or interrupted to permit homeostasis to reestablish a suitable set of physiological parameters.
(6) The protocols are designed to cover treatment periods of at least 24 weeks and may extend for longer periods of time, for example 48 weeks or 52 weeks. The regimens involve daily dosages of the voclosporin component, typically twice daily, although alternative frequencies could be employed, such as once a day, three times a day or four times a day based on reactions of the patient and convenience. As an illustration, the protocol will be described below in terms of a 23.7 mg twice daily (BID) dosage; of course if the voclosporin preparation is administered four times daily, the dosage would be cut in half for each administration and if the administration were only once per day, the dosage for the once a day administration would be double the 23.7 mg administered BID.
(7) In addition, as to the pharmacodynamic protocols of the invention, the dosages may be any combination of the 7.9 mg basic units, and thus can be 7.9 mg, 15.8 mg, 31.6 mg, or 39.5 mg, as well as the exemplified 23.7 mg.
(8) The dosage indicated, for example 23.7 mg, (or any other specified dose) is subject to slight variations, typically ±10% or, alternatively, for 23.7 mg specified between 21 mg and 26 mg BID. This is due to inconsistencies in pharmaceutical manufacture and the ideal dosage is the specified dose—i.e., for example, 23.7 mg BID. Comparable variations applied to the alternative dosages, and to the differential adjustment.
(9) Adjustment Based on eGFR:
(10) One critical parameter used to assess the desirability of dosage reduction is the eGFR using the CKD-EP1 formula or other appropriate method. Chronic kidney disease is defined as eGFR as ≤60 mL/min/1.73 m.sup.2 for ≥three months with or without kidney damage. As noted above, a further decrease in eGFR is a negative side effect that may occur during treatment. If the decrease is too severe, the protocol should be altered in accordance with the prescription of the invention. Typically, a baseline value of the eGFR is established either at the beginning of the protocol or at some “first time point” during the protocol. If the decrease is greater than a target percentage, which is typically between 20%-45% as compared to the first time point, a reduction in dosage is indicated, including a reduction to zero or stopping treatment. If the decrease is less than that target percentage maintenance of treatment at the same level as indicated. In addition to an indication that treatment should be reduced or terminated based on the eGFR reduction, reduction below a certain value is also indicative of a need to modify the treatment. This predetermined value is typically in the range of 50-90 mL/min/1.73 m.sup.2.
(11) As stated above, a baseline value for eGFR is established at the outset of the treatment or during treatment. This is typically done on the first day of the treatment before any administration of the drugs in the protocol. This baseline is used as a criterion for adjusting dosage. However, a first time point could be established at any arbitrarily selected time during the protocol.
(12) In one exemplary protocol, at a second time point subsequent to the first which can be on any day of the treatment, a subject with ≥30% decrease in eGFR from the baseline to <60 ml/min/1.73 m.sup.2 (or, in some cases, a higher cut off) should have the treatment interrupted until a repeat test can be performed, but if the decrease is confirmed and not due to contributing factors (such as a high baseline eGFR, the addition or modification of non-steroidal anti-inflammatory drugs, angiotensin converting enzyme inhibitors, angiotensin 2 inhibitor blockers, or a concurrent state of dehydration, etc.), the treatment should be withheld until a third time point determination typically within 48 hours. If the ≥30% decrease is not maintained, treatment is restored to two-thirds or one-third of the original dosage and increased as tolerated to the 23.7 mg level BID.
(13) For convenience, the 23.7 mg administration is administered orally in the form of three capsules containing 7.9 mg each. Thus, it is easy to provide two-thirds of the standard dosage by administering at any given time only two of the three capsules.
(14) With regard to the second time point, in this exemplary protocol a subject having a decrease of ≥20% in eGFR to ≤60 mL/min/1.73 m.sup.2 but a decrease of less than 30% reduction as compared to baseline, the treatment is not interrupted but the dosage is reduced. Reduction in increments of 7.9 mg is preferred. Again, assessment at an additional time point at any subsequent day during the treatment showing baseline values are restored indicates that the original dosage level of 23.7 mg BID can be resumed.
(15) Adjustment Based on Blood Pressure
(16) An alternative parameter that can be used to determine pharmacodynamic dosage is blood pressure. As voclosporin may increase blood pressure to undesirable levels, at any point during the treatment period if either component of the blood pressure i.e. the cystolic or diastolic pressure of the subject is ≥130/80, the treatment should be reduced, preferably by increments of 7.9 mg. At a later time point if both components of the blood pressure are below 130/80, the treatment can be restored to the original level.
(17) Adjustment Based on UPCR Reduction and/or C3/C4 Normalization
(18) Suitable criteria for early evaluation of the probability of success—i.e. complete or partial remission by the end of a planned protocol, have been identified which permit discontinuation of the treatment earlier than the end point if it is highly unlikely that the subject will benefit from continuing on the dosage schedule. These criteria are reduction in UPCR and normalization of C3/C4. These can be used in combination or in the alternative. It has been found that a determination early in a 24-week or 48 week protocol of probable success can be used to determine whether treatment with voclosporin should continue; such findings are applicable to protocols of any substantial length. By way of illustration, if the UPCR has not been reduced by a satisfactory amount early in the regimen or if C3/C4 has not been normalized early in the regimen, one might conclude that the chances of improvement over an extended treatment period are diminished. Application of these criteria in an exemplary trial is shown in detail in Example 3.
(19) However, a rule for stopping treatment is based either on UPCR reduction or C3/C4 normalization taken alone or in combination. If the combination is used, then failure with respect to both criteria would dictate termination of treatment. Decision would be based on the values of the sensitivity, specificity and positive and negative predictive values shown in the tables set forth in Example 3. These terms are defined in the Example.
(20) As an illustration only, such determination can be made at approximately 8 weeks subsequent to the beginning of the regimen; a time frame of 6-10 weeks could be employed for the approximation of 8 weeks. If a decrease of, for example, ≥25% of UPCR is not achieved, it appears unlikely the subject will benefit from further treatment and the protocol is stopped. As shown in the Example, this can be supplemented with evaluation of C3/C4 normalization—if this is done, it is desirable that both determinations be made at the same early time point.
(21) Auxiliary Therapeutics
(22) The voclosporin treatment of the invention is supplemented with MMF and reduced amounts of corticosteroids.
(23) For example, with respect to corticosteroids, subjects who weigh 45 kg or more may receive 0.5 grams of methylprednisolone on days 1 and 2 of the study intravenously and then beginning on day 3, oral corticosteroid therapy. Subjects weighing ≤45 kg receive only half these dosages.
(24) For oral prednisone, the starting dosage for oral administration is 20 mg/day for subjects <45 kg and 25 mg/day for subjects who weigh ≥45 kg. The dosage is reduced according to the protocol shown in Table 1.
(25) TABLE-US-00001 TABLE 1 Dosing Schedule for IV Methylprednisolone and Daily Oral Prednisone (mg) Subjects Subjects In Case of Prior IV Steroids <45 kg ≥45 kg During Screening (Pre-randomization) Weeks 1-2.sup.(1) Days 1-2.sup.(2) 0.25 g (IV) 0.5 g (IV) 1 g minus prior IV steroids mg or (0.5 g minus prior IV steroids mg for subjects who weigh <45 kg).sup.(3) Days 3-13 20 mg (oral) 25 mg (oral) Week 2 (Day 14) 15 mg (oral) 20 mg (oral) Week 4 (Day 28) 10 mg (oral) 15 mg (oral) Week 6 (Day 42).sup.(4) 10 mg (oral) 10 mg (oral) Week 8 (Day 56) 5 mg (oral) 5 mg (oral) Week 12 (Day 84) 5 mg (oral) 5 mg (oral) Week 16 (Day 112) 15 mg (oral) 2.5 mg (oral) .sup.1Day 0-13; Oral Steroids dosed according to subject weight and then tapered beginning at Day 14. .sup.2Oral corticosteroids may be commenced on Days 1 or 2 if corticosteroids are administered during screening. .sup.3Its recognized that dosing with IV methyprednisolone as described in Section 7.2.2.2, Corticosteroids may not be in the subject's best interest if they have already received therapy within the 3 months pnor to screening. In this case, the Investigayor may be permitted to omit the administration of further IV methylprednisolone but only after discussion with the Medical Monitor. .sup.4Week 6 is not a scheduled study visit, a phone call can be performed to decide further tapering for subjects Notes: Oral prednisone taper should he done within ±3 days of specified timeframe. When clinically indicated, subjects are allowed to be completely titrated off of oral corticosteroids. Abbreviation: IV = intravenous
(26) In contrast to the reducing dose of corticosteroid, the same dose of MMF is maintained throughout the study at a twice daily dosage before meals with a glass of water. Typically, each individual dose is one gram resulting in a total dosage of two grams per day although in the alternative, the subject may be administered 500 mg four times daily.
(27) Low Dosage
(28) In addition to the above-described pharmacodynamic protocols, applicants have found that a substantially lower dosage than expected is effective in large numbers of subjects such that a method to treat lupus nephritis in subjects either with or without pharmacodynamic adjustments can be based on a dosage level of either 15.8 mg BID or 7.9 mg BID. The increments of 7.9 mg are dictated by the availability of capsules containing the 7.9 mg dosage level which provides a convenient platform for dosage alterations.
(29) One additional aspect of the invention is therefore a method to treat lupus nephritis wherein either a logically adjusted dosage or a constant dosage of either 15.8 mg BID or 7.9 mg BID is employed. In these protocols, as would be the case for higher dosages of voclosporin, the above described background administration of MMF and corticosteroids is included in the protocol.
(30) General Factors
(31) In all cases, the subjects are evaluated for success of the treatment both on the completion of the treatment and at extended periods thereafter. Typical treatment periods are at least 24 weeks, but preferably 48 weeks or more. Reevaluation after the termination of the treatment period over a period of 1-2 weeks or longer is also employed. Subjects are evaluated for complete or partial remission. Complete remission (CR) is defined as: Confirmed protein/creatinine ratio of ≤0.5 mg/mg, and eGFR ≥60 mL/min/1.73 m.sup.2 or no confirmed decrease from baseline in eGFR of ≥20%. Partial remission is defined as: 50% reduction in UPCR from baseline.
(32) By establishing a pharmacodynamic dosing regimen, the effectiveness of the protocol in treatment of lupus nephritis can be maximized while minimizing undesirable side effects.
(33) The length of the treatment protocol in all cases will vary from at least 8 weeks to for example 12, 16, 24 and 48 weeks or 52 weeks or even longer, up to 60 weeks including stopping points between the levels mentioned. For example, a treatment protocol of 10 or 11 or 15 or 20 or 29 or 31 or 36 or 43 or 51 or 55 weeks could be employed and is within the scope of the invention. The evaluation described above is conducted at the end of the protocol as well as at a suitable time period or multiple time periods thereafter. These time periods are generally 1-2 weeks to 4-5 months subsequent to terminating the dosage and intervening at time intervals are included within the scope of the invention as well.
(34) This statement regarding time intervals applies to the invention pharmacodynamic treatment protocols, regardless of base dosage levels.
(35) The following examples are to illustrate, not to limit the invention.
EXAMPLE 1
48 Week Study of LN Treatment
(36) The subjects enrolled in the study were divided into three groups, 88 subjects are in a control group who were administered 2 g MMF daily as well as oral corticosteroids—i.e., prednisone in a tapering dosage shown graphically in
(37) Subjects were screened prior to admission to the study by (a) determining that the urine protein creatinine ratio (UPCR) as >1.5 mg/mg as measured by first morning void, and (b) that the eGFR as measured by Chronic Kidney Disease Epidemiology Collaboration equation (CKD-EP1) of >45 ml/min/1.73 m.sup.2. Subjects were assessed after 24 weeks and 48 weeks as well as a subsequent evaluation at 50 weeks.
(38) As shown in
(39) CR in this example is a composite end-point which includes efficacy, safety and low-dose steroids: UPCR ≤0.5 mg/mg (confirmed); eGFR >60 ml/min/1.73 m2 or within 20% of baseline; steroids ≤10 mg/day; no administration of rescue medication.
(40) PR is a composite end-point that includes safety and efficacy: UPCR reduction of 50% from baseline and no use of rescue medication
(41) To determine the efficacy of the pharmacodynamic protocol wherein dosage is reduced or stopped according to the presence or absence of indicators of the decrease in eGFR experienced as a side effect, these three groups of patients were assessed after 24 weeks and 48 weeks of treatment with respect to whether treatment was altered according to the invention protocol. In all three groups, the patients were evaluated according to the criteria set forth in the exemplary protocol above—i.e., wherein the eGFR of each patient was measured immediately prior to administering the first dose of voclosporin and at a second time point at least a day later and (i) if the eGFR of said subject decreased by ≥30% to a value of below 60 mL/min/1.73 m.sup.2 between said first and second time points, stopping the administering of Voclosporin or reducing dosage thereof to said subject; (ii) if the eGFR of said subject decreased by between 20% to 30% to a value of below 60 ml/min/1.73 m.sup.2 between said first and second time points, administering a reduced dosage of voclosporin to said subject; (iii) if the eGFR of said subject decreased by ≤20% between said first and second time points, continuing administering the same predetermined daily dosage of voclosporin to said subject.
(42) The results are shown in Tables 2 and 3 below. Table 2 shows percentages with complete remission (CR) or partial remission (PR) after 24 weeks and Table 3 shows these values after 48 weeks for patients that had no dose reduction and those who did have dose reduction.
(43) TABLE-US-00002 TABLE 2 Patients with a No Dose Reductions (24 weeks): Patient Patients with no Patients with Patients with number Dose Reduction CR at 24 PR at 24 Group (n) n(%) weeks n(%) weeks n(%) Placebo 88 77 (87.5) 14 (18.2) 36 (46.8) Low Dose 89 50 (56.2) 15 (30.0) 34 (68.0) High Dose 88 41 (46.6) 11 (26.8) 24 (58.5) Patients with Dose Reductions (pharmacodynamically dosed): Patient Patients with Patients with Patients with number Dose Reduction CR at 24 PR at 24 Group (n) n(%) weeks n(%) weeks n(%) Placebo 88 11 (12.5) 3 (27.3) 7 (63.6) Low Dose 89 39 (43.8) 14 (35.9) 28 (71.8) High Dose 88 47 (53.4) 13 (27.7) 34 (72.3)
(44) TABLE-US-00003 TABLE 3 Patients with No Dose Reductions (48 weeks): Patient Patients with no Patients with Patients with number Dose Reduction CR at 48 PR at 48 Group (n) n(%) weeks n(%) weeks n(%) Placebo 88 74 (84.1) 18 (24.3) 38 (51.4) Low Dose 89 43 (48.3) 20 (46.5) 26 (60.5) High Dose 88 35 (39.8) 11 (31.4) 22 (62.9) Patients with Dose Reductions (pharmacodynamically dosed): Patient Patients with Patients with Patients with number Dose Reduction CR at 48 PR at 48 Group (n) n(%) weeks n(%) weeks n(%) Placebo 88 14 (15.9) 3 (21.4) 4 (28.6) Low Dose 89 46 (51.7) 24 (52.2) 35 (76.1) High Dose 88 53 (60.2) 24 (45.3) 41 (77.4)
(45) In this study, CR was defined as a composite of UPCR ≤0.5 mg/mg; eGFR >60 mL/min/1.73 m.sup.2 or within 20% of baseline, steroids at ≤10 mg/day and no administration of rescue medication. PR is defined as UPCR reduction of 50% from baseline and no use of rescue medication.
(46) As shown in Table 2, 12.5% of patients on placebo, 43.8% of patients on low dose and 53.4% of patients on high dose voclosporin underwent dose reduction during the treatment. The percentage of patients with complete response after 24 weeks was not affected in either dosage groups by the pharmacodynamic dosage and the percentage with partial response was also roughly the same, although with the high dose group, the percentage with partial reduction improved. Table 3 shows similar results at 48 weeks, although a higher percentage of patients were subjected to dose reduction. Again, no drastic effect on the overall response was exhibited.
EXAMPLE 2
Low Dosage Protocol
(47) In the course of clinical studies similar to those in Example 1, it was observed that a substantial portion of subjects showed substantial remission at a dosage reduced almost immediately to 15.8 mg voclosporin administered twice daily (BID). Accordingly, applicants have analyzed these data and have concluded that a dosage protocol providing 15.8 mg or 7.9 mg voclosporin BID is effective with or without the pharmacodynamic aspects of the protocol.
(48) As the capsules contain 7.9 mg voclosporin, 1 cap represents 7.9 mg voclosporin, 2 caps represent 15.8 mg voclosporin and 3 caps represent 23.7 mg voclosporin, etc. Substantial numbers of subjects showed complete or partial remission even when the dosage was lowered to 7.9 mg voclosporin BID quite early in the treatment and similar results were obtained for administration of 15.8 mg BID.
EXAMPLE 3
Predictability Based on Early Responses
(49) In the study reported in Example 1, the predictability of outcomes based on markers at early time points were determined. These results are shown in Tables 4-12.
(50) In the study described in Example 1, data were obtained to ascertain whether markers evaluated after various time-points during treatment would predict an ultimate favorable outcome or show that continuing treatment was likely to be futile. This is important because it is undesirable to subject a patient to unnecessary treatment, even if the treatment is relatively safe. These data are shown in the tables below.
(51) Based on these data, the sensitivity and specificity of the evaluation of each marker and their counterparts positive predictive value and negative predictive value were determined with respect to whether the patient would or would not show partial remission (PR) after 48 weeks of the treatment protocol. PR is defined as at least 50% reduction in proteinuria (i.e. UPCR). This would also include subjects who showed complete remission (CR).
(52) Sensitivity is defined as the probability that a subject showing PR at 48 weeks would have shown a favorable result with regard to the marker at the designated early time point. In the tables below, this is the ratio of the number of subjects with favorable marker results (early drop or normalization) to the total subjects with 48 week PR.
(53) Specificity is defined as the probability that a subject not showing PR at 48 weeks would have shown an unfavorable result with regard to the marker at the designated early time point. In the tables below, this is the ratio of the number of subjects with unfavorable marker results (no early drop or no normalization) to the total subjects with no 48 week PR.
(54) Positive predictive value is defined as the probability that a subject showing a favorable result with respect to the marker at an earlier time point would show PR at 48 weeks. In the tables below, this is the ratio of the number of subjects with favorable marker results who have 48 week PR to those with favorable marker results (early reduction or yes column).
(55) Negative predictive value is defined as the probability that a subject showing an unfavorable result with respect to the marker at an earlier time point would not show PR at 48 weeks. In the tables below, this is the ratio of the number of subjects with unfavorable marker results who have no PR at 48 weeks to the total subjects with unfavorable marker results (no early reduction or no column).
(56) An ideal marker would show a value of 100 for all of these, but this is generally unattainable. As high as possible value is desirable.
(57) Based on the results in these tables, the protocol will be designed to stop treatment at an earlier time point when the parameters set forth above are the most favorable, but at a reasonable time before the 48 week end point. (Obviously the closer to the end point, the more favorable the indicators become, but the advantage to stopping treatment is correspondingly reduced).
(58) TABLE-US-00004 TABLE 4 Table 4 - Early 15% reduction in UPCR Week 48 No Week 48 Partial Partial Remission Remission Early Positive Negative Treatment Early No Early Early No Early Reduction Predictive Predictive Week Group Drop Drop Drop Drop Yes No Sensitivity Specificity Value Value 2 Placebo 27 15 19 25 46 40 64.3 56.8 58.7 62.5 Voclosporin 45 16 10 14 55 30 73.8 58.3 81.8 46.7 23.7 mg BID Voclosporin 39 21 15 9 54 30 65.0 37.5 72.2 30.0 39.5 mg BID 4 Placebo 36 5 18 23 54 28 87.8 56.1 66.7 82.1 Voclosporin 50 9 12 11 62 20 84.7 47.8 80.6 55.0 23.7 mg BID Voclosporin 49 12 16 5 65 17 80.3 23.8 75.4 29.4 39.5 mg BID 6 Placebo 35 7 22 17 57 24 83.3 43.6 61.4 70.8 Voclosporin 53 6 12 6 65 12 89.8 33.3 81.5 50.0 23.7 mg BID Voclosporin 53 10 16 4 69 14 84.1 20.0 76.8 28.6 39.5 mg BID 8 Placebo 38 4 22 18 60 22 90.5 45.0 63.3 81.8 Voclosporin 55 5 12 7 67 12 91.7 36.8 82.1 58.3 23.7 mg BID Voclosporin 56 5 17 4 73 9 91.8 19.0 76.7 44.4 39.5 mg BID 12 Placebo 39 3 19 21 58 24 92.9 52.5 67.2 87.5 Voclosporin 59 2 15 4 74 6 96.7 21.1 79.7 66.7 23.7 mg BID Voclosporin 57 5 14 4 71 9 91.9 22.2 80.3 44.4 39.5 mg BID 16 Placebo 39 3 19 20 58 23 92.9 51.3 67.2 87.0 Voclosporin 58 3 13 5 71 8 95.1 27.8 81.7 62.5 23.7 mg BID Voclosporin 57 6 15 5 72 11 90.5 25.0 79.2 45.5 39.5 mg BID 20 Placebo 38 4 21 16 59 20 90.5 43.2 64.4 80.0 Voclosporin 60 0 13 3 73 3 100.0 18.8 82.2 100.0 23.7 mg BID Voclosporin 58 4 15 5 73 9 93.5 25.0 79.5 55.6 39.5 mg BID 24 Placebo 37 3 18 17 55 20 92.5 48.6 67.3 85.0 Voclosporin 60 0 12 2 72 2 100.0 14.3 83.3 100.0 23.7 mg BID Voclosporin 57 5 14 5 71 10 91.9 26.3 80.3 50.0 39.5 mg BID 26 Placebo 36 3 16 14 52 17 92.3 46.7 69.2 82.4 Voclosporin 55 0 9 3 64 3 100.0 25.0 85.9 100.0 23.7 mg BID Voclosporin 61 0 12 4 73 4 100.0 25.0 83.6 100.0 39.5 mg BID 36 Placebo 41 1 18 13 59 14 97.6 41.9 69.5 92.9 Voclosporin 60 1 10 3 70 4 98.4 23.1 85.7 75.0 23.7 mg BID Voclosporin 62 1 12 6 74 7 98.4 33.3 83.8 85.7 39.5 mg BID 48 Placebo 37 1 10 16 47 17 97.4 61.5 78.7 94.1 Voclosporin 58 0 9 2 67 2 100.0 18.2 86.6 100.0 23.7 mg BID Voclosporin 61 0 10 6 71 6 100.0 37.5 85.9 100.0 39.5 mg BID
(59) TABLE-US-00005 TABLE 5 Table 5 - Early 20% reduction in UPCR Week 48 No Week 48 Partial Partial Remission Remission Early Positive Negative Treatment Early No Early Early No Early Reduction Predictive Predictive Week Group Drop Drop Drop Drop Yes No Sensitivity Specificity Value Value 2 Placebo 24 18 15 29 39 47 57.1 65.9 61.5 61.7 Voclosporin 44 17 8 16 52 33 72.1 66.7 84.6 48.5 23.7 mg BID Voclosporin 36 24 14 10 50 34 60.0 41.7 72.0 29.4 39.5 mg BID 4 Placebo 32 9 13 28 45 37 78.0 68.3 71.1 75.7 Voclosporin 49 10 12 11 61 21 83.1 47.8 80.3 52.4 23.7 mg BID Voclosporin 47 14 16 5 63 19 77.0 23.8 74.6 26.3 39.5 mg BID 6 Placebo 34 8 22 17 56 25 81.0 43.6 60.7 68.0 Voclosporin 53 6 11 7 64 13 89.8 38.9 82.8 53.8 23.7 mg BID Voclosporin 53 10 15 5 68 15 84.1 25.0 77.9 33.3 39.5 mg BID 8 Placebo 38 4 19 21 57 25 90.5 52.5 66.7 84.0 Voclosporin 55 5 11 8 66 13 91.7 83.3 61.5 23.7 mg BID Voclosporin 55 6 17 4 72 10 90.2 19.0 76.4 40.0 39.5 mg BID 12 Placebo 38 4 19 21 57 25 90.5 52.5 66.7 84.0 Voclosporin 59 2 14 5 73 7 96.7 26.3 80.8 71.4 23.7 mg BID Voclosporin 57 5 14 4 71 9 91.9 22.2 80.3 44.4 39.5 mg BID 16 Placebo 39 3 17 22 56 25 92.9 56.4 69.6 88.0 Voclosporin 58 3 12 6 70 9 95.1 33.3 82.9 66.7 23.7 mg BID Voclosporin 57 6 15 5 72 11 90.5 25.0 79.2 45.5 39.5 mg BID 20 Placebo 38 4 20 17 58 21 90.5 45.9 65.5 81.0 Voclosporin 60 0 12 4 72 4 100.0 25.0 83.3 100.0 23.7 mg BID Voclosporin 58 4 15 5 73 9 93.5 25.0 79.5 55.6 39.5 mg BID 24 Placebo 37 3 16 19 53 22 92.5 54.3 69.8 86.4 Voclosporin 59 1 11 3 70 4 98.3 21.4 84.3 75.0 23.7 mg BID Voclosporin 56 6 14 5 70 11 90.3 26.3 80.0 45.5 39.5 mg BID 26 Placebo 36 3 15 15 51 18 92.3 50.0 70.6 83.3 Voclosporin 55 0 9 3 64 3 100.0 25.0 85.9 100.0 23.7 mg BID Voclosporin 61 0 12 4 73 4 100.0 25.0 83.6 100.0 39.5 mg BID 36 Placebo 41 1 16 15 57 16 97.6 48.4 71.9 93.8 Voclosporin 60 1 10 3 70 4 98.4 23.1 85.7 75.0 23.7 mg BID Voclosporin 61 2 12 6 73 8 96.8 33.3 83.6 75.0 39.5 mg BID 48 Placebo 37 1 9 17 46 18 97.4 65.4 80.4 94.4 Voclosporin 58 0 9 2 67 2 100.0 18.2 86.6 100.0 23.7 mg BID Voclosporin 61 0 10 6 71 6 100.0 37.5 85.9 100.0 39.5 mg BID
(60) TABLE-US-00006 TABLE 6 Table 6 - Early 25% reduction in UPCR Week 48 No Week 48 Partial Partial Remission Remission Early Positive Negative Treatment Early No Early Early No Early Reduction Predictive Predictive Week Group Drop Drop Drop Drop Yes No Sensitivity Specificity Value Value 2 Placebo 18 24 15 29 33 53 42.9 65.9 54.5 54.7 Voclosporin 39 22 8 16 47 38 63.9 66.7 83.0 42.1 23.7 mg BID Voclosporin 33 27 14 10 47 37 55.0 41.7 70.2 27.0 39.5 mg BID 4 Placebo 30 11 11 30 41 41 73.2 73.2 73.2 73.2 Voclosporin 48 11 12 11 60 22 81.4 47.8 80.0 50.0 23.7 mg BID Voclosporin 45 16 16 5 61 21 73.8 23.8 73.8 23.8 39.5 mg BID 6 Placebo 33 9 20 19 53 28 78.6 48.7 62.3 67.9 Voclosporin 51 8 10 8 61 16 86.4 44.4 83.6 50.0 23.7 mg BID Voclosporin 49 14 15 5 64 19 77.8 25.0 76.6 26.3 39.5 mg BID 8 Placebo 35 7 17 23 52 30 83.3 57.5 67.3 76.7 Voclosporin 54 6 10 9 64 15 90.0 47.4 84.4 60.0 23.7 mg BID Voclosporin 55 6 17 4 72 10 90.2 19.0 76.4 40.0 39.5 mg BID 12 Placebo 37 5 17 23 54 28 88.1 57.5 68.5 82.1 Voclosporin 57 4 13 6 70 10 93.4 31.6 81.4 60.0 23.7 mg BID Voclosporin 57 5 14 4 71 9 91.9 22.2 80.3 44.4 39.5 mg BID 16 Placebo 39 3 17 22 56 25 92.9 56.4 69.6 88.0 Voclosporin 58 3 11 7 69 10 95.1 38.9 84.1 70.0 23.7 mg BID Voclosporin 56 7 14 6 70 13 88.9 30.0 80.0 46.2 39.5 mg BID 20 Placebo 38 4 17 20 55 24 90.5 54.1 69.1 83.3 Voclosporin 59 1 11 5 70 6 98.3 31.3 84.3 83.3 23.7 mg BID Voclosporin 58 4 15 5 73 9 93.5 25.0 79.5 55.6 39.5 mg BID 24 Placebo 37 3 13 22 50 25 92.5 62.9 74.0 88.0 Voclosporin 59 1 11 3 70 4 98.3 21.4 84.3 75.0 23.7 mg BID Voclosporin 55 7 12 7 67 14 88.7 36.8 82.1 50.0 39.5 mg BID 26 Placebo 36 3 14 16 50 19 92.3 53.3 72.0 84.2 Voclosporin 55 0 8 4 63 4 100.0 33.3 87.3 100.0 23.7 mg BID Voclosporin 60 1 12 4 72 5 98.4 25.0 83.3 80.0 39.5 mg BID 36 Placebo 41 1 16 15 57 16 97.6 48.4 71.9 93.8 Voclosporin 60 1 10 3 70 4 98.4 23.1 85.7 75.0 23.7 mg BID Voclosporin 61 2 12 6 73 8 96.8 33.3 83.6 75.0 39.5 mg BID 48 Placebo 37 1 9 17 46 18 97.4 65.4 80.4 94.4 Voclosporin 58 0 9 2 67 2 100.0 18.2 86.6 100.0 23.7 mg BID Voclosporin 61 0 7 9 68 9 100.0 56.3 89.7 100.0 39.5 mg BID
(61) TABLE-US-00007 TABLE 7 Table 7 - Early 30% reduction in UPCR Week 48 No Week 48 Partial Partial Remission Remission Early Positive Negative Treatment Early No Early Early No Early Reduction Predictive Predictive Week Group Drop Drop Drop Drop Yes No Sensitivity Specificity Value Value 2 Placebo 14 28 13 31 27 59 33.3 70.5 51.9 52.5 Voclosporin 37 24 6 18 43 42 60.7 75.0 86.0 42.9 23.7 mg BID Voclosporin 31 29 11 13 42 42 51.7 54.2 73.8 31.0 39.5 mg BID 4 Placebo 27 14 10 31 37 45 65.9 75.6 73.0 68.9 Voclosporin 47 12 11 12 58 24 79.7 52.2 81.0 50.0 23.7 mg BID Voclosporin 45 16 15 6 60 22 73.8 28.6 75.0 27.3 39.5 mg BID 6 Placebo 32 10 16 23 48 33 76.2 59.0 66.7 69.7 Voclosporin 49 10 10 8 59 18 83.1 44.4 83.1 44.4 23.7 mg BID Voclosporin 47 16 15 5 62 21 74.6 25.0 75.8 23.8 39.5 mg BID 8 Placebo 34 8 15 25 49 33 81.0 62.5 69.4 75.8 Voclosporin 53 7 10 9 63 16 88.3 47.4 84.1 56.3 23.7 mg BID Voclosporin 54 7 17 4 71 11 88.5 19.0 76.1 36.4 39.5 mg BID 12 Placebo 36 6 16 24 52 30 85.7 60.0 69.2 80.0 Voclosporin 56 5 12 7 68 12 91.8 36.8 82.4 58.3 23.7 mg BID Voclosporin 55 7 14 4 69 11 88.7 22.2 79.7 36.4 39.5 mg BID 16 Placebo 39 3 16 23 55 26 92.9 59.0 70.9 88.5 Voclosporin 58 3 11 7 69 10 95.1 38.9 84.1 70.0 23.7 mg BID Voclosporin 55 8 13 7 68 15 87.3 35.0 80.9 46.7 39.5 mg BID 20 Placebo 38 4 16 21 54 25 90.5 56.8 70.4 84.0 Voclosporin 57 3 9 7 66 10 95.0 43.8 86.4 70.0 23.7 mg BID Voclosporin 57 5 15 5 72 10 91.9 25.0 79.2 50.0 39.5 mg BID 24 Placebo 37 3 11 24 48 27 92.5 68.6 77.1 88.9 Voclosporin 59 1 11 3 70 4 98.3 21.4 84.3 75.0 23.7 mg BID Voclosporin 53 9 12 7 65 16 85.5 36.8 81.5 43.8 39.5 mg BID 26 Placebo 34 5 12 18 46 23 87.2 60.0 73.9 78.3 Voclosporin 54 1 7 5 61 6 98.2 41.7 88.5 83.3 23.7 mg BID Voclosporin 58 3 11 5 69 8 95.1 31.3 84.1 62.5 39.5 mg BID 36 Placebo 41 1 14 17 55 18 97.6 54.8 74.5 94.4 Voclosporin 60 1 10 3 70 4 98.4 23.1 85.7 75.0 23.7 mg BID Voclosporin 61 2 11 7 72 9 96.8 38.9 84.7 77.8 39.5 mg BID 48 Placebo 37 1 5 21 42 22 97.4 80.8 88.1 95.5 Voclosporin 58 0 8 3 66 3 100.0 27.3 87.9 100.0 23.7 mg BID Voclosporin 61 0 5 11 66 11 100.0 68.8 92.4 100.0 39.5 mg BID
(62) TABLE-US-00008 TABLE 8 Table 8 - Early 35% reduction in UPCR Week 48 No Week 48 Partial Partial Remission Remission Early Positive Negative Treatment Early No Early Early No Early Reduction Predictive Predictive Week Group Drop Drop Drop Drop Yes No Sensitivity Specificity Value Value 2 Placebo 13 29 13 31 26 60 31.0 70.5 50.0 51.7 Voclosporin 36 25 6 18 42 43 59.0 75.0 85.7 41.9 23.7 mg BID Voclosporin 28 32 11 13 39 45 46.7 54.2 71.8 28.9 39.5 mg BID 4 Placebo 26 15 9 32 35 47 63.4 78.0 74.3 68.1 Voclosporin 46 13 11 12 57 25 78.0 52.2 80.7 48.0 23.7 mg BID Voclosporin 43 18 13 8 56 26 70.5 38.1 76.8 30.8 39.5 mg BID 6 Placebo 30 12 14 25 44 37 71.4 64.1 68.2 67.6 Voclosporin 47 12 9 9 56 21 79.7 50.0 83.9 42.9 23.7 mg BID Voclosporin 47 16 14 6 61 22 74.6 30.0 77.0 27.3 39.5 mg BID 8 Placebo 34 8 14 26 48 34 81.0 65.0 70.8 76.5 Voclosporin 52 8 9 10 61 18 86.7 52.6 85.2 55.6 23.7 mg BID Voclosporin 53 8 17 4 70 12 86.9 19.0 75.7 33.3 39.5 mg BID 12 Placebo 35 7 14 26 49 33 83.3 65.0 71.4 78.8 Voclosporin 54 7 10 9 64 16 88.5 47.4 84.4 56.3 23.7 mg BID Voclosporin 52 10 14 4 66 14 83.9 22.2 78.8 28.6 39.5 mg BID 16 Placebo 39 3 13 26 52 29 92.9 66.7 75.0 89.7 Voclosporin 57 4 11 7 68 11 93.4 38.9 83.8 63.6 23.7 mg BID Voclosporin 55 8 13 7 68 15 87.3 35.0 80.9 46.7 39.5 mg BID 20 Placebo 38 4 15 22 53 26 90.5 59.5 71.7 84.6 Voclosporin 57 3 8 8 65 11 95.0 50.0 87.7 72.7 23.7 mg BID Voclosporin 56 6 15 5 71 11 90.3 25.0 78.9 45.5 39.5 mg BID 24 Placebo 37 3 10 25 47 28 92.5 71.4 78.7 89.3 Voclosporin 59 1 8 6 67 7 98.3 42.9 88.1 85.7 23.7 mg BID Voclosporin 53 9 12 7 65 16 85.5 36.8 81.5 43.8 39.5 mg BID 26 Placebo 34 5 11 19 45 24 87.2 63.3 75.6 79.2 Voclosporin 52 3 7 5 59 8 94.5 41.7 88.1 62.5 23.7 mg BID Voclosporin 55 6 11 5 66 11 90.2 31.3 83.3 45.5 39.5 mg BID 36 Placebo 41 1 12 19 53 20 97.6 61.3 77.4 95.0 Voclosporin 60 1 9 4 69 5 98.4 30.8 87.0 80.0 23.7 mg BID Voclosporin 61 2 11 7 72 9 96.8 38.9 84.7 77.8 39.5 mg BID 48 Placebo 37 1 3 23 40 24 97.4 88.5 92.5 95.8 Voclosporin 58 0 7 4 65 4 100.0 36.4 89.2 100.0 23.7 mg BID Voclosporin 61 0 4 12 65 12 100.0 75.0 93.8 100.0 39.5 mg BID
(63) Thus it appears the 8 week or 12 week results, for example, are predictions of ultimate outcome, and it is beneficial to stop treatment if there was no reduction in UPCR by >15% at that time.
(64) For completeness, Tables 9a and 9b show similar results for an 8 week early time point when a 25% UPCR reduction is used as a criterion and the protocol extends for 24 or 48 weeks.
(65) TABLE-US-00009 TABLE 9a Probability of attaining a CR by Proteinuria if UPCR reduction of 25% or greater is achieved at 8 weeks: #(%) of patients #(%) of patients who had a who had a # of patients # of patients reduction of reduction of in treatment with UPCR UPCR of ≥25% UPCR of ≥25% arm (number # of CRs by reduction who went on to who went on to with week 8 Proteinuria of ≥25% be a CR by UPCR be a CR by UPCR Group assessment) at 24 weeks at 8 weeks at 24 weeks at 48 weeks Placebo 88 (83) 17 52 16/52 (30.8) 18/52 (34.6) Low Dose 89 (80) 29 64 29/64 (45.3) 40/64 (62.5) High Dose 88 (84) 24 72 24/72 (33.3) 32/72 (44.4)
(66) TABLE-US-00010 TABLE 9b Probability of attaining a CR by Proteinuria if UPCR reduction of 25% or greater is not achieved at 8 weeks: #(%) of patients #(%) of patients who did not who did not # of patients have a have a # of patients without reduction of reduction of in treatment UPCR UPCR of ≥25% UPCR of ≥25% arm (number # of CRs by reduction who went on to who went on to with week 8 Proteinuria of ≥25% be a CR by UPCR be a CR by UPCR Group assessment) at 24 weeks at 8 weeks at 24 weeks at 48 weeks Placebo 88 (83) 17 31 1/31 (3.2) 3/31 (9.7) Low Dose 89 (80) 29 16 0/16 (0.0) 4/16 (25.0) High Dose 88 (84) 24 12 0/12 (0.0) 3/12 (25.0)
(67) Another criterion for effectiveness is normalization of C3 and/or C4 concentration in blood. The normal concentration of C3 is 90 mg/dl or greater and for C4 16 mg/dl or greater. Subjects for the treatment of the invention generally have concentrations below these values. Normalization of C3 is defined as an increase from below 90 mg/dl to above that level or a 25% increase from the baseline (below 90) exhibited by the subject and normalization of C4 is defined as an increase from below 16 mg/dl to above that level or a 25% increase from the baseline (below 16) exhibited by the subject.
(68) Tables 10-12 provide similar data for these criteria to the data in Tables 4-9 for UPCR.
(69) TABLE-US-00011 TABLE 10 Table 10 - Early C3 normalization Week 48 No Week 48 Partial Partial Remission Remission No No Positive Negative Treatment Normal- Normal- Normal- Normal- Normalization Predictive Predictive Week Group ization ization ization ization Yes No Sensitivity Specificity Value Value 12 Placebo 16 24 15 22 31 46 40.0 59.5 51.6 47.8 Voclosporin 23 34 8 10 31 44 40.4 55.6 74.2 22.7 23.7 mg BID Voclosporin 34 28 7 10 41 38 54.8 58.8 82.9 26.3 39.5 mg BID 24 Placebo 17 22 16 18 33 40 43.6 52.9 51.5 45.0 Voclosporin 24 33 6 8 30 41 42.1 57.1 80.0 19.5 23.7 mg BID Voclosporin 35 26 6 12 41 38 57.4 66.7 85.4 31.6 39.5 mg BID 48 Placebo 15 23 14 13 29 36 39.5 48.1 51.7 36.1 Voclosporin 25 30 2 8 27 38 45.5 80.0 92.6 21.1 23.7 mg BID Voclosporin 34 29 7 9 41 38 54.0 56.3 82.9 23.7 39.5 mg BID
(70) TABLE-US-00012 TABLE 11 Table 11 - Early C4 normalization Week 48 No Week 48 Partial Partial Remission Remission No No Positive Negative Treatment Normal- Normal- Normal- Normal- Normalization Predictive Predictive Week Group ization ization ization ization Yes No Sensitivity Specificity Value Value 12 Placebo 15 25 19 18 34 43 37.5 48.6 44.1 41.9 Voclosporin 27 29 10 8 37 37 48.2 44.4 73.0 21.6 23.7 mg BID Voclosporin 40 22 8 9 48 31 64.5 52.9 83.3 29.0 39.5 mg BID 24 Placebo 16 23 18 16 34 39 41.0 47.1 47.1 41.0 Voclosporin 32 25 8 6 40 31 56.1 42.9 80.0 19.4 23.7 mg BID Voclosporin 39 22 5 13 44 35 63.9 72.2 88.6 37.1 39.5 mg BID 48 Placebo 16 22 14 13 30 35 42.1 48.1 53.3 37.1 Voclosporin 29 26 5 5 34 31 52.7 50.0 85.3 16.1 23.7 mg BID Voclosporin 36 27 5 11 41 38 57.1 68.8 87.8 28.9 39.5 mg BID
(71) TABLE-US-00013 TABLE 12 Table 12 - Early C3/C4 normalization Week 48 No Week 48 Partial Partial Remission Remission No No Positive Negative Treatment Normal- Normal- Normal- Normal- Normalization Predictive Predictive Week Group ization ization ization ization Yes No Sensitivity Specificity Value Value 12 Placebo 11 29 14 23 25 52 27.5 62.2 44.0 44.2 Voclosporin 20 37 6 12 26 49 35.1 66.7 76.9 24.5 23.7 mg BID Voclosporin 29 33 7 10 36 43 46.8 58.8 80.6 23.3 39.5 mg BID 24 Placebo 12 27 14 20 26 47 30.8 58.8 46.2 42.6 Voclosporin 23 34 4 10 27 44 40.4 71.4 85.2 22.7 23.7 mg BID Voclosporin 26 35 5 13 31 48 42.6 72.2 83.9 27.1 39.5 mg BID 48 Placebo 10 28 10 17 20 45 26.3 63.0 50.0 37.8 Voclosporin 20 35 2 8 22 43 36.4 80.0 90.9 18.6 23.7 mg BID Voclosporin 27 36 5 11 32 47 42.9 68.8 84.4 23.4 39.5 mg BID
(72) Tables 13-17 make similar calculations for the combined results of UPCR and C3/C4 at 12 weeks. In these tables, the data from the 12 week determinations in Tables 4-8 are meshed with the data from the 12 week time point in Table 12.
(73) Based on the levels of sensitivity, specificity, positive predictive value and negative predicted value shown, decision to stop or continue treatment is made.
(74) TABLE-US-00014 TABLE 13 Table 13 - Early 15% reduction in UPCR or C3/C4 normalization Week 48 No Week 48 Partial Partial Remission Remission Early Early No Early Early No Early Drop or Positive Negative Drop or Drop or Drop or Drop or Normal Predictive Predictive Week Treatment Group Normal Normal Normal Normal Yes No Sensitivity Specificity Value Value 12 Placebo 39 3 26 12 65 15 92.9 31.6 60.0 80.0 Voclosporin 60 1 18 1 78 2 98.4 5.3 76.9 50.0 23.7 mg BID Voclosporin 60 3 16 3 76 6 95.2 15.8 78.9 50.0 39.5 mg BID 24 Placebo 39 2 27 8 66 10 95.1 22.9 59.1 80.0 Voclosporin 61 0 13 1 74 1 100.0 7.1 82.4 100.0 23.7 mg BID Voclosporin 57 5 15 4 72 9 91.9 21.1 79.2 44.4 39.5 mg BID 48 Placebo 37 1 18 9 55 10 97.4 33.3 67.3 90.0 Voclosporin 58 0 10 1 68 1 100.0 9.1 85.3 100.0 23.7 mg BID Voclosporin 62 0 12 4 74 4 100.0 25.0 83.8 100.0 39.5 mg BID
(75) TABLE-US-00015 TABLE 14 Table 14 - Early 20% reduction in UPCR or C3/C4 normalization Week 48 No Week 48 Partial Partial Remission Remission Early Early No Early Early No Early Drop or Positive Negative Treatment Drop or Drop or Drop or Drop or Normal Predictive Predictive Week Group Normal Normal Normal Normal Yes No Sensitivity Specificity Value Value 12 Placebo 38 4 26 12 64 16 90.5 31.6 59.4 75.0 Voclosporin 60 1 17 2 77 3 98.4 10.5 77.9 66.7 23.7 mg BID Voclosporin 60 3 16 3 76 6 95.2 15.8 78.9 50.0 39.5 mg BID 24 Placebo 39 2 25 10 64 12 95.1 28.6 60.9 83.3 Voclosporin 61 0 13 1 74 1 100.0 7.1 82.4 100.0 23.7 mg BID Voclosporin 57 5 15 4 72 9 91.9 21.1 79.2 44.4 39.5 mg BID 48 Placebo 37 1 17 10 54 11 97.4 37.0 68.5 90.9 Voclosporin 58 0 10 1 68 1 100.0 9.1 85.3 100.0 23.7 mg BID Voclosporin 62 0 12 4 74 4 100.0 25.0 83.8 100.0 39.5 mg BID
(76) TABLE-US-00016 TABLE 15 Table 15 - Early 25% reduction in UPCR or C3/C4 normalization Week 48 No Week 48 Partial Partial Remission Remission Early Early No Early Early No Early Drop or Positive Negative Treatment Drop or Drop or Drop or Drop or Normal Predictive Predictive Week Group Normal Normal Normal Normal Yes No Sensitivity Specificity Value Value 12 Placebo 38 4 24 14 62 18 90.5 36.8 61.3 77.8 Voclosporin 58 2 16 3 74 5 96.7 15.8 78.4 60.0 23.7 mg BID Voclosporin 60 3 16 3 76 6 95.2 15.8 78.9 50.0 39.5 mg BID 24 Placebo 39 2 23 12 62 14 95.1 34.3 62.9 85.7 Voclosporin 61 0 13 1 74 1 100.0 7.1 82.4 100.0 23.7 mg BID Voclosporin 57 5 14 5 71 10 91.9 26.3 80.3 50.0 39.5 mg BID 48 Placebo 37 1 17 10 54 11 97.4 37.0 68.5 90.9 Voclosporin 58 0 10 1 68 1 100.0 9.1 85.3 100.0 23.7 mg BID Voclosporin 62 0 10 6 72 6 100.0 37.5 86.1 100.0 39.5 mg BID
(77) TABLE-US-00017 TABLE 16 Table 16 - Early 30% reduction in UPCR or C3/C4 normalization Week 48 No Week 48 Partial Partial Remission Remission Early Early No Early Early No Early Drop or Positive Negative Treatment Drop or Drop or Drop or Drop or Normal Predictive Predictive Week Group Normal Normal Normal Normal Yes No Sensitivity Specificity Value Value 12 Placebo 37 5 24 14 61 19 88.1 36.8 60.7 73.7 Voclosporin 58 2 16 3 74 5 96.7 15.8 78.4 60.0 23.7 mg BID Voclosporin 59 4 16 3 75 7 93.7 15.8 78.7 42.9 39.5 mg BID 24 Placebo 39 2 22 13 61 15 95.1 37.1 63.9 86.7 Voclosporin 61 0 13 1 74 1 100.0 7.1 82.4 100.0 23.7 mg BID Voclosporin 57 5 14 5 71 10 91.9 26.3 80.3 50.0 39.5 mg BID 48 Placebo 37 1 13 14 50 15 97.4 51.9 74.0 93.3 Voclosporin 58 0 9 2 67 2 100.0 18.2 86.6 100.0 23.7 mg BID Voclosporin 62 0 8 8 70 8 100.0 50.0 88.6 100.0 39.5 mg BID
(78) TABLE-US-00018 TABLE 17 Table 17 - Early 35% reduction in UPCR or C3/C4 normalization Week 48 No Week 48 Partial Partial Remission Remission Early Early No Early Early No Early Drop or Positive Negative Treatment Drop or Drop or Drop or Drop or Normal Predictive Predictive Week Group Normal Normal Normal Normal Yes No Sensitivity Specificity Value Value 12 Placebo 36 6 23 15 59 21 85.7 39.5 61.0 71.4 Voclosporin 56 4 14 5 70 9 93.3 26.3 80.0 55.6 23.7 mg BID Voclosporin 57 6 16 3 73 9 90.5 15.8 78.1 33.3 39.5 mg BID 24 Placebo 39 2 21 14 60 16 95.1 40.0 65.0 87.5 Voclosporin 61 0 10 4 71 4 100.0 28.6 85.9 100.0 23.7 mg BID Voclosporin 57 5 14 5 71 10 91.9 26.3 80.3 50.0 39.5 mg BID 48 Placebo 37 1 12 15 49 16 97.4 55.6 75.5 93.8 Voclosporin 58 0 8 3 66 3 100.0 27.3 87.9 100.0 23.7 mg BID Voclosporin 62 0 7 9 69 9 100.0 56.3 89.9 100.0 39.5 mg BID
EXAMPLE 4
Low Dose Corticosteroid
(79) Applicants have also found that the dosage of corticosteroid can effectively be reduced as compared to “standard of care” as shown in Tables 8 and 9, and can be reduced further to 4 mg per day or less.
(80) TABLE-US-00019 TABLE 18 Standard of Care Dosing Schedule for IV methylprednisolone and daily oral prednisone: Patients Patients Time <45 kg (daily dosage) ≥45 kg (daily dosage) Days 1-3 0.5 g IV 1 g IV methylprednisolone methylprednisolone Days 3-112 1 mg/kg tapered down 1 mg/kg (maximum 80 mg) tapered down
(81) TABLE-US-00020 TABLE 19 Lowered Dosing Schedule for IV methylprednisolone and daily oral prednisone: Patients Patients Time <45 kg (daily dosage) ≥45 kg (daily dosage) Days 1-2 0.25 g IV 0.5 g IV methylprednisolone methylprednisolone Days 3-13 20 mg oral prednisone 25 mg oral prednisone Week 3 15 mg oral prednisone 20 mg oral prednisone Week 4 10 mg oral prednisone 15 mg oral prednisone Week 6 10 mg oral prednisone 10 mg oral prednisone Week 8 5 mg oral prednisone 5 mg oral prednisone Week 12 5 mg oral prednisone 5 mg oral prednisone Week 16 2.5 mg oral prednisone 2.5 mg oral prednisone