NZ615539B2 - Treatment of hepatitis c virus infection with alisporivir - Google Patents
Treatment of hepatitis c virus infection with alisporivir Download PDFInfo
- Publication number
- NZ615539B2 NZ615539B2 NZ615539A NZ61553912A NZ615539B2 NZ 615539 B2 NZ615539 B2 NZ 615539B2 NZ 615539 A NZ615539 A NZ 615539A NZ 61553912 A NZ61553912 A NZ 61553912A NZ 615539 B2 NZ615539 B2 NZ 615539B2
- Authority
- NZ
- New Zealand
- Prior art keywords
- alisporivir
- treatment
- weeks
- amount
- per day
- Prior art date
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- 238000011277 treatment modality Methods 0.000 description 1
- 229960005486 vaccine Drugs 0.000 description 1
- HPAPGONEMPZXMM-CMWVUSIZSA-N vaniprevir Chemical compound O=C([C@H]1C[C@@H]2OC(=O)N3CC=4C=CC=C(C=4C3)CCCCC(C)(C)COC(=O)N[C@@H](C(N1C2)=O)C(C)(C)C)N[C@]1(C(=O)NS(=O)(=O)C2CC2)C[C@H]1C=C HPAPGONEMPZXMM-CMWVUSIZSA-N 0.000 description 1
- 229950000843 vaniprevir Drugs 0.000 description 1
- 229920002554 vinyl polymer Polymers 0.000 description 1
- 230000029812 viral genome replication Effects 0.000 description 1
- XLYOFNOQVPJJNP-UHFFFAOYSA-N water Substances O XLYOFNOQVPJJNP-UHFFFAOYSA-N 0.000 description 1
- 229920003169 water-soluble polymer Polymers 0.000 description 1
Classifications
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K31/00—Medicinal preparations containing organic active ingredients
- A61K31/70—Carbohydrates; Sugars; Derivatives thereof
- A61K31/7042—Compounds having saccharide radicals and heterocyclic rings
- A61K31/7052—Compounds having saccharide radicals and heterocyclic rings having nitrogen as a ring hetero atom, e.g. nucleosides, nucleotides
- A61K31/7056—Compounds having saccharide radicals and heterocyclic rings having nitrogen as a ring hetero atom, e.g. nucleosides, nucleotides containing five-membered rings with nitrogen as a ring hetero atom
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K38/00—Medicinal preparations containing peptides
- A61K38/04—Peptides having up to 20 amino acids in a fully defined sequence; Derivatives thereof
- A61K38/12—Cyclic peptides, e.g. bacitracins; Polymyxins; Gramicidins S, C; Tyrocidins A, B or C
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K38/00—Medicinal preparations containing peptides
- A61K38/04—Peptides having up to 20 amino acids in a fully defined sequence; Derivatives thereof
- A61K38/12—Cyclic peptides, e.g. bacitracins; Polymyxins; Gramicidins S, C; Tyrocidins A, B or C
- A61K38/13—Cyclosporins
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K38/00—Medicinal preparations containing peptides
- A61K38/16—Peptides having more than 20 amino acids; Gastrins; Somatostatins; Melanotropins; Derivatives thereof
- A61K38/17—Peptides having more than 20 amino acids; Gastrins; Somatostatins; Melanotropins; Derivatives thereof from animals; from humans
- A61K38/19—Cytokines; Lymphokines; Interferons
- A61K38/21—Interferons [IFN]
- A61K38/212—IFN-alpha
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
- A61P1/00—Drugs for disorders of the alimentary tract or the digestive system
- A61P1/16—Drugs for disorders of the alimentary tract or the digestive system for liver or gallbladder disorders, e.g. hepatoprotective agents, cholagogues, litholytics
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
- A61P31/00—Antiinfectives, i.e. antibiotics, antiseptics, chemotherapeutics
- A61P31/12—Antivirals
- A61P31/14—Antivirals for RNA viruses
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
- A61P43/00—Drugs for specific purposes, not provided for in groups A61P1/00-A61P41/00
Abstract
Disclosed is the use of alisporivir in the manufacture of a medicament for the treatment of a Hepatitis C virus genotype 1 infected patient, wherein the medicament is adapted for administration in combination with standard of care; wherein the patient is a relapser; wherein the medicament is adapted for administration of alisporivir during an initial phase in an amount of about 600 mg twice per day, followed by a second phase in an amount of about 600 to about 1000 mg once per day; and wherein the standard of care is a combination of interferon with ribavirin. for administration of alisporivir during an initial phase in an amount of about 600 mg twice per day, followed by a second phase in an amount of about 600 to about 1000 mg once per day; and wherein the standard of care is a combination of interferon with ribavirin.
Description
W0 2012/140082
ENT OF TIS C VIRUS ION WITH ALISPORIVIR
The present disclosure relates to a non-immunosuppressive cyclosporin which binds to
cyclophilin, which are cyclophilin inhibitors, in particular to their pharmaceutical use of
in the treatment of Hepatitis C virus infection.
The cyclosporins comprise a class of structurally distinctive, cyclic, poly—N—methylated
undecapeptides, commonly possessing pharmacological, in particular
immunosuppressive, or anti-inflammatory activity. The first of the cyclosporins to be
isolated was the naturally occurring fungal metabolite Ciclosporin or Cyclosporine, also
known as cyclosporin A (CsA).
Cyclosporins which bind strongly to cyclophilin but are not immunosuppressive have
been fied. PCT/EP 2004/009804, , or disclose
non-immunosuppressive cyclosporins which bind to cyclophilin have also been found to
have an inhibitory effect on Hepatitis C virus (HCV). , incorporated
herein by reference in its entirety, describes methods and compositions for the use of
alisporivir in the treatment of HCV. Alisporivir (DEBOZS or Debio-025) is a cyclophilin
(Cyp) inhibitor and its mode of action as an CV agent is via inhibition of host
proteins, in particular of cyclophilin A, that are directly involved in HCV replication.
tis C virus (HCV) is an enveloped single stranded (+) RNA virus that belongs to
the separate genus Hepacivz’rus of the family Flavivz'rz'dae. HCV causes acute and chronic
liver disease, ing chronic hepatitis, cirrhosis, and hepatocellular carcinoma.
Worldwide more than 170 million people are chronically infected with HCV and are thus
at sed risk of developing serious life~threatening liver disease.
The current standard of care in HCV ts consists of a combination of interferon and
ribavirin. Treatment on and ribavirin dose depend on the genotype treated.
Sustained viral response (SVR) in ts with genotypes 2 and 3 after standard of care
treatment reaches 80-90%, but only 40-50% in patients with genotype 1. rmore,
side effects are cant and include myalgia, arthralgia, headache, fever, severe
depression, leucopenia and haemolytic anaemia.
As a result, there is currently a large proportion of chronic HCV infected ts that
have failed previous treatment and that are in high need for new treatment modalities that
would allow them to e SVR and halt the further evolution of their chronic liver
disease. Persistent infection by HCV, which has been identified as the major causative
agent of non-A, non-B hepatitis has been considered closely d to liver diseases such
as chronic hepatitis, liver cirrhosis or hepatocellular carcinoma. The development of these
liver diseases is a major public health problem.
Despite the ve indications in the art of the use of CsA and non-immunosuppressive
cyclosporins in treatment of HCV, there is a significant class of HCV patients that
remains refractory to the current standard of care therapies. Non-responders to standard
of care treatment represent an important medical challenge. For these patients, no
ative antiviral regimen is available and a substantial percentage of them will
p progressive disease with cirrhosis and end stage liver e, sometimes
complicated by hepatocellular carcinoma resulting in orthotopic liver transplantation.
Thus, despite existing therapies, there remains a significant need for methods and
itions for the treatment of HCV.
Failure to achieve a can also be a consequence of relapse. Relapse is defined as
reappearance of HCV RNA during the post—treatment follow—up after having achieved
undetectable HCV RNA at end of treatment. Relapse is a significant clinical problem,
especially for the genotype 1 c hepatitis C population. Therefore, there is a need to
provide therapy regimens which will improve efficacy for both, relapsers and non—
responders patients.
Surprisingly we have found out that cyclophilin tors, in particular alisporivir, can be
used effectively in the ent of HCV. In particular, we have found that satisfactory
treatment s of Hepatitis C virus genotype 1 infection in relapser or non—responder
patients to standard of care can be obtained when using alisporivir.
Accordingly, the present invention provides new anti-HCV treatments using alisporivir,
in particular methods of treating hepatitis C virus genotype 1 infection in a er or
non-responder patient comprising stering to the patient alisporivir, during an initial
phase in an amount of about 600 mg twice a day; followed by stering alisporivir
during a second phase in an amount of about 600 to about 1000 mg once per day.
(followed by page 2a)
In a particular aspect, the present invention provides the use of rivir in the
manufacture of a medicament for the treatment of a Hepatitis C Virus genotype 1 infected
patient, wherein the medicament is d for administration in combination with
standard of care wherein
(i) the t is a relapser, and
(ii) the medicament is adapted for administration of alisporivir during an initial phase in
an amount of about 600 mg, twice per day; followed by a second phase in an amount of
about 600 to about 1000 mg once per day, and wherein the standard of care is a
combination of interferon with ribavirin.
1O [FOLLOWED BY PAGE 3]
W0 2012/140082
The ion further provides alisporivir for use in the treatment or prevention of
Hepatitis C virus genotype 1 infections or HCV induced ers in a relapser or a nonresponder
patient.
SUMMARY OF THE DISCLOSURE
Further, the following is described:
1.1 A method for preventing or treating Hepatitis C ions or HCV induced
disorders in a relapser or a non-responder patient, comprising administering to said
patient rivir during an initial phase in an amount of about 600 mg twice a day;
followed by stering rivir during a second phase in an amount of about 600 to
about 800 mg once per day.
1.2 A method for inhibiting HCV replication in a relapser or a non-responder,
comprising administering alisporivir during an initial phase in an amount of 600 mg twice
a day; followed by administering alisporivir during a second phase in an amount of about
600 to about 800 mg once per day.
1.3. A method for preventing or treating Hepatitis C infections or HCV induced
disorders in a relapser or a non—responder patient, comprising administering to said
patient rivir in an amount of about 400 mg twice a day.
1.4. Any method as defined above, wherein the HCV infection is Hepatitis C
virus genotype 1 infection.
2. Use of alisporivir in the preparation of a ceutical composition for use
in any method as defined above.
3. Use of alisporivir in the preparation of a medicament for use in any method
as defined above.
4. A pharmaceutical composition for use in any method as defined above,
comprising alisporivir, together with one or more pharmaceutically acceptable diluents or
carriers therefor.
. A therapeutic regimen comprising administering alisporivir during an initial
phase in an amount of about 600 mg, twice per day followed by administering alisporivir
during a second phase in an amount of about 600 to about 800 mg per day and wherein
W0 2012/140082
rivir is administered in combination with standard of care hout the initial and
second phases.
6. A package comprising the pharmaceutical composition comprising
alisporivir as defined above, in combination with instructions to administer said
composition during an initial phase in an amount of about 600 mg twice a day; followed
by administering alisporivir during a second phase in an amount of about 600 to about
800 mg per day.
7. A kit for the treatment of chronic hepatitis C infection.
Also plated herein is a method of reducing the HCV RNA in a relapser or a non-
responder patient comprising administering to the patient: alisporivir, an interferon; and
ribavirin in which alisporivir is administered during an l phase in an amount of about
600 mg twice a day; followed by administering alisporivir during a second phase in an
amount of about 600 or about 800 mg once per day.
onal embodiments of the present invention relate to methods of treating hepatitis C
genotype 1 ions in a patient that is resistant to standard of care therapy for HCV
ent comprising administering to the patient: alisporivir in combination with
standard of care, wherein alisporivir is administered during an initial phase in an amount
of about 600 mg twice a day; followed by administering rivir during a second phase
in an amount of about 600 to about 800 mg once per day.
Also contemplated herein is a pharmaceutical combination comprising a first
pharmaceutically acceptable formulation comprising alisporivir, a second
phamiaceutically acceptable formulation comprising an interferon and a third
pharmaceutically acceptable formulation sing ribavirin, wherein the first, second
and third formulations are packaged in a kit for the treatment of chronic hepatitis C
~25 infection.
DETAILED DESCRIPTION OF THE DISCLOSURE
Figure 1 shows the HCV RNA (loglO IU/mL), by visits for all treatment arms, up 12
weeks tment.
In the above embodiments and throughout this specification, the standard of care
treatment is a treatment that is used to treat Hepatitis C infections. The currently used
W0 2012/140082
standard of care treatment involves administration of interferon, in particular pegylated
interferon in ation with ribavirin.
In the above embodiments and throughout this specification, the initial phase is
a period
of 3, 4, 5, 6, or 7 days. Preferably the l phase is a period of at least 3 days, preferred
of 7 days.
In the above embodiments and throughout this specification, the second phase is
a period
of 23, 47 or 71 weeks. Preferably the second phase is a period of 47 weeks.
In the present application, the term ser” is intended to
mean a t or subject who
relapse to rd of care treatment for HCV. More specifically, a relapser to standard of
care patient is a patient with undetectable HCV RNA < 10 IU/rnL levels at the end of
treatment which become detectable again during post-treatment follow
up, at any time
point after treatment end, in particular within 24 weeks of post-treatment follow-up after
previous undetectable HCV RNA at end of ent.
In the present application, the term “non~responder” is intended to mean a patient or
subject who is a non-responder to standard of care treatment for HCV. More specifically,
a non-responder to standard of care patient is a patient who has not responded to
treatment with standard of care given over a 12 weeks treatment period. The non-
responder to standard of care includes the following subsets of patients —— null responders
and partial ders.
Typically, a patient who has a “null response” may, for example, be defined as one in
whom the HCV~RNA reduction is observed to be less than 2 loglO IU/mL after 12 weeks
of ent with standard of care.
A patient that has a “partial” response or partial responder is
one in whom the A
reduction of more than 2 loglO IU/mL is observed after 12 weeks of treatment with
standard of care but the A is still detectable at the end of treatment.
In the present invention, an interferon may be pegylated or non-pegylated and may
include interferons such as: Intron-A®, interferon alfa-2b (Schering Corporation,
Kenilworth, NJ); PEG-lntron®, peginteferon alfa-Zb ing Corporation, Kenilworth,
NJ); n®, recombinant interferon alfa-2a (Hoffinann~La Roche, Nutley, NJ);
Pegasys®, peginterferon alfa—Za (Hoffmann—La Roche, Nutley, NJ); Berefor®, interferon
W0 2012/140082
alfa 2 available (Boehringer lngelheim Pharmaceutical, Inc, eld, CT);
Sumiferon®, a purified blend of l alpha interferons (Sumitomo, Japan);
ron®, blastoid interferon alpha n1 (GlaxoSmithKline); Infergen®,
CA and Amgen,
sus alpha interferon (InterMune Pharmaceuticals, Inc, Brisbane,
Inc, Newbury Park, CA); Alferon®, a mixture of natural alpha interferons (Interferon
Sciences, and Purdue Frederick Co., CT); Viraferon®; and combinations of these
interferons.
Conjugated interferons that may be used include, for example, Albuferon (Human
Genome Science) which is conjugated to human albumin. Interferon conjugated to a
water—soluble polymer or polyalkylene oxide homopolymers such as polyethylene glycol
(PEG) or polypropylene glycols, polyoxyethylenated polyols, copolymers thereof and
block copolymers f. As an alternative to polyalkylene oxide-based polymers,
effectively non-antigenic materials such as dextran, polyvinyl idones,
polyacrylamides, polyvinyl alcohols, carbohydrate-based rs and the like can be
used. Interferon—polymer conjugates are described in US 4766106, US 4917888, EPA 0
236 987, EPA O 510 356 and WO 95/13090. Since the polymeric modification
sufficiently reduces antigenic responses, the foreign interferon need not be completely
autologous. Interferon used to prepare polymer conjugates may be prepared from a
mammalian extract, such as human, ruminant or bovine interferon, or recombinantly
produced. Other forms of interferons include eron beta, gamma, tau and omega,
such as Rebif ( Interferon beta la) by Serono, Omniferon al interferon) by Viragen,
or Omega Interferon by Boehringer Ingelheim. Oral interferons such as oral interferon
alpha by Amarillo Biosciences.
Additional examples of interferons that may be used include pegylated interferon alpha,
for e pegylated interferon u-Za, pegylated interferon u-Zb, pegylated consensus
eron or pegylated purified interferon~oc product. Pegylated interferon u~2a is
described in an Patent 593,868 (incorporated herein by reference in its entirety)
and commercially available e. g. under the trade name PEGASYS® (Hoffmann—La
Roche). ted interferon-a-Zb is described, eg. in an Patent 975,369
(incorporated herein by reference in its entirety) and commercially available e.g. under
the trade name PEG— INTRON A® (Schering Plough). Pegylated consensus interferon is
described in WO 96/11953 (incorporated herein by reference in its entirety).
W0 40082
In preferred embodiments, the interferon used in the methods of the invention is
pegylated interferon. In other embodiments, the interferon is selected from the group
consisting of interferon alpha-2a, Interferon alpha-2b, a consensus interferon, a purified
interferon alpha product or a pegylated interferon alpha-2a, pegylated interferon alpha-2b,
and pegylated consensus interferon, a mixture of natural alpha and combinations thereof.
Preferably the methods using interferon alpha use a pegylated interferon alpha-2b and the
amount of ted interferon 2b is from 0,5 to 2.0 micrograms/kilogram per week
on a weekly, three times a week, every other day or daily basis.
As used herein, "microgram/kilogram" means micrograrn drug per kilogram body weight
1O ofthe mammal - including man - to be treated.
As used herein, the term “treatment” or “treat” refer to both prophylactic or preventative
treatment as well as curative or disease modifying treatment, including treatment of
patient at risk of contracting the disease or suspected to have contracted the disease as
well as patients who are ill or have been diagnosed as suffering from a disease or l
ion, and includes suppression of clinical relapse. The treatment may be
administered to a subject having a medical disorder or who ultimately may acquire the
disorder, in order to prevent, cure, delay the onset of, reduce the severity of, or ameliorate
one or more symptoms of a disorder or recurring disorder, or in order to prolong the
survival of a subject beyond that expected in the absence of such treatment.
By “therapeutic regimen” is meant the pattern of treatment of an illness, e.g., the pattern
of dosing used during HCV ey. A therapeutic regimen may e an induction
regimen and a nance regimen.
The phrase “induction regimen" or “induction period” refers to a therapeutic n (or
the portion of a therapeutic regimen) that is used for the initial treatment of a disease. The
general goal of an induction regimen is to provide a high level of drug to a patient during
the l period of a treatment regimen. An induction regimen may employ (in part or in
whole) a ng regimen”, which may include stering a greater dose of the drug
than a physician would employ during a nance n, administering a drug more
frequently than a physician would ster the drug during a maintenance regimen, or
both.
W0 2012/140082
The phrase “maintenance regimen” or “maintenance period” refers to a therapeutic
regimen (or the portion of a therapeutic regimen) that is used for the maintenance of a
patient during treatment of an illness, e.g., to keep the t in remission for long
periods of time s or years). A maintenance n may employ continuous
therapy (e.g., administering a drug at a regular intervals, e.g., weekIy, monthly, yearly,
etc.) or intermittent y (e.g., interrupted treatment, intermittent treatment, treatment
at relapse, or treatment upon achievement of a particular predetermined criteria [e.g.,
pain, e manifestation, etc.]).
As used herein, the term “about”, unless the context es otherwise, is used to mean a
'10 range of+ or — 10%.
In other embodiments, the interferon alpha is a pegylated interferon alpha-2a and the
amount of pegylated interferon alpha-2a administered is from 20 to 250
micrograms/kilogram per week on a weekly, three times a week, every other day or daily
basis. Preferably, the interferon peg-IFNa2a is administered at an amount of 180
micrograms once per week.
In specific ments, the ary interferon used in the methods herein is
interferon selected from the group consisting of Intron~A®; PEG-lntron®; Roferon®;
Pegasys®; Berefor®; ron®; Wellferon®; Infergen®; Alferon®; Viraferon®;
Albuferon® (Human Genome Science); Rebif; Omniferon; Omega and combinations
2O thereof.
In some embodiments, the patient may be administered ribavirin or a ribavirin derivative
(e.g., a ribavirin analog or prodrug, such as ribamidine, taribavirin (viramidine), ICN
17261, les disclosed in WO/2008/052722, which is incorporated by reference in its
entirety, etc.)
In some embodiments, ribavirin is administered at between about 800 mg to about 1200
mg per day, e.g., 800 mg, 900 mg, 1000 mg, 1100 mg, 1200 mg per day. In some
embodiments, rin is administered based on the weight of the patient.
In another embodiment, alisporivir may be administered with additional agents of the
standard of care that promote the antiviral efficacy of the therapy treatment. The standard
of care may include additional agents that promote the antiviral efficacy of the therapy
W0 2012/140082
treatment, such as substrate-based protease tors of HCV NS3-4A serine protease,
non-substrate-based NS3 protease inhibitors; phenanthrenequinones, thiazolidines and
benzanilides, nucleosides analogs, antisense molecules directed against HCV genome or
any cellular component that is ed for viral replication, vaccine or antibody-based
ches to HCV treatment. Direct acting antiviral agents, is used herein to mean
agents that interfere with specific steps in the hepatitis C virus (HCV) replication cycle.
Such agents may be, e.g., ribavirin derivatives, se inhibitors, polymerase inhibitors
(e.g., nucleoside and non~nucleoside inhibitors), and cyclophiilin inhibitors. Exemplary
antiviral include: boceprevir, telaprevir, ART-072, ABT—450, ABT—333 by ,
ACH1625 by Achillion, ANA598 by Anadys Pharmaceuticals, AZD-7295 by
AstraZeneca, BI20l335, B1207127 by nger Ingelheim Pharma, BMS650032,
BMS790052, BMS791325, BMSSZ4383 by Bristol Myers Squibb, Clemizole by Eiger
BioPharmacetucials, Filibuvir by Pfizer, GS9190 (Tegobuvir), GS9256 by ,
IDX375 by , INX—189 by Inhibitex, PSI-7851, PSI—938 by Pharmasset, PSI-7977,
RG7128 by Pharmasset/Genethec, 1 by Presidio RG7227 (Danoprevir) by
InterMune/Genentech, SCH900518 (Narlaprevir), Vaniprevir by Merck, TMC435 by
Medivir/Tibotec, VX-222, VX-759, , VX-916 by Vertex.
In some embodiments, alisporivir may be administered once per day (daily), twice per
day, three times per day, every other day, every three days, Weekly (once per week), once
every other week, once every three weeks, once monthly, etc.
In one embodiment, the present invention r provides alisporivir for use in
combination with standard of care in treatment of a Hepatitis C Virus infected patient, the
alisporivir to be administered in an amount of about 400 to about 600 mg (e.g., about 350
about 600 mg, about 650
mg, about 400 mg, about 450 mg, about 500 mg, about 550 mg,
mg) twice per day.
As used herein “twice per day” means twice in any period of about 24 hour period.
As used herein “once per week” is used to mean once in any period of about seven days.
In still another aspect, alisporivir is to be administered for up to 24, 48 or 72 weeks. As
used herein “up to 24, 48 or 72 weeks” is used to mean that rivir is administered on
about 48
a continuous basis (e.g., twice per day, once per week, etc.) for about 24 weeks,
weeks, or about 72 weeks. It will be understood that therapy need not end at exactly the
24, 48 or 72 week time period. For example, therapy may end a day or a few days before
the 24 week period, and still be an equivalent Within the scope and range of the current
disclosure.
In one embodiment, the present invention further es alisporivir for use in
combination with standard of care in treatment of a Hepatitis C virus genotype 1 infected
relapser or a non-responder patient, the rivir being administered during an l
phase in an amount of about 600 mg, twice per day; ed by administering alisporivir
during a second phase in an amount of about 600 to about 800 mg once per day. In still
another aspect, the initial phase is a period of 7 days; the second phase is a period of 23,
1O 47 or 71 weeks.
In one embodiment, the present invention further provides alisporivir for use in
combination with an interferon (e.g., pegylated interferon alpha 2a or pegylated interferon
alpha 2b) and ribavirin in treatment of a Hepatitis C virus genotype 1 infected relapser or
non—responder patient, the alisporivir being administered during an initial phase in an
amount of about 600 mg, twice per day for 7 days; followed by administering alisporivir
during a second phase in an amount of about 600 or about 800 mg once per day for up to
23, 47 or 71 weeks.
In one embodiment, the present invention further provides alisporivir for use in
combination with interferon and ribavirin in treatment of a Hepatits C virus genotype l
infected relapser or sponder t, the alisporivir being administered during an
initial phase in an amount of about 600 mg, twice per day for 7 days; ed by
administering alisporivir during a second phase in an amount of 600 mg once per day for
up to 71 weeks, preferably up to 23 weeks, most red up to 47 weeks.
In one embodiment, the present invention further provides alisporivir for use in
combination with interferon and ribavirin in treatment of a Hepatitis C virus genotype 1
infected relapser or non-responder patient, the alisporivir being stered during an
l phase in an amount of about 600 mg, twice per day for 7 days; followed by
administering alisporivir during a second phase in an amount of 800 mg once per day for
up to 47 weeks.
In one embodiment, the t invention further provides alisporivir for use in
combination with standard of care, preferably with pegylated interferon alpha—2a and
W0 2012/140082
ribavirin in treatment of a Hepatitis C virus genotype 1 infected relapser or non-responder
patient, the alisporivir being administered in an amount of about 400 mg, for up to 24, 48
or 72 weeks.
In one embodiment, the present invention further provides alisporivir for use in
combination with standard of care, preferably with pegylated interferon 2a and
rin in treatment of a Hepatitis C Virus genotype 1 infected relapser or non-responder
patient, the alisporivir being is administered during an initial phase in an amount of about
600 mg, twice per day; followed by stering alisporivir during a second phase in an
amount of about 600 to about 800 mg once per day for up to 23 or 47 or 71 weeks. In still
1O another aspect, the ted interferon alpha-2a and is administeredin an amount of 180
rams once per week.
In one embodiment, the present invention further es alisporivir for use in
combination with pegylated interferon alpha—2a and ribavirin in ent of a Hepatitis C
virus genotype 1 ed relapser or non—responder patient, the alisporivir being
administered during an initial phase in an amount of about 600 mg, twice per day;
followed by administering alisporivir during a second phase in an amount of about 600 to
about 800 mg once per day for up to 23, 47 or 71 weeks. In still another aspect, the
ribavirin is administered at between 1000 mg to 1200 mg per day and the pegylated
interferon alpha-2a is administered in an amount of 180 micrograms once per week.
In one aspect, the present invention further es a method of treating of a Hepatitis C
Virus genotype 1 ed relapser or non—responder patient with alisporivir in
combination with standard of care, preferably with interferon and ribavirin, the method
comprising administering alisporivir during an initial phase in an amount of about 600
mg, twice per day; ed by administering alisporivir during a second phase in an
amount of about 600 to about 800 mg once per day for up to 23, 47 or 71 weeks. In still
other aspects, the l phase is a period of at least 3 days, ably of 5 days, most
preferred of 7 days.
In one aspect, the present invention further provides use of alisporivir in the manufacture
of a medicament for treatment of a Hepatitis C virus genotype 1 infected relapser or non-
responder patient wherein alisporivir is administered during an initial phase in an amount
of about 600 mg, twice per day; followed by administering alisporivir during a second
W0 2012/140082
phase in an amount of about 600 to about 800 mg once per day for up 23, 47 or 71 weeks
and n alisporivir is administered in combination with interferon and ribavirin
hout the l and second phases. In still other aspects, the initial phase a period of
at least 3 days, preferably of 5 days, most preferred of 7 days.
In one aspect, the present invention further provides use of rivir in the preparation
of a pharmaceutical composition for treatment of a Hepatitis C Virus genotype 1 infected
relapser or non—responder patient characterized in that alisporivir is administered during
an initial phase in an amount of about 600 mg, twice per day; followed by stering
alisporivir during a second phase in an amount of about 600 to about 800 mg once per day
1O for up to 23, 47 or 71 weeks and wherein alisporivir is administered in combination with
interferon and ribavirin throughout the l and second phases. In still another aspects,
the l phase is a period of at least 3 days, preferably of 5 days, most preferred of 7
days.
In one aspect, the present invention further provides a combination of alisporivir with
standard of care, preferably with interferon and ribavirin for use in ent of a
Hepatitis C virus genotype 1 infected relapser or non-responder patient, wherein
alisporivir is administered during an initial phase in an amount of about 600 mg, twice per
day for 7 days; followed by administering alisporivir during a second phase in an amount
of about 600 to about 800 mg once per day for up to 23, 47 or 71 weeks.
In one , the present invention further provides a therapeutic regimen comprising
administering alisporivir during an initial phasein an amount of about 600 mg, twice per
day for one week; followed by stering alisporivir during a second phase in an
amount of about 600 to about 800 mg once per day for up to 23, 47 or 71 weeks and
wherein alisporivir is administered in combination with interferon and ribavirin
throughout the initial and second phases.
In one aspect, the present invention further provides pharmaceutical compositions
comprising alisporivir for uses as defined above. In still other aspects, the present
invention provides a package comprising the pharmaceutical ition comprising
alisporivir for uses as defined above in combination with instructions to ster said
composition.
W0 2012/140082
In exemplary ments, alisporivir is stered at a dosage of from about 600 to
about 1000 mg twice daily for 7 days followed by administering alisporivir at a dosage of
from about 600 to about 1000 mg once per day for up to 23, 47 or 71 weeks.
In exemplary embodiments, the treatment of the present invention involves administration
of interferon alpha that is a pegylated interferon alpha—2a and the amount of pegylated
interferon alpha-2a administered is from 20 to 250 micrograms per week on a weekly,
three times a week, every other day or daily basis. The current approved dose is 180
micrograms per week. In other exemplary embodiments, the interferon alpha is a
ted interferon 2b and the amount of pegylated interferon alpha-2b is from 0.5
to 2.0 micrograms/kilogram per week on a weekly, three times a week, every other day or
daily basis. Exemplary descriptions of such treatments are described in US. Patent No.
7,1 15,578, incorporated herein by reference in its entirety.
An exemplary NaZa used in the treatment protocols described herein is Pegasys®.
PEGASYS® is a pegylated form of IFNor2a (peg—IFNorZa) and utilizes a 40 kDa branched
PEG (polyethylene ) to provide sustained serum concentrations for a full week (168
hours). PEGASYS® is commercially available, presented as single use, pie-filled
syringes containing 180 rig/0.5 mL peg—IFNaZa for SC. injection. The standard package
contains 1 syringe of 180ug/0.5 mL.
In some embodiments, it may be desirable to modify the dose of NuZa. If dose
modification is required for moderate to severe adverse reactions (clinical and/or
laboratory), initial dose reduction from 180 to 135 ug is generally adequate (adjustment to
the corresponding graduation mark on pre—filled syringe). r, in some cases, dose
reduction to 90 pg may be needed. Following improvement, re~escalation of the dose may
be considered.
In treatment described above effective dosages of the rd of care agents are
stered in itions, i.e. they may be administered together (i.e.,
simultaneously), but may also be administered separately or sequentially. In general,
combination therapy is typically administered together, the rationale being that such
simultaneous administration induces multiple aneous stresses on the virus. The
, specific dosages given will depend on tion, inactivation and excretion rate of the
drugs as well as other factors. It is to be noted that dosage values will also vary with the
severity of the condition to be alleviated.
The terms "co-administration" or "combined administration" or “administered in
combination with” or the like as utilized herein are meant to encompass administration of
the selected therapeutic agents to a single patient, and are intended to include treatment
regimens in which the agents are not necessarily administered by the same route of
administration or at the same time. Fixed combinations are also within the scope of the
present invention. The administration of a pharmaceutical combination of the invention
results in a beneficial , e.g. a synergistic or additive eutic effect, compared to
a monotherapy applying only one of its pharmaceutically active ingredients or as
ed to the current standard of care therapy. The treatment used in the methods
described herein may be administered by any conventional route. One or more
components may be stered parentally, e.g., in the form of injectable solutions or
suspensions, or in the form of injectable t formulations. Preferably, alisporivir will
. be administered orally in the form of solutions or suspensions for drinking, tablets or
capsules. Pharmaceutical compositions for oral administration comprising alisporivir
typically r comprise one or more pharmaceutically acceptable carrier nces.
Typically, these compositions are concentrated and need to be ed with an
riate t, e.g., water, prior to stration. Pharmaceutical compositions for
parenteral administration typically also include one or more ents. Optional
excipients include an isotonic agent, a buffer or other pH— controlling agent, and a
preservative. These excipients may be added for nance of the composition and for
the attainment of preferred ranges of pH (about 6.5—7.5) and osmolarity (about 300
mosm/L).
The efficacy of the therapy regimen may be monitored using standard protocols.
Treatment may be followed by determinations of HCV in serum and ement of
serum ALT levels. For example, the patients may be assessed for the presence of HCV
RNA in their plasma. HCV RNA (IU/mL) can be measured at regular intervals during
the treatment, e.g., at Day 1 (pre-dose and 4, 8, and 12 hours post-dose) and pre-dose at
Day 2, Day 3, Day 8, Day 15, Day 29, and at Week 12, Week 24, Week 36, Week 48,
Week 72 (when applicable), and at follow up. In addition, the HCV strains in the patient
can be sequenced and assessed for identification of mutations selecting for resistance.
W0 2012/140082
The endpoint of treatment is a virological response, i.e., the e ofHCV at the end of
a treatment course, several months after initiation of treatment, or l months after
completion of treatment. HCV in serum may be measured at the RNA level by methods
such as quantitative RT-PCR or northern blots or at the protein level by enzyme
immunoassay or enhanced chemiluminescence immunoassay of viral proteins. The
endpoint may also include a determination ofa serum ALT level in the normal range.
Exemplary treatment ns are given in the es. 111 one exemplary regimen a
subject in need of treatment is provided with pegylated interferon alfa 2a at a dose of 180
pg subcutaneously (S.C.) once weekly for 48 weeks in combination with ribavirin
1O administered in an oral dosage of 1000/1200 mg daily (weight based) for 48 weeks and
600 mg alisporivir orally twice daily for 7 days, followed by 600 to 800 mg alisporivir
orally once daily for 47 weeks.
In another exemplary ol a subject in need of treatment is provided with pegylated
interferon alfa 2a at a dose of 180 pg subcutaneously (S.C.) once weekly for 48 weeks in
combination with ribavirin administered in an oral dosage of 1000/1200 mg daily (weight
based) for 48 weeks and 600 mg orivir orally twice daily for 7 days, followed by
800 mg alisporivir orally once daily for 47 weeks.
After a 4 week ent period, based on t response, the administration of
alisporivir may be continued up to 48 or 72 weeks from the start of treatment at 600 or
800 mg per day orally or preferably the dose of alisporivir is reduced to a lesser amount in
a daily dose (e.g., 400 or 600 mg) or more preferably, the administration of alisporivir is
discontinued. The treatment with pegylated interferon alfa 2a and ribavirin is preferably
continued for up to 48 or 72 weeks from the initiation of treatment. For example between
weeks 5 to 48 or 72, the patient is stered 180 ug pegylated interferon alfa 2a S.C.
orally once weekly and ribavirin administered in an oral dosage of 1000/1200 mg daily
(weight based).
The following Examples illustrate the invention described hereinbefore.
EXAMPLES
1. Compounds
Na2a is a pegylated form of interferon alfa 2a and utilizes 40 kDa branched PEG
(polyethylene ) to provide sustained serum trations for a full week (168
hours). PEGASYS® is commercially available from Roche.
Ribavirin is a synthetic nucleoside analogue and is also commercially available, e.g., as
COPEGUS® from Roche.
2. Clinical Study and Results
This is an international, entre, randomized, -blind, placebo-controlled, 4—
arm, parallel’group phase II study ing therapy with three doses of DEB025 (600
mg OD, 800 mg OD and 400 mg BID) plus SOC (peg-IFNuZa once weekly plus RBV
BID) versus triple therapy with placebo matching DEBOZS plus SOC in chronic HCV
GT1 patients who were non—responders to prior SOC treatment, or who have relapsed
after SOC treatment.
Approximately 344 patients will be randomized into one of 4 treatment arms (A, B, C
(Cl/C2) and D) in a l:l:l:l ratio. Cl and C2 patients will be randomized in a 1:1 ratio
within arm C.
The randomization will be stratified by response status to us treatment (non—
responders/relapsers), BMI (< 25 kg/m2 or Z 25 kg/m2) and IL28B rphism (CC or
CT/'IT) at screening.
The ratio non-responders and relapsers should be kept at 50% (172 patients) of the study
population.An international, multicentre, randomized, double—blind, placeboecontrolled,
4-arm, parallel-group phase II study comparing triple therapy with three doses of
alisporivir (400 mg, 600 mg or 800 mg) + standard of care (SOC) versus triple therapy
with placebo matching alisporivir plus SOC in 258 chronic HCV GT1 patients who were
non-responders to prior SOC treatment, or relapsers after SOC treatment is provided.
Patients are randomized into one of 4 treatment arms as described below in a l
ratio. The randomization will be stratified by response status to previous treatment (non—
responders/relapsers), BMI (< 25 kg/m2 or _>_ 25 kg/mZ) and IL28B polymorphism (CC or
CT/TT) at screening. The ratio non-responders and relapsers should be kept at 50% (172
patients) of the study population.
W0 2012/140082
Treatment A
Alisporivir/Placebo 3 capsules of 200 mg (600 mg) alisporivir 2x/day (BID) orally for l
week (loading dose) followed by 3 capsules of 200 mg (600 mg)
alisporivir once per day (QD) plus 1 capsule of placebo QD for 47
weeks. Only in week 17 (dummy loading) patients receive 3
capsules of 200 mg (600 mg) alisporivir in the morning and 3
es of placebo in the g.
Peg— a 180 ug subcutaneously (5.0.) once weekly for 48 weeks
Ribavirin 1000 mg/day (<75 kg) or 1200 mg/day (_>_75 kg) orally in two
divided doses for 48 weeks
Treatment B
alisporivir/Placebo 3 capsules of 200 mg (600 mg) alisporivir 2x/day orally for 1 week
(loading dose) followed by 4 capsules alisporivir (800 mg) QD for
47 weeks. Only in week 17 (dummy loading) patients receive 3
capsules of 200 .mg (600 mg) rivir in the morning and 1
capsule of 200 mg alisporivir plus 2 capsules of placebo in the
evening.
Peg-IFNaZa 180 ug subcutaneously (s.c.) once weekly for 48 weeks
Ribavirin 1000 mg/day (<75 kg) or 1200 mg/day (275 kg) orally in two
divided doses for 48 weeks
Treatment C1 (will change to active treatment ifCBVR not reached == arm CIA)
Placebo 3 capsules of placebo BID orally for 1 week (loading dose)
followed by 4 capsules placebo QD for 47 weeks. Only in week 17
(dummy loading) ts receive 3 es of placebo in the
morning and 3 capsules of placebo in the evening
Peg-IFNaZa 180 ug so. once weekly for 48 weeks
Ribavirin 1000 mg/day (<75 kg) or 1200 mg/day (275 kg) orally in two
divided doses for 48 weeks
W0 2012/140082
Treatment C]A
Placebo alisporivir 3 capsules of placebo BID orally for 1 week (loading dose)
followed by 4 capsules placebo QD for 16 weeks. After week 16
switch to:
3 es of 200 mg (600 mg) alisporivir 2x/day orally for 1 week
ng dose) followed by 3 capsules of 200 mg (600 mg)
alispon'vir QD plus 1 capsule placebo QD for 47 weeks
Peg-IFNdZa 180 ug aneously (s.c.) once weekly for 16 weeks plus 48
weeks
Ribavirin 1000 mg/day (<75 kg) or 1200 mg/day (275 kg) orally in two
divided doses for 16 weeks plus 48 weeks
ent D
Placebo alisporivir 1 capsule of placebo QB (in the morning) orally for 48 weeks
2 capsules of 200 mg (400 mg) alisporivir 2x/day orally for 48
weeks
Peg~ IFNaZa
180 pg so. once weekly for 48 weeks
Ribavirin 1000 mg/day (<75 kg) or 1200 mg/day (275 kg) orally in two
divided doses for 48 weeks
Treatment C2 (will change to active treatment ifcEVR not reached = arm CZA)
DEBOZS placebo 3 capsules of placebo orally in the morning and 2 capsules of
placebo in the evening for 48 weeks.
Peg-IFNaZa 180 ug so. once weekly for 48 weeks
Ribavirin 1000 mg/day (<75 kg) or 1200 mg/day (275 kg) orally in two
divided doses for 48 weeks
Treatment CZA
Placebo 3 capsules of placebo orally as morning dose and 2 capsules of
placebo as evening dose for 16 weeks. After week 16 switch to:
alisporivir 2 capsules of 200 mg (400 mg) alisporivir BID orally plus 1 capsule
of o in the morning for 48 weeks
Peg—IFNaZa 180 pg subcutaneously (s.c.) once weekly for 16 weeks plus 48
weeks
rin 1000 mg/day (<75 kg) or 1200 mg/day (275 kg) orally in two
divided doses for 16 weeks plus 48 weeks
Primary efficacy endpoint: proportion of patients ing cEVR (complete early
virologic response) after 12 week triple therapy with DEB025 600 mg QD plus SOC
versus triple therapy with placebo matching DEB025 plus SOC.
461 patients have been randomized into one of 4 treatment arms (A, B, C ) and D)
in a 121:1:1 ratio. C1 and C2 patients have been randomized in a 1:1 ratio within
arm C.
Arm A corresponds to treatment A above (DEB 600 QD);
Arm B corresponds to ent B above (DEB 800 QD);
Arm C corresponds to treatment C above, is a control arm with peg-IFNaZa/RBV plus
o (Placebo+PR);
Arm D corresponds to treatment D above (DEB 400 BID).
The randomization was stratified by response status to previous treatment (non-
responders/relapsers), BMI (< 25 kg/m2 or 2 25 kg/m2) and 1L28B polymorphism (CC or
CT/TT) at screening.
In the fill] randomized study population 57% of the patients are sponder and 43%
relapser.
Out of the total 461 patients randomized in the study, we report the results of the first 337
randomized patients with up to week 12 on—treatrnent data.
Of all the 337 patients in randomized set, 38.9% was relapser while 55.2% was non-
responder.
W0 2012/140082
At Week 4, all the DEBO25 treatment arms had > 20% patients achieved RVR While
.3% of Placebo patients achieved RVR. At Week 12, all the DEB025
treatment arms had
2 79% patients achieved EVR While 62.7% of Placebo patients achieved RVR. Among
the 4 treatment arms, DEB 400 BID arm had the highest proportion in achieving
(37.2%), CBVR (70.5%) and EVR (80.8%) while the Placebo arm had the lowest
proportion in achieving RVR, cEVR and EVR.
Table 1 ts who achieved virologic
response by limit of quantitation (LOQ)
Arm A Arm B Arm C Arm D
DEB 600 GB DEB 800 OD o DEB 400 BID
N=81 N=84 N=75 N=78
Variable n (%) n (%) n (%) n M)
.. Ryafifz ; g 5/» 4912335):.:,=~:f_:2 _» r. 33:1,8g‘(2.1;4)1' *
pEVR 28 (34.6) 24 (28.6) 27 (36.0) 8 (10.3)
EVR 64 (79.0) 72 (85.7) 47 (62.7) 63 (80.8)
cEVRé(primary'endpoint)r‘ > .36 (44.4)} ~25} '1' >
.48‘:“(57,1.)é15j§ 3,;"1’ 203(26;7)';i11':§7i;T\A:3:Zf55;..(.l0}5)- 7’s '1
- RVR (rapid virologic response) is defined as HCV RNA < LOQ (25 IU/mL) after4 weeks of
1O treatment.
- pEVR al early virologic response) is defined as HCV RNA decrease >=2 [0910 from
baseline and > LOQ (25 lU/mL)
after 12 weeks of treatment.
- - EVR is defined as HCV RNA decrease >=2 log? 0 from baseline
or < LOQ (25 lU/mL) after 12 weeks of treatment.
- cEVR (complete early virologic response) is the y endpoint of the study, defined
as HCV RNA < LOQ (25
lU/mL) after 12 weeks of treatment.
Claims (6)
1. Use of alisporivir in the manufacture of a medicament for the treatment of a Hepatitis C Virus pe 1 infected t, wherein the medicament is adapted for administration in combination with rd of care wherein (i) the patient is a relapser, and (ii) the medicament is adapted for administration of alisporivir during an initial phase in an amount of about 600 mg, twice per day; followed by a second phase in an amount of about 600 to about 1000 mg once per day, and wherein the standard of care is a combination of interferon with ribavirin. 10
2. Use according to claim 1 n the medicament is adapted for administration of alisporivir during an initial phase in an amount of about 600 mg, twice per day for 7 days; followed by a second phase in an amount of about 600 or about 1000 mg or 800 mg once per day for up to 23, 47 or 71 weeks.
3. Use according to claim 2 wherein the medicament is adapted for 15 administration of alisporivir during an initial phase in an amount of about 600 mg, twice per day for 7 days; followed by a second phase in an amount of 600 mg once per day for up to 47 weeks.
4. Use according to claim 1, wherein said interferon is pegylated interferon alpha-2a, and is d for administration in an amount of 180 micrograms once per 20 week.
5. Use according to claim 1, wherein said ribavirin is adapted for administration at between 1000 mg to 1200 mg per day.
6. Use according to claim 1, substantially as herein described with reference to any one of the es and/or
Applications Claiming Priority (3)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| US201161474946P | 2011-04-13 | 2011-04-13 | |
| US61/474,946 | 2011-04-13 | ||
| PCT/EP2012/056577 WO2012140082A1 (en) | 2011-04-13 | 2012-04-11 | Treatment of hepatitis c virus infection with alisporivir |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| NZ615539A NZ615539A (en) | 2016-01-29 |
| NZ615539B2 true NZ615539B2 (en) | 2016-05-03 |
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