Miljöpåverkan
Brinzolamid
Miljörisk:
Risk för miljöpåverkan av brinzolamid kan inte uteslutas då ekotoxikologiska data saknas.
Nedbrytning:
Det kan inte uteslutas att brinzolamid är persistent, då data saknas.
Bioackumulering:
Brinzolamid har låg potential att bioackumuleras.
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Detaljerad miljöinformation
Environmental Risk Classification
Predicted Environmental Concentration (PEC)
PEC is calculated according to the following formula:
PEC (μg/L) = (A*109*(100-R))/(365*P*V*D*100) = 1.37*10-6 * A * (100 - R) = 1.37*10-6 * 23.7 * 100 = 0.0032 μg/L
Where:
A = 23.6637 kg brinzolamide (total sold amount API in Sweden year 2021, data from IQVIA).
R = 0 % removal rate (due to loss by adsorption to sludge particles, by volatilization, hydrolysis or biodegradation) = 0, if no data is available.
P = number of inhabitants in Sweden = 10 *106
V (L/day) = volume of wastewater per capita and day = 200 (ECHA default) (ECHA 2008)
D = factor for dilution of waste water by surface water flow = 10 (ECHA default) (ECHA 2008)
Predicted No Effect Concentration (PNEC)
Ecotoxicological studies
Algae: no data available
Crustacean (Daphnia magna): no data available
Fish: no data available
Other ecotoxicity data: No data available
PNEC derivation:
No PNEC can be calculated since there is no environmental toxicity data available
Environmental risk classification (PEC/PNEC ratio)
Calculation of a risk ratio is not possible, due to the lack of environmental toxicity data. Therefore, the following phrase is used: "Risk of environmental impact of brinzolamide cannot be ruled out as ecotoxicological data are missing."
According to the European Medicines Agency guideline on environmental risk assessment of medicinal products (EMA/CHMP/SWP/4447/00), use of brinzolamide is unlikely to represent a risk for the environment, because the predicted environmental concentration (PEC) at the time of registration was below the action limit 0.01 μg/L.
Degradation
Biotic degradation
Ready degradability: no data available
Justification of chosen degradation phrase:
As no data on biological degradation is available the following phrase is used: ‘The potential for persistence of brinzolamide cannot be excluded, due to lack of data.’
Bioaccumulation
Partitioning coefficient:
logKow = 0.817 (method unknown) (Alcon Technical Report No. 136:60:0900)
Justification of chosen bioaccumulation phrase:
As log Kow < 4, the following statement is used for Brinzolamide: ‘Brinzolamide has low potential for bioaccumulation.’
Excretion (metabolism)
Following topical or systemic administration, brinzolamide undergoes metabolic reactions that include N-dealkylation, O-dealkylation and oxidation of the N-propyl side chain, all CYP-450 catalyzed reactions. N-desethyl brinzolamide is the major metabolite of brinzolamide in primates and human whole blood and is the only quantifiable metabolite in human whole blood. (Alcon Technical Report No. 025:38570:0596, Alcon Technical Report No. 027:38570:0596, Alcon Technical Report No. 029:38570:0596, Alcon Technical Report No. 037:38570:0796) Studies with radioactive 14C-brinzolamide revealed that after 24 hours following an IV does, that approximately 50-60% of brinzolamide was excreted unchanged from the body and that approximately 42% remained in the blood and the carcass. (Alcon Technical Report No. 014:38570:0496)
PBT/vPvB assessment
Based on screening information, brinzolamide cannot be considered a potential PBT substance as the octanol-water partition coefficient remains significantly below the trigger level for a bioaccumulative substance.
References
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ECHA 2008, European Chemicals Agency. 2008 Guidance on information requirements and chemical safety assessment. http://guidance.echa.europa.eu/docs/guidance_document/information_requirements_en.htm
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EMA 2006, European Medicines Agency. European Medicines Agency guideline on environmental risk assessment of medicinal products (EMA/CHMP/SWP/4447/00). https://www.ema.europa.eu/en/documents/scientific-guideline/guideline-environmental-risk-assessment-medicinal-products-human-use-first-version_en.pdf
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Alcon Technical Report No. 136:60:0900
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Alcon Technical Report No. 025:38570:0596
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Alcon Technical Report No. 027:38570:0596
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Alcon Technical Report No. 029:38570:0596
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Alcon Technical Report No. 037:38570:0796
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Alcon Technical Report No. 014:38570:0496
Timolol
Miljörisk:
Risk för miljöpåverkan av timolol kan inte uteslutas då ekotoxikologiska data saknas.
Nedbrytning:
Det kan inte uteslutas att timolol är persistent, då data saknas.
Bioackumulering:
Timolol har låg potential att bioackumuleras.
Läs mer
Detaljerad miljöinformation
Environmental Risk Classification
Predicted Environmental Concentration (PEC)
PEC is calculated according to the following formula:
PEC (μg/L) = (A*109*(100-R))/(365*P*V*D*100) = 1.37*10-6 * A * (100 - R) = 1.37*10-6 * 2.4 kg * 100 = 0.004142 μg/L = 4.1423 ng/L
Where:
A = 30.2354 kg (sum of 7.1842 kg timolol and 31.5077 kg timolol maleat, equaling 23.0512 kg timolol) (total sold amount API in Sweden year 2022, data from IQVIA).
R = 0 % removal rate (due to loss by adsorption to sludge particles, by volatilization, hydrolysis or biodegradation) = 0, if no data is available.
P = number of inhabitants in Sweden = 10 * 106
V (L/day) = volume of wastewater per capita and day = 200 (ECHA default) (ECHA 2008)
D = factor for dilution of waste water by surface water flow = 10 (ECHA default) (ECHA 2008).
Predicted No Effect Concentration (PNEC)
Ecotoxicological studies
Algae: no data available
Crustacean (Daphnia magna): no data available
Fish: no data available
Other ecotoxicity data: No data available
PNEC derivation:
No PNEC can be calculated since there is no environmental toxicity data available
Environmental risk classification (PEC/PNEC ratio)
Calculation of a risk ratio is not possible, due to the lack of environmental toxicity data. Therefore, the following phrase is used: "Risk of environmental impact of timolol cannot be excluded, since no ecotoxicity data are available."
Degradation
Biotic degradation
Ready degradability: no data available
Justification of chosen degradation phrase:
As no data on biological degradation is available the following phrase is used: The potential for persistence of timolol cannot be excluded, due to lack of data.
Bioaccumulation
Partitioning coefficient:
logKow = 1.8 (method unknown) (Clarkes’s Analysis of Drugs and Poisons, 2017)
Justification of chosen bioaccumulation phrase:
As the logKow remains below the trigger level for a bioaccumlative substance (logKow < 4.0), the following statement is used for timolol: Timolol has low potential for bioaccumulation.
Excretion (metabolism)
Approximately 80% of timolol is metabolized in the liver to inactive metabolites. The unchanged drug and its metabolites are excreted in urine. Only small amounts of the drug are removed by hemodialysis. (AHFS Drug Information, 2017).
PBT/vPvB assessment
Based on screening information, timolol cannot be considered a potential PBT substance as the octanol-water partition coefficient remains below the trigger level for a bioaccumulative substance.
References
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ECHA 2008, European Chemicals Agency. 2008 Guidance on information requirements and chemical safety assessment. http://guidance.echa.europa.eu/docs/guidance_document/information_requirements_en.htm
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Clarkes’s Analysis of Drugs and Poisons, 2017. Medicines Complete. Pharmaceutical Press. https://www.medicinescomplete.com/mc/clarke/current/CLK1616.htm?q=timolol&t=search&ss=text&tot=31&p=1#_hit
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AHFS Drug Information, 2017. Medicines Complete. Pharmaceutical Press.https://www.medicinescomplete.com/mc/ahfs/current/a384029.htm#pkin