Tumor-agnostic data supporting approval
demonstrated an overall response rate (ORR) of 44% across multiple
tumor types
FDA simultaneously grants traditional approval
in adults with locally advanced or metastatic non-small cell lung
cancer (NSCLC) with a RET gene fusion, as detected by an
FDA-approved test
INDIANAPOLIS, Sept. 21,
2022 /PRNewswire/ -- Eli Lilly and Company (NYSE:
LLY) today announced the U.S. Food and Drug Administration (FDA)
has granted approval to Retevmo® (selpercatinib, 40 mg
& 80 mg capsules) for adult patients with locally advanced or
metastatic solid tumors with a rearranged during transfection
(RET) gene fusion that have progressed on or following prior
systemic treatment or who have no satisfactory alternative
treatment options. This indication is approved under accelerated
approval based on ORR and duration of response (DOR). Continued
approval for this indication may be contingent upon verification
and description of clinical benefit in the confirmatory trial.
"In the LIBRETTO-001 trial, selpercatinib demonstrated
clinically meaningful and durable responses across a variety of
tumor types in patients with RET-driven cancers, including
pancreatic, colon and other cancers in need of new treatment
options," said Vivek Subbiah, M.D.,
associate professor of Investigational Cancer Therapeutics at The
University of Texas MD Anderson Cancer
Center and co-investigator for LIBRETTO-001. "These data and
FDA approval of the tumor-agnostic indication underscore the
importance of routine, comprehensive genomic testing for patients
across a wide variety of tumor types."
In addition to the tumor-agnostic approval, the FDA has granted
traditional approval for Retevmo in adult patients with
locally advanced or metastatic non-small cell lung cancer (NSCLC)
with a RET gene fusion, as detected by an FDA-approved test.
This FDA action broadens the Retevmo label to include patients with
locally advanced disease and converts the May 2020 accelerated approval for NSCLC to a
traditional approval.
The labeling for Retevmo contains warnings and precautions for
hepatotoxicity (evidence of liver dysfunction), interstitial lung
disease (ILD)/pneumonitis, hypertension, QT interval prolongation,
hemorrhagic events, hypersensitivity, tumor lysis syndrome, risk of
impaired wound healing, hypothyroidism, and embryo-fetal
toxicity.
"Since its initial accelerated approval, Retevmo has shifted the
treatment paradigm for patients with RET-altered cancers,"
said David Hyman, M.D., chief
medical officer, Loxo@Lilly. "Retevmo is the first and only RET
inhibitor to receive both tumor-agnostic accelerated approval and
traditional approval in NSCLC, further supporting its ability to
deliver meaningful clinical benefit for patients across
diverse tumor types."
The two approvals are supported by data from the pivotal
LIBRETTO-001 trial, which is the largest clinical trial of patients
with RET-driven cancers treated with a RET inhibitor. The
multicenter, open-label, multi-cohort study enrolled patients with
locally advanced or metastatic RET-driven solid tumors,
including NSCLC. Major efficacy outcomes were ORR and DOR, assessed
by a blinded independent review committee (BIRC). Prespecified
secondary endpoints included central nervous system (CNS) ORR and
CNS DOR.
RET Fusion-Positive Solid Tumors
Among the 41
patients in the tumor-agnostic data set, the most common cancers
were pancreatic adenocarcinoma (27%), colorectal (24%), salivary
(10%), and unknown primary (7%). Thirty-seven patients (90%)
received prior systemic therapy (median 2 [range 0 – 9]; 32%
received 3 or more). Efficacy results are summarized
below:
|
RET
Fusion-Positive
Solid Tumors
|
|
No. of
patients
|
41
|
|
Overall Response
Rate1 (95% CI)
|
44 %(28,
60)
|
|
Complete
response
|
4.9 %
|
|
Partial
response
|
39 %
|
|
Duration of
Response
|
|
|
Median in months (95%
CI)
|
24.5 (9.2,
NE)
|
|
% with ≥ 6
months2
|
67 %
|
|
1
Confirmed overall response rate assessed by BIRC.
2 Based on observed duration of
response.
NE = not estimable
|
Efficacy results by tumor type are summarized below:
|
Tumor
Type
|
Patients
(n =
41)
|
ORR1,2
|
DOR
Range
(months)
|
|
|
n (%)
|
95%
CI
|
|
|
Pancreatic
adenocarcinoma
|
11
|
6
(55 %)
|
(23, 83)
|
2.5, 38.3+
|
|
Colorectal
|
10
|
2
(20 %)
|
(2.5, 56)
|
5.6, 13.3
|
|
Salivary
|
4
|
2
(50 %)
|
(7, 93)
|
5.7, 28.8+
|
|
Unknown
primary
|
3
|
1
(33 %)
|
(0.8, 91)
|
9.2
|
|
Breast
|
2
|
PR, CR
|
NA
|
2.3+, 17.3
|
|
Sarcoma (soft
tissue)
|
2
|
PR, SD
|
NA
|
14.9+
|
|
Xanthogranuloma
|
2
|
NE, NE
|
NA
|
NA
|
|
Carcinoid
(bronchial)
|
1
|
PR
|
NA
|
24.1+
|
|
Carcinoma of the
skin
|
1
|
NE
|
NA
|
NA
|
|
Cholangiocarcinoma
|
1
|
PR
|
NA
|
5.6+
|
|
Ovarian
|
1
|
PR
|
NA
|
14.5+
|
|
Pulmonary
carcinosarcoma
|
1
|
NE
|
NA
|
NA
|
|
Rectal
neuroendocrine
|
1
|
NE
|
NA
|
NA
|
|
Small
intestine
|
1
|
CR
|
NA
|
24.5
|
|
+ denotes ongoing
response.
1 Confirmed overall response rate assessed
by BIRC.
2 Best overall response for each patient is
presented for tumor types with ≤2 patients.
CI = confidence interval, CR = complete response, DOR = duration of
response, NA = not applicable, NE = not evaluable, ORR = overall
response rate, PR = partial response, SD = stable
disease.
|
"Today's announcement of Retevmo's expanded label reflects an
opportunity to bring more targeted treatment options to a broader
set of difficult-to-treat solid tumors, such as pancreatic cancer,"
said Julie Fleshman, president and
chief executive officer, the Pancreatic Cancer Action Network
(PanCAN). "This news further highlights the importance of broad
biomarker testing, which may open the door to new therapy options
for more patients."
Retevmo may affect both healthy cells and tumor cells, which can
result in side effects, some of which can be serious.
RET Fusion-Positive NSCLC
Efficacy results for
patients with both platinum chemotherapy treated and
treatment-naïve RET fusion-positive NSCLC are summarized
below:
|
RET
Fusion-Positive NSCLC
|
|
Treatment-Naïve
|
Platinum
Chemotherapy
Treated
|
|
No. of
patients
|
69
|
247
|
|
Overall Response
Rate1
(95% CI)
|
84% (73%,
92%)
|
61% (55%,
67%)
|
|
Complete
response
|
5.8 %
|
7.3 %
|
|
Partial
response
|
78 %
|
54 %
|
|
Duration of
Response
|
|
|
|
Median in months (95%
CI)
|
20.2 (13,
NE)
|
28.6 (20,
NE)
|
|
% with ≥ 12
months2
|
50 %
|
63 %
|
|
1 Confirmed overall response
rate assessed by BIRC.
2 Based on observed duration of
response.
NE = not estimable
|
The activity of Retevmo in patients with CNS metastases was also
evaluated. Among the 247 patients with previously treated
RET fusion-positive NSCLC, 16 had measurable CNS metastases
at baseline as assessed by BIRC. One patient received radiation
therapy (RT) to the brain within two months prior to study entry.
Responses in intracranial lesions were observed in 87.5% (14 of 16)
of patients; 39% of responders had an intracranial DOR of 12 months
or greater. Among the 69 patients with treatment-naïve RET
fusion-positive NSCLC, five had measurable CNS metastases at
baseline as assessed by BIRC. Two patients received RT to the brain
within two months prior to study entry. Responses in intracranial
lesions were observed in four of these five patients; 38% of
responders had an intracranial DOR of 12 months or greater.
"Retevmo's accelerated approval played an important role in
providing earlier access for patients who needed new treatment
options. We are now pleased to see the conversion from an
accelerated approval to a traditional approval," said Andrea Ferris, president and chief executive
officer, LUNGevity Foundation. "As a targeted treatment, this
traditional approval further reinforces the need for comprehensive
biomarker testing for lung cancer patients, with the hope that as
many patients as possible can benefit from receiving treatments
tailored to their specific tumor mutations."
In the full LIBRETTO-001 safety population (n=796) with advanced
solid tumors, the most common adverse reactions (≥25%) were edema,
diarrhea, fatigue, dry mouth, hypertension, abdominal pain,
constipation, rash, nausea, and headache. The most common Grade 3
or 4 laboratory abnormalities (≥5%) were decreased lymphocytes,
increased alanine aminotransferase (ALT), increased aspartate
aminotransferase (AST), decreased sodium, and decreased calcium.
For more information, see "IMPORTANT SAFETY INFORMATION FOR
RETEVMO® (selpercatinib)" below.
About LIBRETTO-001
The Phase 1/2 LIBRETTO-001 trial is
the largest clinical trial of patients with RET-driven
cancers treated with a RET inhibitor. The trial, which spans 16
countries and 85 sites, included a dose escalation phase (Phase 1)
and a dose expansion phase (Phase 2). The primary objective was to
determine ORR by blinded independent review committee (BIRC) and
other objectives included DOR, CNS ORR & DOR, safety and
PFS.
About Retevmo® (selpercatinib, 40 mg & 80 mg
capsules)
Retevmo (selpercatinib, formerly known as
LOXO-292) (pronounced ret-tév-mo) is a selective and potent RET
kinase inhibitor. Retevmo may affect both tumor cells and healthy
cells, which can result in side effects. RET-driver
alterations are predominantly mutually exclusive from other
oncogenic drivers. Retevmo is a U.S. FDA-approved oral prescription
medicine, 120 mg or 160 mg dependent on weight (<50 kg or ≥50
kg, respectively), taken twice daily until disease progression or
unacceptable toxicity.
IMPORTANT SAFETY INFORMATION FOR
RETEVMO® (selpercatinib)
Hepatotoxicity: Serious hepatic adverse reactions
occurred in 3% of patients treated with Retevmo. Increased
aspartate aminotransferase (AST) occurred in 59% of patients,
including Grade 3 or 4 events in 11% and increased alanine
aminotransferase (ALT) occurred in 55% of patients, including Grade
3 or 4 events in 12%. Monitor ALT and AST prior to initiating
Retevmo, every 2 weeks during the first 3 months, then monthly
thereafter and as clinically indicated. Withhold, reduce dose, or
permanently discontinue Retevmo based on the severity.
Severe, life-threatening, and fatal interstitial lung disease
(ILD)/pneumonitis can occur in patients treated with Retevmo.
ILD/pneumonitis occurred in 1.8% of patients who received Retevmo,
including 0.3% with Grade 3 or 4 events, and 0.3% with fatal
reactions. Monitor for pulmonary symptoms indicative of
ILD/pneumonitis. Withhold Retevmo and promptly investigate for ILD
in any patient who presents with acute or worsening of respiratory
symptoms which may be indicative of ILD (e.g., dyspnea, cough, and
fever). Withhold, reduce dose, or permanently discontinue Retevmo
based on severity of confirmed ILD.
Hypertension occurred in 41% of patients, including
Grade 3 hypertension in 20% and Grade 4 in one (0.1%) patient.
Overall, 6.3% had their dose interrupted and 1.3% had their dose
reduced for hypertension. Treatment-emergent hypertension was most
commonly managed with anti-hypertension medications. Do not
initiate Retevmo in patients with uncontrolled hypertension.
Optimize blood pressure prior to initiating Retevmo. Monitor blood
pressure after 1 week, at least monthly thereafter, and as
clinically indicated. Initiate or adjust anti-hypertensive therapy
as appropriate. Withhold, reduce dose, or permanently discontinue
Retevmo based on the severity.
Retevmo can cause concentration-dependent QT interval
prolongation. An increase in QTcF interval to >500 ms was
measured in 7% of patients and an increase in the QTcF interval of
at least 60 ms over baseline was measured in 20% of patients.
Retevmo has not been studied in patients with clinically
significant active cardiovascular disease or recent myocardial
infarction. Monitor patients who are at significant risk of
developing QTc prolongation, including patients with known long QT
syndromes, clinically significant bradyarrhythmias, and severe or
uncontrolled heart failure. Assess QT interval, electrolytes,
and thyroid-stimulating hormone (TSH) at baseline and
periodically during treatment, adjusting frequency based upon risk
factors including diarrhea. Correct hypokalemia, hypomagnesemia,
and hypocalcemia prior to initiating Retevmo and during treatment.
Monitor the QT interval more frequently when Retevmo is
concomitantly administered with strong and moderate CYP3A
inhibitors or drugs known to prolong QTc interval. Withhold and
dose reduce or permanently discontinue Retevmo based on the
severity.
Serious, including fatal, hemorrhagic events can occur
with Retevmo. Grade ≥3 hemorrhagic events occurred in 3.1% of
patients treated with Retevmo including 4 (0.5%) patients with
fatal hemorrhagic events, including cerebral hemorrhage (n=2),
tracheostomy site hemorrhage (n=1), and hemoptysis (n=1).
Permanently discontinue Retevmo in patients with severe or
life-threatening hemorrhage.
Hypersensitivity occurred in 6% of patients
receiving Retevmo, including Grade 3 hypersensitivity in 1.9%. The
median time to onset was 1.9 weeks (range: 5 days to 2 years).
Signs and symptoms of hypersensitivity included fever, rash and
arthralgias or myalgias with concurrent decreased platelets or
transaminitis. If hypersensitivity occurs, withhold Retevmo and
begin corticosteroids at a dose of 1 mg/kg prednisone (or
equivalent). Upon resolution of the event, resume Retevmo at a
reduced dose and increase the dose of Retevmo by 1 dose level each
week as tolerated until reaching the dose taken prior to onset of
hypersensitivity. Continue steroids until patient reaches target
dose and then taper. Permanently discontinue Retevmo for recurrent
hypersensitivity.
Tumor lysis syndrome (TLS) occurred in 0.6% of
patients with medullary thyroid carcinoma receiving Retevmo.
Patients may be at risk of TLS if they have rapidly growing tumors,
a high tumor burden, renal dysfunction, or dehydration. Closely
monitor patients at risk, consider appropriate prophylaxis
including hydration, and treat as clinically indicated.
Impaired wound healing can occur in patients who
receive drugs that inhibit the vascular endothelial growth factor
(VEGF) signaling pathway. Therefore, Retevmo has the potential to
adversely affect wound healing. Withhold Retevmo for at least 7
days prior to elective surgery. Do not administer for at least 2
weeks following major surgery and until adequate wound healing. The
safety of resumption of Retevmo after resolution of wound healing
complications has not been established.
Retevmo can cause hypothyroidism. Hypothyroidism occurred
in 13% of patients treated with Retevmo; all reactions were Grade 1
or 2. Hypothyroidism occurred in 13% of patients (50/373) with
thyroid cancer and 13% of patients (53/423) with other solid tumors
including NSCLC. Monitor thyroid function before treatment with
Retevmo and periodically during treatment. Treat with thyroid
hormone replacement as clinically indicated. Withhold Retevmo until
clinically stable or permanently discontinue Retevmo based on
severity.
Based on data from animal reproduction studies and its mechanism
of action, Retevmo can cause fetal harm when administered to
a pregnant woman. Administration of selpercatinib to pregnant rats
during organogenesis at maternal exposures that were approximately
equal to those observed at the recommended human dose of 160 mg
twice daily resulted in embryolethality and malformations. Advise
pregnant women and females of reproductive potential of the
potential risk to a fetus. Advise females of reproductive potential
and males with female partners of reproductive potential to use
effective contraception during treatment with Retevmo and for 1
week after the last dose. There are no data on the presence of
selpercatinib or its metabolites in human milk or on their 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 Retevmo and
for 1 week after the last dose.
Severe adverse reactions (Grade 3-4) occurring in ≥20% of
patients who received Retevmo in LIBRETTO-001, were
hypertension (20%), diarrhea (5%), prolonged QT interval (4.8%),
dyspnea (3.1%), fatigue (3.1%), hemorrhage (2.6%), abdominal pain
(2.5%), vomiting (1.8%), headache (1.4%), nausea (1.1%),
constipation (0.8%), edema (0.8%), rash (0.6%), and arthralgia
(0.3%).
Serious adverse reactions occurred in 44% of
patients who received Retevmo. The most frequently reported
serious adverse reactions (in ≥2% of patients) were pneumonia,
pleural effusion, abdominal pain, hemorrhage, hypersensitivity,
dyspnea, and hyponatremia.
Fatal adverse reactions occurred in 3% of patients; fatal
adverse reactions included sepsis (n=6), respiratory failure (n=5),
hemorrhage (n=4), pneumonia (n=3), pneumonitis (n=2), cardiac
arrest (n=2), sudden death (n=1), and cardiac failure (n=1).
Common adverse reactions (all grades) occurring in ≥20% of
patients who received Retevmo in LIBRETTO-001, were edema
(49%), diarrhea (47%), fatigue (46%), dry mouth (43%), hypertension
(41%), abdominal pain (34%), rash (33%), constipation (33%), nausea
(31%), headache (28%), cough (24%), vomiting (22%), dyspnea (22%),
hemorrhage (22%), arthralgia (21%), and prolonged QT interval
(21%).
Laboratory abnormalities (all grades ≥20%; Grade 3-4)
worsening from baseline in patients who received Retevmo in
LIBRETTO-001, were increased AST (59%; 11%), decreased calcium
(59%; 5.7%), increased ALT (56%; 12%), decreased albumin (56%;
2.3%), increased glucose (53%; 2.8%), decreased lymphocytes (52%;
20%), increased creatinine (47%; 2.4%), decreased sodium
(42%; 11%), increased alkaline phosphatase (40%; 3.4%), decreased
platelets (37%; 3.2%), increased total cholesterol (35%; 1.7%),
increased potassium (34%; 2.7%), decreased glucose (34%; 1.0%),
decreased magnesium (33%; 0.6%), increased bilirubin (30%; 2.8%),
decreased hemoglobin (28%; 3.5%), and decreased neutrophils (25%;
3.2%).
Concomitant use of acid-reducing agents decreases
selpercatinib plasma concentrations which may reduce Retevmo
anti-tumor activity. Avoid concomitant use of proton-pump
inhibitors (PPIs), histamine-2 (H2) receptor antagonists, and
locally-acting antacids with Retevmo. If coadministration cannot be
avoided, take Retevmo with food (with a PPI) or modify its
administration time (with a H2 receptor antagonist or a
locally-acting antacid).
Concomitant use of strong and moderate CYP3A
inhibitors increases selpercatinib plasma concentrations
which may increase the risk of Retevmo adverse reactions including
QTc interval prolongation. Avoid concomitant use of strong and
moderate CYP3A inhibitors with Retevmo. If concomitant use of a
strong or moderate CYP3A inhibitor cannot be avoided, reduce the
Retevmo dosage as recommended and monitor the QT interval with ECGs
more frequently.
Concomitant use of strong and moderate CYP3A
inducers decreases selpercatinib plasma concentrations which
may reduce Retevmo anti-tumor activity. Avoid coadministration of
Retevmo with strong and moderate CYP3A inducers.
Concomitant use of Retevmo with CYP2C8 and CYP3A
substrates increases their plasma concentrations which may
increase the risk of adverse reactions related to these substrates.
Avoid coadministration of Retevmo with CYP2C8 and CYP3A substrates
where minimal concentration changes may lead to increased adverse
reactions. If coadministration cannot be avoided, follow
recommendations for CYP2C8 and CYP3A substrates provided in their
approved product labeling.
Retevmo is a P-glycoprotein (P-gp) inhibitor. Concomitant use of
Retevmo with P-gp substrates increases their plasma
concentrations, which may increase the risk of adverse reactions
related to these substrates. Avoid coadministration of Retevmo with
P-gp substrates where minimal concentration changes may lead to
increased adverse reactions. If coadministration cannot be avoided,
follow recommendations for P-gp substrates provided in their
approved product labeling.
No dosage modification is recommended for patients with mild
to severe renal impairment (estimated Glomerular Filtration
Rate [eGFR] ≥15 to 89 mL/min, estimated by Modification of Diet in
Renal Disease [MDRD] equation). A recommended dosage has not been
established for patients with end-stage renal disease.
Reduce the dose when administering Retevmo to patients with
severe hepatic impairment (total bilirubin greater than 3 to
10 times upper limit of normal [ULN] and any AST). No dosage
modification is recommended for patients with mild or moderate
hepatic impairment. Monitor for Retevmo-related adverse reactions
in patients with hepatic impairment.
Please see full Prescribing
Information for Retevmo.
SE HCP ISI LA_21SEP22
About Lilly
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P-LLY
Retevmo® is a registered trademark owned by or
licensed to Eli Lilly and Company, its subsidiaries, or
affiliates.
PP-SE-US-1166 09/2022
©Lilly USA, LLC 2022. ALL
RIGHTS RESERVED.
Lilly Cautionary Statement Regarding Forward-Looking
Statements
This press release contains forward-looking
statements (as that term is defined in the Private Securities
Litigation Reform Act of 1995) about Retevmo®
(selpercatinib) for the treatment of locally advanced and
metastatic RET fusion-positive NSCLC and other RET
fusion-positive solid tumors, and reflects Lilly's current beliefs
and expectations. However, as with any pharmaceutical product,
there are substantial risks and uncertainties in the process of
development and commercialization. Among other things, there is no
guarantee that future study results will be consistent with study
findings to date or that Retevmo will receive additional regulatory
approvals. For further discussion of these and other risks and
uncertainties, see Lilly's Form 10-K and Form 10-Q filings with the
United States Securities and Exchange Commission. Except as
required by law, Lilly undertakes no duty to update forward-looking
statements to reflect events after the date of this release.
Refer to: Kyle Owens;
owens_kyle@lilly.com; (332) 259-3932 – media
Joe Fletcher; jfletcher@lilly.com; (317)
296-2884 – investors
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