UNITED STATES ENVIRONMENTAL PROTECTION AGENCY WASHINGTON, D.C. 20460 Office of Prevention, Pesticides and Toxic Substances MEMORANDUM SUBJECT: Lindane; Chemical No. 009001. Revised Assessment of Risk from Use of Lindane for Treatment of Lice and Scabies
DP Barcode: D284188; Submission No. S605841Reregistration Case #: 0315
Becky DaissEnvironmental Health ScientistReregistration Branch 4Health Effects Division (7509C)
THROUGH: Susan Hummel
Branch Senior ScientistReregistration Branch 4Health Effects Division (7509C)
Mark HowardReregistration Branch 3Special Review & Reregistration Division (7508C)
This provides HED’s revised assessment of risk from use of lindane for treatment of
scabies and lice. The revised assessment incorporates additional information and commentsprovided by the Food and Drug Administration (FDA). ASSESSMENT OF RISK FROM USE OF LINDANE TO TREAT SCABIES
HED’s assessment of risk from use of lindane to treat scabies uses data from both animal
and human studies and provides a range of risk estimates. EPA conducted analyses using: 1) aMargin of Exposure (MOE) approach based on animal toxicity data, and 2) a comparison oflindane blood levels from one study which documents cases of accidental lindane ingestion bytoddlers in which blood levels were determined after ingestion, and a second study whichprovides data on blood levels of lindane following application of lindane to treat scabies. HEDbased its assessment on directions provided in the current label for scabies treatment. It isimportant to note, however, that FDA is planning to make a number of changes to the labelincluding statements that restrict the use to patients who have attained adult stature (i.e., > 60 kgbody weight). Therefore, HED also considered pending label changes in its assessment of lindaneas a scabies treatment.
Under this approach, an estimated MOE is calculated based on a toxicological endpoint
recommended by HED’s Hazard Identification and Assessment Committee (HIARC) andcompared with the target MOE for short-term dermal exposure/risk to determine whether there isan exposure of concern. The MOE is the ratio of the appropriate No Observed Adverse EffectLevel (NOAEL) to estimated exposure. For the short-term dermal endpoint, a NOAEL of 6mg/kg/day was selected from an acute oral neurotoxicity study in rats. For residential exposures,uncertainty factors are used to determine target MOEs. The target MOE for exposure to lindanefrom pharmaceutical use is 100 based on uncertainty factors (UF) used to account for differencesamong humans (intraspecies variability - UF of 10), and for differences between the test animalsand humans (interspecies extrapolation - UF of 10).
Since the NOAEL is based on an oral toxicity study, dermal absorption data are required
to adjust the oral dose. Two different dermal absorption factors were used to calculate estimatedexposure. One was taken from a 1989 article published in Journal of Toxicological andEnvironmental Health, which reported data from a dermal absorption study on rhesus monkeys todetermine if lindane applied for treatment of lice and scabies is absorbed into the blood stream (1). A second was taken from a study in Toxicology and Applied Pharmacology, 1974, in whichlindane was tested on human subjects to quantify dermal penetration (2).
The monkey study involved topical application of 1% lotion, at label prescribed rates, to
the forehead, forearm, or forepaw of monkeys for 24 hours. Percent absorption was determinedbased on urinary excretion of 14C-lindane. Study results indicated that 18, 34, and 54% of theapplied dose was absorbed after application to the forearm, forehead, and palm, respectively. Aweighted average of 20% was derived based on the body surface area corresponding to theapplicable dermal absorption factor from the monkey study.
For the human study, C14-labeled lindane was applied topically (4µg/cm2) to the forearm
and via the intravenous route (1µCi). Excretion of the chemical was then monitored by collecting
and analyzing urine samples during the 5 day testing period. All results were calculated as percentof the injected or applied dose. Data from the IV dosing was used to correct the skin penetrationdata for incomplete urinary recovery. Lindane was shown to have a dermal penetration factor of9.3% ± 3.7 (SD).
Results of the scabies MOE assessment for children and young adults using both monkey
and human dermal absorption data are provided in Tables 1 and 2 respectively. The analysisindicates MOEs of concern (MOE<100) from both high and low-end treatment scenarios. Table 1. Assessment of Use of Lindane for Scabies - DAF from Product Specific Monkey Study
daily dermal dose (mg/kg/day) x dermal absorption factor (%)
Daily Dermal Dose = applied dose (mg) ÷ body weight (kg)Applied Dose = 20-60g of 1% lotion (high-end); 10-30 g of 1% lotion (low-end) depending on age groupDermal Absorption Factor = 20% (weighted avg)
Palm Dermal Absorption Factor = 54% -- DAF from monkey study; Used for hands which are assumed to be 6% ofDosed Body Surface Area based on % of Surface Area/Body Part from EPA Exposure Factor Handbook (EFH)Vol IForearm Dermal Absorption Factor = 18% -- DAF from monkey study; Used for 94% of Dosed Body Surface Area(all but hands) based on % of Total Surface Area/Body Part from EPA EFH Vol IDosed Body Surface Area = entire body from neck down
Table 2. Assessment of Lindane for Scabies - DAF from Pesticide Exposure in Human Study
daily dermal dose (mg/kg/day) x dermal absorption factor (%)
Daily Dermal Dose = applied dose (mg) ÷ body weight (kg)Applied Dose = 20-60 g of 1% lotion (high-end); 10-30 g of 1% lotion (low-end) depending on age groupDermal Absorption Factor = 10% from human pesticide application dermal absorption study
1 Application rates are based on pending label for young adults and current label/estimated body sizes for small children. 2 Young adult BW is based on pending label changes. Child and toddler BW is avg from EPA EFH3 Does not include an FQPA safety factor which, if applied, would increase the Target MOE to 300 for infants and children
Uncertainties Associated with the MOE AssessmentToxicity Endpoint - The toxicity endpoint used in the MOE assessment is based on an
acute oral neurotoxicity study where the test material was administered by gavage. An oralgavage dose may be absorbed more rapidly than the dermal dose, producing a higher peakconcentration of lindane in the blood and target tissues than a dermal dose. Use of a toxicityendpoint based on an oral dose (adjusted to reflect 10% or 20% dermal absorption) may thereforeoverestimate toxicity from a dermal dose.
Since adult animals were used in the acute oral study and children are more susceptible to
exposure than adults, use of a toxicity endpoint based on the acute study may underestimate risksto children who are exposed to lindane. Dermal Absorption - HED calculated MOEs assuming 20% and 10% dermal absorption.
The 20% absorption value is derived from a study of the absorption of the scabies lotion appliedto monkeys. The lotion was left on for 24 hours in the monkey assessment and therefore mayoverestimate dermal absorption for scabies treatment, which has a 12 hour exposure duration limitbased on label restrictions. In addition, monkeys may not absorb the scabies lotion in the samemanner as humans. The 10% absorption values is from a study of absorption of pesticides appliedto humans. Humans may absorb the pesticide and lotion formulations at different rates. Sincethere are no data to evaluate the relative absorption of the scabies lotion by monkeys vs. humansor the relative absorption by humans of the pesticide vs. scabies lotion, it is not possible to assesswhether these dermal absorption factors tend to overstate or understate potential risk. However,use of both studies provides a range of dermal absorption and probably provides an adequatebounding of potential exposure. Anticipated Label Changes - According to the FDA, the label for the 1% scabies
treatment lotion will be revised to restrict use to, “patients who have attained adult stature, orapproximately 60 kg”. The label will also be revised to recommend only that a thin layer of lotionbe applied. The current label prescribes the following; “Use only enough to cover the body in athin layer. 1 ounce (half a 2 ounce container) should be all that is needed for children under 6years of age: 1-2 ounces for older children and adults”. HED conducted its scabies MOEassessment based on directions provided in the current label. Given anticipated label changes, usein accordance with the revised label would eliminate risks to young children (less than 60 kg). Also, according to FDA, pending label changes to the amount of lotion required should result inlower application rates for both older children and adults.
HED also analyzed potential risk from lindane used as a scabies treatment based on data
on lindane blood levels provided in two published literature studies. One study documents casesof accidental lindane ingestion by toddlers in which blood levels were determined after ingestion. The second study provides data on blood levels of lindane in children after application of 1%
lindane lotion to treat scabies. The blood level associated with acute accidental ingestion whichresulted in short-term adverse effects according to the accidental ingestion case study is 0.32ug/mL. The highest measured blood concentration from the clinical study of levels associated withprescribed uses of lindane to treat scabies was 0.064 ug/mL. The studies are described in moredetail below. Acute Accidental Lindane Ingestion
Case reports published in the November, 1995, edition of the Annals of EmergencyMedicine provide data on blood levels, adverse effects, and time and level of recovery resultingfrom acute accidental lindane ingestion in toddlers.(3) As noted in the Annals publication, mostcases reported in the literature involve dermal lindane toxicity; ingestion toxicity is infrequentlydocumented and data on blood levels associated with ingestion are rare. The article presentsthree cases in which blood levels were obtained and documented after ingestion. The highestlindane blood concentrations documented in the case studies in which the patient exhibited fullrecovery was 0.32 ug/mL (Case 1). This case involved a 13 month old boy who accidentlyingested part of the contents of a bottle of Kwell lotion. The following description of Case 1 isexcerpted from the 1995 article.
In this case, a 13 month old boy was brought to a local emergency departmentafter being found with an open bottle of Kwell lotion. He was described as glassyeyed, he vomited twice, and had a generalized tonic-clonic seizure. The child wastransported to the hospital where he was somnolent. Shortly after arrival, he hadanother seizure. He was treated and laboratory analyses were conducted.
Blood lindane concentrations were determined with the method of Dale et al inaccordance with Environmental Protection Agency procedures. The lindane levelwas 0.32 ug/mL (4 hours after ingestion) and 0.02 ug/mL (20 hours afteringestion). The child was transferred to a children’s hospital ICU, where hismental status progressively improved. The next day the child had slightlydecreased activity. During observation over the next 2 days his conditionprogressively improved, and he was discharged home.
The Physicians Desk Reference (PDR) provides the following statement on clinical
pharmacology regarding 1% lindane cream, “Dale, et al reported a blood level of 290 ng/mlassociated with convulsions following the accidental ingestion of a lindane containing product”. Lindane Blood Levels in Children Following Application of 1% Lotion for Scabies
A 1977 article in The Journal of Pediatrics provides data from a study conducted in the
Acute Care Clinic of Children’s Medical Center, Dallas, Texas which documents blood levels oflindane in infants and children who were treated with 1% lindane lotion for scabies. (4)
In this study, serum concentrations of lindane were determined in infants and children with
and without scabies infection following application of 1% lindane lotion. Studies were performedin 20 infected and noninfected patients who averaged 33 to 64 months of age with averageweights ranging from 13 to 17 kg. After a pretreatment blood sample was obtained, 1% lindaneproduct was applied to the body surface area prescribed by the label. Twenty four hours afterapplication of the lotion, all patients were given a warm soapy bath. The current label for lindanelotion applied for scabies specifies that the lotion should not be left on for more than 12 hours. This may result in an overestimation of blood concentrations, however, it is likely not relevant tothe risk assessment since the blood level measured at 6 hours was used for risk assessmentpurposes. Specimens of blood for determination of lindane concentrations were obtained at 0, 2,4, 6, 8, 12, 24, and 48 hours after topical application of 1% lotion. Patient characteristics arepresented in Table 3 and results are presented in Table 4. TABLE 3. Characteristics of Scabies Treatment Patients TABLE 4. Blood Concentrations of Lindane After Scabies Treatment
Concentrations of Lindane in Blood (ug/ml)
Discussion of Uncertainties Associated with Blood Level AnalysisAllowable Blood Level in Children (i.e., non-exceedance levels based on evidence of
adverse effects) - It is uncertain whether the levels of 320 ng/ mL and 290 ng/mL represent themaximum levels of lindane in the subjects' blood. Given that the measured level of 320 ng/mL inthe cited clinical study was taken at least 4 hours after ingestion, it is likely that initial blood levelswere higher. It is also uncertain what blood level is associated with the effects observed in thecase study patient. To the extent that observed effects are attributable to higher than measuredlindane blood levels, the assessment tends to overstate potential risk. To the extent that adverseeffects may be associated with lindane blood levels lower than 320 ng/mL, the assessment maytend to underestimate risk.
The subjects in the clinical study received a bath with warm soapy water prior to
application of the lindane lotion. Wet skin tends to exhibit greater dermal absorption than dryskin. Use of the blood levels from the study may therefore overstate potential exposure forindividuals who have dry skin at the time of application.
In the clinical study, the lindane lotion was left on for 24 hours after application. The
current label for scabies treatment specifies that the lotion should not be left on for more than 12hours. This prolonged exposure may result in an overestimation of blood concentrations seenafter 12 hours. However, it should not effect the 6 hour peak level used in the risk assessment.
The potential contribution of other lotion components to observed effects is not known. Anticipated Label Changes - Based on the average age, the clinical scabies study looked
only at infants and small children (up to 8 yrs old). Average amounts of lindane applied in thestudy were 129-158 mg. Given that the current label prescribes up to 300 mg (1 oz) for infantsand up to 600 mg (2 oz) for children 6 and older, the amount of product applied in the study was2-4 times less than the currently allowable amount. However, the label for the 1% scabies lotionwill be revised to prescribe against use of the product for small children (i.e., children less than 60kg). Given anticipated label changes, use in accordance with the revised label would eliminaterisks to young children (<60 kg). Also, according to FDA, pending label changes on the amountof lotion required should result in lower application rates for both older children and adults. Although there is insufficient data to indicate a correlation between amount applied dermally andcorresponding blood levels, it is reasonable to assume that use of a lower amount of product willproduce lower lindane blood levels. Finally, the new label will direct that lindane be applied todry skin which will reduce the amount of lindane absorbed into the blood stream. Children vs. Adults - The blood level comparison analysis pertains and is applicable only
to small children. HED has no data on blood levels associated with adverse effects in adults nordo we have data on blood levels associated with prescribed use of lindane to treat scabies inadults. Based on available toxicity data, children are more sensitive than adults. Thereforeadverse effects would occur at higher blood levels in adults and older children than in youngchildren. In addition, blood levels associated with prescribed use (under both current and revisedlabels) would be lower in older children and adults due to differences in weight to body surfacearea ratios between young children and adults/young adults.
HED’s analysis using the MOE approach indicates MOEs of concern from both high and
low-end treatment scenarios for all ages assessed using either monkey or human dermalabsorption data. For the blood concentration analysis, HED compared blood concentrations fromthe scabies study with the blood concentration associated with short-term adverse effects inchildren. HED is concerned that there is an inadequate margin of safety between the blood levelsassociated with scabies treatment (0.064 ug/mL) and the blood levels resulting in short term
effects in children (0.29 - 0.32 ug/mL). Given variability of responses in humans, an uncertaintyfactor of 10 is considered reasonable for this risk assessment. There is a 4-5 fold differencebetween blood levels in treated patients and allowable blood levels identified based on evidenceof adverse effects. While this assessment does consider mitigation efforts being undertaken byFDA, it is important to note that it does not consider the medical benefits of scabies treatment.
FDA will approve a drug that it finds is safe and effective for a specific population with a
specific condition when the drug is used in accordance with its proposed labeling. Safe and effective does not mean without risks, it means that the benefit of the treatmentoutweighs the risk for the patient group specified in the label. As described below, FDAconducted a risk/benefit analysis of the use of lindane as second line prescription medication forscabies and concluded, based on that analysis, that lindane is safe and effective for treatment ofscabies when used in a manner consistent with its labeling. Second line therapy is defined as aproduct that should be used only if another treatment has already failed, or if the patient cannottolerate another available therapy.
Lindane has been on the market since 1947, but was labeled a second line therapy in 1995
after review by the FDA. It is similar in action to other approved therapies, but has a higherpercutaneous absorption than other approved scabicides and pediculocides. This greater systemicexposure may translate to a greater potential for serious adverse events, such as seizure. Thissystemic exposure can be exaggerated in patients with an immature or compromised cutaneousbarrier. Animal data have demonstrated that the young are more sensitive to the neurotoxiceffects of lindane.
FDA assessed the safety and potential risks from use of lindane as a drug based on safety
information from the spontaneous adverse event reporting system (AERS) and current literature. The AERS database is a collection of spontaneous, voluntarily submitted reports of adverseevents associated with drug products submitted by consumers, healthcare professionals,manufacturers, and others. One of the limitations of a voluntary system of reporting is asubstantial amount of under-reporting. FDA estimates that between one and 10% of all adverseevents are reported to FDA. Other limitations include the variability in the quality and quantity ofinformation reported. In spite of known limitations, the spontaneous system has value. Thesystem is sensitive to rare, unexpected events, is simple to use, and is relatively inexpensive. However, the AERS database does not include the total number of patients who have beentreated, with or without adverse events. Because of this, it is not possible to quantify thepercentage of patients who have had adverse events. Most of the serious adverse events in theAERs database occurred in patients who had already labeled contraindications to the use oflindane, who used lindane in excessive amounts, or who ingested lindane.
Moreover, even though there appears to be a narrow therapeutic index, there isn’t much
evidence that labeled use leads to serious adverse events. The 290 ng/ml plasma level in thePhysician’s Desk Reference (PDR) and the 320 ng/ml plasma level from the Aks article areplasma levels that were obtained several hours after acute ingestion of the lindane product. Thetwo levels are from pediatric patients who ingested lindane and had seizures. This information ishelpful to a physician in determining if the patient’s seizure was secondary to lindane ingestion, orif there is another etiology. The plasma levels may provide a tool to determine the etiology of apatient’s seizure upon presentation to the Emergency Room but are not a “No observed adverseevent level (NOAEL).”
The data for lindane indicate that there is a two-compartment pharmacokinetic model.
After ingestion, there is a steep rise in the serum level, followed by a rapid decline during thedisposition phase when some lindane distributes to lipid tissues and some is excreted. Thedisposition phase is followed by a prolonged beta elimination phase. Based on this model, it isprobable that the patients’symptoms (seizure) occurred at a higher serum level than those levelsobtained 4 hours after the initial ingestion. In addition, the marketed formulation contains otheringredients that may contribute to the toxicity in acute ingestions. Ingredients for lotion include:glycerol monostearate, cetyl alcohol, stearic acid, trolamine, carrageenan, 2-amino-2-methyl-1-propanol, methylparaben, butylparaben, perfume and water. Ingredients for shampoo include:trolamine lauryl sulfate, polysorbate 60, acetone and water
It is important to emphasize that the blood levels listed in the PDR and the article by Aks
are single cases following ingestion by toddlers of an unknown quantity of lindane. The youngdo appear to be more sensitive to the neurotoxic effects of lindane, as seen in studies acrossspecies. The serum lindane level that may lead to a seizure in a small child is most likely lowerthan the level that would cause an equal effect in an adult. The labeling is being changed to reflectthis concern, indicating that lindane should be used only in patients who have achieved adultstature, or approximately 60 kilograms.
FDA recognizes that all drugs have associated risks. Therefore, FDA must determine if
the potential risks of adverse side effects associated with a drug treatment outweigh the overallhealth benefits of treating the condition. Although not life threatening, scabies can pose significantproblems if left untreated, including severe itching and secondary infections. In underdevelopedareas of the world where treatments are not available or medical care is inaccessible, scabies canbe pandemic and accounts for significant morbidity. FDA has concluded that there is no questionthat the standard of care for these patients is to administer scabicidal treatment for theirinfestation.
FDA considers alternative therapies when evaluating the benefit of a drug. Although the
FDA has determined that there are other products for the treatment of scabies that may have lessrisk and should be used first in a patient, FDA also recognizes that there are patients “who have
either failed to respond to adequate doses, or are intolerant of, other approved therapies.” Thesepatients would have documented failed prior treatment with other approved products, ordocumented reactions – either local or systemic, to those products or drugs that would beexpected to cross-react with those products. Although there are other therapies available forfirst-line use in the treatment of scabies, FDA believes it is in the best interest of public health tohave several alternatives available for this subset of patients. The approved treatment options forscabies are limited. They are:
permethrin cream, 5% (Acticin and Elimite),
lindane cream 1% (not marketed in the U.S.), lindane lotion 1%, and
Precipitated sulfur ointment, 5-10%, is occasionally compounded and used for scabies. For safety reasons, crotamiton and precipitated sulfur ointment are reasonable options foryoung children and pregnant women, but the efficacy of these products is much lower thanother products, and re-treatment is frequently necessary. There is information available onthe internet about other alternative treatments that include soaking in borax. The efficacyof these therapies is unknown.
Resistance to products must also be considered when evaluating drugs. There are
currently only three approved treatments for scabies, and as mentioned earlier, crotamiton is notas effective as lindane or permethrin. Lindane is labeled for second line therapy and should onlybe used in the event that there is treatment failure or if the patient is intolerant to the other twotreatments. If a patient has persistent infestation after one form of treatment, there should first bean assessment for appropriate use, and if it is determined that the failure wasn’t due to misuse,then the patient should be retreated with an alternative agent. There is a public health benefit tohaving several treatment options for a condition where a patient may require re-treatment with adifferent therapy, especially when there may be emerging or transient resistance.
Lindane has been available since 1947, and there are some case reports that the scabies
mite has recently developed resistance to it. A literature search did not reveal any reports ofscabies mite resistance to permethrin, but it has been on the market for a much shorter period oftime than lindane. There is one case report in the literature of resistance to crotamiton. It is notunreasonable to expect that resistance to permethrin will develop over time. If this resistancedoes occur, and lindane is not available, physicians would not have alternative approved andeffective therapies for patients infested with scabies.
FDA has concluded that lindane is safe and effective for treatment of scabies when used in
a manner consistent with its labeling. Although lindane is already labeled as a second line therapy,the current label is being revised to indicate that lindane is for use only in patients who haveattained adult stature (approximately 60 kilograms). This emphasizes that it should not be used inyoung pediatric patients, and that patients should be post-pubescent. In addition, physicians are
instructed to use caution when they are prescribing this product to patients who have underlyingconditions (HIV/AIDS) or are on medications that may result in a lowered seizure threshold, andpatients who have skin conditions that may allow enhanced absorption.
Extensive information will be provided for the physician and the patient regarding the
potential risk of applying the product more than once. The new label also includes a medicationguide that must, by law, be given to each patient with the lindane prescription. This medicationguide explains in plain language the potential for harm if the lindane is used other than asinstructed. It also includes clear instructions for use. The high volume container sizes are beingdiscontinued to limit the amount per prescription. It is anticipated that this will decrease over-usethe product. ASSESSMENT OF RISK FROM USE OF LINDANE TO TREAT LICE
HED’s assessment of risk from use of lindane to treat head lice relies on data provided in
two published literature studies. One study documents cases of accidental lindane ingestion bytoddlers in which blood levels were determined after ingestion. The second study provides dataon blood levels of lindane in children and young adults following application of Kwell Shampoo totreat head lice. Acute Accidental Lindane Ingestion in Toddlers
See case study and PDR data described above for scabies assessment. (3)
Absorption of Lindane Following Application of Kwell Shampoo to Treat Lice
EPA has a published study on blood levels of lindane in children and young adults
following standard application of Kwell Shampoo. An 1983 article in Pediatric Dermatologyprovides data from a study conducted in the Outpatient Clinic of Children’s Medical Center,Dallas, Texas. (4)
In this study, serum concentrations of lindane were determined in children with pediculosis
capititis following application of 1% Kwell shampoo. Studies were performed in 9 patients whowere from 3.5 to 18 years of age with weights ranging from 13.6 to 35 kg, and heights rangingfrom 99 to 163 cm. After a pretreatment blood sample was obtained, 1% lindane product wasapplied to dry hair using a sufficient amount of medication to thoroughly saturate the hair andscalp. After 10 minutes, small quantities of water were added until a lather formed. Shampooingwas continued for an additional 4 minutes after which the hair was rinsed and blown dry with ahair dryer. The current label for Kwell shampoo specifies that the shampoo should remain inplace on dry hair for 4 minutes only before water is added to form lather. Consequently, the studymay result in higher absorption than would occur following label directions. Four patients were
retreated because of persistence of living lice after 5 days. Specimens of blood were obtained at 0,2, 4, 6, and 24 hours after topical application of Kwell shampoo. Patient characteristics arepresented in Table 5 and results are presented in Table 6. TABLE 5. Characteristics of the Lice Patients TABLE 6. Blood Concentrations of Lindane After Lice Treatment
Mean Concentrations of Lindane in Blood (ng/mL)
Discussion of Uncertainties Associated with Blood Level Analysis
It is uncertain whether the levels of 320 ng/mL and 290 ng/mL represent the maximum
levels of lindane in the subjects' blood. Given that the measured level of 320 ng/mL in the citedclinical study was taken at least 4 hours after ingestion, it is likely that initial blood levels werehigher. It is uncertain what blood level is associated with the effects observed in the case studypatient. To the extent that observed effects are attributable to higher than measured lindane bloodlevels, the assessment tends to overstate potential risk. To the extent that adverse effects may beassociated with lindane blood levels of 320 ng/mL or lower, the assessment may tend tounderestimate risk.
The current label for Kwell shampoo specifies that the shampoo should remain in place on
dry hair for 4 minutes only before water is added to form lather. In the clinical study, theshampoo was left in place for 10 minutes before water was added. Consequently, the study mayresult in higher absorption than would occur following label directions.
The highest measured blood concentration obtained following single and double
treatments of head lice at label rates but at longer than label specified treatment durations was0.00613 ug/mL. This is significantly lower than 0.32 ug/mL, the blood level associated with acuteaccidental ingestion which resulted in short-term adverse effects according to the cited case study
article. Therefore, HED does not believe that lindane pharmaceutical products used for treatmentof lice pose human health risks of concern when used in accordance with directions provided onthe label.
Based on its assessment of safety and potential risks from use of lindane as a prescription
medication for scabies and lice, FDA has concluded that lindane is safe and effective for treatmentof lice when used as labeled. References
(1) Moody, R.P., and Ritter, L., J. Tox and Env Hlth, 28:161-169, 1989(2) Feldman, R.J. and Maibach, H.I., Tox and Applied Pharmacology 28, 126-132, 1974(3) Aks, S.E., Krantz A., Hryhorczuk, D.O., Wagner, S., and Mock, J., Ann Emerg Med, 26:647-651, 1995(4) Ginsburg, C.M. and Lowry, W., Pediatric Dermatology Vol 1. No. 1 74-76, 1983
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