I guess while we're on the subject of some of the most difficult things melanoma patients can deal with, we might as well roll with it. LMD is certainly that. Here are previous posts: Leptomeningeal Disease
Now there is this:
Intrathecal (IT) and intravenous (IV) nivolumab (N)
for metastatic melanoma (MM) patients (pts) with leptomeningeal disease (LMD). John, Foster, Haymaker, et al. ASCO 2021.
Background: MM pts
with LMD have a dismal prognosis, with median overall survival (OS) less than 3
months, no approved therapies and extremely limited clinical trial options. We
previously reported initial safety findings from an open label, single arm,
single center phase I/IB trial (NCT03025256), in which IT and IV N were well
tolerated, without any CNS-specific or unexpected toxicity. Here we report an
update on safety and maximum tolerated dose (MTD) for all patients enrolled,
and efficacy for the completed dose cohorts.
Methods: MM patients
aged greater than 18 with evidence of LMD by MRI and/or CSF cytology, ECOG PS greater than/= to 2 were
treated with IT and IV N. Dexamethasone less than/= to 4 mg/daily and concurrent BRAF/MEK
inhibitor(i) treatment was allowed. For cycle 1, IT N was administered via
intraventricular reservoir on day (D)1. For subsequent cycles (every 14 days),
pts received IT N on D1, followed by IV N 240 mg on D2. IT N doses evaluated
were 5, 10, 20 mg and 50 mg. Blood and CSF were collected at multiple time
points for translational research. The primary objectives of this
first-in-human study were to determine the safety and MTD of IT N given with IV
N in MM pts with LMD. Bayesian mTPI methodology was used to define the MTD.
Results: To date, 23
pts have been treated: two at 5, three at 10, fourteen at 20 mg and four at 50
mg IT N. Median age at LMD diagnosis was 42 (28-73); 12 pts are male. All pts
had radiographic evidence of LMD and neurological symptoms; 14 pts had positive
CSF cytology at baseline. 21 pts received prior therapies for their metastatic
melanoma: anti-PD1 (n = 19), BRAFi/MEKi (n = 14), chemo (n = 2), IT IL2 (n = 4)
other (n = 2). 19 pts had prior XRT, including whole brain RT (n = 7). Two pts
were treatment-naïve. The median number of IT N doses was five (1- 66). The
combination regimen was well tolerated by all evaluable pts (n=23), with only
five pts (22%) experiencing gr 3 AEs, and no reported gr 4 or 5 toxicities.
Nausea (30%), diarrhea (26%), and rash (22%) were the most common AEs. Eight
pts (23%) experienced AEs after IT N administration, all gr 1. Initial efficacy
analysis included only pts (n=19) treated with first three dose levels
(5-20mg). Median follow-up for these pts is 4.5 months (mos) (1.1, 31.5 mos)
and median OS is 63 % at 3 mos, 42 % at 6 mos and 30% at 12 mos.
Conclusions: The
trial demonstrates the feasibility and safety of IT administration of modern
immunotherapy for MM pts with LMD. No unexpected systemic or neurological
toxicity was observed with 20mg IT N. 2 additional patients are required to
complete the 50mg IT N cohort. OS rates at 6 and 12 mos are encouraging and
support further evaluation of IT administration of immunotherapy agents for pts
with MM and LMD. Final presentation will include results of LMD for all dose
cohorts, composite response assessment and comparative analysis of longitudinal
CSF samples to assess immunologic effects. Clinical trial information:
NCT03025256.
Holding Rob and Adriana in my heart always. ~ les
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