Diabetic Macular Edema Clinical Trial
Official title:
Combination OZURDEX® & EyLea® vs. OZURDEX® Monotherapy in IncompLete-Responders wIth Diabetic Macular Edema (COLLIDE)
COLLIDE is a multi-center, open-label, 1:1 randomized study looking at the effects of aflibercept (AFL; 2.0mg) plus OZURDEX (DEX; 0.7mg) implant combination therapy versus DEX monotherapy in phakic or pseudophakic eyes with center-involved DME that have demonstrated prior incomplete response to 3-6 anti-VEGF treatment in 3-9 months. The primary outcome will be 24 week central subfield thickness. Secondary outcomes include the change in ETDRS BCVA letters, number of re-injections and re-injection interval, proportion of eyes with 15- and 10- ETDRS letter gained/lost, proportion of eyes with PDR as per Optos color and FA at the study completion (24+/- 2 weeks) and OCT and OCT angiography biomarkers.
Diabetic macular edema (DME) is a common cause of vision loss in patients with diabetes. The
pathophysiology of DME is complex and likely multifactorial, where some of the most important
features include the accumulation of advanced glycation end products, reactive oxygen
species, protein kinase C and diacylglyceride activation, up-regulation of the
renin-angiotensin-aldosterone system and up-regulation of vascular endothelial growth factor
(VEGF). Additionally, inflammation has also been identified as an important etiological
factor because breakdown of the retinal pigment epithelium - a physiologic barrier to fluid
flow from the choriocapillaris and active retinal fluid pump, has been linked to increased
levels of pro-inflammatory mediators including VEGF and processes that support leukostasis.
In Canada, LUCENTIS® (0.5 mg ranibizumab or RBZ, an anti-neovascular VEGF-A inhibitor,
Novartis Pharmaceuticals Canada Inc.) was the first approved medical treatment for DME.
Health Canada's decision for regulatory approval of RBZ (0.5 mg) for treatment of DME was
based on 12-month results from the RESOLVE (Phase II trial investigating RBZ (0.3 mg or 0.5
mg) vs. sham injection) and RESTORE (Phase IIIb trial investigating RBZ (0.5 mg) + sham laser
or RBZ (0.5 mg) + laser vs. laser + sham injection) trials. In the RESOLVE trial, pooled RBZ
treatment arms resulted in significant and continuous improvement compared to sham treatment
in both BCVA (mean improvement of 7.8 letters with RBZ treatment compared to a mean decline
of 0.1 letters with sham treatment) and CRT (mean reduction of -194.2 µm with RBZ treatment
vs. -48.4±153.4 µm with sham treatment). Similarly in the RESTORE trial, RBZ monotherapy and
RBZ treatment with adjunctive laser yielded a statistically significantly greater mean
average change in BCVA letter score compared to laser monotherapy through 12-months of study
(+6.1 and +5.9 vs. +0.8 BCVA letters, respectively) along with a significantly greater
improvement in CRT change from baseline vs. laser (-118.7 µm and -128.3 µm vs. -61.3 µm,
respectively). Additionally, RBZ treatment arms in both RESOLVE and RESTORE demonstrated
comparable safety with controls permitting conclusions that RBZ 0.5 mg is well-tolerated in
the management of DME.
Diabetic Retinopathy Clinical Research Network (DRCR.net) published in 2015 their Protocol T:
Comparison of RBZ with Eylea (Aflibercept or AFL, Regeneron Pharmaceuticals) and Avastin
(Bevacizumab or BCZ, Roche) in DME. At 1 year, the patients treated with AFL had a
statistically improved visual acuity of 13.3 letters as compared to BCZ (9.7 letters) and RBZ
(11.2 letters). The same cohort of AFL treated DME had greater improvement on Ocular
Coherence Tomography central subfield thickness with 169 micron change vs 101 um with BCZ and
147 um with RBZ. However, in all treatment arms, a large number of patients 46% required
rescue laser therapy as per study protocol.
While anti-VEGF agents are a mainstay for the management of DME, a subgroup of eyes having
partial or incomplete response to AVASTIN® (bevacizumab or BCZ), EYLEA® (intravitreal
aflibercept injection or AFL) and RBZ exist.
RISE and RIDE, two phase III trials for registration of RBZ in the USA randomized DME
patients on a basis of 1:1:1 to receive monthly 0.3 mg or 0.5 mg RBZ intravitreal treatments
or sham injections over 24 months. Upon completion of the 24-month study (time point for
primary efficacy outcome, namely the proportion of patients gaining ≥ 15 Early Treatment
Diabetic Retinopathy Study (ETDRS) letters in BCVA from baseline), patients within the sham
arm were eligible to receive delayed monthly 0.5 mg RBZ treatments over the next 12 months.
Although strong vision gains were observed in patients originally randomized to RBZ arms at
month 24 and sustained through month 36, sham controls receiving delayed RBZ treatment had
vision improvements to a lesser extent than those receiving continuous RBZ treatment
throughout the 36 month study, thereby suggesting benefits with initiation of DME treatment
early in the course of DME management.
In a prospective study comparing the efficacy of monthly BCZ (1.5 mg) vs. monthly RBZ (0.5
mg) in eyes with baseline center-involved DME > 300 µm, Nepomuceno and colleagues reported
59% and 37% of eyes had persistent DME (> 275 µm) by week 48. Moreover, 28% and 14% of BCZ-
and RBZ-treated eyes qualified for rescue therapy, respectively.
Results from the phase 3 VIVID and VISTA trials demonstrated that 42% eyes with central
involved DME treated with Eylea (Aflibercept) 2.0 mg administered either every 4 or 8 weeks
(after 5 initial monthly doses) failed to achieve 2-lines of vision gain.
In the RESOLVE and RESTORE trials there were 39.2% and 59.7% of RBZ-treated eyes that
respectively failed to achieve 2-lines of vision gain at 12 months of study, while in RISE
and RIDE, 23% of patients had CRT >250 µm and 40% of patients failed to achieve a
best-corrected visual acuity (BCVA) ≥ 20/40 despite 2 years of monthly RBZ injections.
Adjunctive treatment regimens that offer ability to resolve DME and improve vision in eyes
with incomplete response to anti-VEGF monotherapy will be of great value. Given that the
treatment effects observed with delayed treatment in RISE and RIDE were less than that seen
in the continuous (early) RBZ treatment arms, one may reason it is beneficial to readily
identify eyes with incomplete response to anti-VEGF monotherapy to best allow functional
vision improvement with an effective adjunctive treatment option.
Intravitreal corticosteroids may be useful in the treatment of DME because they block
production of VEGF and other inflammatory mediators, inhibit leukostasis, and enhance the
barrier function of vascular endothelial cell tight junctions. Off-label treatment with IVTA
has been shown to be more effective than placebo in improving vision in patients with
refractory DME. Sustained-release corticosteroids have been developed to reduce the need for
frequent retreatments associated with anti-VEGF monotherapy regimens.
OZURDEX® (DEX implant; Allergan Inc. Irvine, CA, USA) is a sustained-release biodegradable
implant approved for treatment of ME following central retinal vein occlusion, non-infectious
uveitis affecting the posterior segment and pseudophakic DME in adult patients. DEX implant
releases the corticosteroid dexamethasone, which possesses 5-6 times greater
anti-inflammatory potency than triamcinolone, into the vitreous over a period of 6 months. In
previous studies, DEX implant has demonstrated efficacy in the treatment of persistent DME,
DME resistant to anti-VEGF treatment and DME in difficult-to-treat vitrectomized eyes.
Recently, the results of two identical phase III, multi-center, international, masked,
randomized, sham-controlled trials of DEX implants (0.35 mg and 0.7 mg) in DME demonstrated
that an average of 4-5 DEX implant injections administered at ≥ 6-month intervals over 3
years provides rapid and sustained functional and anatomical improvements. Retreatment with
the 0.7 mg DEX implant in phakic DME eyes was associated with significant 67.9%
cataract-related adverse events and 59.2% cataract surgery rate vs. only 20.4% and 7.2% rates
observed in sham-controls. These cataract-related adverse event rates are comparatively lower
for a DEX implant than for other commonly used intravitreal corticosteroids. As such, a DEX
implant may have a better benefit to risk safety profile. A meta-analysis on
corticosteroid-induced IOP elevation for the three commonly used intravitreal corticosteroids
including off-label KENALOG® (intravitreal triamcinolone acetonide or IVTA (4.0 mg),
Bristol-Myers Squibb, Canada. Montreal, Quebec), DEX implant and RETISERT® (intravitreal
fluocinolone acetonide or IFA (0.59 mg) non-biodegradable implant, Bausch & Lomb Canada Inc.,
Vaughan, Ontario) found the incidence of ocular hypertension to be lowest among eyes treated
with DEX implant (15%) followed by IVTA (32%) and IFA (66%).
DRCR.net Protocol U studied the effect of adding Ozurdex to patients who had incomplete
response to at least 3 anti-VEGF injections. The authors randomized 116 phakic and
pseudophakic patients with DME to either Ozurdex plus RBZ or RBZ alone. Change in OCT
subfoveal thickness was significantly different between both groups with 110 um reduction in
the ozurdex arm vs 62 um in the monotherapy RBZ arm.
The present study seeks to compare the effects of a combination treatment regimen consisting
of AFL (2.0 mg) + DEX implant vs. DEX implant monotherapy in phakic or pseudophakic eyes with
center-involved DME deemed to have incomplete response to 3-6 prior anti-VEGF treatments.
It is hypothesized that phakic or pseudophakic center-involved DME eyes with incomplete
response to 3-6 anti-VEGF injections (i.e., RBZ, BCZ or IAI) will show a greater reduction in
central subfield thickness (CST) at 24 weeks when treated with a combination treatment
regimen consisting of AFL (2.0 mg) and DEX implant (0.7 mg) vs. a monotherapy treatment
regimen with DEX implant (0.7 mg).
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