Abstract
Clozapine (CLZ) is the drug of choice for the treatment of resistant schizophrenia; however, its suitable use is limited by the complex adverse effects’ profile. The best-described adverse effects in the literature are represented by agranulocytosis, myocarditis, sedation, weight gain, hypotension, and drooling; nevertheless, there are other known adverse effects that psychiatrists should readily recognize and manage. This review covers the “rare” and “very rare” known adverse effects of CLZ, which have been accurately described in literature. An extensive search on the basis of predefined criteria was made using CLZ and its combination with adverse effects as keywords in electronic databases. Data show the association between the use of CLZ and uncommon adverse effects, including ischemic colitis, paralytic ileus, hematemesis, gastroesophageal reflux disease, priapism, urinary incontinence, pityriasis rosea, intertriginous erythema, pulmonary thromboembolism, pseudo-pheochromocytoma, periorbital edema, and parotitis, which are influenced by other variables including age, early diagnosis, and previous/current pharmacological therapies. Some of these adverse effects, although unpredictable, are often manageable if promptly recognized and treated. Others are serious and potentially life-threatening. However, an adequate knowledge of the drug, clinical vigilance, and rapid intervention can drastically reduce the morbidity and mortality related to CLZ treatment.
Introduction
Clinical use
Clozapine (CLZ) is the “prototypical” of second-generation antipsychotics (APs), also named “atypical antipsychotics” (AAPs).Citation1 It was synthesized in 1958, developed by Sandoz in 1961, and introduced in Europe in 1970. Hence, CLZ was widely viewed as the most important advance in the treatment of schizophrenia since the discovery of the first AP drugs (chlorpromazine and haloperidol in the 1950s and 1960s, respectively).
In 1975, 17 patients out of 2,660 (0.7%) exposed to CLZ in Finland developed agranulocytosis, defined as an absolute neutrophil count <500/mm3, and eight (50%) of them subsequently died from secondary infections; CLZ was voluntarily withdrawn by the manufacturer.Citation2
The effectiveness of CLZ in cases of conventional treatment-resistant schizophreniaCitation3 has allowed the molecule to be reintroduced into clinical use. About 25%–60% of patients are unresponsive to conventional or combined pharmacological treatment (AP combined with electroconvulsive therapy or AP combined with psychotherapy).Citation4,Citation5 In these forms, which are defined as being “resistant”, CLZ was considered the most effective APCitation6 for the management of severely ill schizophrenic patients who fail to respond adequately to standard APs. It was approved by the US Food and Drug Administration and health authorities in most countries, under regular hematological monitoring aimed to detect early granulocytopenia, and was first marketed in the US in January 1990.Citation7
Pharmacological properties
In comparison to traditional neuroleptics, CLZ has more robust effectiveness trials than other APs in all symptomatic schizophrenia dimensionsCitation8 and a lower incidence of extrapyramidal symptoms;Citation9 it also has greater specificity for the limbic system, improving negative symptoms and cognitive impairment associated with schizophrenia.Citation10–Citation12
CLZ belongs to the family of dibenzodiazepines (8-chloro-11-(4-methyl-piperazinyl)-5H-dibenzo-[1,4]-diazepine). It interacts with several different subtypes of dopamine receptors (D1, D2, D3, D4), serotonin receptors (5-HT1A, 5-HT2A, 5-HT2C, 5-HT3, 5-HT6, 5-HT7), adrenergic receptors (alpha-1, alpha-2), histaminergic receptor (H1), and muscarinic receptor (M1).Citation13
It is often mentioned that CLZ simultaneously blocks the serotonin 5-HT2A receptors or other serotonin receptors as well as dopamine D2 receptors, suggesting that the block of serotonin receptors may prevent the Parkinson-like motor side effects of APs.Citation14
The greater difference between the serotonin 5-HT2A receptor and D2 receptor affinities in atypical APs was not due to higher 5-HT2A affinities but due to lower D2 affinities.Citation15
It has also been demonstrated that CLZ possesses the ability to modulate the production of pro-inflammatory cytokines such as interleukin-10 and interferon-γ in peripheral blood cells, which also supports its potential neuroprotective effect.Citation16,Citation17 Moreover, an increase in plasma concentrations of CLZ leads to a significant decrease in the presence of free radicals (reactive oxygen species), which may also contribute to this latter effect.Citation18
In addition to its indication in the treatment of resistant schizophrenia, CLZ has other important therapeutic uses. It has demonstrated efficacy in ameliorating tardive dyskinesia, mood disorders, and some neurological disorders, as well as psychosis in patients with dementia and parkinsonism.Citation19 Only CLZ has level A evidence to support its use in Parkinson’s disease patients with psychosis, whether demented or not.Citation20 Moreover, CLZ drastically reduces mortality rates for suicide in patients with schizophrenia; in contrast, it increases the mortality rate in psychiatric patients for other rare drug-related causes, such as pulmonary embolism (PE) and CLZ-related heart problems.Citation21
Side effects
Despite all this effectiveness, similar to many other available drugs, it has side effects that can be serious and bothersome.Citation22 In agreement, the use of CLZ in schizophrenia is limited by the potentially fatal side effects and contraindications, which is the reason why it requires frequent monitoring.Citation22 Approximately 17% of patients taking CLZ discontinue the treatment because of adverse effects.Citation23
Since clinical trials are conducted under widely varying conditions, adverse reaction rates observed in clinical trials may not reflect the rates observed in clinical practice.
The most commonly reported adverse effects (≥5%) across CLZ clinical trialsCitation24 were central nervous system reactions (sedation, dizziness/vertigo, headache, and tremor), cardiovascular reactions (tachycardia, hypotension, and syncope), autonomic nervous system reactions (hypersalivation, weight gain, drooling, sweating, dry mouth, and visual disturbances), and gastrointestinal reactions (constipation and nausea). Other adverse effects are rare or less frequent.
Adverse reactions are divided by frequency, using the following parameters: very common (≥1/10), common (≥1/100, <1/10), uncommon (≥1/1,000, <1/100), rare (≥1/10,000, <1/1,000), very rare (<1/10,000), and not known (cannot be estimated from the available data).Citation25 shows other adverse reactions of CLZ according to their currently established frequency.
Table 1 Adverse reactions divided by frequency regarding patients and treatment: very common (≥1/10), common (≥1/100, <1/10), uncommon (≥1/1,000, <1/100), rare (≥1/10,000, <1/1,000), very rare (<1/10,000), and not known (cannot be estimated from the available data) (Agenzia Italiana del Farmaco [AIFA] document 06/06/2014)Citation25
Among uncommon adverse reactions, severe cardiovascular effects are connected with the appearance of myocarditis, with 0.015%–1.3% of cases occurring in more than 50% of cases within the first 2 weeks of treatment,Citation26 as well as the appearance of pericarditis and cardiomyopathy, and the lengthening of the corrected QT.Citation27,Citation28 The clinical presentation generally consists of heart failure including shortness of breath (60%) and palpitations (36%). Echocardiography at presentation showed dilated cardiomyopathy in 39% of cases.Citation29
Furthermore, CLZ is associated with a significant incidence of drug-induced diabetes mellitus and dyslipidemia.Citation30,Citation31
On the other hand, there are many other related contraindications, such as active liver disease, progressive liver disease and hepatic failure, uncontrolled epilepsy, preexisting cardiovascular disease, and severe central nervous system depression or comatose state, in alcoholic/toxic psychosis and previous hypersensitivity to CLZ.Citation32 CLZ is also contraindicated in patients with myeloproliferative disorders and a history of toxic or idiosyncratic agranulocytosis or severe granulocytopenia.Citation33 The underutilization of CLZ is likely related to uneasiness on the part of physicians in managing adverse effects, particularly agranulocytosis, and a reluctance by patients to submit to frequent blood sampling.Citation34
However, an early recognition of more serious side effects may allow a better therapy management. For example, the monitoring system has been effective in reducing both the incidence of CLZ-related agranulocytosis and the associated mortality rate.Citation34 Therefore, patients generally tolerate most common side effects associated with CLZ use, and appropriate medical management facilitates a maximization of the treatment benefits. Conversely, some adverse effects are not described in the data sheet, and less known by most psychiatrists because of their presence in case reports only; however, some of them are potentially fatal.
The aim of the present review is to describe the “rare” and “very rare” adverse effects related to CLZ’s treatment, which are often not described in the data sheet but potentially life-threatening; we also describe strategies for their management according to literature reports, in order to provide psychiatrists and physicians with a quick reference tool that contains appropriate therapeutic measures to be taken in the case of these kinds of adverse effects. Anticipating and managing these adverse effects may be essential for a valuable therapeutic outcome.
Methods
This review considered articles and case reports that better describe rare and very rare adverse effects of CLZ, at any dose; common side effects are widely described.
The following scientific databases were consulted to find studies published in English without year limits: Medline (OvidSP), CINAHL (Ebsco), EMBASE (Ovid), PsychINFO (Ebsco), AgeLine, Cochrane Database of Systematic Reviews, and the Database of Abstracts of Reviews of Effects. Additional references were identified from the bibliographies of published articles.
Three reviewers independently inspected all study citations identified by the searches. The search was made using the terms “clozapine” and “clozapine and adverse effects” as keywords. Studies were included on the basis of the following inclusion criteria: studies in English language that clearly linked CLZ treatment with rare and very rare adverse effects and also included strategies for an early recognition and management of them. Articles focusing on widely known physical adverse effects or on psychiatric side effects and studies that considered CLZ in association with other psychotropic drugs were excluded. The search produced 4,090 results. Only 56 studies fulfilled the inclusion criteria and thus were selected for this review at the end of the selection, and were considered on the basis of frequency of every rare and very rare adverse effect.
Results
Gastrointestinal adverse effects
Rare adverse effects affecting the gastrointestinal system have been described in CLZ-treated patients.Citation35–Citation37 CLZ can affect the entire gastrointestinal system, from esophagus to rectum, and may cause bowel obstruction, ischemia, perforation, and aspiration.Citation38
Due to its anticholinergic properties, the use of CLZ was related to varying degrees of impairment of intestinal peristalsis ranging from chronic constipation, paralytic ileus, and intestinal obstruction to fecal impaction. Epidemiological data on the occurrence of chronic constipation in treated patients are conflicting. Some surveys reported incidence between 22.8% and 33.3% of acute events of constipation in patients receiving chronic treatment,Citation39 whereas in other studies, such incidence was as high as 60%.Citation40 So far, seven deaths due to severe gastrointestinal complications have been reported in patients treated with CLZ (). The strategies needed to prevent the occurrence of gastrointestinal complications are a recommended dietary fiber intake, an adequate intake of liquids, especially in the presence of drooling, and adequate regular physical activity. In patients with a high risk of developing constipation, therapeutic options should always consider low doses of CLZ or association with a second AP.Citation41 These strategies are similar to those used in the treatment of constipation caused by opioids,Citation42 which could be useful in reducing morbidity and mortality from CLZ-induced adverse gastrointestinal effects. The use of prolonged-release formulations of naloxone or methylnaltrexone was considered by some authors for the agonist action exerted by norclozapine on opioid receptors.Citation43,Citation44 Another severe and rare CLZ-related effect is hematemesis (vomiting of blood). The possible pathophysiological mechanisms by which CLZ may cause severe esophagitis and subsequent hematemesis are not fully understood, but a role for the anticholinergic activity of the drug can be assumed. Antagonism of cholinergic receptors may be responsible for the reduction until abolition of esophageal motility, increased pressure in the lower sphincter tone, and overall reduction in esophageal tone.Citation45,Citation46
Table 2 Death due to clozapine-associated gastrointestinal hypomotility
Another hypothesized pathophysiological mechanism regards the effects of CLZ on the regulation of vagal tone in esophageal peristalsis and consequent abolition and sialorrhea (excessive flow of saliva) not due to anticholinergic effects.Citation47
Although the number of cases of esophageal reflux is small, it still represents the most common gastrointestinal effect reported in CLZ-treated patients.Citation35,Citation48,Citation49 It was estimated that approximately 11% of patients treated with CLZ develop gastrointestinal symptoms similar to reflux esophagitis with endoscopic evidence within 6 weeks of treatment.Citation35 Reflux symptoms could be due to the association between CLZ and proton pump inhibitor drugs, rather than only the use of CLZ;Citation46 in fact, there is a temporal association between gastroesophageal reflux symptoms onset and CLZ–proton pump inhibitor drug association.Citation49,Citation50
Ogilvie’s syndrome is reported in some CLZ-treated schizophrenic patients.Citation51 Ogilvie’s syndrome is a massive dilatation of the loops of the bowel without radiological evidence of mechanical obstruction. This condition occurs more frequently in hospitalized or institutionalized patients with significant medical and surgical conditions and metabolic disorders, and in cases of spinal or retroperitoneal cord injuries. These injuries are the basis of altered regulation of the autonomic parasympathetic nervous system with suppression and enhancement of sympathetic tone; they cause intestinal atony and massive expansion of the loops.
Recognition and proper therapeutic management are essential to reduce the mortality rate, which is around 40%, when it evolves to ischemia and colonic perforation.Citation52
There are reported cases of gastrointestinal adverse events that cause acute abdomen, and so, it must be remembered that schizophrenic patients may have an altered sensitivity to painful stimuli and poor compliance during clinic visits.Citation53 This event is very important for the acute abdomen differential diagnosis.Citation54,Citation55 APs can often have a sedative and modulating effect on a patient’s nociceptive threshold. Another possibility is that pain perception is normal but that schizophrenic patients have difficulties in verbalizing their expression of pain.Citation56
Urogenital adverse effects
The genitourinary adverse events described in CLZ-treated patients are mainly priapism and urinary incontinence. Priapism is a prolonged and persistent penile erection, independent from stimulation or sexual desire.Citation57 It is a urological emergency that, if not treated in a timely and appropriate manner, can cause permanent damage such as impotence, necrosis, and acute urinary retention.Citation58 Most typical and atypical APs can cause priapism.Citation53 The first case of CLZ-induced priapism was reported in 1992; this was probably caused by many factors including prolactin increase.Citation59 In 2010, another case of a patient with CLZ-treated schizophrenia who developed a severe case of priapism was described; in this circumstance, he required surgical decompression and drug suspension. After a relative clinical stabilization period, the same patient was treated with CLZ for a new episode of psychosis and again developed pria-pism.Citation60 Another patient was treated with hormone replacement therapy (3.5 mg goserelin acetate every 28 days) that resolved the urological condition and allowed the patient to continue treatment with CLZ. Regular goserelin acetate administration is the pharmacological treatment of choice in patients with recurrent priapism due to its antagonistic action on testosterone plasma levels.Citation61
Urinary continence requires a perfect balance between urethral closure and bladder detrusor muscle activity.Citation62 CLZ-induced urinary incontinence often occurs as nocturnal enuresisCitation63 and generally develops within the first few days after starting therapy. It may also occur after weeks or months. For some patients, this condition is temporary and self-limiting, while for others, it is permanent and requires treatment.Citation64 The mechanism of CLZ-induced urinary incontinence is multifactorial:Citation65 CLZ can reduce the internal bladder sphincter tone through its adrenergic blocking action. Incontinence can also be caused by intrinsic CLZ activity, that is, antimuscarinic action, and 5-HT2A and 5-HT2C receptor antagonisms.Citation66,Citation67
CLZ can cause an overactive bladder tone that results in continence impairment due to acting as a dopamine antagonist.Citation68
CLZ α-adrenergic receptor antagonism can be considered the major cause of urinary incontinence;Citation65 in fact, the efficacy of pseudoephedrine has been demonstrated in incontinence due to CLZ treatment. Fifty-seven patients with schizophrenia who began CLZ treatment and developed urinary incontinence were treated with ephedrine; the dose was gradually increased to 150 mg/day until the resolution of urologic adverse effects. Sixteen patients were treated with ephedrine, and 15 of them showed improvement after optimization of the assay. Twelve patients had complete resolution of symptoms, three a partial resolution, and only one had no response to treatment. Ephedrine did not alter patients’ psychopathology.
Dermatological adverse effects
Many medications can cause skin rashes that occur in various forms and severity levels. Most of these reactions are mild; however, severe cases can lead to a decrease in the patient’s quality of life. Serious reactions may include angioedema, acute generalized exanthematous reactions, Stevens–Johnson syndrome, and toxic epidermal necrolysis. Two cases of CLZ-treated patients with schizophrenia who developed angioneurotic edema have been reported; discontinuation of the drug resulted in resolution of the clinical symptoms.Citation69
Although minor skin reactions may occur in 5% of APs-treated patients, a 54-year-old patient with schizophrenia treated for 28 days with CLZ developed a generalized rash compatible with pityriasis rosea (skin rash that usually begins as one large circular or oval spot on your chest, abdomen, or back), hyperthermia, and abnormal liver function tests. Discontinuation of the drug, together with corticosteroids and antihistamine treatment, led to the resolution of the clinical symptoms.Citation70 A case of CLZ-induced flexural intertrigo (inflammation of the body folds) has also been reported, although the correlation between autoimmune mechanism and CLZ was not clarified; discontinuation of treatment resulted in resolution of the dermatological condition.Citation71
Pulmonary adverse effects
Case reports exist linking CLZ use and onset of pulmonary thromboembolism.Citation72–Citation75 These events were related considering the lack of important risk factors such as hypercoagulability or previous surgery in patients who have had an adverse event. There is no definitive proof of a biological mechanism through which CLZ induces PE. It is believed that there is an indirect effect via weight increase and sedation, which correlate positively with abolition of physical activity, a recognized risk factor in the development of thromboembolic disease.Citation76 Risk of developing PE is a rare event, but it is about 28 times higher in CLZ-treated patients compared to the general population.Citation77 Although it is not an absolute contraindication, the potential risk of developing PE should be assessed at the beginning of CLZ treatment. The creation of a link between CLZ and PE has been described in a study in which death causes were investigated, including PE, by examining medical records of 67,072 patients with previous or current CLZ treatment. The rate ratio of deaths attributed to PE for current CLZ exposure was 5.2.Citation21 Two case-control studies have explored the relationship between the use of first-generation APs and PE occurrence. There is no definitive evidence about a causal link between PE and use of first-generation APs, but it can be assumed that the use of low-potency first-generation APs is able to produce higher rates of PE compared to high-potency first-generation APs.Citation78 In the case of nonspecific symptoms in CLZ-treated patients, such as dyspnea, caution is important for the suspect of PE even when there are no other critical elements.Citation79
Other “very rare” adverse effects
Pseudopheochromocytoma (severe paroxysmal hypertension)
The rise of norepinephrine plasma levels in CLZ-treated patients is an expected effect caused by α2-adrenergic receptor antagonism.Citation80–Citation82 Increased catecholamine plasma levels cause nonspecific symptoms; however, there may be clinical scenarios that can be classified as pseudopheochromocytoma. Clinical manifestations are related to paroxysmal or continuous catecholamine plasma secretion with hypertensive crises. Other detectable symptoms are hyperglycemia, panic attacks, and weight loss.Citation83 There have been cases of pseudopheochromocytoma reported in CLZ-treated patients aged between 22 years and 51 years suffering from treatment-resistant schizophrenia.Citation84 These patients were treated with CLZ (300–900 mg) for 2–18 months, and all had elevated urinary catecholamine levels and severe hypertension with no other organic causes. CLZ was discontinued resulting in normalization of blood pressure and urinary catecholamine concentration.Citation85–Citation87 This evidence suggests the need for routine urinary catecholamine screening and blood pressure monitoring.
Periorbital edema
There have been three reported cases of periorbital edema associated with CLZ treatment; in two cases, CLZ-treated patients (150 mg/day and 50 mg/day) developed fever, blisters, and periorbital edema after few days. In both patients, laboratory tests showed neutrophilic leukocytosis. CLZ treatment was discontinued, and introduction of corticosteroids and antihistamine drugs caused complete symptoms remission within a few days; an IgE-mediated reaction to CLZ was assumed.Citation69
Another case report describes a pretibial and periorbital edema in a CLZ-treated patient (400 mg daily) after 6 weeks of treatment. Laboratory tests showed a modest eosinophilia only. Halving the dose led to a regression of the allergic reaction; the CLZ antagonistic effect on the D4 receptor resulting in sodium retention and hypertension could explain the regression.Citation88
Parotitis (inflammation of one or both parotid glands)
Sialorrhea in CLZ-treated patients is a known side effect,Citation89 but it can occur in a secondary form caused by parotitis.Citation90,Citation91 Drug-induced parotitis is a rare adverse drug reaction. Based on the quantitative and qualitative evidence collected from the case reports, medications that are associated with drug-induced parotitis include L-asparaginase, CLZ, and phenylbutazone.Citation92
Parotid gland inflammation is among the least prominent side effects reported in CLZ-treated patients. The UK Medicines and Healthcare Products Regulatory Agency has collected 32 reports of parotitis in 504 cases of sialorrhea prior to January 2012. Most of the treatments were aimed at resolving sialorrhea and consequently the parotid swelling. There are no intervention protocols for these cases, and treatment can be anticholinergic drugs with the aim of blocking muscarinic receptors, and adrenergic drugs (α2 agonists/α1 antagonists) for the suppression of sympathetic stimulation.Citation93
To the best of our knowledge, there is only one randomized trial that demonstrated a better response to treatment associated with terazosin (α1 lytic) and benztropine (antimuscarinic) rather than monotherapy with either drug.Citation94
Conclusion
It was not possible to provide details regarding the dosage and associations of CLZ with other APs in each study.
Despite the benefits in relieving positive and negative symptoms in treatment-resistant schizophrenia and other psychiatric and neurological disorders,Citation19 the use of CLZ has been strongly limited by the possibility of the onset of severe adverse effects.
Clinical research has to concentrate on the presence, early recognition, and treatment of CLZ-related adverse effects.Citation95 Clinical monitoring, laboratory tests, and instrumental controls for these adverse effects are very strict to limit possible complications, which may be fatal.
Some of these adverse effects are predictable, less serious, and more common and are directly related to the receptor-mediated mechanisms that can often be managed medically.
Others are rare and less known, and the hypothesized pathophysiology is not completely clear. The presence of adverse effects should not deter psychiatrists from using CLZ when it is necessary.
In the studies included in our review, many important outcomes were described. Monitoring both common and rare adverse effects could significantly reduce the disability and mortality associated to CLZ treatment. An early recognition of both more common and rare adverse effects may allow a better therapy management.
Furthermore, adherence to CLZ treatment can be significantly enhanced if patients are adequately informed about the nature and risk of its adverse effects and if the clinician recognizes and attempts to treat them. The appropriate management of other CLZ adverse effects facilitates a maximization of the benefits of CLZ treatment. Physicians and patients alike should be aware that there is a range of benefits of CLZ use that is wider than its risk.
Disclosure
All authors declare that they have no competing interests relevant to this work.
References
- StahlSEssential Psychopharmacology Neuroscientific Basis and Practical Applications (Essential Psychopharmacology Series)CambridgeCambridge University Press2008
- Indanpaan-HeikkilaJAlhavaEOlkinuoraMPalvaIPAgranulocytosis during treatment with clozapineEur J Clin Pharmacol1977113193198856603
- KaneJHonigfeldGSingerJMeltzerHClozapine for the treatment-resistant schizophrenic. A double-blind comparison with chlorpromazineArch Gen Psychiatry19884597897963046553
- SolankiRKSinghPMunshiDCurrent perspectives in the treatment of resistant schizophreniaIndian J Psychiatry200951425426020048449
- TaylorSElectroconvulsive therapy: a review of history, patient selection, technique, and medication managementSouth Med J2007100849449817534086
- MalhotraAKPharmacogenomics and schizophrenia: clinical implicationsPharmacogenomics J20011210911411911437
- KaneJHonigfeldGSingerJMelzerHthe Clozaril Collaborative Study GroupClozapine for treatment-resistant schizophrenic: a double-blind comparison with chlorpromazine/benztropineArch Gen Psychiatry19984597897963046553
- GareriPDe FazioPRussoEMariglianoNDe FazioSDe SarroGThe safety of clozapine in the elderlyExpert Opin Drug Saf20087552553818759705
- KumraSKranzlerHGerbino-RosenGClozapine and “high-dose” olanzapine in refractory early-onset schizophrenia: a 12-week randomized and double-blind comparisonBiol Psychiatry200863552452917651705
- MeltzerHYMcGurkSRThe effects of clozapine, risperidone, and olanzapine on cognitive function in schizophreniaSchizophr Bull199925223325510416729
- LindenmayerJPIskanderAParkMClinical and neurocognitive effects of clozapine and risperidone in treatment-refractory schizophrenic patients: a prospective studyJ Clin Psychiatry199859105215279818633
- BrarJSChengappaKNParepallyHThe effects of clozapine on negative symptoms in patients with schizophrenia with minimal positive symptomsAnn Clin Psychiatry1997942272349511946
- GareriPDe FazioPDe FazioSNorma MariglianoNFerreri IbbaduGDe SarroGAdverse effects of atypical antiphychotics in the elderlyDrugs Aging2006231293795617154659
- MelzerHYMatsubaraSLeeJCClassification of typical and atypical antipsychotic drugs on the basis of dopamine D1, D2 and serotonin2 pKi valuesJ Pharmacol Exp Ther198925112382462571717
- KapurSSeemanPDoes fast dissociation from the dopamine D2 receptor explain the action of atypical antipsychotics? A new hypothesisAm J Psychiatry2001158336036911229973
- SongCLinAKenisGBosmansEMaesMImmunosuppressive effects of clozapine and haloperidol: enhanced production of the interleukin-1 receptor antagonistSchizophr Res200042215716410742653
- PatersonGJOhashiYReynoldsGPPrattJAMorrisBJSelective increases in the cytokine, TNFalpha, in the prefrontal cortex of PCP-treated rats and human schizophrenic subjects: influence of antipsychotic drugsJ Psychopharmacol200620563664216478754
- GrossAJoffeGJoutsiniemiSLNybergPRimόnRAppelbergBDecreased production of reactive oxygen species by blood monocytes caused by clozapine correlates with EEG slowing in schizophrenic patientsNeuropsychobiology2003472737712707488
- CohenSAUnderwoodMTThe use of clozapine in a mentally retarded and aggressive populationJ Clin Psychiatry199455104404447961521
- FriedmanJHParkinson disease psychosis: updateBehav Neurol201327446947723242358
- WalkerAMLanzaLLArellanoFRothmanKJMortality in current and former users of clozapineEpidemiology1997866716779345668
- KruppPBarnesPClozapine-associated agranulocytosis: risk and aetiologyBr J Psychiatry Suppl19921738401418887
- YoungCRBowersMBMazureCMManagement of the adverse effects of clozapineSchizophr Bull19982433813909718630
- GardnerDMBaldessariniRJWaraichPModern antipsychotic drugs: a critical overviewCMAJ2005172131703171115967975
- Farmaciemedici.it [homepage on the Internet]A.I.F.A. [updated June 6, 2014] Available from: http://www.farmaciemedici.it/farmaci/bugiardino/leponex/aifa/Accessed February 19, 2015
- KamphuisHArendsJTimmermanLvan MarleJKappertJMyocarditis and cardiomyopathy: underestimated complications resulting from clozapine therapyTijdschr Psychiatr201052422323320503163
- CrewsMPDhillonGSMacCabeJHClozapine rechallenge following clozapine-induced pericarditisJ Clin Psychiatry201071795996120667298
- RathoreSMasaniNDCallaghanPOClozapine-induced effuso-constrictive pericarditisCase report and review of the literature. Cardiology200710818318517085936
- AlawamiMWasywichCCicovicAKenediCA systematic review of clozapine induced cardiomyopathyInt J Cardiol2014176231532025131906
- LambertiJSOlsonDCrillyJFPrevalence of the metabolic syndrome among patients receiving clozapineAm J Psychiatry200616371273127616816234
- SaffermanALiebermanJKaneJSzymanskiSKinonBUpdate on the clinical efficacy and side effects of clozapineSchizophr Bull19911722472611882209
- NaheedMGreenBFocus on clozapineCurr Med Res Opin200117322322911900316
- VelayudhanRKakkanSLate onset clozapine induced agranulocytosisIndian J Psychol Med201436442542725336778
- AlvirJMLiebermanJAAgranulocytosis: incidence and risk factorsJ Clin Psychiatry199455suppl B1371387961558
- LakerMCooksonJReflux oesophagitis and clozapineInt Clin Psychopharmacol199712137399179632
- TownsendGCurtisDCase report: rapidly fatal bowel ischaemia on clozapine treatmentBMC Psychiatry200664317052340
- RegeSLaffertyTLife-threatening constipation associated with clozapineAustralas Psychiatry200816321621918568631
- PalmerSEMcLeanRMEllisPMHarrison-WoolrychMLife-threatening clozapine-induced gastrointestinal hypomotility: an analysis of 102 casesJ Clin Psychiatry200869575976818452342
- LiebermanJASaffermanAZPollackSClinical effects of clozapine in chronic schizophrenia: response to treatment and predictors of outcomeAm J Psychiatry199415112174417527977880
- HayesGGiblerBClozapine-induced constipation (letter)Am J Psychiatry199515222987840373
- AlexopoulosGSStreimJCarpenterDDochertyJPExpert Consensus Panel for Using Antipsychotic Drugs in Older PatientsUsing antipsychotic agents in older patientsJ Clin Psychiatr200465suppl 2599
- HolzerPAhmedzaiSHNiederleNOpioid-induced bowel dysfunction in cancer-related pain: causes, consequences, and a novel approach for its managementJ Opioid Manag20095314515119662924
- BakerDEMethylnaltrexone bromide: new drug for the treatment of opioid induced bowel dysfunctionRev Gastroenterol Disord200993E84E9319898269
- OnaliPOlianasMCN-Desmethylclozapine, a major clozapine metabolite, acts as a selective and efficacious delta-opioid agonist at recombinant and native receptorsNeuropsychopharmacology200732477378516841075
- TomerTJonathanBAlanMDeath from clozapine-induced constipation: case report and literature reviewPsychosomatics2002431717311927763
- Van SoestEDielemanJKuipersEThe effect of anticholinergic agents on gastrooesophageal reflux and related disordersExpert Opin Drug Saf20087217318018324880
- PraharajSKAroraMGandotraSClozapine-induced sialorrhea: pathophysiology and management strategiesPsychopharmacology (Berl)2006185326527316514524
- BakerRWChengappaKNGastroesophageal reflux as a possible result of clozapine treatmentJ Clin Psychiatry19985952579632041
- van VeggelMOlofinjanaODaviesGTaylorDClozapìne and gastrooesophageal reflux disease (GORD) – an investigation of temporal associationActa Psychiatr Scand20121271697722901096
- TaylorDOlofinjanaORahimiTUse of antacid medication in patients receiving clozapine: a comparison with other second generation antipsychoticsJ Clin Psychopharmacol201030446046120631564
- de BruinGJBacDJvan PuijenbroekEPvan der KloosterJMOgilvie Syndrome induced by clozapineNed Tijdschr Geneeskd2009153B43720051163
- SaundersMDKimmeyMBSystematic review: acute colonic pseudo-obstructionAliment Pharmacol Ther2005221091792516268965
- DworkinRHPain insensitivity in schizophrenia: a neglected phenomenon and some implicationsSchizophr Bull19942022352488085127
- BickerstaffLKHarrisSCLeggettRSCheahKCPain insensitivity in schizophrenic patientsA surgical dilemma. Arch Surg1988123149513337657
- RosenthalSHPorterKACoffeyBPain insensitivity in schizophreniaCase report and review of the literature. Gen Hosp Psychiatry19901253193222210350
- PotvinSStipETempierAPain perception in schizophrenia: no changes in diffuse noxious inhibitory controls (DNIC) but a lack of pain sensitizationPsychiatr Res2008421210101016
- KeoghaneSRSullivanMEMillerMAThe aetiology, pathogenesis and management of priapismBJU Int200290214915412081756
- ReifRVýbornýKPriapism: a urological emergencyActa Univ Palacki Olomuc Fac Med199313559637976678
- ComptonMTMillerAHSexual side effects associated with conventional and atypical antipsychoticsPsychopharmacol Bull20013538910812397881
- SeftelASaenz de TejadaISzetelaBColeJGoldsteinIClozapine-associated priapism: a case reportJ Urol199214711461481729510
- MulhallJPKaminetskyJCAlthofSECorrelations with satisfaction measures in men treated with phosphodiesterase inhibitors for erectile dysfunctionAm J Mens Health20115326127121406491
- HanesALee DemlerTLeeCCamposAPseudoephedrine for the treatment of clozapine-induced incontinenceInnov Clin Neurosci2013104333523696957
- Harrison-WoolrychMSkeggKAshtonJHerbisonPSkeggDCNocturnal enuresis in patients taking clozapine, risperidone, olanzapine, and quetiapine: comparative cohort studyBr J Psychiatry2011199214014421653944
- LinCCBaiYMChenJYLinCYLanCYLanTHA retrospective of clozapine and urinary incontinence in Chinese in-patientsActa Psychatr Scand19991002158161
- FullerMABorovickaMCJaskiwGESimonMRKwonKKonickiPEClozapine-induced urinary incontinence: incidence and treatment with ephedrineJ Clin Psychiatry199657115145188968299
- WarnerJPHarveyCABarnesTRClozapine and urinary incontinenceInt Clin Psychopharmacol1994932072097814831
- ThorKBDonatucciCCentral nervous system control of the lower urinary tract: new pharmacological approaches to stress urinary incontinence in womenJ Urol20041721273315201731
- ClarkNConventional antipsychotic and clozapine-induced urinary incontinenceJ Coll Psychiatr Neurolog Pharma2003218
- MishraBSahooSSarkarSAkhtarSClozapine-induced angioneurotic edemaGen Hosp Psychiatry2007291788017189753
- LaiYWChouCYShenWWLuMLPityriasis rosea-like eruption associated with clozapine: a case reportGen Hosp Psychiatry201234e5e7
- RaoAFrancisNMorarNClozapine-induced symmetrical drug-related intertriginous and flexural exanthema: first reported casesBr J Dermatol201216651142114322121994
- SrihariVHLeeTWPulmonary embolism in a patient taking clozapineBMJ200833676591499150118583682
- TrippACNon-fatal pulmonary embolus associated with clozapine treatment: a case seriesGen Hosp Psychiatry2011331e5e621353146
- JoksovicPMChilesCCardiac arrest and pulmonary embolism after clozapine titrationPrim Care Companion CNS Disord2011132MC3184584
- MunoliRNPraharajSKBhatSMClozapine-induced recurrent pulmonary thromboembolismJ Neuropsychiatry Clin Neurosci2013253E50E5124026744
- HäggSJönssonAKSpigsetORisk of venous thromboembolism due to antipsychotic drug therapyExpert Opin Drug Saf20098553754719569978
- PaciulloCAEvaluating the association between clozapine and venous thromboembolismAm J Health Syst Pharm200865191825182918796423
- ZornbergGLJickHAntipsychotic drug use and risk of first-time idiopathic venous thromboembolism: a case-control studyLancet200035692371219122311072939
- ParkinLSkeggDCHerbisonGPPaulCPsychotropic drugs and fatal pulmonary embolismPharmacoepidemiol Drug Saf200312864765214762980
- DavidsonMKahnRSSternRGTreatment with clozapine and its effect of plasma homovanillic acid and norepinephrine concentrations in schizophreniaPsychiatry Res19934621511638483974
- BreierABuchananRWWaltripRWListwakSHolmesCGoldsteinDSThe effect of clozapine on plasma norepinephrine: relationship to clinical efficacyNeuropsychopharmacology1994101178179790
- PickarDOwenRRLitmanREKonickiEGutierrezRRapaportMHClinical and biologic response to clozapine in patients with schizophrenia: Cross-over comparison with fluphenazineArch Gen Psychiatry19924953453531375019
- WaltherMMKeiserHRLinehanWMPheochromocytoma: evaluation, diagnosis, and treatmentWorld J Urol1999171353910096149
- KrentzAJMikhailSCantrellPHillGMPseudophaeochromocytoma syndrome associated with clozapineBMJ20013227296121311358774
- LiJKYeungVTLeungCMClozapine: a mimicry of phaeochromocytomaAust NZ J Psychiatry1997316889891
- PrasadSEKennedyHGPseudophaeochromocytoma associated with clozapine treatmentIr J Psych Med200320132134
- AkinsolaOOngKPseudophaeochromocytoma associated with Clozapine Therapy: a case reportAfr J Psychiatry2011145406408
- DurstRRaskinSKatzGZislinJDurstRPedal edema associated with clozapine useIsr Med Assoc J20002648548610897248
- SockalingamSShammiCRemingtonGClozapine-induced hypersalivation: a review of treatment strategiesCan J Psychiatry200752637738417696024
- BrodkinEPeltonGPriceLTreatment of clozapine-induced parotid gland swellingAm J Psychiatry199615234458610845
- RobinsonDFennHYesavageJPossible association of parotitis with clozapineAm J Psychiatry199515222972987840372
- BrooksKGThompsonDFA review and assessment of drug-induced parotitisAnn Pharmacother201246121688169923249870
- ImmadisettyVAgrawalPA successful treatment strategy for clozapine-induced parotid swelling: a clinical case and systematic reviewTher Adv Psychopharmacol20122623523923983982
- ReinsteinMSirotovskyaLChasonovMComparative efficacy and tolerability of benzatropine and terazosin in the treatment of hypersalivation secondary to clozapineClin Drug Investig19991797102
- ConleyRRKellyDLSecond-generation antipsychotics for schizophrenia: a review of clinical pharmacology and medication-associated side effectsIsr J Psychiatry Relat Sci2005421516016134407
- ThéretLGermailMLBurdeACurrent aspects of the use of clozapine in the Chalons-surMarn Psychiatric Hospital: intestinal occlusion with clozapineAnn Med Psychol19951537474477
- DrewLHerdsonPClozapine and constipation: a serious issueAust NZ J Psychiatry1997311149150
- ShammiCMRemingtonGClozapine-induced necrotizing colitisJ Clin Psychopharmacol19971732302329169975
- LevinTTBarrettJMendelowitzADeath from clozapine-induced constipation: a case report and literature reviewPsychosomatics2002431717311927763
- FerslewKEHagardornANHarlanGCMcCormickWFA fatal drug interaction between clozapine and fluoxetienJ Forensic Sci1998435108210859729831
- FlanaganRJBallRYGastrointestinal hypomobility: an under-recognised life-threatening adverse effect of clozapineForensic Sci Int20112061–3e31e3620719440