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Ростовский Государственный Медицинский Университет

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Ординатура / Офтальмология / Английские материалы / Retinal Pharmacotherapy_Rodrigues, Nguyen, Farah_2010.pdf

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		100
		90	83% 86%			Anec Acet 15 mg
		80		75%		PDT
		70		69%
	loss	70			61%
					61%
		60			56%	51%50%
	-line	60			56%		45% 49%
	-line	50					45% 49%
	<3	40
chaptecortave• 31 An	% With	40
		30
		20
		10
		0	Week 6	Month 3	Month 6	Month 9	Month 12
Acetate			Week 6	Month 3	Month 6	Month 9	Month 12
	A
		100
		100	89%86%
		90	89%86%			Anec Acet 15 mg
		80		71% 75%		PDT
		80		71% 75%
	loss	70			62% 61%	59%
		60			62% 61%	59%	57%
							57%

	-line					50%	49%
		50				50%	49%
		50
	<3	40
	% With	40
	% With	30
		20
		10
		0	Week 6	Month 3	Month 6	Month 9	Month 12
			Week 6	Month 3	Month 6	Month 9	Month 12
	C

	20
	15
	10
Percentage	5
	0
	−5
	−5	−7%
		−7%
	−10
	−15	−14%
	−20	Week 6	Month 3	Month 6	Month 9	Month 12
		Week 6	Month 3	Month 6	Month 9	Month 12
B

	20
	15
	10
Percentage	5
	0
	−5
	−5	−7%
		−7%
	−10
	−15	−14%
	−20	Week 6	Month 3	Month 6	Month 9	Month 12
		Week 6	Month 3	Month 6	Month 9	Month 12
D

Figure 31.8 Results of the anecortave acetate (AA) versus photodynamic therapy (PDT) comparison trial. Percentage of eyes avoiding moderate (3 lines) visual acuity loss (left) and difference between groups over time with 95% confidence intervals (right) with dashed lines representing 7% (planned noninferiority criteria for this study) and 14% confidence limits. Results shown are for all subjects (A and B) and a retrospective subgroup excluding eyes with reflux and those with >6 months between injections (C and D). (Reprinted from Slakter JS, Bochow TW, D’Amico DJ, et al. Anecortave acetate (15 milligrams) versus photodynamic therapy for treatment of subfoveal neovascularization in age-related macular degeneration. Ophthalmology 2006;113:3–13, with permission from Ophthalmology.)

Figure 31.9 Counterpressure device for minimizing drug reflux during posterior juxtascleral depot injection.

and 40.3%, respectively, compared to 64.3% (P < 0.001) and 5.6% (P < 0.001), respectively, in the PDT group. Even accounting for reflux and missed dosing windows, a side-by-side comparison of the ANCHOR data with those from the anecortave acetate versus PDT comparison trial would seem to suggest that ranibizumab is a more effective treatment (Figure 31.10). This comparison is, however, provided only for illustrative purposes, and it is difficult to make firm conclusions based on such comparisons across trials owing to probable differences between study populations and other baseline conditions. Of note, the PDT group also fared better in the ANCHOR trial than in the anecortave acetate comparison trial, highlighting the probable existence of such differences.

CONTRAINDICATIONS

OCULAR COMPLICATions AND TOXICITY

Preclinical safety studies performed on rabbits and monkeys revealed a transient mild episcleral inflammation at the PJD site in some eyes.40

214

	100	P<0.001
months)	90
	80
	70
(12	70
(12	60				P=0.193
loss	60				P=0.193
loss	50				P=0.43
VA	50
VA
3 lines	40
3 lines	30
<	30
<
Percent	20
Percent	10
	0	ANCHOR-	ANCHOR-	C-01-99-	C-01-99-	C-01-99-
		ANCHOR-	ANCHOR-	C-01-99-	C-01-99-	C-01-99-
		PDT	RAN 0.5 mg	PDT	AA 15 mg	AA 15 mg
						(adjusted)

Figure 31.10 Side-by-side comparison of the percentage of eyes avoiding moderate (3 lines) visual acuity loss in a trial of photodynamic therapy (PDT) versus ranibizumab (ANCHOR39) and a trial of PDT versus anecortave acetate (AA) (C-01-9931). For the latter, data on the AA group are shown for all subjects and for the subgroup (adjusted), excluding those eyes with reflux and/or >6-month treatment interval.

Otherwise slit-lamp biomicroscopy, indirect ophthalmoscopy, IOP measurement and electroretinogram testing revealed no ocular toxicity with various doses and at various timepoints.

Pooled safety data from the major clinical trials of anecortave acetate were reported by Regillo et al.41 With respect to ocular complications, the most frequent adverse events when anecortave acetate was used as either primary therapy (Table 31.2) or adjunctive therapy (Table 31.3) included visual acuity decrease, cataract, and eye pain, among others. None of these ocular adverse events differed significantly in frequency between the anecortave acetate and placebo groups. Particular attention was paid to the incidence of cataract and IOP increase, as both of these are known ocular complication of glucocorticoid therapy. The incidence of cataract was less frequent among 313 subjects receiving anecortave acetate (15%) than among 267 subjects receiving PDT (18%) or 30 subjects receiving vehicle (40%). The incidence of IOP increase was 5.4%, 6.7%, and 0% among those receiving anecortave acetate, PDT, and vehicle, respectively. The most frequent adverse events related to the PJD procedure when anecortave acetate was given as primary therapy included eye pain (8.9%), eye discomfort (4.8%), eye hyperemia (3.2%), and subconjunctival hemorrhage (3.2%). The only serious ocular adverse event reported was retinal detachment in one subject receiving a PJD injection. Based on these data, it was concluded that anecortave acetate does not exhibit glucocorticoid-mediated side-effects and is well tolerated from an ocular standpoint.

SYSTEMIC COMPLICATions AND TOXICITY

Preclinical safety studies in a number of in vitro and in vivo models revealed no toxicity in any organ system, no genotoxicity, no carcinogenicity, and no reproductive toxicity or teratogenicity.40

Table 31.2 Most frequent ocular adverse events in subjects receiving anecortave acetate as primary therapy. Listed are all reported adverse events (top) and treatment-related adverse events (bottom)

Adverse event	Anecortave		PDT		P (15 mg	Vehicle		P (15 mg
	acetate 15 mg		(n = 267)		versus PDT)	(n = 30)		versus
	(n = 313)							vehicle)
All ocular
Visual acuity decrease	108	(34.5%)	92	(34.5%)	0.9904	13 (43.3%)		0.3337
Cataract	47 (15%)		48	(18%)	0.3368	12 (40%)		0.0005
Ocular pain	38 (12.1%)		25	(9.4%)	0.2840	5	(16.7%)	0.5606
Vitreous detachment	27	(8.6%)	1	(0.4%)	<0.0001	3	(10%)	0.7363
Foreign-body sensation	23	(7.3%)	15	(5.6%)	0.4013	3	(10%)	0.4864
Abnormal vision	21	(6.7%)	21	(7.9%)	0.5924	1	(3.3%)	0.7069
Pupil disorder	20	(6.4%)	18	(6.7%)	0.8645	4	(13.3%)	0.1461
IOP increase	17	(5.4%)	18	(6.7%)	0.5089	0	(0%)	0.3805
Treatment-related
ocular
Visual acuity decrease	17	(5.4%)	7	(2.6%)	0.0904	0	(0%)	0.3805
Eye pain	8	(2.6%)	6	(2.2%)	0.8092	1	(3.3%)	0.5657
Cataract	6	(1.9%)	6	(2.2%)	0.7806	2	(6.7)	0.1488
IOP decrease	4	(1.3%)	0	(0%)	0.1284	0	(0%)	1.0000
Foreign-body sensation	3	(1%)	4	(1.5%)	0.7087	1	(3.3%)	0.3077
Eye hyperemia	3	(1%)	2	(0.7%)	1.0000	0	(0%)	1.0000
Ptosis	3	(1%)	1	(0.4%)	0.6284	2	(6.7%)	0.0627
Conjunctival cicatrix	3	(1%)	0	(0%)	0.2534	0	(0%)	1.0000

Adapted from data reported in Regillo CD, D’Amico DJ, Mieler WF, et al. Clinical safety profile of posterior juxtascleral depot administration of anecortave acetate 15 mg suspension as primary therapy or adjunctive therapy with photodynamic therapy for treatment of wet age-related macular degeneration. Surv Ophthalmol 2007;52(Suppl. 1):S70–S78.

PDT, photodynamic therapy; IOP, intraocular pressure.

Diseases Retinal in Mechanisms and Drugs • 4 section

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