Does methylphenidate cause a cytogenetic effect in children with attention deficit hyperactivity disorder?BACKGROUND AND OBJECTIVE: Attention deficit hyperactivity disorder attention deficit hyperactivity disorder (ADHD), formerly called hyperkinesis or minimal brain dysfunction, a chronic, neurologically based syndrome characterized by any or all of three types of behavior: hyperactivity, distractibility, and impulsivity. (ADHD Attention-Deficit/Hyperactivity Disorder (ADHD) Definition Attention-deficit/hyperactivity disorder (ADHD) is a developmental disorder characterized by distractibility, hyperactivity, impulsive behaviors, and the inability to remain focused on tasks or ) is the most common psychiatric disorder in children and adolescents (6-12% affected). Treatment with methylphenidate methylphenidate /meth·yl·phen·i·date/ (meth?il-fen´i-dat) a central stimulant, used in the form of the hydrochloride salt in the treatment of attention-deficit in children and narcolepsy. (MPH) in the United States United States, officially United States of America, republic (2005 est. pop. 295,734,000), 3,539,227 sq mi (9,166,598 sq km), North America. The United States is the world's third largest country in population and the fourth largest country in area. has increased to a current prescription rate of > 5 million per year. However, a 2005 study by El-Zein and co-workers [Cancer Lett 230:284-291] reporting a 3-fold increase in genomic damage in all 12 analyzed children after 3 months of therapy with MPH resulted in much concern about potential carcinogenic carcinogenic having a capacity for carcinogenesis. effects. Here we provide new information concerning the cytogenetic cytogenetic /cy·to·ge·net·ic/ (-je-net´ik) 1. pertaining to chromosomes. 2. pertaining to cytogenetics. cytogenetic pertaining to or originating from the origin and development of the cell. effect of MPH in children. DESIGN, PARTICIPANTS, AND METHODS: In a prospective study, we analyzed the genomic damage in children with ADHD (initial sample size 38 children) before and 1 (30 children), 3 (21 children), and 6 (8 children) months after initiation of MPH therapy. In addition, we investigated a group of 9 children receiving chronic MPH therapy. Patients were recruited within a study of our Clinical Research Group on ADHD in the Department of Child and Adolescent Psychiatry A branch of psychiatry that specialises in work with children, teenagers, and their families. History An important antecedent to the specialty of child psychiatry was the social recognition of childhood as a special phase of life with its own developmental stages, starting with and Psychotherapy of the University of Wurzburg. Assessment and treatment of patients were performed during inpatient or outpatient health care. The measure for genomic damage was the frequency of micronuclei, a subset of chromosomal aberrations, in peripheral lymphocytes Lymphocytes Small white blood cells that bear the major responsibility for carrying out the activities of the immune system; they number about 1 trillion. . RESULTS: MPH treatment resulted in no significant alteration in the micronucleus micronucleus /mi·cro·nu·cle·us/ (-noo´kle-us) 1. in ciliate protozoa, the smaller of two types of nucleus in each cell, which functions in sexual reproduction; cf. macronucleus. 2. a small nucleus. frequency. CONCLUSIONS: Because the findings published in 2005 by El-Zein and co-workers could not be replicated, the concern regarding a potential increase in the risk of developing cancer later in life after long-term MPH treatment is not supported. KEY WORDS: ADHD, cytogenetic effects, methylphenidate, micronuclei, psychostimulants. Environ Health Perspect 115:936-940 (2007). doi:10.1289/ehp.9866 available via http://dx.doi.org/ [Online 21 February 2007] ********** Attention deficit hyperactivity disorder (ADHD) is the most common psychiatric disorder in children and adolescents, with 6-12% being affected worldwide according to according to prep. 1. As stated or indicated by; on the authority of: according to historians. 2. In keeping with: according to instructions. 3. the Diagnostic and Statistical Manual of Mental Disorders Diagnostic and Statistical Manual of Mental Disorders /Di·ag·nos·tic and Sta·tis·ti·cal Man·u·al of Men·tal Dis·or·ders/ (DSM) a categorical system of classification of mental disorders, published by the American Psychiatric Association, that delineates objective , 4th text revision (DSM-IVTR 2000; see also Biederman and Faraone 2005). Methylphenidate (MPH), a central nervous system stimulant, is the most frequently prescribed drug for the symptomatic treatment Symptomatic treatment is any medical therapy of a disease that only affects its symptoms, not its cause, i.e., its etiology. It is usually aimed at reducing the signs and symptoms for the comfort and well-being of the patient, but it also may be useful in reducing organic of ADHD and has consistently shown efficacy and safety. Although MPH was introduced about 50 years ago, no conclusive data are currently available to assess the long-term benefits and risks. A recent report (El-Zein et al. 2005) on cytogenetic effects observed in peripheral lymphocytes (PBL PBL Problem-Based Learning PBL Phi Beta Lambda PBL Performance Based Logistics PBL Planetary Boundary Layer PBL Publishing and Broadcasting Limited (Australia) PBL Philippine Basketball League PBL Peripheral Blood Leukocyte ) from 12 ADHD children treated for 3 months with MPH raised questions about the genetic toxicity of this drug. On average, 3.0-, 4.3-, and 2.4-fold increases were found in chromosome aberrations (12 cases), sister chromatid exchanges (11 cases), and micronuclei frequencies (11 cases), respectively. The authors (El-Zein et al. 2005) cautioned that "the data should be replicated and expanded" but also stated that "the lack of research on long-term effects of methylphenidate use in humans warrants great concern." This great concern arose because cohort studies have shown an association between the frequency of cells with structural chromosomal aberrations or micronuclei in peripheral blood lymphocytes Peripheral Blood Lymphocytes (PBL): These are the mature lymphocytes (small white immune cells) that are found circulating in the blood, as opposed to organs, such as the lymph nodes, spleen, thymus, liver or bone marrow. These cells consist of T cells, NK cells and B cells. and cancer risk (Bonassi et al. 2004, 2006; Hagmar et al. 2004). Considering the extremely high current estimated prescription rate of MPH of over 5 million per year in the United States (Physician Drug and Diagnosis Audit 2003), a thorough investigation of the safety of this important medication for children with ADHD is essential. Using a standard genotoxicity Genotoxic substances are a type of carcinogen, specifically those capable of causing genetic mutation and of contributing to the development of tumors. This includes both certain chemical compounds and certain types of radiation. test battery, Teo et al. (2003) evaluated the activity of MPH in the bacterial reverse mutation assay and mouse lymphoma mammalian mutation assay with and without metabolic activation, and in a bone marrow micronucleus test A micronucleus test is a test used in toxicological screening for potential genotoxic compounds. In vitro culture cells are checked for induced micronucleus formation. A micronucleus is the erratic (third) nucleus that is formed during the anaphase of mitosis. in male and female CD-1 mice. Although substance-associated toxicity was observed in the mammalian tests, no mutagenic mutagenic inducing genetic mutation. or clastogenic effects were induced. This was recently further supported by negative genotoxicity findings in the in vitro in vitro /in vi·tro/ (in ve´tro) [L.] within a glass; observable in a test tube; in an artificial environment. in vi·tro adj. In an artificial environment outside a living organism. human lymphocyte lymphocyte: see blood; immunity. lymphocyte Type of leukocyte fundamental to the immune system, regulating and participating in acquired immunity. Each has receptor molecules on its surface that bind to a specific antigen. chromosomal aberration assay and the mouse bone marrow micronucleus test (Suter et al. 2006). Epidemiologic data are limited to one report of a cohort study of 143,574 patients; the researchers screened MPH, among other prescription drugs, for possible carcinogenicity carcinogenicity /car·ci·no·ge·nic·i·ty/ (kahr?si-no-je-nis´i-te) the ability or tendency to produce cancer. carcinogenicity the ability or tendency to produce cancer. and found no increase in cancer (Selby et al. 1989). However, the small sample size of 529 MPH-treated patients (15 cancer cases instead of 32.7 expected cases) and the short observation period of up to 15 years limit the interpretation. According to recent overviews responding to the findings of elevated genomic damage in children (Holtmann et al. 2006; Preston et al. 2005), MPH was not found to be carcinogenic in a long-term rat bioassay Bioassay A method for the quantitation of the effects on a biological system by its exposure to a substance, as well as the quantitation of the concentration of a substance by some observable effect on a biological system. , but yielded an increase in hepatic neoplasms in B6C3[F.sub.1] mice at the highest test dose of 56-66 mg/kg body weight/day, which is about 60-fold above the recommended doses for ADHD patients (Taylor et al. 2004). Because of these hepatic neoplasms, MPH was judged by the National Toxicology Program National Toxicology Program Environment A program that conducts toxicologic tests on substances frequently found at the EPA's National Priorities List sites, which have the greatest potential for human exposure (NTP (Network Time Protocol) A TCP/IP protocol used to synchronize the real time clock in computers, network devices and other electronic equipment that is time sensitive. It is also used to maintain the correct time in NTP-based wall and desk clocks. ) of the National Institute of Environmental Health Sciences The National Institute of Environmental Health Sciences (NIEHS) is one of 27 Institutes and Centers of the National Institutes of Health (NIH),which is a component of the Department of Health and Human Services (DHHS). The Director of the NIEHS is Dr. David A. Schwartz. to yield "some evidence of carcinogenic activity" (NTP 1995). The aim of this study is to provide new data on the potential mutagenicity mutagenicity /mu·ta·ge·nic·i·ty/ (-je-nis´it-e) the property of being able to induce genetic mutation. mutagenicity the property of being able to induce genetic mutation. of MPH in children. We assessed the cytogenetic effects of MPH treatment by evaluating the frequency of micronuclei, a subgroup of chromosomal aberrations, in ADHD children. We present data on the results before and 1 month (30 children), 3 months (21 children), and 6 months (8 children) after initiation of MPH treatment. Additionally, we analyzed 9 patients who had been medicated medicated /med·i·cat·ed/ (med´i-kat?id) imbued with a medicinal substance. medicated contains a medicinal substance. with MPH between 6 and 24 months. Methods Participants. The study was approved by the ethics committee ethics committee A multidisciplinary hospital body composed of a broad spectrum of personnel–eg, physicians, nurses, social workers, priests, and others, which addresses the moral and ethical issues within the hospital. See DNR, Institutional review board. of the University of Wurzburg (study no. 140/03), and written informed parental consent Parental consent laws (also known as parental involvement or parental notification laws) in some countries require that one or more parents consent to or be notified before their minor child can legally engage in certain activities. was obtained for all patients before participation in the study. Children with ADHD and no previous medication were recruited between May 2005 and April 2006. The patients were characterized by a team of consultant child and adolescent psychiatrists at the Department of Child and Adolescent Psychiatry and Psychotherapy of the University of Wurzburg. The patients were assessed and treated during inpatient or outpatient health care; semistructured interview and the Schedule for Affective Disorders Affective disorders A group of psychiatric conditions, also known as mood disorders, characterized by disturbances of affect, emotion, thinking, and behavior. and Schizophrenia for School-Aged Children (K-SADS K-SADS Kiddie-Schedule for Affective Disorders and Schizophrenia ) (Kaufman et al. 1997) were used as diagnostic inventories. The recruitment was done within a study of our Clinical Research Group on ADHD with the objective of family-based association and genome-wide linkage studies. Exclusion criteria exclusion criteria AIDS Donor exclusion criteria, see there were current smoking, current infection or an infection in the 14 days before blood sampling, or extreme food patterns (e.g., vegans) of the children. Psychiatric diagnoses such as anorexia nervosa, schizophrenia, any pervasive developmental disorders Pervasive Developmental Disorders Definition Pervasive developmental disorders include five different conditions: Asperger's syndrome, autistic disorder, childhood disintegrative disorder (CDD), pervasive developmental disorder not otherwise specified , neurologic disorders such as epilepsy, a history of any acquired brain damage, or evidence of a fetal alcohol syndrome fetal alcohol syndrome (FAS), pattern of physical, developmental, and psychological abnormalities seen in babies born to mothers who consumed alcohol during pregnancy. , premature deliveries and/or maternal reports of severe prenatal, perinatal, or postnatal postnatal /post·na·tal/ (-na´t'l) occurring after birth, with reference to the newborn. post·na·tal adj. Of or occurring after birth, especially in the period immediately after birth. complications, as well as severe diseases were also regarded as exclusion criteria. We investigated an additional sample consisting of nine children, who had been medicated with MPH for more than 6 months (chronic treatment). Four of them had received comedications (three risperidone and one valproic acid valproic acid /val·pro·ic ac·id/ (-ik) an anticonvulsant used particularly for the control of absence seizures. val·pro·ic acid n. An anticonvulsive drug used to treat seizure disorders. ) before the beginning of the study. Except for the medication, the same recruitment and exclusion criteria were applied. The MPH treatment (organized by sex) for the prospective study and the chronic treatment group is given in the tables. Group description and missing data of the prospective investigation. All children fulfilled the diagnostic criteria for ADHD according to DSM-IV-TR DSM-IV-TR Diagnostic and Statistical Manual of Mental Disorders-Fourth Edition (Text Revision) (American Psychiatric Association) (2000) and were completely drug naive before being enrolled in the study. Of the 38 patients who were identified as potential participants, 8 patients (group A) were not medicated with MPH or did not want to participate further in the study. Two patients withdrew because of nonresponse to MPH and change of treatment to amphetamine amphetamine (ămfĕt`əmēn), any one of a group of drugs that are powerful central nervous system stimulants. Amphetamines have stimulating effects opposite to the effects of depressants such as alcohol, narcotics, and barbiturates. and atomoxetine, respectively, and 7 patients were lost at follow-up. These circumstances both occurred after the 1-month visit. Therefore, 9 patients (group B) could be placed in the 1-month follow-up, 13 patients (group C) could be included in the 1- and 3-month follow-up, and 8 more patients were analyzed after 1, 3, and 6 months (group D). Thus the groups A, B, C, and D represent patients from whom we could collect one, two, three, and four blood samples, respectively, during the course of the study (Tables 1 and 2). Collection of blood samples. Blood samples (7.5 mL each) were collected 1 day before, and 1, 3, and 6 months after MPH treatment for micronucleus analysis. From each participant of the chronic treatment group, one blood sample was analyzed. Blood samples were taken via an in-dwelling cannula cannula /can·nu·la/ (kan´u-lah) a tube for insertion into a vessel, duct, or cavity; during insertion its lumen is usually occupied by a trocar. can·nu·la or can·u·la n. pl. and collected in coded tubes containing heparin. When blood samples were collected before 1700 hr, the samples were transported at room temperature to the nearby Department of Toxicology, University of Wurzburg, for immediate isolation of peripheral blood peripheral blood Cardiology Blood circulating in the system/body mononuclear mononuclear /mono·nu·cle·ar/ (-noo´kle-er) 1. having but one nucleus. 2. a cell having a single nucleus, especially a monocyte of the blood or tissues. mon·o·nu·cle·ar adj. cells (PBMCs); when samples were taken after 1700 hr, they were stored at room temperature pending isolation of PBMC PBMC Peripheral Blood Mononuclear Cell the following morning. Cell isolation. PBMCs were isolated by standard density gradient Density gradient is a variation in density over an area. The term is used in the natural sciences to describe varying density of matter, but can apply to any quantity whose density can be measured. centrifugation Centrifugation A mechanical method of separating immiscible liquids or solids from liquids by the application of centrifugal force. This force can be very great, and separations which proceed slowly by gravity can be speeded up enormously in centrifugal using FicoLite H (Linaris-H, Wertheim, Germany). In brief, the blood was layered (1:1) onto FicoLite H (Linaris) and centrifuged at 1,600 rpm (370 x g) for 30 min at room temperature. The PBMC layer was removed and the cells were washed twice (1,300 rpm; 250 x g; 10 min) with RPMI-1640 (Sigma-Aldrich Chemie GmbH, Steinheim, Germany). Culture conditions. PBMCs were cultured at a cell density of 1 Mio (millions)/mL in 5 mL of culture medium at 37[degrees]C in a humified hu·mi·fied adj. Converted into humus. Adj. 1. humified - converted to humus; "humified soil" , 5% carbon dioxide carbon dioxide, chemical compound, CO2, a colorless, odorless, tasteless gas that is about one and one-half times as dense as air under ordinary conditions of temperature and pressure. incubator. The culture medium consisted of RPMI-1640, supplemented with 15% fetal bovine serum Fetal bovine serum ( or foetal bovine serum) is serum taken from the fetuses of cows. Fetal Bovine Serum (or FBS) is the most widely used serum in the culturing of cells. In some papers the expression foetal calf serum is used. , 2 mM L-glutamine, 1 mM Na-pyruvate, nonessential amino acids nonessential amino acid n. An alpha-amino acid that is required for protein synthesis and can be synthesized by humans. , and antibiotics (penicillin/streptomycin/tylosin). To stimulate the lymphocytes for proliferation, PHA PHA abbr. phytohemagglutinin PHA phytohemagglutinin, a plant lectin. (phytohemagglutinine; final concentration 10 [micro]g/mL) was added. Micronucleus assay. The micronucleus scoring was carried out by a single scorer six times for each sample in a blinded manner. Because DNA DNA: see nucleic acid. DNA or deoxyribonucleic acid One of two types of nucleic acid (the other is RNA); a complex organic compound found in all living cells and many viruses. It is the chemical substance of genes. damage can be expressed as micronuclei only after going through mitosis, the analysis was limited to actively dividing lymphocytes. These were identified as binucleated bi·nu·cle·ate also bi·nu·cle·at·ed or bi·nu·cle·ar adj. Having two nuclei. Adj. 1. binucleated - having two nuclei binuclear, binucleate cells on addition of the cytokinesis-inhibitor cytochalasin B Cytochalasin B is a cell-permeable mycotoxin. It inhibits cytoplasmic division by blocking the formation of contractile microfilaments. It inhibits cell movement and induces nuclear extrusion. (final concentration 5 [micro]g/mL). Cytochalasin B was added to the cultures 44 hr after stimulation with PHA. At 72 hr after culture initiation, the cells were spun on glass slides with a cytocentrifuge cytocentrifuge designed for hypocellular fluids; it spins at lower speeds and has more gradual acceleration and deceleration than normal centrifuges. Some are able to deposit cells directly onto a slide for examination. (Cytospin 3; Shandon/Thermo, Dreieich, Germany; 1,000 rpm; 145 x g, 5 min). Subsequently, fixation in cold (-20[degrees]C) methanol was performed for at least 2 hr. Slides were stored at -20[degrees]C in sealed boxes. Before evaluation, slides were stained with acridine orange acridine orange n. A basic fluorescent dye used as a metachromatic stain for nucleic acids and in screening cervical smears for abnormal cells. (0.00625% in Sorensen buffer, w/v, pH 6.8) for 5 min, and washed twice in Sorensen buffer [67 mM [Na.sub.2]HP[O.sub.4]/K[H.sub.2]P[O.sub.4] (pH 6.8)]. Sample preparation (cell culture, slide preparation) was limited to two laboratory members, staining of slides to one. From each blood sample, 6,000 binucleated lympocytes (6 slides, 1,000 cells per slide) were screened for the presence of micronuclei with fluorescence microscopy Noun 1. fluorescence microscopy - light microscopy in which the specimen is irradiated at wavelengths that excite fluorochromes microscopy - research with the use of microscopes at 400x magnification. The scoring criteria corresponded to those described by Fenech et al. (2003). In addition, from 6,000 cells of each sample, we determined the cytokinesis cytokinesis: see mitosis. Cytokinesis The physical partitioning of a plant or animal cell into two daughter cells during cell reproduction. block proliferation index (CBPI CBPI Competency-Based Performance Improvement ) [(number of mononucleate cells + 2x number of binucleate bi·nu·cle·ate or bi·nu·cle·ar adj. Having two nuclei. cells + 3x number of multinucleate mul·ti·nu·cle·ate or mul·ti·nu·cle·at·ed adj. Having two or more nuclei. multinuclear, multinucleate cells having more than one nucleus. cells)/(sum of mononucleate, binucleate, and multinucleate cells)]. Statistics. Data are shown as mean [+ or -] SD of micronucleated cells per 1,000 binucleated cells. Microsoft Excel was used to organize data. WinStat (demo version; R. Fitch Software, Bad Krozingen, Germany; Statistics for Excel, Microsoft Corporation, Redmond, WA, USA) was applied for calculation of correlations (Pearson). Because data were not strictly normally distributed (as analyzed by WinStat) we applied both the paired t-test and Wilcoxon test Wilcoxon test a test used in statistics to compare paired data. Has the advantage of incorporating the size of the difference between the two sets of data in the comparison. for comparison of each sampling time with values before initiation of therapy. An overall analysis and an analysis of the most informative subgroup across three sampling times (before, 1 month, 3 months) were performed with Kruskal-Wallis. Independent groups were compared with the two-sample t-test and the two-sample Wilcoxon test. A p-value of [less than or equal to] 0.05 was considered significant. Results The mean ([+ or -] SD) age of the children in the initial study group (n = 38; groups A-D A-D Advance-Decline, or measurement of the number of issues trading above their previous closing prices less the number trading below their previous closing prices over a particular period. , Tables 1, 2; Figure 1) was 10.0 [+ or -] 2.8 years (range, 4.9-17.0 years). The sample included 29 male and 9 female children (all of German origin). The mean age of the 21 patients from whom at least three blood samples were collected (groups C + D; Tables 1, 2; Figure 1), was 9.7 [+ or -] 2.8 years (range, 4.9-17.0 years). The average of children's body weight was 34.5 [+ or -] 13.5 kg (range, 23.6-82.0 kg). During the first month, the children were medicated with an individual dose of MPH, ranging from 5 to 40 mg/day, equivalent to a mean of 0.54 mg/body weight/day, and during the subsequent 3 months with a dose of MPH ranging from 15 to 45 mg/body weight/day, equivalent to 0.74 mg/body weight/day. Sex, individual MPH doses, and pharmaceutical preparation (short-acting, long-acting) are given in Table 1. Comparable to our investigation, in the study of El-Zein et al. (2005) the patients received therapeutic dosages ranging from 20 to 54 mg/day after 3 months. In our chronic treatment group (Table 3), consisting of nine boys with long-term medication of MPH (6 months to 2 years) the mean age was 11.2 [+ or -] 2.8 years (range, 7.1-16.0 years). All of them had been medicated with a dose ranging from 15 to 60 mg/day. The average body weight was 45.5 [+ or -] 16.2 kg (range, 22.8-77.1 kg), and the average dose of MPH was equivalent to a mean of 0.83 mg/body weight/day. Three of these patients had additionally received risperidone (range, 0.5-1.5 mg/day) and one of them valproic acid (1,500 mg/day) for longer than 6 months. From the prospective study, 38 pretreatment pretreatment, n the protocols required before beginning therapy, usually of a diagnostic nature; before treatment. pretreatment estimate, n See predetermination. blood samples were available for micronucleus analysis in binucleated lymphocytes (groups A-D; Table 2, Figure 1). In untreated children we determined 6.1 [+ or -] 4.3/1,000 binucleated cells. There was no correlation between basal micronucleus numbers and sample admission date (r = -0.22; p = 0.10), suggesting no seasonal influences on micronucleus numbers. Within this age group, donor age did not correlate with micronucleus frequency (r = 0.02; p = 0.45). Because of limited sample size (nine female patients), we performed no analysis for influence of sex. Figure 1 and Table 2 give the number of micronucleated cells before and after MPH treatment at three different follow-up time points. The micronucleated cell frequencies at each follow-up compared with the baseline value did not demonstrate any significant increase (paired t-test and Wilcoxon test). Analysis of all groups with Kruskal-Wallis yielded no significant alterations. Table 2 also indicates that there was no significant alteration (t-test and Wilcoxon test) in the cell proliferation capability in response to phytohemagglutinine stimulation in vitro (CBPI) after initiation of MPH therapy. In addition, we gathered samples (one time point) from children who had received MPH for at least 6 months (6 months-2 years of chronic treatment). This group of nine children (Table 2) did not show a significantly different (p = 0.49/0.69; t-test/Wilcoxon; two sample tests performed separately) mean micronucleated lymphocyte frequency compared with the pre-treatment mean of our study group. In addition to the assessment of micronucleus numbers, we measured safety by analyzing changes in vital signs, electrocardiograms, and clinical laboratory values such as white and red blood count, electrolytes, and transaminases according to the recommendations for MPH therapy (Warnke and Walitza 2004). No abnormal parameters were observed except slightly reduced values of total iron, without signs of hypochromic microcytic anemia microcytic anemia n. Anemia in which the average size of red blood cells is smaller than normal. microcytic anemia An anemia in which the RBCs are < 6. , which occurred in some patients before and during the treatment, independent of micronucleus deviation. We could not detect reasons for increased micronucleus frequencies of individual children at isolated time points such as pathologic laboratory parameters, eating behavior, weight, or dose per weight. We reconsulted all patients with micronucleus frequencies of [greater than or equal to] 10/1,000 binucleated cells to ascertain whether they had been exposed to radiation, such as medical X-ray exposure or cosmic radiation within the preceding 2 years. Because only one patient reported one flight 2 years before the study, one patient had been hiking higher than 3,000 m, and another patient had one maxilla maxilla /max·il·la/ (mak-sil´ah) pl. maxil´las, maxil´lae [L.] the irregularly shaped bone that with its fellow forms the upper jaw. max´illary max·il·la n. pl. X ray for getting a brace, radiation exposure does not explain these isolated elevated micronucleus frequencies at single time points. Discussion In this study we did not find any alteration in the number of micronucleated cells after MPH treatment at three follow-up intervals (up to 6 months). These results suggest no induction of genomic damage and are in contrast to a recent report by El-Zein et al. (2005) showing elevated genomic damage 3 months after initiation of MPH therapy using three cellular genotoxicity end points--frequency of micronucleus formation, chromosomal aberrations, and sister-chromatid exchanges (SCE SCE (in Scotland) Scottish Certificate of Education SCE n abbr (= Scottish Certificate of Education) → Schulabschlusszeugnis in Schottland ). A micronucleus is formed during cell division, expressing previously induced chromosomal damage, and contains chromosomal fragments and--less frequently--whole chromatids or chromosomes. SCE analysis detects exchanges between sister chromatids harboring identical genetic information, thus not directly representing a mutagenic effect. Although chromosomal aberration studies are very common in human genetic analysis and cancer research, micronuclei are the cytogenetic end point most often used for current human exposure biomonitoring studies. For example, HUMN (Human MicroNucleus; http://ehs.sph.berkeley.edu/holland/humn/) is an international collaborative project of > 40 laboratories from all over the world documenting micronucleus frequencies in human populations. HUMN is currently focusing on human lymphocytes and exfoliated epithelial cells Epithelial cells Cells that form a thin surface coating on the outside of a body structure. Mentioned in: Corneal Transplantation as biomonitors for exposure to toxic substances, and as potential predictors of adverse health effects (Fenech et al. 1999). Recently, Bonassi et al. (2006) found that an increased micronucleus frequency in peripheral blood lymphocytes predicts the risk of cancer in humans. El-Zein et al. (2005) reported an average micronucleus frequency of 3.55 [+ or -] 0.68/1,000 binucleated cells in drug-naive patients, whereas we found 6.1 [+ or -] 4.3 micronucleated cells/1,000 in this study. As with El-Zein et al., some researchers prefer to score the number of micronuclei per 1,000 cells rather than the number of micronucleated cells, as recommended for genotoxicity testing in the Organisation for Economic Co-operation and Development The Organisation for Economic Co-operation and Development (OECD), (in French: Organisation de coopération et de développement économiques; OCDE) is an international organisation of thirty countries that accept the principles of representative democracy and a free market (OECD OECD: see Organization for Economic Cooperation and Development. ) guideline draft (OECD 2006). Because cells with more than one micronucleus are rare, the difference between these variants is small, and the number of micronuclei would be higher than the number of micronucleated cells. In a metaanalysis aimed at providing reference values ref·er·ence values pl.n. A set of laboratory test values obtained from an individual or from a group in a defined state of health. for basal micronucleus frequencies (no exposure to genotoxic genotoxic /ge·no·tox·ic/ (je´no-tok?sik) damaging to DNA: pertaining to agents known to damage DNA, thereby causing mutations, which can result in cancer. ge·no·tox·ic adj. agents, no disease), data from 13 publications with micronucleus data of children (440 children 0-19 years of age) gives an overall mean of 4.48 [+ or -] 0.66 micronuclei/ 1,000 binucleated cells (Neri et al. 2005). Based on the data collection from 12 laboratories for a pooled analysis of individual data (332 referents, 0-18 years of age; data from HUMN database) an overall mean [+ or -] SE of 5.23 [+ or -] 5.07 micronuclei/1,000 binucleated cells was calculated (Neri et al. 2005). Specifically, the age groups of 5-9 and 10-14 years had pooled estimated means of 5.62 and 6.02, respectively. Thus, our data (mean age, 10.0 years) are in excellent agreement with the published literature. Searching for possible explanations for the difference between our study and that of El-Zein et al. (2005), we are not aware of variations between the methods and procedures; El-Zein et al. (2005) did not describe methods in detail because of space limitations, so they denoted them as "standard procedures" in a later comment (El-Zein et al. 2006). In that comment, they excluded changes in the patients' health, environment, diet, or lifestyle as reasons for the observed elevation in the level of cytogenetic damage. Seasonal influences could be excluded in our database; it is not known whether this was also possible in their study. Differences concerning doses of MPH or type of pharmaceutical preparation, potentially increasing the contact time between MPH and peripheral lymphocytes, are not apparent between both studies, but El-Zein et al. (2005) do not describe individual dosage and pharmaceutical preparation of the medication. Although there is no evidence of cytochrome cytochrome (sī`təkrōm'), protein containing heme (see coenzyme) that participates in the phase of biochemical respiration called oxidative phosphorylation. P450 (CYP CYP In currencies, this is the abbreviation for the Cyprus Pound. Notes: The currency market, also known as the Foreign Exchange market, is the largest financial market in the world, with a daily average volume of over US $1 trillion. 450)-dependent reactions in the metabolism of MPH in humans, Le Nedelec and Rosengren (2002) have found that MPH decreased total hepatic CYP450 in the mouse and altered the catalytic activity and/or the polypeptide polypeptide: see peptide. levels of CYP1A CYP1A Cytochrome P450 1A , CYP2E1, and CYP3A. Thus, CYP450 polymorphisms may influence the effects of MPH. Because polymorphisms are not distributed equally among populations worldwide, we cannot exclude different extends of polymorphisms between the El-Zein study (2005) and ours. This presumption is supported by the fact that the investigated group of El-Zein et al. consisted of patients with different ethnicities (six Caucasians, four African Americans, and two Hispanic children), whereas our sample includes only patients of German origin. Based on our results, concern about a potential increase in the cancer risk later in life after long-term MPH treatment needs to be reconsidered. This is also supported by the fact that our "chronic treatment" group did not show a significant difference in micro-nucleated cells compared with the pretreatment values of the study group. Nonetheless, the widespread use of MPH still suggests a need for further research on this important topic, including extension of this study to examine potential long-term effects. REFERENCES Biederman J, Faraone SV. 2005. Attention-deficit hyperactivity disorder Attention-deficit hyperactivity disorder (ADHD) A condition in which a person (usually a child) has an unusually high activity level and a short attention span. People with the disorder may act impulsively and may have learning and behavioral problems. . Lancet 366:237-248. Bonassi S, Znaor A, Ceppi M, Lando C, Chang WP, Holland N, et al. 2006. An increased micronucleus frequency in peripheral blood lymphocytes predicts the risk of cancer in humans. Carcinogenesis car·ci·no·gen·e·sis n. The production of cancer. carcinogenesis production of cancer. biological carcinogenesis viruses and some parasites are capable of initiating neoplasia. ; doi:10.1093/carcin/bgl177 [Online 14 September 2006]. Bonassi S, Znaor A, Norppa H, Hagmar L. 2004. Chromosomal aberrations and risk of cancer in humans: an epidemiologic perspective. Cytogenet Genome Res 104:376-382. DSM-IV-TR. 2000. Diagnostic and Statistical Manual of Mental Disorders. 4th ed., Text Revision. Washington, DC:American Psychiatric Association The American Psychiatric Association (APA) is the main professional organization of psychiatrists and trainee psychiatrists in the United States, and the most influential world-wide. Its some 148,000 members are mainly American but some are international. . El-Zein RA, Abdel-Rahman SZ, Hay MJ, Lopez MS, Bondy ML, Morris DL, et al. 2005. Cytogenetic effects in children treated with methylphenidate. Cancer Lett 230:284-291. El-Zein RA, Hay MJ, Lopez MS, Bondy ML, Morris DL, Legator le·ga·tor n. One that makes a will; a testator. [Latin l  g MS, et
al. 2006. Response to comments on "Cytogenetic effects in children
treated with methylphenidate" by El-Zein et al. Cancer Lett
231:146-148.
Fenech M, Chang WP, Kirsch-Volders M, Holland N, Bonassi S, Zeiger E. 2003. HUMN project: detailed description of the scoring criteria for the cytokinesis-block micronucleus assay using isolated human lymphocyte cultures. Mutat Res 534(1-2):65-75. Fenech M, Holland N, Chang WP, Zeiger E, Bonassi S. 1999. The HUman MicroNucleus Project--An international collaborative study on the use of the micronucleus technique for measuring DNA damage in humans. Mutat Res 428:271-283. Available: http://ehs.sph.berkeley.edu/holland/humn/ [accessed 20 April 2007]. Hagmar L, Stromberg U, Bonassi S, Hansteen IL, Knudsen LE, Lindholm C, et al. 2004. Impact of types of lymphocyte chromosomal aberrations on human cancer risk: results from Nordic and Italian cohorts. Cancer Res 64:2258-2263. Holtmann M, Kaina B, Poustka F. 2006. Methylphenidate-induced cytogenetic alterations? [in German]. Z Kinder Jugendpsychiatr Psychother 34:215-220. Kaufman J, Birmaher B, Brent D, Rao U, Flynn C, Moreci P, et al. 1997. Schedule for affective disorders and schizophrenia for school-age children-present and lifetime version (K-SADS-PL): initial reliability and validity data. J Am Acad Child Adolesc Psychiatry 36:980-987. Le Nedelec MJ, Rosengren RJ. 2002. Methylphenidate inhibits cytochrome P450 in the Swiss Webster mouse. Hum Exp Toxicol 21:273-280. Neri M, Ceppi M, Knudsen LE, Merlo DF, Barale R, Puntoni R, et al. 2005. Baseline micronuclei frequency in children: estimates from meta- and pooled analyses. Environ Health Perspect 113:1226-1229. National Toxicology Program. 1995. Toxicology and Carcinogenesis Studies of Methylphenidate Hydrochloride methylphenidate hydrochloride Concerta, Daytrana, Equasym (UK), Metadate CD, Metadate ER, Methylin, Methylin ER, PHL-Methylphenidate (CA), PMS-Methylphenidate (CA), Riphenidate (CA), Ritalin, Ritalin LA, Ritalin-SR Pharmacologic class: (CAS no. 298-59-9) in F344/N Rats and B6C3F C3F Commander Third Fleet 1 Mice (feed studies). TR 439. Research Triangle Park Research Triangle Park, research, business, medical, and educational complex situated in central North Carolina. It has an area of 6,900 acres (2,795 hectares) and is 8 × 2 mi (13 × 3 km) in size. Named for the triangle formed by Duke Univ. , NC:National Toxicology Program. OECD (Organisation for Economic Co-operation and Development). 2006. OECD Guideline for The Testing of Chemicals. Draft Proposal for a New Guideline 487: In Vitro Micronucleus Test. Available: http://www.oecd.org/dataoecd/33/22/37865944.pdf [accessed 18 April 2007]. Physician Drug and Diagnosis Audit. 2003. Physician Drug and Diagnosis Audit. Newton, MA:Scott-Levin Associates. Preston RJ, Kollins SH, Swanson JM, Greenhill LL, Wigal T, Elliott GR, et al. 2005. Comments on "Cytogenetic effects in children treated with methylphenidate" by El-Zein et al. Cancer Lett 230:292-294. Selby JV, Friedman GD, Fireman BH. 1989. Screening prescription drugs for possible carcinogenicity: eleven to fifteen years of follow-up. Cancer Res 49:5736-5747. Suter W, Martus HJ, Elhajouji A. 2006. Methylphenidate is not clastogenic in cultured human lymphocytes and in the mouse bone-marrow micronucleus test. Mutat Res 607:153-159. Taylor E, Dopfner M, Sergeant J, Asherson P, Banaschewski T, Buitelaar J, et al. 2004. European clinical guidelines for hyperkinetic hyperkinetic pertaining to or marked by hyperkinesia. hyperkinetic episodes see Scottie cramp. hyperkinetic circulatory disorders disorder--first upgrade. Eur Child Adol Psychiatry 13(suppl 1):17-30. Teo SK, San RH, Wagner VO, Gudi R, Stirling DI, Thomas SD, et al. 2003. D-Methylphenidate is nongenotoxic in in vitro and in vivo in vivo /in vi·vo/ (ve´vo) [L.] within the living body. in vi·vo adj. Within a living organism. in vivo adv. assays. Mutat Res 537:67-79. Warnke A, Walitza S. 2004. Methylphenidat in der Behandlung der Aufmerksamkeits-Defizit/Hyperaktivitatsstorung [in German]. In: Methylphenidat (Schulte-Markwort M, Warnke A, eds). Stuttgart:Thieme, 14-33. Susanne Walitza, (1) Birgit Werner, (2) Marcel Romanos, (1) Andreas Warnke, (1) Manfred Gerlach, (1) and Helga Stopper (2) (1) Department of Child and Adolescent Psychiatry and Psychotherapy, and (2) Department of Toxicology, University of Wurzburg, Wurzburg, Germany Address correspondence to H. Stopper, Department of Toxicology, University of Wurzburg, Versbacher Strasse 9, D-97078 Wurzburg, Germany. Telephone: +49 931 201 48427. Fax: +49 931 201 48446. E-mail: stopper@toxi.uni-wuerzburg.de We gratefully acknowledge the technical assistance of M. Kessler and A. Nowak. This study was partially funded by grants from the German Research Foundation (Deutsche Forschungsgemeinschaft; KFO 125/1-1) and from the Interdisciplinary Center for Clinical Research [IZKF N-5 (1)] and was performed independent of financial or other support by companies producing or selling methylphenidate. The authors declare they have no competing financial interests. Received 30 October 2006; accepted 21 February 2007.
Table 1. Individual dosage of MPH analyzed after 1, 3, and 6 months for
all children of groups B, C, and D.
Dosage of MPH
(mg/day)
Sex 1 month 3 months 6 months
Group B
F 15
M 40
M 30
M 20
M 5
M 10
M 20 long-acting
F 18 long-acting, 5 short-acting
M 10
Group C
M 20 30
F 10 20
M 30 long-acting 40 long-acting
M 40 long-acting 40 long-acting
M 18 long-acting 36 long-acting
M 20 30
M 15 20
M 15 15
F 20 30
F 10 20
M 15 40
M 5 20
M 18 18
Group D
F 15 20 25 long-acting
M 20 20 30
M 20 20 30
M 10 15 15
F 36 long-acting 36 long-acting 54 long-acting
M 20 20 20
F 15 20 20
M 20 25 20 long-acting
Abbreviations: F, female; M, male. Unless otherwise noted, the
short-acting pharmaceutical preparation has been given.
Table 2. Individual frequencies of micronucleated lymphocytes of
children with ADHD before and after MPH treatment at three follow-up
intervals.
Before treatment
Group (no. of subjects) Mn-Cells CBPI
A (8) 10.00 [+ or -] 2.00 1.73
8.00 [+ or -] 4.73 1.73
5.83 [+ or -] 0.75 1.70
5.00 [+ or -] 0.89 1.69
4.00 [+ or -] 2.97 1.75
4.00 [+ or -] 2.00 1.73
3.67 [+ or -] 0.82 1.69
2.00 [+ or -] 0.89 1.88
B (9) 17.00 [+ or -] 4.69 1.82
7.83 [+ or -] 4.12 1.70
7.00 [+ or -] 1.55 1.74
6.00 [+ or -] 3.58 1.92
5.67 [+ or -] 1.21 1.63
5.33 [+ or -] 2.07 1.78
4.00 [+ or -] 1.29 1.77
3.00 [+ or -] 0.89 1.58
2.67 [+ or -] 0.82 1.77
C (13) 16.00 [+ or -] 4.34 1.88
11.67 [+ or -] 4.08 1.70
8.83 [+ or -] 2.32 1.76
8.00 [+ or -] 0.89 1.69
7.00 [+ or -] 2.19 1.67
7.00 [+ or -] 1.41 1.79
6.00 [+ or -] 1.27 1.77
4.83 [+ or -] 2.14 1.75
4.00 [+ or -] 1.27 1.76
4.00 [+ or -] 2.00 1.73
3.00 [+ or -] 3.03 1.74
2.83 [+ or -] 2.14 1.75
2.00 [+ or -] 0.89 1.80
D (8) 21.00 [+ or -] 5.22 1.76
6.17 [+ or -] 1.17 1.81
4.17 [+ or -] 1.47 1.73
3.17 [+ or -] 2.86 1.65
3.00 [+ or -] 1.79 1.78
2.67 [+ or -] 1.75 1.74
2.00 [+ or -] 0.63 1.80
2.00 [+ or -] 0.63 1.69
Total no. of patients 38 38
Mean [+ or -] SD 6.06 [+ or -] 4.29 1.75 [+ or -] 0.07
p-Value (t-test/Wilcoxon)
After 1 month
Group (no. of subjects) Mn-Cells CBPI
A (8)
B (9) 4.00 [+ or -] 1.79 1.79
15.00 [+ or -] 6.13 1.74
3.00 [+ or -] 0.89 1.85
2.50 [+ or -] 0.84 1.56
4.67 [+ or -] 1.03 1.63
2.17 [+ or -] 1.33 1.69
2.67 [+ or -] 0.82 1.78
5.33 [+ or -] 1.03 1.67
3.67 [+ or -] 0.82 1.68
C (13) 14.00 [+ or -] 2.37 1.81
6.67 [+ or -] 1.63 1.68
13.00 [+ or -] 2.53 1.74
8.17 [+ or -] 3.60 1.74
4.00 [+ or -] 3.03 1.75
3.00 [+ or -] 2.53 1.72
10.00 [+ or -] 2.83 1.85
7.83 [+ or -] 2.32 1.80
6.67 [+ or -] 1.03 1.85
4.33 [+ or -] 1.21 1.66
3.00 [+ or -] 1.55 1.73
3.00 [+ or -] 1.27 1.84
2.83 [+ or -] 1.47 1.85
D (8) 10.00 [+ or -] 5.37 1.74
5.33 [+ or -] 1.03 1.81
2.00 [+ or -] 2.28 1.77
3.00 [+ or -] 1.41 1.74
16.00 [+ or -] 2.19 1.85
3.00 [+ or -] 1.27 1.72
8.17 [+ or -] 3.76 1.78
2.00 [+ or -] 1.27 1.70
Total no. of patients 30 30
Mean [+ or -] SD 5.97 [+ or -] 4.12 1.76 [+ or -] 0.08
p-Value (t-test/Wilcoxon) 0.75/0.75 0.53/0.41
After 3 months
Mn-Cells CBPI
A (8)
B (9)
C (13) 5.00 [+ or -] 1.78 1.75
5.50 [+ or -] 1.38 1.66
7.33 [+ or -] 2.50 1.76
6.00 [+ or -] 1.67 1.70
8.00 [+ or -] 1.79 1.84
5.17 [+ or -] 2.32 1.82
1.67 [+ or -] 1.03 1.72
5.00 [+ or -] 2.10 1.78
3.67 [+ or -] 1.21 1.92
5.33 [+ or -] 1.37 1.66
3.67 [+ or -] 1.63 1.69
7.67 [+ or -] 2.94 1.73
9.67 [+ or -] 4.41 1.81
D (8) 13.67 [+ or -] 3.50 1.85
6.50 [+ or -] 1.38 1.84
11.50 [+ or -] 4.85 1.77
1.50 [+ or -] 1.05 1.67
2.00 [+ or -] 1.41 1.72
4.83 [+ or -] 2.48 1.78
5.50 [+ or -] 2.34 1.68
27.83 [+ or -] 3.71 1.78
Total no. of patients 21 21
Mean [+ or -] SD 7.00 [+ or -] 5.65 1.76 [+ or -] 0.07
p-Value (t-test/Wilcoxon) 0.60/0.96 0.61/0.78
After 6 months
Mn-Cells CBPI
A (8)
B (9)
C (13)
D (8) 5.00 [+ or -] 0.89 1.71
5.67 [+ or -] 0.82 1.78
3.50 [+ or -] 1.64 1.80
3.33 [+ or -] 0.52 1.67
5.67 [+ or -] 1.37 1.79
5.17 [+ or -] 1.17 1.74
4.33 [+ or -] 1.03 1.64
3.67 [+ or -] 0.82 1.70
Total no. of patients 8 8
Mean [+ or -] SD 4.54 [+ or -] 0.96 1.73 [+ or -] 0.06
p-Value (t-test/Wilcoxon) 0.67/0.55 0.54/0.81
Values for micronucleated lymphocytes (Mn-Cells) are mean [+ or -] SD
from 6 analyses of 1,000 binucleated lymphocytes. The cytokinesis block
proliferation index (CBPI) from 6,000 cells is indicated for each time
point. Significance was analyzed using the paired t-test and the
Wilcoxon test to compare data from each time point with the same
individuals before therapy initiation.
Table 3. Individual frequencies of micronucleated lymphocytes of
children with ADHD who had received chronic MPH treatment for at least 6
months.
Dosage
Treatment duration of MPH
(months) Sex (mg/day) Mn-Cells CBPI
13 M (a) 60 3.67 [+ or -] 0.82 1.70
6 M (b) 35 4.00 [+ or -] 0.89 1.67
8 M 45 5.83 [+ or -] 1.47 1.73
24 M (c) 25 2.00 [+ or -] 1.79 1.63
15 M 54 long- 5.33 [+ or -] 1.21 1.60
acting
11 M 25 7.67 [+ or -] 0.82 1.67
6 M 40 1.83 [+ or -] 1.33 1.62
12 M (d) 40 8.83 [+ or -] 1.47 1.79
24 M 15 6.00 [+ or -] 0.89 1.75
Total no. of 9 9
patients
Mean [+ or -] SD 5.02 [+ or -] 2.38 1.69 [+ or -]
0.06
M, male. Values for micronucleated lymphocytes (Mn-Cells) are mean
[+ or -] SD from 6 analyses of 1,000 binucleated lymphocytes. The
cytokinesis block proliferation index (CBPI) from 6,000 cells is
indicated.
(a) Risperidone: 0.5 mg/day. (b) Risperidone: 1 mg/day. (c) Risperidone:
1.5 mg/day. (d) Valproic acid: 1,500 mg/day.
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