Clinical and genetic determinants of chronic visual pathway changes after methanol - induced optic neuropathy: four-year follow-up study

Olga Nurieva; Jaroslav A Hubacek; Pavel Urban; Jiri Hlusicka; Pavel Diblik; Pavel Kuthan; Petr Sklenka; Martin Meliska; Jan Bydzovsky; Jarmila Heissigerova; Katerina Kotikova; Tomas Navratil; Martin Komarc; Zdenek Seidl; Manuela Vaneckova; Lucie Vojtova; Sergey Zakharov

doi:10.1080/15563650.2018.1532083

Clinical and genetic determinants of chronic visual pathway changes after methanol - induced optic neuropathy: four-year follow-up study

Clin Toxicol (Phila). 2019 Jun;57(6):387-397. doi: 10.1080/15563650.2018.1532083. Epub 2018 Nov 17.

Authors

Olga Nurieva¹, Jaroslav A Hubacek², Pavel Urban^{1

3}, Jiri Hlusicka¹, Pavel Diblik⁴, Pavel Kuthan⁴, Petr Sklenka⁴, Martin Meliska⁴, Jan Bydzovsky⁴, Jarmila Heissigerova⁴, Katerina Kotikova¹, Tomas Navratil^{5

6}, Martin Komarc⁷, Zdenek Seidl⁸, Manuela Vaneckova⁸, Lucie Vojtova⁹, Sergey Zakharov¹

Affiliations

¹ a Toxicological Information Centre, Department of Occupational Medicine, First Faculty of Medicine , Charles University and General University Hospital , Prague , Czech Republic.
² b Center for Experimental Medicine , Institute for Clinical and Experimental Medicine , Prague , Czech Republic.
³ c Centre for Industrial Hygiene and Occupational Medicine , National Institute of Public Health , Prague , Czech Republic.
⁴ d Clinic of Ophthalmology, First Faculty of Medicine , Charles University and General University Hospital , Prague , Czech Republic.
⁵ e Department of Biomimetic Electrochemistry , J. Heyrovský Institute of Physical Chemistry of the Czech Academy of Sciences , Prague , Czech Republic.
⁶ f Institute of Medical Biochemistry and Laboratory Medicine, First Faculty of Medicine , Charles University and General University Hospital in Prague , Prague , Czech Republic.
⁷ g Department of Methodology, Faculty of Physical Education and Sport , Charles University , Prague , Czech Republic.
⁸ h Department of Radiology, First Faculty of Medicine , Charles University in Prague and General University Hospital , Prague , Czech Republic.
⁹ i First Faculty of Medicine, Institute of Clinical Biochemistry and Laboratory Diagnostics , Charles University and General University Hospital , Prague , Czech Republic.

PMID: 30451020
DOI: 10.1080/15563650.2018.1532083

Abstract

Context: Methanol poisoning induces acute optic neuropathy with possible long-term visual damage.

Objective: To study the dynamics and key determinants of visual pathway functional changes during 4 years after acute methanol poisoning.

Methods: A total of 42 patients with confirmed methanol poisoning (mean age 45.7 ± 4.4 years) were examined 4.9 ± 0.6, 25.0 ± 0.6, and 49.9 ± 0.5 months after discharge. The following tests were performed: visual evoked potential (VEP), retinal nerve fiber layer (RNFL) measurement, brain magnetic resonance imaging (MRI), complete ocular examination, biochemical tests, and apolipoprotein E (ApoE) genotyping.

Results: Abnormal VEP P1 latency was registered in 18/42 right eyes (OD) and 21/42 left eyes (OS), abnormal N1P1 amplitude in 10/42 OD and OS. Mean P1 latency shortening during the follow-up was 15.0 ± 2.0 ms for 36/42 (86%) OD and 14.9 ± 2.4 ms for 35/42 (83%) OS, with maximum shortening up to 35.0 ms. No significant change of mean N1P1 amplitude was registered during follow-up. A further decrease in N1P1 amplitude ≥1.0 mcV in at least one eye was observed in 17 of 36 patients (47%) with measurable amplitude (mean decrease -1.11 ± 0.83 (OD)/-2.37 ± 0.66 (OS) mcV versus -0.06 ± 0.56 (OD)/-0.83 ± 0.64 (OS) mcV in the study population; both p < .001). ApoE4 allele carriers had lower global and temporal RNFL thickness and longer initial P1 latency compared to the non-carriers (all p < .05). The odds ratio for abnormal visual function was 8.92 (3.00-36.50; 95%CI) for ApoE4 allele carriers (p < .001). The presence of ApoE4 allele was further associated with brain necrotic lesions (r = 0.384; p = .013) and brain hemorrhages (r = 0.395; p = .011).

Conclusions: Improvement of optic nerve conductivity occurred in more than 80% of patients, but evoked potential amplitude tended to decrease during the 4 years of observation. ApoE4 allele carriers demonstrated lower RNFL thickness, longer P1 latency, and more frequent methanol-induced brain damage compared to non-carriers.

Keywords: Toxic optic neuropathy; apolipoprotein E; chronic axonal neurodegeneration; long-term visual sequelae; methanol poisoning; remyelination; visual evoked potential.

MeSH terms

Adult
Apolipoprotein E4 / genetics*
Case-Control Studies
Czech Republic
Evoked Potentials, Visual
Female
Follow-Up Studies
Gene Frequency
Genetic Predisposition to Disease
Humans
Longitudinal Studies
Male
Methanol / poisoning*
Middle Aged
Optic Nerve / drug effects*
Optic Nerve / physiopathology
Optic Nerve Diseases / chemically induced*
Optic Nerve Diseases / diagnosis
Optic Nerve Diseases / genetics
Optic Nerve Diseases / physiopathology
Prognosis
Prospective Studies
Reaction Time
Risk Factors
Time Factors
Vision Disorders / chemically induced*
Vision Disorders / diagnosis
Vision Disorders / genetics
Vision Disorders / physiopathology
Vision, Ocular / drug effects*
Vision, Ocular / genetics

Substances

Apolipoprotein E4
Methanol