HYDROQUINONE
HAZARDTEXT ®
Information to help in the initial response for evaluating chemical incidents
-IDENTIFICATION
SYNONYMS
HYDROQUINONE AIDA ARCTUVIN BENZENE, p-DIHYDROXY- p-BENZENEDIOL 1,4-BENZENEDIOL BENZOHYDROQUINONE BENZOQUINOL BLACK and WHITE BLEACHING CREAM DIAK 5 1,4-DIHYDROXY-BENZEEN (Dutch) 1,4-DIHYDROXYBENZEN (Czech) DIHYDROXYBENZENE p-DIHYDROXYBENZENE 1,4-DIHYDROXYBENZENE 1,4-DIHYDROXY-BENZOL (German) 1,4-DIIDROBENZENE (Italian) p-DIOXOBENZENE p-DIOXYBENZENE ELDOPAQUE ELDOQUIN HE 5 HYDROCHINON (Czech, Polish) HYDROQUINOL HYDROQUINOLE alpha-HYDROQUINONE p-HYDROQUINONE 4-HYDROXYPHENOL p-HYDROXYPHENOL IDROCHINONE (Italian) PHIAQUIN PYROGENTISIC ACID QUINNONE QUINOL beta-QUINOL QUINOLE TECQUINOL TENOX HQ TEQUINOL
IDENTIFIERS
SYNONYM REFERENCE
- (Budavari, 1989; CHRIS , 1990; EPA, 1985; OHM/TADS , 1990; RTECS , 1991)
USES/FORMS/SOURCES
Hydroquinone is a reducing agent (ILO, 1983) and it oxidizes to form QUINONE in air (Clayton & Clayton, 1994). It is used as a photographic developer, antioxidant, stabilizer in paints, fuels, oils, and polymers, as a chemical intermediate, in pharmaceuticals, and as a skin depigmenting agent (HSDB, 1996; (ACGIH, 1992; ILO, 1983; Lewis, 1993).
HYDROQUINONE, also called p-DIHYDROXYBENZENE or p-HYDROXYPHENOL, is a colorless, hexagonal prism solid with a sweet taste (HSDB, 1996). The technical grade is a tan to light gray crystalline solid. It is soluble in 14 parts of water, is freely soluble in chloroform, alcohol, ether, and carbon tetrachloride, and is very soluble in acetone (HSDB, 1996; (ACGIH, 1992). A solution of hydroquinone turns brown in air due to oxidation; the reaction is very rapid under alkaline conditions (Budavari, 1996).
Hydroquinone occurs in cigarette smoke, and in nature as arbutin, the beta-D-glucopyranoside conjugate. Arbutin is found in wheat, pears, coffee and tea; free hydroquinone has been detected in coffee, red wine, wheat cereals, and broccoli (Deisinger et al, 1996). Hydroquinone may occur at concentrations greater than 1 percent in blueberry, red whortleberry, cranberry, or bearberry leaves which may be used in herbal teas (Clayton & Clayton, 1994). Hydroquinone is also a metabolite of benzene(Morimoto et al, 1980)
-CLINICAL EFFECTS
GENERAL CLINICAL EFFECTS
- POTENTIAL HEALTH HAZARDS - EMERGENCY RESPONSE GUIDEBOOK, GUIDE 153 (ERG, 2004)
TOXIC; inhalation, ingestion or skin contact with material may cause severe injury or death. Contact with molten substance may cause severe burns to skin and eyes. Avoid any skin contact. Effects of contact or inhalation may be delayed. Fire may produce irritating, corrosive and/or toxic gases. Runoff from fire control or dilution water may be corrosive and/or toxic and cause pollution.
ACUTE CLINICAL EFFECTS
Hydroquinone is a SEVERE IRRITANT of the skin at concentrations of 5 percent or greater (RTECS). The vapor can cause eye irritation, photophobia, tearing, and corneal ulceration (HSDB, 1996). Hydroquinone is more dangerous to the eye than the more irritating substance, quinone, because tearing is not sufficient to wash away the material and the irritation is not sufficient warning to prevent corneal ulceration (HSDB, 1996). Hydroquinone has caused fatality in at least one case of ingestion (Saito et al, 1994). Ingestions in the range of 5 to 12 grams have been fatal (ACGIH, 1992). Ingestion of hydroquinone in amounts as small as 1 gram can cause tinnitus, nausea, dizziness, a sense of suffocation, vomiting, abdominal cramps, diarrhea, pallor, twitching, headache, breathing difficulty, cyanosis, delirium, and cardiovascular collapse (ILO, 1983) HSDB, 1996). The urine may be a green or brown-green color which darkens upon standing (ILO, 1983; Clayton & Clayton, 1994). Other systemic effects of hydroquinone are liver and kidney damage, bronchopneumonia, and induction of METHEMOGLOBINEMIA (Clayton & Clayton, 1994). Methemoglobinemia may be secondary to hemolysis of red blood cells (Oettel, 1936), but it unclear whether or not methemoglobinemia has been documented in exposed humans. Hydroquinone can generate reactive oxygen species (hydroxyl radicals or the equivalent) in the presence of a copper-redox cycling mechanism, and this reactive oxygen may play a role in its toxicity (Li et al, 1995). Hydroquinone is oxidized to more toxic QUINONE in the body (Clayton & Clayton, 1994). A 5 percent aqueous solution of hydroquinone was absorbed through human skin at the relatively slow rate of 0.52 +/- 0.13 mcg/cm(2)/hour (Barber et al, 1995).
CHRONIC CLINICAL EFFECTS
Hydroquinone did not produce any overt signs of toxicity in subjects who ingested 300 to 500 mg/day for 3 to 5 months (Hathaway et al, 1991). Hydroquinone is a skin sensitizer and can cause dermatitis in humans (Anon, 1986; Hathaway et al, 1991). Repeated skin contact causes depigmentation similar in appearance to vitiligo (Frenk & Loi-Zedda, 1980) because it inhibits synthesis of new melanin pigment (HSDB, 1996). Chronic exposure to hydroquinone dust at airborne concentrations in the range of 10 to 30 mg/m(3) has caused staining of the conjunctiva (ILO, 1983) and alterations in the corneal curvature (Anderson, 1947), as well as pitting and erosion of the corneal surface (HSDB, 1996). These conditions require at least five years of exposure to develop, but may persist for some time after removal from exposure (ACGIH, 1992).
- ANIMAL STUDIES - In a 2-year feeding study in rats, hydroquinone caused aplastic anemia and atrophy of the liver (HSDB, 1996). It has caused photosensitization following ingestion in a dog (HSDB, 1996). Other systemic effects in experimental animals have been anemia, hemolysis, hypoglycemia, and tremors (HSDB, 1996).
-FIRST AID
FIRST AID AND PREHOSPITAL TREATMENT
- EMESIS/ NOT RECOMMENDED -
-MEDICAL TREATMENT
LIFE SUPPORT
- Support respiratory and cardiovascular function.
SUMMARY
- FIRST AID - EMERGENCY RESPONSE GUIDEBOOK, GUIDE 153 (ERG, 2004)
Move victim to fresh air. Call 911 or emergency medical service. Give artificial respiration if victim is not breathing. Do not use mouth-to-mouth method if victim ingested or inhaled the substance; give artificial respiration with the aid of a pocket mask equipped with a one-way valve or other proper respiratory medical device. Administer oxygen if breathing is difficult. Remove and isolate contaminated clothing and shoes. In case of contact with substance, immediately flush skin or eyes with running water for at least 20 minutes. For minor skin contact, avoid spreading material on unaffected skin. Keep victim warm and quiet. Effects of exposure (inhalation, ingestion or skin contact) to substance may be delayed. Ensure that medical personnel are aware of the material(s) involved and take precautions to protect themselves.
INHALATION EXPOSURE - Carefully observe patients with inhalation exposure for the development of any systemic signs or symptoms and administer symptomatic treatment as necessary. ACUTE LUNG INJURY: Maintain ventilation and oxygenation and evaluate with frequent arterial blood gases and/or pulse oximetry monitoring. Early use of PEEP and mechanical ventilation may be needed. SEIZURES: Administer a benzodiazepine; DIAZEPAM (ADULT: 5 to 10 mg IV initially; repeat every 5 to 20 minutes as needed. CHILD: 0.1 to 0.5 mg/kg IV over 2 to 5 minutes; up to a maximum of 10 mg/dose. May repeat dose every 5 to 10 minutes as needed) or LORAZEPAM (ADULT: 2 to 4 mg IV initially; repeat every 5 to 10 minutes as needed, if seizures persist. CHILD: 0.05 to 0.1 mg/kg IV over 2 to 5 minutes, up to a maximum of 4 mg/dose; may repeat in 5 to 15 minutes as needed, if seizures continue). Consider phenobarbital or propofol if seizures recur after diazepam 30 mg (adults) or 10 mg (children greater than 5 years). Monitor for hypotension, dysrhythmias, respiratory depression, and need for endotracheal intubation. Evaluate for hypoglycemia, electrolyte disturbances, and hypoxia.
METHEMOGLOBINEMIA: Determine the methemoglobin concentration and evaluate the patient for clinical effects of methemoglobinemia (ie, dyspnea, headache, fatigue, CNS depression, tachycardia, metabolic acidosis). Treat patients with symptomatic methemoglobinemia with methylene blue (this usually occurs at methemoglobin concentrations above 20% to 30%, but may occur at lower methemoglobin concentrations in patients with anemia, or underlying pulmonary or cardiovascular disorders). Administer oxygen while preparing for methylene blue therapy. METHYLENE BLUE: INITIAL DOSE/ADULT OR CHILD: 1 mg/kg IV over 5 to 30 minutes; a repeat dose of up to 1 mg/kg may be given 1 hour after the first dose if methemoglobin levels remain greater than 30% or if signs and symptoms persist. NOTE: Methylene blue is available as follows: 50 mg/10 mL (5 mg/mL or 0.5% solution) single-dose ampules and 10 mg/1 mL (1% solution) vials. Additional doses may sometimes be required. Improvement is usually noted shortly after administration if diagnosis is correct. Consider other diagnoses or treatment options if no improvement has been observed after several doses. If intravenous access cannot be established, methylene blue may also be given by intraosseous infusion. Methylene blue should not be given by subcutaneous or intrathecal injection. NEONATES: DOSE: 0.3 to 1 mg/kg. Concomitant use of methylene blue with serotonergic drugs, including serotonin reuptake inhibitors (SRIs), selective serotonin reuptake inhibitors (SSRIs), serotonin and norepinephrine reuptake inhibitors (SNRIs), tricyclic antidepressants (TCAs), norepinephrine-dopamine reuptake inhibitors (NDRIs), triptans, and ergot alkaloids may increase the risk of potentially fatal serotonin syndrome.
EYE EXPOSURE - DECONTAMINATION: Remove contact lenses and irrigate exposed eyes with copious amounts of room temperature 0.9% saline or water for at least 15 minutes. If irritation, pain, swelling, lacrimation, or photophobia persist after 15 minutes of irrigation, the patient should be seen in a healthcare facility.
DERMAL EXPOSURE - ORAL EXPOSURE - Although not as irritating as phenol, dilution with water or milk is indicated. Because of possible esophageal or gastrointestinal tract irritation or burns following ingestion, emesis should not be induced. DILUTION: If no respiratory compromise is present, administer milk or water as soon as possible after ingestion. Dilution may only be helpful if performed in the first seconds to minutes after ingestion. The ideal amount is unknown; no more than 8 ounces (240 mL) in adults and 4 ounces (120 mL) in children is recommended to minimize the risk of vomiting.
ACTIVATED CHARCOAL: Administer charcoal as a slurry (240 mL water/30 g charcoal). Usual dose: 25 to 100 g in adults/adolescents, 25 to 50 g in children (1 to 12 years), and 1 g/kg in infants less than 1 year old. SEIZURES: Administer a benzodiazepine; DIAZEPAM (ADULT: 5 to 10 mg IV initially; repeat every 5 to 20 minutes as needed. CHILD: 0.1 to 0.5 mg/kg IV over 2 to 5 minutes; up to a maximum of 10 mg/dose. May repeat dose every 5 to 10 minutes as needed) or LORAZEPAM (ADULT: 2 to 4 mg IV initially; repeat every 5 to 10 minutes as needed, if seizures persist. CHILD: 0.05 to 0.1 mg/kg IV over 2 to 5 minutes, up to a maximum of 4 mg/dose; may repeat in 5 to 15 minutes as needed, if seizures continue). Consider phenobarbital or propofol if seizures recur after diazepam 30 mg (adults) or 10 mg (children greater than 5 years). Monitor for hypotension, dysrhythmias, respiratory depression, and need for endotracheal intubation. Evaluate for hypoglycemia, electrolyte disturbances, and hypoxia.
METHEMOGLOBINEMIA: Determine the methemoglobin concentration and evaluate the patient for clinical effects of methemoglobinemia (ie, dyspnea, headache, fatigue, CNS depression, tachycardia, metabolic acidosis). Treat patients with symptomatic methemoglobinemia with methylene blue (this usually occurs at methemoglobin concentrations above 20% to 30%, but may occur at lower methemoglobin concentrations in patients with anemia, or underlying pulmonary or cardiovascular disorders). Administer oxygen while preparing for methylene blue therapy. METHYLENE BLUE: INITIAL DOSE/ADULT OR CHILD: 1 mg/kg IV over 5 to 30 minutes; a repeat dose of up to 1 mg/kg may be given 1 hour after the first dose if methemoglobin levels remain greater than 30% or if signs and symptoms persist. NOTE: Methylene blue is available as follows: 50 mg/10 mL (5 mg/mL or 0.5% solution) single-dose ampules and 10 mg/1 mL (1% solution) vials. Additional doses may sometimes be required. Improvement is usually noted shortly after administration if diagnosis is correct. Consider other diagnoses or treatment options if no improvement has been observed after several doses. If intravenous access cannot be established, methylene blue may also be given by intraosseous infusion. Methylene blue should not be given by subcutaneous or intrathecal injection. NEONATES: DOSE: 0.3 to 1 mg/kg. Concomitant use of methylene blue with serotonergic drugs, including serotonin reuptake inhibitors (SRIs), selective serotonin reuptake inhibitors (SSRIs), serotonin and norepinephrine reuptake inhibitors (SNRIs), tricyclic antidepressants (TCAs), norepinephrine-dopamine reuptake inhibitors (NDRIs), triptans, and ergot alkaloids may increase the risk of potentially fatal serotonin syndrome.
-RANGE OF TOXICITY
MINIMUM LETHAL EXPOSURE
One gram in an adult has caused symptoms, and death has occured after 5 g (Merck Index, 1984). Fatal acute cases have been in the 5 to 12 g range (Deichmann & Keplinger, 1981).
MAXIMUM TOLERATED EXPOSURE
- Carcinogenicity Ratings for CAS123-31-9 :
ACGIH (American Conference of Governmental Industrial Hygienists, 2010): A3 ; Listed as: Hydroquinone A3 :Confirmed Animal Carcinogen with Unknown Relevance to Humans: The agent is carcinogenic in experimental animals at a relatively high dose, by route(s) of administration, at site(s), of histologic type(s), or by mechanism(s) that may not be relevant to worker exposure. Available epidemiologic studies do not confirm an increased risk of cancer in exposed humans. Available evidence does not suggest that the agent is likely to cause cancer in humans except under uncommon or unlikely routes or levels of exposure.
EPA (U.S. Environmental Protection Agency, 2011): Not Assessed under the IRIS program. ; Listed as: Hydroquinone IARC (International Agency for Research on Cancer (IARC), 2016; International Agency for Research on Cancer, 2015; IARC Working Group on the Evaluation of Carcinogenic Risks to Humans, 2010; IARC Working Group on the Evaluation of Carcinogenic Risks to Humans, 2010a; IARC Working Group on the Evaluation of Carcinogenic Risks to Humans, 2008; IARC Working Group on the Evaluation of Carcinogenic Risks to Humans, 2007; IARC Working Group on the Evaluation of Carcinogenic Risks to Humans, 2006; IARC, 2004): 3 ; Listed as: Hydroquinone 3 : The agent (mixture or exposure circumstance) is not classifiable as to its carcinogenicity to humans. This category is used most commonly for agents, mixtures and exposure circumstances for which the evidence of carcinogenicity is inadequate in humans and inadequate or limited in experimental animals. Exceptionally, agents (mixtures) for which the evidence of carcinogenicity is inadequate in humans but sufficient in experimental animals may be placed in this category when there is strong evidence that the mechanism of carcinogenicity in experimental animals does not operate in humans. Agents, mixtures and exposure circumstances that do not fall into any other group are also placed in this category.
NIOSH (National Institute for Occupational Safety and Health, 2007): Not Listed ; Listed as: Hydroquinone MAK (DFG, 2002): Category 2 ; Listed as: Hydroquinone NTP (U.S. Department of Health and Human Services, Public Health Service, National Toxicology Project ): Not Listed
TOXICITY AND RISK ASSESSMENT VALUES
- EPA Risk Assessment Values for CAS123-31-9 (U.S. Environmental Protection Agency, 2011):
Oral: Inhalation: Drinking Water:
References: RTECS, 1991 LD50- (ORAL)CAT: LD50- (ORAL)DOG: LD50- (ORAL)GUINEA_PIG: LD50- (INTRAPERITONEAL)MOUSE: LD50- (ORAL)MOUSE: LD50- (SUBCUTANEOUS)MOUSE: LD50- (INTRAPERITONEAL)RABBIT: LD50- (ORAL)RABBIT: LD50- (INTRAPERITONEAL)RAT: LD50- (INTRAVENOUS)RAT: LD50- (ORAL)RAT: LDLo- (SUBCUTANEOUS)CAT: LDLo- (INTRAVENOUS)DOG: LDLo- (INTRAPERITONEAL)GUINEA_PIG: LDLo- (SUBCUTANEOUS)GUINEA_PIG: LDLo- (ORAL)HUMAN: LDLo- (SUBCUTANEOUS)RAT: TDLo- (ORAL)HUMAN:
-STANDARDS AND LABELS
WORKPLACE STANDARDS
- ACGIH TLV Values for CAS123-31-9 (American Conference of Governmental Industrial Hygienists, 2010):
Editor's Note: The listed values are recommendations or guidelines developed by ACGIH(R) to assist in the control of health hazards. They should only be used, interpreted and applied by individuals trained in industrial hygiene. Before applying these values, it is imperative to read the introduction to each section in the current TLVs(R) and BEI(R) Book and become familiar with the constraints and limitations to their use. Always consult the Documentation of the TLVs(R) and BEIs(R) before applying these recommendations and guidelines.
- AIHA WEEL Values for CAS123-31-9 (AIHA, 2006):
- NIOSH REL and IDLH Values for CAS123-31-9 (National Institute for Occupational Safety and Health, 2007):
Listed as: Hydroquinone REL: TWA: STEL: Ceiling: 2 mg/m(3) [15-minute] Carcinogen Listing: (Not Listed) Not Listed Skin Designation: Not Listed Note(s):
IDLH: IDLH: 50 mg/m3 Note(s): Not Listed
- OSHA PEL Values for CAS123-31-9 (U.S. Occupational Safety, and Health Administration (OSHA), 2010):
- OSHA List of Highly Hazardous Chemicals, Toxics, and Reactives for CAS123-31-9 (U.S. Occupational Safety and Health Administration, 2010):
ENVIRONMENTAL STANDARDS
- EPA CERCLA, Hazardous Substances and Reportable Quantities for CAS123-31-9 (U.S. Environmental Protection Agency, 2010):
- EPA CERCLA, Hazardous Substances and Reportable Quantities, Radionuclides for CAS123-31-9 (U.S. Environmental Protection Agency, 2010):
- EPA RCRA Hazardous Waste Number for CAS123-31-9 (U.S. Environmental Protection Agency, 2010b):
- EPA SARA Title III, Extremely Hazardous Substance List for CAS123-31-9 (U.S. Environmental Protection Agency, 2010):
Listed as: Hydroquinone Reportable Quantity, in pounds: 100 Threshold Planning Quantity, in pounds: Note(s): f f: Chemicals on the original list that do not meet toxicity criteria but because of their acute lethality, high production volume and known risk are considered chemicals of concern ("Other chemicals"). (November 17, 1986, and February 15, 1990.)
- EPA SARA Title III, Community Right-to-Know for CAS123-31-9 (40 CFR 372.65, 2006; 40 CFR 372.28, 2006):
- DOT List of Marine Pollutants for CAS123-31-9 (49 CFR 172.101 - App. B, 2005):
- EPA TSCA Inventory for CAS123-31-9 (EPA, 2005):
SHIPPING REGULATIONS
- DOT -- Table of Hazardous Materials and Special Provisions for UN/NA Number 2662 (49 CFR 172.101, 2005):
- DOT -- Table of Hazardous Materials and Special Provisions for UN/NA Number 3435 (49 CFR 172.101, 2005):
- ICAO International Shipping Name for UN2662 (ICAO, 2002):
- ICAO International Shipping Name for UN3435 (ICAO, 2002):
LABELS
- NFPA Hazard Ratings for CAS123-31-9 (NFPA, 2002):
Listed as: Hydroquinone Hazard Ratings: Health Rating (Blue): 2 Flammability Rating (Red): 1 Instability Rating (Yellow): 0 Oxidizer/Water-Reactive Designation: Not Listed
-PERSONAL PROTECTION
SUMMARY
- RECOMMENDED PROTECTIVE CLOTHING - EMERGENCY RESPONSE GUIDEBOOK, GUIDE 153 (ERG, 2004)
Wear positive pressure self-contained breathing apparatus (SCBA). Wear chemical protective clothing that is specifically recommended by the manufacturer. It may provide little or no thermal protection. Structural firefighters' protective clothing provides limited protection. fire situations ONLY; it is not effective in spill situations where direct contact with the substance is possible.
RESPIRATORY PROTECTION
- Refer to "Recommendations for respirator selection" in the NIOSH Pocket Guide to Chemical Hazards on TOMES Plus(R) for respirator information.
PROTECTIVE CLOTHING
- CHEMICAL PROTECTIVE CLOTHING. Search results for CAS 123-31-9.
-PHYSICAL HAZARDS
FIRE HAZARD
- FLAMMABILITY CLASSIFICATION
- NFPA Flammability Rating for CAS123-31-9 (NFPA, 2002):
Listed as: Hydroquinone Flammability Rating: 1
- FIRE CONTROL/EXTINGUISHING AGENTS
- SMALL FIRE PRECAUTIONS - EMERGENCY RESPONSE GUIDEBOOK, GUIDE 153 (ERG, 2004)
- LARGE FIRE PRECAUTIONS - EMERGENCY RESPONSE GUIDEBOOK, GUIDE 153 (ERG, 2004)
Dry chemical, CO2, alcohol-resistant foam or water spray. Move containers from fire area if you can do it without risk. Dike fire control water for later disposal; do not scatter the material.
- TANK OR CAR/TRAILER LOAD FIRE PRECAUTIONS - EMERGENCY RESPONSE GUIDEBOOK, GUIDE 153 (ERG, 2004)
Fight fire from maximum distance or use unmanned hose holders or monitor nozzles. Do not get water inside containers. Cool containers with flooding quantities of water until well after fire is out. Withdraw immediately in case of rising sound from venting safety devices or discoloration of tank. ALWAYS stay away from tanks engulfed in fire.
- NFPA Extinguishing Methods for CAS123-31-9 (NFPA, 2002):
EXPLOSION HAZARD
- Reacts violently with sodium hydroxide.
REACTIVITY HAZARD
- Reacts with oxidizing materials.
EVACUATION PROCEDURES
- Editor's Note: This material is not listed in the Table of Initial Isolation and Protective Action Distances.
- SPILL - PUBLIC SAFETY EVACUATION DISTANCES - EMERGENCY RESPONSE GUIDEBOOK, GUIDE 153 (ERG, 2004)
Increase, in the downwind direction, as necessary, the isolation distance of at least 50 meters (150 feet) for liquids and at least 25 meters (75 feet) for solids in all directions.
- FIRE - PUBLIC SAFETY EVACUATION DISTANCES - EMERGENCY RESPONSE GUIDEBOOK, GUIDE 153 (ERG, 2004)
If tank, rail car or tank truck is involved in a fire, ISOLATE for 800 meters (1/2 mile) in all directions; also, consider initial evacuation for 800 meters (1/2 mile) in all directions.
- PUBLIC SAFETY MEASURES - EMERGENCY RESPONSE GUIDEBOOK, GUIDE 153 (ERG, 2004)
CALL Emergency Response Telephone Number on Shipping Paper first. If Shipping Paper not available or no answer, refer to appropriate telephone number: MEXICO: SETIQ: 01-800-00-214-00 in the Mexican Republic; For calls originating in Mexico City and the Metropolitan Area: 5559-1588; For calls originating elsewhere, call: 011-52-555-559-1588.
CENACOM: 01-800-00-413-00 in the Mexican Republic; For calls originating in Mexico City and the Metropolitan Area: 5550-1496, 5550-1552, 5550-1485, or 5550-4885; For calls originating elsewhere, call: 011-52-555-550-1496, or 011-52-555-550-1552; 011-52-555-550-1485, or 011-52-555-550-4885.
ARGENTINA: CIQUIME: 0-800-222-2933 in the Republic of Argentina; For calls originating elsewhere, call: +54-11-4613-1100.
BRAZIL: PRÓ-QUÍMICA: 0-800-118270 (Toll-free in Brazil); For calls originating elsewhere, call: +55-11-232-1144 (Collect calls are accepted).
COLUMBIA: CISPROQUIM: 01-800-091-6012 in Colombia; For calls originating in Bogotá, Colombia, call: 288-6012; For calls originating elsewhere, call: 011-57-1-288-6012.
CANADA: UNITED STATES:
For additional details see the section entitled "WHO TO CALL FOR ASSISTANCE" under the ERG Instructions. As an immediate precautionary measure, isolate spill or leak area in all directions for at least 50 meters (150 feet) for liquids and at least 25 meters (75 feet) for solids. Keep unauthorized personnel away. Stay upwind. Keep out of low areas. Ventilate enclosed areas.
- AIHA ERPG Values for CAS123-31-9 (AIHA, 2006):
- DOE TEEL Values for CAS123-31-9 (U.S. Department of Energy, Office of Emergency Management, 2010):
Listed as Hydroquinone TEEL-0 (units = mg/m3): 2 TEEL-1 (units = mg/m3): 3 TEEL-2 (units = mg/m3): 20 TEEL-3 (units = mg/m3): 50 Definitions: TEEL-0: The threshold concentration below which most people will experience no adverse health effects. TEEL-1: The airborne concentration (expressed as ppm [parts per million] or mg/m(3) [milligrams per cubic meter]) of a substance above which it is predicted that the general population, including susceptible individuals, could experience notable discomfort, irritation, or certain asymptomatic, nonsensory effects. However, these effects are not disabling and are transient and reversible upon cessation of exposure. TEEL-2: The airborne concentration (expressed as ppm or mg/m(3)) of a substance above which it is predicted that the general population, including susceptible individuals, could experience irreversible or other serious, long-lasting, adverse health effects or an impaired ability to escape. TEEL-3: The airborne concentration (expressed as ppm or mg/m(3)) of a substance above which it is predicted that the general population, including susceptible individuals, could experience life-threatening adverse health effects or death.
- AEGL Values for CAS123-31-9 (National Research Council, 2010; National Research Council, 2009; National Research Council, 2008; National Research Council, 2007; NRC, 2001; NRC, 2002; NRC, 2003; NRC, 2004; NRC, 2004; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2006; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2007; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2005; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2005; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2007; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2006; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2006; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2006; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2006; 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National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2008; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2009; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2008; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2008; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2008; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2009; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2008; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2008; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2008; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2008; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2008; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2008; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2008; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2007; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2006; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2006; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2006; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2007; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2007; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2007; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2007; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2007; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2005; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2005; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2005; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2005; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2005; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2005; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2005; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2005; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2007; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2005; National Advisory Committee for Acute Exposure Guideline Levels for Hazardous Substances, 2006; 62 FR 58840, 1997; 65 FR 14186, 2000; 65 FR 39264, 2000; 65 FR 77866, 2000; 66 FR 21940, 2001; 67 FR 7164, 2002; 68 FR 42710, 2003; 69 FR 54144, 2004):
- NIOSH IDLH Values for CAS123-31-9 (National Institute for Occupational Safety and Health, 2007):
IDLH: 50 mg/m3 Note(s): Not Listed
CONTAINMENT/WASTE TREATMENT OPTIONS
SPILL OR LEAK PRECAUTIONS - EMERGENCY RESPONSE GUIDEBOOK, GUIDE 153 (ERG, 2004) ELIMINATE all ignition sources (no smoking, flares, sparks or flames in immediate area). Do not touch damaged containers or spilled material unless wearing appropriate protective clothing. Stop leak if you can do it without risk. Prevent entry into waterways, sewers, basements or confined areas. Absorb or cover with dry earth, sand or other non-combustible material and transfer to containers. DO NOT GET WATER INSIDE CONTAINERS.
RECOMMENDED PROTECTIVE CLOTHING - EMERGENCY RESPONSE GUIDEBOOK, GUIDE 153 (ERG, 2004) Wear positive pressure self-contained breathing apparatus (SCBA). Wear chemical protective clothing that is specifically recommended by the manufacturer. It may provide little or no thermal protection. Structural firefighters' protective clothing provides limited protection. fire situations ONLY; it is not effective in spill situations where direct contact with the substance is possible.
PHYSICAL TREATMENT: A method was developed that used "salting out" as a technique to remove phenol and hydroquinone from aqueous solution. The method used the combination of an organic solvent and inorganic salt to extract the chemicals (Jones et al, 1993).
Liquid can be atomized into an incinerator for disposal. It may be necessary to mix with a more flammable solvent (OHM/TADS , 1990). Solid should be packaged in paper or other flammable material and incinerated. Alternatively, the solid may be dissolved in a flammable solvent and incinerated (OHM/TADS , 1990).
-ENVIRONMENTAL HAZARD MANAGEMENT
POLLUTION HAZARD
- Runoff from fire control or dilution water may cause pollution.
ABIOTIC DEGRADATION
- No information found at the time of this review.
BIODEGRADATION
- The BOD for hydroquinone is 53%; for 5 days is 25%; for 0.5 days as catechol (CHRIS , 1990).
- Hydroquinone is subject to biodegradation (OHM/TADS , 1990).
BIOACCUMULATION
ENVIRONMENTAL TOXICITY
- No information found at the time of this review.
-PHYSICAL/CHEMICAL PROPERTIES
MOLECULAR WEIGHT
DESCRIPTION/PHYSICAL STATE
- Hydroquinone occurs as colorless or white to light tan or gray odorless crystals with a sweet taste (EPA, 1985; CHRIS , 1990; Deichmann & Keplinger, 1981).
VAPOR PRESSURE
- 4 mmHg (at 150 degrees C) (EPA, 1985)
DENSITY
- OTHER TEMPERATURE AND/OR PRESSURE
- TEMPERATURE AND/OR PRESSURE NOT LISTED
FREEZING/MELTING POINT
BOILING POINT
- 285-287 degrees C; 545-549 degrees F (EPA, 1985)
FLASH POINT
- 329 degrees F (closed cup) (HSDB , 1990)
SOLUBILITY
ALCOHOL: Soluble (HSDB , 1990) ETHER: Soluble (HSDB , 1990) ACETONE: Very soluble (HSDB , 1990) CARBON TETRACHLORIDE: Very soluble (HSDB , 1990)
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