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. 2018 May 22;2018(5):CD011977. doi: 10.1002/14651858.CD011977.pub2

Monnet 2009.

Methods Study design: RCT
Study grouping: parallel group, with one eye per participant randomised to one of the interventions
Exclusions after randomisation: Two IOLs in Group 3 (blue‐light filtering IOL group) were placed with one haptic in the capsular bag and one haptic outside the capsular bag; these two participants were also excluded from the final statistical analyses.
Losses to follow‐up: one participant in Group 2 (one of the two non‐blue‐light filtering IOL groups) was lost to follow‐up and was not included in the final statistical analyses.
How missing data were handled: it appears that missing data were excluded from the analysis.
Reported power size calculation? yes
Participants Baseline characteristics
Blue‐light filtering IOL (Group 3)

  • Number of participants: number of people (number of eyes): 19 (19)

  • Sex (number of women/number of men): unclear

  • Age (mean): 72.9 years (unit of error not specified)


Non‐blue‐light filtering IOL1 ‐ MA60AC (Group 1)

  • Number of participants: number of people (number of eyes): 20 (20)

  • Sex (number of women/number of men): 8/12

  • Age (mean): 72.8 years (unit of error not specified)


Non‐blue‐light filtering IOL2 ‐ SA60AT (Group 2)

  • Number of participants: number of people (number of eyes): 20 (20)

  • Sex (number of women/number of men): 11/9

  • Age (mean): 72.6 years (unit of error not specified)


Inclusion criteria: people ≥ 60 years, of either sex, of any race, and scheduled for cataract surgery; in good general and ocular health, willing to attend all postoperative visits, and expected to achieve postoperative visual acuities of 20/40 or better
Exclusion criteria: people with a history of uveitis, uncontrolled diabetes, diabetic retinopathy, Sjogren syndrome, trauma to the operative eye, use of anti‐inflammatory medications for any reason, use of topical prostaglandin analogues for ocular hypertension or glaucoma, bleeding tendencies, congenital ocular abnormality, or a nonfunctioning fellow eye. people with intraoperative complications including capsule tears, significant anterior chamber hyphema, zonule rupture, or out‐of‐the‐bag IOL implantation. people at risk for intraoperative complications by virtue of pseudoexfoliation syndrome or poor pupil dilation (6.0 mm). people having multiple planned procedures (i.e. cataract and trabeculectomy or corneal transplantation), except those having concurrent relaxing keratotomy for astigmatism correction.
Comparison of study groups at baseline: no statistically significant differences between groups in any parameter at baseline, but no data reported for those participants who appear to be excluded from the analyses (n = 1 participant from Group 2, and n = 2 participants from Group 3, but all of Group 2 were included in the demographic data).
Interventions Intervention characteristics
Blue‐light filtering IOL (Group 3)

  • Type of IOL: AcrySof SN60AT (Alcon)


Non‐blue‐light filtering IOL1 ‐ MA60AC (Group 1)

  • Type of IOL: Acrysof MA60AC (Alcon)


Non‐blue‐light filtering IOL2 ‐ SA60AT (Group 2)

  • Type of IOL: Acrysof 60AT (Alcon)
Outcomes Postoperative evaluations were performed at one week, one month and three months. All visits included assessment of distance BCVA after manifest refraction, cells, flare, and adverse events.
The primary objective of the study was to compare postoperative inflammation (presence of anterior chamber cells and flare) between the three IOL models. Anterior chamber cells were initially graded on a 5‐point scale (0‐4); however, because all eyes were graded 0 or 1, except for 1 eye that was graded 2, values were dichotomised into 2 categories: (1) cell or (2) no cell.
Identification Sponsorship source:
Funding sources: not reported
Declaration of interest: no author has a financial or proprietary interest in any material or method mentioned
Country: France
Setting: Service d’Ophtalmologie, Universite ´Paris Descartes Hospital Cochin, Paris, France
Comments:
Date study conducted: not reported
Trial registration number: not reported
Contacting study investigators: study authors not contacted; no additional information used for review
Corresponding author's name: Antoine P. Brezin, MD, PhD
Institution: Universite ´ Paris Descartes, Assistance Publique Hopitaux de Paris, Hopital Cochin, Service d’Ophtalmologie
Email: antoine.brezin@cch.aphp.fr
Corresonding author's address:
Antoine P. Brezin
Universite ´ Paris Descartes, Assistance Publique Hopitaux de ParisHopital Cochin, Service d’Ophtalmologie
27 rue du Faubourg Saint‐Jacques 75014 Paris, France
Notes None
Risk of bias
Bias Authors' judgement Support for judgement
Random sequence generation (selection bias) Unclear risk Quote: "Patients were randomly assigned in a 1:1:1 ratio to receive one of the IOL models according to a randomization list."
Judgement comment: not reported how list was generated. Study is described as “randomised” but with no further details
Allocation concealment (selection bias) Unclear risk Judgement comment: not reported how allocation administered. Study is described as “randomised” but with no further details
Blinding of participants and personnel (performance bias) 
 All outcomes High risk Quote: "single‐center unmasked 3‐month study"
Judgement comment: study is described as "unmasked"
Blinding of outcome assessment (detection bias) 
 All outcomes High risk Quote: "single‐center unmasked 3‐month study"
Judgement comment: study is described as "unmasked"
Incomplete outcome data (attrition bias) 
 All outcomes Low risk Judgement comment: missing data < 20% (i.e. more than 80% follow‐up) and equal follow‐up in the intervention groups
Selective reporting (reporting bias) Unclear risk Judgement comment: no access to protocol or trials registry entry
Other bias Low risk Judgement comment: no other apparent sources of bias