- Only systemic treatment for relapsed or refractory (r/r) CTCL
to target the IL-2 receptor on malignant T-cells and Tregs
- LYMPHIR is expected to launch within the next five months
- LYMPHIR's approval marks the first novel targeted systemic
therapy approved by the FDA r/r CTCL since 2018
- Approval based on Phase 3 Pivotal Study 302 results that
demonstrated 36% ORR, reduction in skin disease in 84% of patients,
clinically significant pruritis improvement, and no cumulative
toxicity
CRANFORD, N.J., Aug. 8, 2024
/PRNewswire/ -- Citius Pharmaceuticals, Inc. (NASDAQ: CTXR)
("Citius", "Citius Pharma"), announced today that the U.S. Food and
Drug Administration (FDA) has approved LYMPHIR™ (denileukin
diftitox-cxdl), a novel immunotherapy for the treatment of r/r
cutaneous T-cell lymphoma (CTCL) after at least one prior systemic
therapy. LYMPHIR is the only CTCL therapy that targets the
interleukin-2 (IL-2) receptor found on malignant T-cells and Tregs.
This is the first indication for LYMPHIR and the first FDA-approved
product for Citius Pharma.
"LYMPHIR offers new hope for patients suffering from cutaneous
T-cell lymphoma, a rare and chronic cancer characterized by
debilitating skin lesions and severe itching. This approval is a
significant milestone for CTCL patients. The introduction of
LYMPHIR, with its potential to rapidly reduce skin disease and
control symptomatic itching without cumulative toxicity, is
expected to expand the CTCL treatment landscape and grow the
overall market, currently estimated to be $300-$400 million,"
stated Leonard Mazur, Chief
Executive Officer of Citius Pharmaceuticals.
"LYMPHIR, with an initial indication in the treatment of CTCL,
is the first of our pipeline candidates to receive FDA approval.
Citius is dedicated to working closely with healthcare providers to
ensure that all r/r CTCL patients have timely access to this
important new therapy. We are preparing to launch LYMPHIR in the
U.S. market within the next five months," added Mazur.
"We are grateful to the clinicians, patients, and researchers
who contributed to the development of LYMPHIR. We believe LYMPHIR's
unique IL-2 receptor-targeted treatment, which kills tumor cells
directly, and concurrently depletes host Tregs in order to boost
the body's immune response, is an important differentiator and
offers clinically meaningful benefits to a significant percentage
of r/r patients. As the only IL-2 receptor-targeted immunotherapy
for CTCL, LYMPHIR provides a novel and non-cross-resistant
treatment option without cumulative toxicity for Stage I-III r/r
patients for whom symptomatic skin involvement interferes with
their daily quality of life. LYMPHIR's median time-to-response of
only 1.4 months (min, max: 0.7, 5.6) offers many patients rapid
skin relief," added Dr. Myron
Czuczman, Chief Medical Officer of Citius
Pharmaceuticals.
CTCL is a rare and often debilitating chronic non-Hodgkin
lymphoma that primarily affects the skin. Approximately 2,500-3,000
patients are diagnosed each year with an estimated 40,000 living
with the disease. Patients with r/r CTCL have limited treatment
options. No universally defined single treatment is used to treat
these patients with incurable cancer. Patients typically cycle
through several skin-directed therapies before the cancer becomes
resistant and/or progressive at which point systemic agents are
needed to achieve effective disease control. Reducing and
controlling skin plaques and itching without cumulative toxicity is
a primary goal of CTCL treatment. Systemic medicines are prescribed
until the disease progresses again or when dose-limiting toxicity
occurs, after which HCPs prescribe a different systemic medicine.
LYMPHIR provides another viable option in the treatment landscape
with unique benefits to patients. It offers a novel mechanism of
action designed to target and eradicate malignant T-cells while
preserving healthy tissue. It is the only treatment option that
targets the IL-2 receptors found in T-cell lymphomas and Tregs.
"As a treating oncologist, I have seen the
profound negative effect on the quality of life in patients with
r/r CTCL. Given the long-term nature of the disease, pruritus,
ulceration of the tumors, and secondary pyogenic skin infection, it
is vital to get this skin involvement under control. LYMPHIR is the
first therapeutic option in many years to offer hope of reducing
skin disease, bringing us one step closer to filling the need for
CTCL patients, particularly those that are not able to complete or
continue prior therapies," stated Dr. Francine Foss, Professor of Hematology and
Director of the Multidisciplinary T-cell Lymphoma Program at Yale
Cancer Center, New Haven, CT.
The approval of LYMPHIR is based on results from the Phase 3
Pivotal Study 302 (NCT01871727) of CTCL patients who had previously
received at least one systemic treatment. Actual study patients
received a median of 4 (min, max: 1, 18) prior anticancer
therapies. The primary efficacy population includes 69 patients
with stage I-III CTCL who were treated with denileukin
diftitox-cxdl (9 μg /kg/day). The primary efficacy outcome measure
was Objective Response Rate (ORR), as assessed by an Independent
Review Committee (IRC). The ORR was 36.2%, (95% CI: 25.0-48.7),
with 8.7% achieving a Complete Response (CR).
The median time to response was rapid at 1.41 months, with the
majority of responders (~70%) seeing results after 1–2 cycles of
treatment. Duration of response was at least 6 months for 52.0% of
the patients. 84.4% (54/64) of skin evaluable subjects had a
decrease in skin tumor burden and 12.5% (8/64) saw complete
clearing of skin disease. Pruritis was evaluated as an exploratory
endpoint with 31.7% of patients demonstrating clinically
significant pruritus improvement. Importantly, no cumulative
toxicity was observed in patients receiving LYMPHIR.
LYMPHIR's safety profile is consistent with the known safety
profile for denileukin diftitox. Across three studies of 119 CTCL
patients receiving 9 μg dose of denileukin diftitox, the most
common (≥20%) adverse reactions, including laboratory
abnormalities, were increased transaminases, albumin decreased,
nausea, edema, hemoglobin decreased, fatigue, musculoskeletal pain,
rash, chills, constipation, pyrexia, and capillary leak syndrome
(CLS).
The U.S. Prescribing Information for LYMPHIR contains a boxed
warning that CLS, including life-threatening or fatal reactions,
can occur in patients receiving LYMPHIR. Monitor patients for signs
and symptoms of CLS during treatment. Withhold LYMPHIR until CLS
resolves, or permanently discontinue based on severity. Additional
"Important Safety Information" is available below and LYMPHIR's
full prescribing information may be accessed here in the next few
days.
This approval includes a postmarketing requirement from the FDA
to characterize the risk of visual impairment in CTCL patients
treated with LYMPHIR. Citius is committed to the safety of
patients and will continue to monitor all safety data as it
emerges.
About Study 302
The efficacy of LYMPHIR was evaluated in Study 302, an
open-label, single-arm, multicenter trial in patients with r/r
Stage I to IV CTCL. Eligible patients were required to have
expression of CD25 on ≥ 20% of biopsied malignant cells by
immunohistochemistry. The study excluded patients with
significant cardiac disease or uncontrolled infections. Patients
received LYMPHIR at 9 mcg/kg as an intravenous infusion daily from
Day 1 through Day 5 of each 21-day cycle. Patients continued to
receive LYMPHIR until disease progression or unacceptable
toxicity.
The efficacy population includes 69 patients with r/r Stage I to
III CTCL. Of the 69 patients, the median age was 64 years
(range: 28 to 87 years), 65% were male, 73% were White, 19% Black
or African American, 1% Asian, and 14% Hispanic or Latino. The CTCL
disease stage was IA in 7%, IB in 23%, IIA in 13%, IIB in 35%, IIIA
in 12%, and IIIB in 10%. The median number of prior therapies was 4
(range: 1 to 18), including both skin-directed and systemic
therapies. Prior therapies included photodynamic therapy (56%),
total skin electron beam therapy (42%), systemic retinoids (49%),
methotrexate/pralatrexate (49%), histone deacetylase inhibitor
(35%), brentuximab vedotin (26%) and mogamulizumab (12%).
Efficacy was established based on ORR, according to ISCL/EORTC
Global Response Score (GRS) per Independent Review Committee (Olsen
2011). Efficacy results are shown in the table below.
Table: Efficacy
Results of Study 302
|
Efficacy
Endpoint
|
LYMPHIR
9
mcg/kg/day
(N=69)
|
ORR
(GRS)%a
(95%
CIb)
|
36%
(25,
49)
|
Complete
Response
|
9 %
|
Partial
Response
|
27 %
|
Duration of
Responsec
Range,
months
Duration ≥ 6 months, n
(%)
Duration ≥ 12 months,
n (%)
|
3.0+, 23.5+
13 (52%)
5 (20%)
|
a ORR,
objective response rate per Olsen, et al (2011) Global Response
Score (GRS), by
Independent Review Committee (IRC).
|
b CI,
confidence interval
|
c The median
(95% CI) DOR using Kaplan-Meier (KM) estimate was not estimable
(NE) among
the 25 subjects due to censoring.
|
Median time to response
was 1.4 months (range: 0.7 to 5.6 months).
|
Among responders, the
median follow-up for duration of response was 6.5 months (range:
3.5+,
23.5+ months).
|
About LYMPHIR™ (denileukin diftitox-cxdl)
LYMPHIR is a targeted immune therapy for r/r (R/R) CTCL
indicated for use in Stage I-III disease after at least one prior
systemic therapy. It is a recombinant fusion protein that combines
the IL-2 receptor binding domain with diphtheria toxin fragments.
The agent specifically binds to IL-2 receptors on the cell surface,
causing diphtheria toxin fragments that have entered cells to
inhibit protein synthesis. After uptake into the cell, the DT
fragment is cleaved and the free DT fragments inhibit protein
synthesis, resulting in cell death. Denileukin diftitox-cxdl
demonstrated the ability to deplete immunosuppressive regulatory T
lymphocytes (Tregs) and antitumor activity through a direct
cytocidal action on IL-2R-expressing tumors.
In 2021, denileukin diftitox received regulatory approval in
Japan for the treatment of CTCL
and PTCL. Subsequently, in 2021, Citius acquired an exclusive
license with rights to develop and commercialize LYMPHIR in all
markets except for Japan and
certain parts of Asia.
About Cutaneous T-cell Lymphoma
Cutaneous T-cell lymphoma is a type of cutaneous non-Hodgkin
lymphoma (NHL) that comes in a variety of forms and is the most
common type of cutaneous lymphoma. In CTCL, T-cells, a type of
lymphocyte that plays a role in the immune system, become cancerous
and develop into skin lesions, leading to a decrease in the quality
of life of patients with this disease due to severe pain and
pruritus. Mycosis Fungoides (MF) and Sézary Syndrome (SS) comprise
the majority of CTCL cases. Depending on the type of CTCL,
the disease may progress slowly and can take anywhere from several
years to upwards of ten to potentially reach tumor stage. However,
once the disease reaches this stage, the cancer is highly malignant
and can spread to the lymph nodes and internal organs, resulting in
a poor prognosis. Given the duration of the disease, patients
typically cycle through multiple agents to control disease
progression. CTCL affects men twice as often as women and is
typically first diagnosed in patients between the ages of 50 and 60
years of age. Other than allogeneic stem cell transplantation, for
which only a small fraction of patients qualify, there is currently
no curative therapy for advanced CTCL.
INDICATION
LYMPHIR is an IL2-receptor-directed cytotoxin indicated for the
treatment of adult patients with r/r Stage I-III cutaneous T-cell
lymphoma (CTCL) after at least one prior systemic therapy.
IMPORTANT SAFETY INFORMATION
BOXED WARNING: CAPILLARY LEAK SYNDROME
Capillary leak syndrome (CLS), including life-threatening or
fatal reactions, can occur in patients receiving LYMPHIR. Monitor
patients for signs and symptoms of CLS during treatment. Withhold
LYMPHIR until CLS resolves, or permanently discontinue based on
severity.
WARNINGS AND PRECAUTIONS
Capillary Leak Syndrome
LYMPHIR can cause capillary leak syndrome (CLS), including
life-threatening or fatal reactions. CLS was defined in the
clinical trials as the occurrence of at least 2 of the following
symptoms at any time during LYMPHIR therapy: hypotension, edema,
and serum albumin <3 g/dL. These symptoms were not required to
occur simultaneously to be characterized as capillary leak
syndrome.
As defined, CLS occurred in 27% of patients in the pooled
population across 3 clinical trials, including 8% with Grade 3.
There was one (0.8%) fatal occurrence of CLS. Of the patients with
CLS, 22% had recurrence. The majority of CLS events (81%) occurred
within the first 2 cycles of treatment. The median time to onset
from Cycle 1, Day 1 was 6.5 days (range: 1 to 77), the median
duration of CLS was 14 days (range: 2 to 40), and 75% of patients
had resolution. The most common symptoms included edema,
hypoalbuminemia, and hypotension. Pleural effusion, pericardial
effusion, and dehydration also occurred.
Regularly assess patients for weight gain, new onset or
worsening of edema, dyspnea, and hypotension (including orthostatic
changes). Monitor serum albumin levels prior to the initiation of
each cycle of therapy and more often as clinically indicated.
Withhold, reduce dose, or permanently discontinue based on
severity. If LYMPHIR is withheld, resume LYMPHIR following
resolution of CLS and when serum albumin is greater than or equal
to 3 g/dL.
Visual Impairment
LYMPHIR can cause serious visual impairment, including changes
in visual acuity and color vision. In the pooled population across
3 clinical trials, visual impairment occurred in 9%, with Grade 1
in 8% and Grade 2 in 1%. The most commonly reported symptom was
blurred vision. Of the patients with visual impairment, 67% had
resolution of their visual impairment.
Perform baseline ophthalmic examination and monitor as
clinically indicated. If patients experience symptoms of visual
impairment, such as changes in visual acuity, changes in color
vision, or blurred vision, refer for ophthalmologic evaluation.
Withhold LYMPHIR until visual impairment resolves or permanently
discontinue based on severity.
Infusion-Related Reactions
LYMPHIR can cause serious infusion-related reactions.
Infusion-related reactions were reported in 69% of patients in the
pooled population across 3 clinical trials of patients who received
LYMPHIR, with Grade 3 infusion-related reactions in 3.4% [see
Adverse Reactions (6.1)]. Eighty-three percent of infusion-related
reactions occurred in Cycles 1 and 2. The most common symptoms
included nausea, fatigue, chills, musculoskeletal pain, vomiting,
fever, and arthralgia.
Premedicate patients for the first three cycles prior to
starting a LYMPHIR infusion [see Dosage and Administration (2.3)].
Monitor patients frequently during infusion. For Grade 2 or higher
infusion reactions, premedicate at least 30 minutes prior to each
subsequent infusion with a systemic steroid for at least 3
cycles.
Interrupt or discontinue LYMPHIR based on severity [see Dosage
and Administration (2.4)]. Institute appropriate medical
management.
Hepatotoxicity
LYMPHIR can cause hepatotoxicity. In the pooled safety
population, elevated ALT occurred in 70% of patients, with Grade 3
ALT occurring in 22%; elevated AST occurred in 64% of patients,
with Grade 3 AST elevation occurring in 9%. For Grade 3 events,
median time to onset was 8 days (range: 1 to 15 days); median time
to resolution was 15 days (range: 7 to 50 days); all cases of Grade
3 ALT or AST elevations resolved [see Adverse Reactions (6.1)].
Elevated total bilirubin occurred in 5% of patients, with Grade 3
occurring in 0.9%.
Monitor liver enzymes and bilirubin at baseline and during
treatment as clinically indicated. Withhold, reduce dose, or
permanently discontinue LYMPHIR based on severity.
Embryo-Fetal Toxicity
Based on its mechanism of action, LYMPHIR can cause fetal harm
when administered to a pregnant woman. Verify the pregnancy status
of females of reproductive potential prior to the initiation of
LYMPHIR. Advise pregnant women of the potential risk to the fetus.
Advise females of reproductive potential to use effective
contraception during treatment and for 7 days following the last
dose of LYMPHIR.
ADVERSE REACTIONS
The most common adverse reactions (≥20%), including laboratory
abnormalities, are increased transaminases, albumin decreased,
nausea, edema, hemoglobin decreased, fatigue, musculoskeletal pain,
rash, chills, constipation, pyrexia, and capillary leak
syndrome
USE IN SPECIFIC POPULATIONS
Pregnancy
Risk Summary
Based on its mechanism of action, LYMPHIR can cause fetal harm when
administered to a pregnant woman. There are no available data on
the use of LYMPHIR in pregnant women to evaluate for a
drug-associated risk. No animal reproductive and developmental
toxicity studies have been conducted with denileukin diftitox.
Denileukin diftitox-cxdl causes depletion of regulatory T
lymphocytes (Treg), immune activation, and capillary leak syndrome,
compromising pregnancy maintenance. Advise pregnant women of the
potential risk to a fetus.
In the U.S. general population, the estimated background risk of
major birth defects and miscarriage in clinically recognized
pregnancies are 2-4% and 15-20%, respectively.
Lactation
Risk Summary
No data are available regarding the presence of denileukin
diftitox-cxdl in human milk, the effects on the breastfed child, or
on milk production. Because of the potential for serious adverse
reactions in breastfed children, advise women not to breastfeed
during treatment with LYMPHIR and for 7 days after the last
dose.
Females and Males of Reproductive Potential
Based on its mechanism of action, LYMPHIR can cause fetal harm
when administered to a pregnant woman.
Pregnancy Testing
Verify the pregnancy status of females of reproductive potential
prior to initiating LYMPHIR.
Contraception
Females
Advise females of reproductive potential
to use effective contraception during treatment with LYMPHIR and
for 7 days after the last dose.
Infertility
Males
Based on findings in rats, male fertility may be
compromised by treatment with. The reversibility of the effect on
fertility is unknown.
Pediatric Use
Safety and effectiveness of LYMPHIR in pediatric patients have not
been established.
Geriatric Use
Of the 69 patients with Stage I-III r/r CTCL who received LYMPHIR,
34 patients (49%) were 65 years of age and older and 10 patients
(14%) were 75 years of age and older. Clinical studies of LYMPHIR
did not include sufficient numbers of patients 65 years of age and
older to determine whether they respond differently from younger
adult patients.
You may report side effects to the FDA at 1-800-FDA-1088
or www.fda.gov/medwatch. You may also report side
effects to Citius Pharmaceuticals at 1-844-459-6744.
Please read Important Safety Information and full Prescribing
Information, including Boxed WARNING, for LYMPHIR™ which will be
available in the next few days
About Citius Pharmaceuticals, Inc.
Citius Pharmaceuticals, Inc. is a biopharmaceutical company
dedicated to the development and commercialization of
first-in-class critical care products. In August 2024, the FDA approved LYMPHIR, a targeted
immunotherapy for an initial indication in the treatment of
cutaneous T-cell lymphoma. Citius Pharma's late-stage pipeline also
includes Mino-Lok®, an antibiotic lock solution to salvage
catheters in patients with catheter-related bloodstream infections,
and CITI-002 (Halo-Lido), a topical formulation for the relief of
hemorrhoids. A Pivotal Phase 3 Trial for Mino-Lok and a Phase
2b trial for Halo-Lido were completed
in 2023. Mino-Lok met primary and secondary endpoints of its Phase
3 Trial. Citius is actively engaged with the FDA to outline next
steps for both programs. For more information, please visit
www.citiuspharma.com.
Forward-Looking Statements
This press release may contain "forward-looking statements"
within the meaning of Section 27A of the Securities Act of 1933 and
Section 21E of the Securities Exchange Act of 1934. Such statements
are made based on our expectations and beliefs concerning future
events impacting Citius. You can identify these statements by the
fact that they use words such as "will," "anticipate," "estimate,"
"expect," "plan," "should," and "may" and other words and terms of
similar meaning or use of future dates. Forward-looking statements
are based on management's current expectations and are subject to
risks and uncertainties that could negatively affect our business,
operating results, financial condition and stock price.
Factors that could cause actual results to differ materially from
those currently anticipated are: our ability to commercialize
LYMPHIR and any of our other product candidates that may be
approved by the FDA; the estimated markets for our product
candidates and the acceptance thereof by any market; the ability of
our product candidates to impact the quality of life of our target
patient populations; the planned transaction between TenX Keane
Acquisition and Citius Pharma to form Citius Oncology, Inc. may not
be completed for failure to meet closing conditions or other
reasons; our need for substantial additional funds; risks relating
to the results of research and development activities, including
those from our existing and any new pipeline assets; our dependence
on third-party suppliers; our ability to procure cGMP
commercial-scale supply; our ability to obtain, perform under and
maintain financing and strategic agreements and relationships;
uncertainties relating to preclinical and clinical testing; the
early stage of products under development; market and other
conditions; risks related to our growth strategy; patent and
intellectual property matters; our ability to identify, acquire,
close and integrate product candidates and companies successfully
and on a timely basis; government regulation; competition; as well
as other risks described in our SEC filings. These risks have been
and may be further impacted by Covid-19 and could be impacted by
any future public health risks. Accordingly, these forward-looking
statements do not constitute guarantees of future performance, and
you are cautioned not to place undue reliance on these
forward-looking statements. Risks regarding our business are
described in detail in our Securities and Exchange Commission
("SEC") filings which are available on the SEC's website at
www.sec.gov, including in our Annual Report on Form 10-K for the
year ended September 30, 2023, filed
with the SEC on December 29, 2023,
and updated by our subsequent filings with the Securities and
Exchange Commission. These forward-looking statements speak only as
of the date hereof, and we expressly disclaim any obligation or
undertaking to release publicly any updates or revisions to any
forward-looking statements contained herein to reflect any change
in our expectations or any changes in events, conditions or
circumstances on which any such statement is based, except as
required by law.
Investor Relations for Citius Pharmaceuticals:
Investor Contact:
Ilanit
Allen
ir@citiuspharma.com
908-967-6677 x113
Media Contact:
STiR-communications
Greg Salsburg
Greg@STiR-communications.com
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