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==Characteristics==
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The diagnosis of '''bipolar disorder in children''' has many similarities to that of the [[bipolar disorder|same disease in adults]] (BD), a type of mood disorder previously called manic-depressive disorder.  All forms of BD are characterized by periods of extremely elevated or irritable mood, which can sometimes alternate with episodes of [[depression]].  Bipolar disorder can be diagnosed in children as young as preschool.<ref name=Carr> Carr A. 2009. Bipolar disorder in young people: Description, assessment and evidence-based treatment. Devel. Neurorehabilitation. 12: 427-441</ref> The lifetime prevalence of BD is between 0.5 to 1.6%, and the prevalence may be as high as 1% in youths alone.<ref name=McCl> McClellan J, Kowatch R, Findling R (2008) Practice Parameter for the Assessment and Treatment of Children and Adolescents With Bipolar Disorder  J Am Acad Child Adolesc Psychiatry 1: 107-125</ref>  When diagnosed in children, BD is most commonly characterized by increased energy, distractibility, pressured speech, irritable mood, grandiosity, and elevated mood.<ref name=Carr> Carr A. 2009. Bipolar disorder in young people: Description, assessment and evidence-based treatment. Devel. Neurorehabilitation. 12: 427-441</ref>  BD is an increasingly common diagnosis in children, due to several factors including an expansion of diagnosis criteria from classic manic depressive symptoms to more general manic symptoms, availability of knowledge about BD in children, and desire for insurance reimbursement for treating symptomatic behaviors of bipolar disorder.<ref name=Carr> Carr A. 2009. Bipolar disorder in young people: Description, assessment and evidence-based treatment. Devel. Neurorehabilitation. 12: 427-441</ref><ref name=McCl> McClellan J, Kowatch R, Findling R (2008) Practice Parameter for the Assessment and Treatment of Children and Adolescents With Bipolar Disorder  J Am Acad Child Adolesc Psychiatry 1: 107-125</ref><ref name=Cum>Cummings CM and Fristad MA (2008)  Pediatric bipolar disorder: recognition in primary care Current Opinion in Pediatrics 20: 560-565</ref>


===Signs and Symptoms===
The diagnosis of bipolar disorder in children is a highly controversial issue, as the disease was previously thought to rarely occur in youths.<ref name=McCl> McClellan J, Kowatch R, Findling R (2008) Practice Parameter for the Assessment and Treatment of Children and Adolescents With Bipolar Disorder J Am Acad Child Adolesc Psychiatry 1: 107-125</ref><ref name=Cum>Cummings CM and Fristad MA (2008) Pediatric bipolar disorder: recognition in primary care Current Opinion in Pediatrics 20: 560-565</ref> However, more than 60% of adults with BD report having their first mood episode before the age of 19, as the typical age of onset is during adolescence.<ref name=Nand>Nandagopal JJ and DelBello MP (2010)  Pharmacotherapy for Pediatric Bipolar Disorder  Psychiatric Annals 4:221-230</ref> When the [[DSM-IV]] was published in 1994, pediatric bipolar disorder was not included as a diagnosis.   Currently, the American Psychological Association is currently working on criteria and classification for a new subset of BD, Pediatric Bipolar Disorder (PBD), to be included in the 2013 publication of DSM-V.<ref name=faw>Fawcett J (2009) Report of the DSM-V Mood Disorders Work Group American Psychiatric Association. Available: http://www.psych.org/MainMenu/Research/DSMIV/DSMV/DSMRevisionActivities/DSM-V-Work-Group-Reports/Mood-Disorders-Work-Group-Report.aspx. Accessed 15 March 2011.</ref> One of the main challenges in categorizing PBD as a separate diagnosis in DSM-V is understanding the symptomology of BD in children, for it has been poorly studied in the past but is now beginning to be more thoroughly understood.<ref name=faw>Fawcett J (2009) Report of the DSM-V Mood Disorders Work Group American Psychiatric Association. Available: http://www.psych.org/MainMenu/Research/DSMIV/DSMV/DSMRevisionActivities/DSM-V-Work-Group-Reports/Mood-Disorders-Work-Group-Report.aspx.  Accessed 15 March 2011.</ref>
Pediatric Bipolar Disorder (PBD) causes a significant impairment in the ability of children to function normally, especially in academics and psychosocial areas, and it is a chronic disorder that persists throughout the lifetime.[6.7] Children with PBD experience chronic periods of mania, characterized by elevated and irritable moods, or depression. PBD patients are ten times more likely to commit suicide than healthy children.[4, 8]  Severe manic and depressive symptoms are associated with early age of diagnosis, meaning children often display more acute symptoms than adults.[8] In children, mania often presents with psychotic symptoms and mixed manic depressive episodes.[2] Such a  presentation of mania often differs from classic descriptions of mania in adults, yet children who are diagnosed with bipolar disorder show the same brain abnormalities as adults, further complicating diagnosis. [2, 7] Children with PBD display anger, dysphoria, irritability, belligerence, and mixed-manic depressive symptoms more commonly and for more erratic time periods than adults. [2]


==Characteristics==


===Brain Structure===
Functional magnetic resonance imaging (fMRI) is a non-invasive tool used to show concrete links between brain functioning and psychiatric disorders.  Changes in blood flow in the brain, which are indicators of neural activity, can be viewed using fMRI technology.  Using fMRI images, altered mechanisms of brain functioning have been seen in PBD patients in brain areas such as the ventral prefrontal cortex, cingulated cortex, amygdalae, and hippocampus.[7] In fMRI comparisons of healthy children with previously unmediated PBD patients, treatment of the PBD patients with a second generation antipsychotic then an anticonvulsant resulted in increased activity in affective brain regions while cognitive regions showed decreased brain activity.[9]  Prescription of antipsychotics may permanently alter the brain development in children, as shown by fMRI studies, and is a reason why treatment plans should be carefully monitored.


===Signs and symptoms===
Pediatric bipolar disorder (PBD) causes a significant impairment in the ability of children to function normally, especially in academics and psychosocial areas, and it is a chronic disorder that persists throughout the lifetime.<ref name=sch>Scheffer RE, Tripathi A, Kirkpatrick FG, Schultz T (2010) Rapid Quetiapine Loading in Youths with Bipolar Disorder J. Child Adol. Psychop 20:441-445  </ref><ref name=man>Mana S, Martinot MLP, Martinot JL  (2010) Brain Imaging Findings in Children and Adolescents with Mental Disorders: A Cross-sectional Review  J Eurpsy 25: 345-354</ref> Children with PBD experience chronic periods of mania, characterized by elevated and irritable moods, or depression. PBD patients are ten times more likely to commit suicide than healthy children.<ref name=Nand>Nandagopal JJ and DelBello MP (2010)  Pharmacotherapy for Pediatric Bipolar Disorder  Psychiatric Annals 4:221-230</ref><ref name=wag>Wagner KD, Redden L, Kowatch RA, Willens T, Segal S, et al. (2009) A double-blind, randomized, placebo-controlled trial of divalproex extended-release in the treatment of bipolar disorder in children and adolescents J Am Acad Child Adolesc Psychiatry 48: 519-532 </ref>  Severe manic and depressive symptoms are associated with early age of diagnosis, meaning children often display more acute symptoms than adults.<ref name=wag>Wagner KD, Redden L, Kowatch RA, Willens T, Segal S, et al. (2009) A double-blind, randomized, placebo-controlled trial of divalproex extended-release in the treatment of bipolar disorder in children and adolescents J Am Acad Child Adolesc Psychiatry 48: 519-532 </ref>  Children with PBD display anger, dysphoria, irritability, belligerence, and mixed-manic depressive symptoms more commonly and for more erratic time periods than adults.<ref name=McCl> McClellan J, Kowatch R, Findling R (2008) Practice Parameter for the Assessment and Treatment of Children and Adolescents With Bipolar Disorder  J Am Acad Child Adolesc Psychiatry 1: 107-125</ref><ref name=man>Mana S, Martinot MLP, Martinot JL  (2010) Brain Imaging Findings in Children and Adolescents with Mental Disorders: A Cross-sectional Review  J Eurpsy 25: 345-354</ref> In children, mania often presents with psychotic symptoms and mixed manic depressive episodes, yet these symptoms differ from classical descriptions of mania in adults.<ref name=McCl> McClellan J, Kowatch R, Findling R (2008) Practice Parameter for the Assessment and Treatment of Children and Adolescents With Bipolar Disorder  J Am Acad Child Adolesc Psychiatry 1: 107-125</ref> Although the presentation of manic periods in children is unique,children who are diagnosed with bipolar disorder show the same brain abnormalities as adults, further complicating diagnosis.<ref name=McCl> McClellan J, Kowatch R, Findling R (2008) Practice Parameter for the Assessment and Treatment of Children and Adolescents With Bipolar Disorder  J Am Acad Child Adolesc Psychiatry 1: 107-125</ref>
===Brain structure===
[[Functional magnetic resonance imaging]] (fMRI) is a non-invasive tool used to show concrete links between brain functioning and psychiatric disorders.  fMRI technology produces images which show how blood flow in the brain changes. Neural activity can therefore be visualized because it causes changes of blood flow in the brain.    Using fMRI images, altered mechanisms of brain functioning have been seen in PBD patients in brain areas such as the ventral prefrontal cortex, cingulated cortex, amygdalae, and hippocampus.<ref name=man>Mana S, Martinot MLP, Martinot JL  (2010) Brain Imaging Findings in Children and Adolescents with Mental Disorders: A Cross-sectional Review  J Eurpsy 25: 345-354</ref> In fMRI comparisons of healthy children with previously unmediated PBD patients, treatment of the PBD patients with a second generation antipsychotic and an anticonvulsant resulted in increased activity in affective brain regions and decreased activity in cognitive brain regions.<ref name=pavu>Pavuluri MN, Passarotti AM, Parnes SA, Fitzgerald JM, Sweeney JA (2010)  A Pharmacological Functional Magnetic resonance imaging Study Probing the Interface of Cognitive and Emotional Brain Systems in Pediatric Bipolar Disorder J Child Adol Psychop 20: 395-406  </ref>  fMRI studies show prescription of antipsychotics may permanently alter the brain development in children, and it is a reason why treatment plans should be carefully monitored.


==Treatment==
==Treatment==
Prompt treatment of PBD is important because it minimizes developmental delays and dysfunctions; however, current treatment recommendations are based off of adult treatment models.<ref name=sch>Scheffer RE, Tripathi A, Kirkpatrick FG, Schultz T (2010) Rapid Quetiapine Loading in Youths with Bipolar Disorder J. Child Adol. Psychop 20:441-445  </ref><ref name=man>Mana S, Martinot MLP, Martinot JL  (2010) Brain Imaging Findings in Children and Adolescents with Mental Disorders: A Cross-sectional Review  J Eurpsy 25: 345-354</ref> 


===Pscychopharmacology===
===Psychopharmacology===
Prompt treatment of PBD is important because it minimizes developmental delays and dysfunctions; however, current treatment recommendations are based off of adult treatment models.[6, 7]  Increasingly, psychopharmacology is being looked to for treatment of PBD, but studies showing the safety and efficacy of psychopharmacology in treating PBD are rare.  From 1993 to 2003, 90.6% of pediatric bipolar patients who visited an outpatient physician practice were prescribed a psychotropic medication.[10] Although doctors are prescribing medication to treat PBD, there is no standard treatment for it because the current research available has found high rates of adverse events in many pharmacological treatment options and that children are at greater risk for adverse events when taking such medications.  Current treatment options for bipolar disorder in children include antipsychotics, atypical antipsychotics, second generation antipsychotics, mood stabilizers, or anticonvulsants.  The only FDA medications approved to treat bipolar disorder in children are: lithium, risperidone, aripiprazole, olanzinpine, and aripriprazole; however, even these drugs have negative side effects such as sedation, somnolence, and weight gain.[4,8]   
Increasingly, psychopharmacology is being looked to for treatment of PBD, but studies showing the safety and efficacy of psychopharmacology in treating PBD are rare.  From 1993 to 2003, 90.6% of pediatric bipolar patients who visited an outpatient physician practice were prescribed a psychotropic medication.<ref name=more>Moreno C, Gonzaol L, Blanco C, Huiping J, Schmidt AB, et al. (2007) National Trends in the Outpatient Diagnosis and Treatment of Bipolar Disorder in Youth  Arch Gen Psychiatry 64: 1032-1039</ref> Although doctors are prescribing medication to treat PBD, there is no standard treatment for it because the current research available has found high rates of adverse events in many pharmacological treatment options, and children have been found to be at greater risk for adverse events when taking psychotropic medications.  Current treatment options for bipolar disorder in children include [[antipsychotic]]s, atypical antipsychotics, second generation antipsychotics, mood stabilizers, and [[anticonvulsant]]s.  The only FDA medications approved to treat bipolar disorder in children are: lithium, risperidone, aripiprazole, olanzinpine, and aripriprazole; however, even these FDA approved drugs have negative side effects such as sedation, somnolence, and weight gain.<ref name=Nand>Nandagopal JJ and DelBello MP (2010) Pharmacotherapy for Pediatric Bipolar Disorder  Psychiatric Annals 4:221-230</ref><ref name=wag>Wagner KD, Redden L, Kowatch RA, Willens T, Segal S, et al. (2009) A double-blind, randomized, placebo-controlled trial of divalproex extended-release in the treatment of bipolar disorder in children and adolescents J Am Acad Child Adolesc Psychiatry 48: 519-532 </ref>
 
 
===Alternative Treatments===
Alternative treatments have been shown to reduce bipolar symptoms while causing few side effects.  One current theory is omega-3 fatty acids eicosapentaenoic acid (EPA) and docosahexaenoic acid (DHA) may help to manage bipolar disorder in children.[11] Both EPA, which can be metabolized into DHA, and DHA are components of cell membranes, and abnormalities of these phospholipids in cell membranes have been found in bipolar disorder.[11]    PBD patients who supplemented their diet with omega-3 fatty acids saw a reduction of mania symptoms.[8] Other alternative treatments, such as a micronutrient diet, have found similar results.  In one study of using micronutrients to treat PBD, parents purchased a 36-ingredient micronutrient product and monitored their child’s progress over six months.[12]  Symptoms were reduced by 50% in almost half of the subjects, with few side effects. [12]
 


===Pscyhotherapy===
===Alternative treatments===
Psychotherapy has also been shown to be helpful in treatment of BD. [3] In individual psychotherapy, children are closely monitored for symptoms and progress while gaining life skills.[2] Because PBD impacts children’s academic, social, and family life, psychotherapy is also used to help mange functional and developmental impairments.[2] Through educating and informing parents and family members, children with PBD are able to maintain treatment gains.[3]  By educating family members, medication adherence and communication within the family is improved, leading to greater treatment gains.[2]  
Alternative treatments have been shown to reduce bipolar symptoms while causing few side effects.  One current theory is omega-3 [[fatty acid]]s eicosapentaenoic acid (EPA) and docosahexaenoic acid (DHA) may help to manage bipolar disorder in children.<ref name=woz>Wozniak J, Biederman J, Mick E, Waxmonsky J, Hantsoo L et al. (2007) Omega-3 fatty acid monotherapy for pediatric bipolar disorder: A prospective open-label trial J Euro Neuro17: 440-447</ref> Both EPA, which can be metabolized into DHA, and DHA are [[phospholipid]] components of cell membranes, and abnormalities of these phospholipids in [[cell membrane]]s have been found in bipolar disorder.<ref name=woz>Wozniak J, Biederman J, Mick E, Waxmonsky J, Hantsoo L et al. (2007) Omega-3 fatty acid monotherapy for pediatric bipolar disorder: A prospective open-label trial J Euro Neuro17: 440-447</ref>    PBD patients who supplemented their diet with omega-3 fatty acids saw a reduction of mania symptoms.<ref name=wag>Wagner KD, Redden L, Kowatch RA, Willens T, Segal S, et al. (2009) A double-blind, randomized, placebo-controlled trial of divalproex extended-release in the treatment of bipolar disorder in children and adolescents J Am Acad Child Adolesc Psychiatry 48: 519-532 </ref> Other alternative treatments, such as a micronutrient diet, have found similar resultsIn one study of using micronutrients to treat PBD, parents purchased a 36-ingredient micronutrient product and monitored their child’s progress over six months.<ref name=ruc>Rucklidge JJ, Gately D, Kaplan BJ (2010) Database Analysis of Children and Adolescents with Bipolar Disorder Consuming a Micronutrient Formula  BMC Psychiatry 10: 74-88</ref>  Symptoms were reduced by 50% in almost half of the subjects, and there were few side effects.<ref name=ruc>Rucklidge JJ, Gately D, Kaplan BJ (2010) Database Analysis of Children and Adolescents with Bipolar Disorder Consuming a Micronutrient Formula BMC Psychiatry 10: 74-88</ref>


 
===Psychotherapy===
[[Psychotherapy]] has also been shown to be helpful in treatment of PBD.<ref name=Cum>Cummings CM and Fristad MA (2008)  Pediatric bipolar disorder: recognition in primary care Current Opinion in Pediatrics 20: 560-565</ref>  In individual psychotherapy, children are closely monitored for symptoms and progress,and they are also taught life skills by a therapist.<ref name=McCl> McClellan J, Kowatch R, Findling R (2008) Practice Parameter for the Assessment and Treatment of Children and Adolescents With Bipolar Disorder  J Am Acad Child Adolesc Psychiatry 1: 107-125</ref>  Because PBD impacts children’s academic, social, and family life, psychotherapy is also used to help manage functional and developmental impairments.<ref name=McCl> McClellan J, Kowatch R, Findling R (2008) Practice Parameter for the Assessment and Treatment of Children and Adolescents With Bipolar Disorder  J Am Acad Child Adolesc Psychiatry 1: 107-125</ref>  One additional aspect of psychotherapy in treating PBD is family therapy.  Through educating and informing parents and family members, children with PBD are able to maintain treatment gains.<ref name=Cum>Cummings CM and Fristad MA (2008)  Pediatric bipolar disorder: recognition in primary care Current Opinion in Pediatrics 20: 560-565</ref>  Additionally, by educating family members, medication adherence and communication within the family is improved, leading to greater treatment gains.<ref name=McCl> McClellan J, Kowatch R, Findling R (2008) Practice Parameter for the Assessment and Treatment of Children and Adolescents With Bipolar Disorder  J Am Acad Child Adolesc Psychiatry 1: 107-125</ref>


==References==
==References==
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[[User:Jessica Kelly|Jessica Kelly]] 01:03, 23 March 2011 (UTC)

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The diagnosis of bipolar disorder in children has many similarities to that of the same disease in adults (BD), a type of mood disorder previously called manic-depressive disorder. All forms of BD are characterized by periods of extremely elevated or irritable mood, which can sometimes alternate with episodes of depression. Bipolar disorder can be diagnosed in children as young as preschool.[1] The lifetime prevalence of BD is between 0.5 to 1.6%, and the prevalence may be as high as 1% in youths alone.[2] When diagnosed in children, BD is most commonly characterized by increased energy, distractibility, pressured speech, irritable mood, grandiosity, and elevated mood.[1] BD is an increasingly common diagnosis in children, due to several factors including an expansion of diagnosis criteria from classic manic depressive symptoms to more general manic symptoms, availability of knowledge about BD in children, and desire for insurance reimbursement for treating symptomatic behaviors of bipolar disorder.[1][2][3]

The diagnosis of bipolar disorder in children is a highly controversial issue, as the disease was previously thought to rarely occur in youths.[2][3] However, more than 60% of adults with BD report having their first mood episode before the age of 19, as the typical age of onset is during adolescence.[4] When the DSM-IV was published in 1994, pediatric bipolar disorder was not included as a diagnosis. Currently, the American Psychological Association is currently working on criteria and classification for a new subset of BD, Pediatric Bipolar Disorder (PBD), to be included in the 2013 publication of DSM-V.[5] One of the main challenges in categorizing PBD as a separate diagnosis in DSM-V is understanding the symptomology of BD in children, for it has been poorly studied in the past but is now beginning to be more thoroughly understood.[5]

Characteristics

Signs and symptoms

Pediatric bipolar disorder (PBD) causes a significant impairment in the ability of children to function normally, especially in academics and psychosocial areas, and it is a chronic disorder that persists throughout the lifetime.[6][7] Children with PBD experience chronic periods of mania, characterized by elevated and irritable moods, or depression. PBD patients are ten times more likely to commit suicide than healthy children.[4][8] Severe manic and depressive symptoms are associated with early age of diagnosis, meaning children often display more acute symptoms than adults.[8] Children with PBD display anger, dysphoria, irritability, belligerence, and mixed-manic depressive symptoms more commonly and for more erratic time periods than adults.[2][7] In children, mania often presents with psychotic symptoms and mixed manic depressive episodes, yet these symptoms differ from classical descriptions of mania in adults.[2] Although the presentation of manic periods in children is unique,children who are diagnosed with bipolar disorder show the same brain abnormalities as adults, further complicating diagnosis.[2]

Brain structure

Functional magnetic resonance imaging (fMRI) is a non-invasive tool used to show concrete links between brain functioning and psychiatric disorders. fMRI technology produces images which show how blood flow in the brain changes. Neural activity can therefore be visualized because it causes changes of blood flow in the brain. Using fMRI images, altered mechanisms of brain functioning have been seen in PBD patients in brain areas such as the ventral prefrontal cortex, cingulated cortex, amygdalae, and hippocampus.[7] In fMRI comparisons of healthy children with previously unmediated PBD patients, treatment of the PBD patients with a second generation antipsychotic and an anticonvulsant resulted in increased activity in affective brain regions and decreased activity in cognitive brain regions.[9] fMRI studies show prescription of antipsychotics may permanently alter the brain development in children, and it is a reason why treatment plans should be carefully monitored.

Treatment

Prompt treatment of PBD is important because it minimizes developmental delays and dysfunctions; however, current treatment recommendations are based off of adult treatment models.[6][7]

Psychopharmacology

Increasingly, psychopharmacology is being looked to for treatment of PBD, but studies showing the safety and efficacy of psychopharmacology in treating PBD are rare. From 1993 to 2003, 90.6% of pediatric bipolar patients who visited an outpatient physician practice were prescribed a psychotropic medication.[10] Although doctors are prescribing medication to treat PBD, there is no standard treatment for it because the current research available has found high rates of adverse events in many pharmacological treatment options, and children have been found to be at greater risk for adverse events when taking psychotropic medications. Current treatment options for bipolar disorder in children include antipsychotics, atypical antipsychotics, second generation antipsychotics, mood stabilizers, and anticonvulsants. The only FDA medications approved to treat bipolar disorder in children are: lithium, risperidone, aripiprazole, olanzinpine, and aripriprazole; however, even these FDA approved drugs have negative side effects such as sedation, somnolence, and weight gain.[4][8]

Alternative treatments

Alternative treatments have been shown to reduce bipolar symptoms while causing few side effects. One current theory is omega-3 fatty acids eicosapentaenoic acid (EPA) and docosahexaenoic acid (DHA) may help to manage bipolar disorder in children.[11] Both EPA, which can be metabolized into DHA, and DHA are phospholipid components of cell membranes, and abnormalities of these phospholipids in cell membranes have been found in bipolar disorder.[11] PBD patients who supplemented their diet with omega-3 fatty acids saw a reduction of mania symptoms.[8] Other alternative treatments, such as a micronutrient diet, have found similar results. In one study of using micronutrients to treat PBD, parents purchased a 36-ingredient micronutrient product and monitored their child’s progress over six months.[12] Symptoms were reduced by 50% in almost half of the subjects, and there were few side effects.[12]

Psychotherapy

Psychotherapy has also been shown to be helpful in treatment of PBD.[3] In individual psychotherapy, children are closely monitored for symptoms and progress,and they are also taught life skills by a therapist.[2] Because PBD impacts children’s academic, social, and family life, psychotherapy is also used to help manage functional and developmental impairments.[2] One additional aspect of psychotherapy in treating PBD is family therapy. Through educating and informing parents and family members, children with PBD are able to maintain treatment gains.[3] Additionally, by educating family members, medication adherence and communication within the family is improved, leading to greater treatment gains.[2]

References

  1. 1.0 1.1 1.2 Carr A. 2009. Bipolar disorder in young people: Description, assessment and evidence-based treatment. Devel. Neurorehabilitation. 12: 427-441
  2. 2.0 2.1 2.2 2.3 2.4 2.5 2.6 2.7 2.8 McClellan J, Kowatch R, Findling R (2008) Practice Parameter for the Assessment and Treatment of Children and Adolescents With Bipolar Disorder J Am Acad Child Adolesc Psychiatry 1: 107-125
  3. 3.0 3.1 3.2 3.3 Cummings CM and Fristad MA (2008) Pediatric bipolar disorder: recognition in primary care Current Opinion in Pediatrics 20: 560-565
  4. 4.0 4.1 4.2 Nandagopal JJ and DelBello MP (2010) Pharmacotherapy for Pediatric Bipolar Disorder Psychiatric Annals 4:221-230
  5. 5.0 5.1 Fawcett J (2009) Report of the DSM-V Mood Disorders Work Group American Psychiatric Association. Available: http://www.psych.org/MainMenu/Research/DSMIV/DSMV/DSMRevisionActivities/DSM-V-Work-Group-Reports/Mood-Disorders-Work-Group-Report.aspx. Accessed 15 March 2011.
  6. 6.0 6.1 Scheffer RE, Tripathi A, Kirkpatrick FG, Schultz T (2010) Rapid Quetiapine Loading in Youths with Bipolar Disorder J. Child Adol. Psychop 20:441-445
  7. 7.0 7.1 7.2 7.3 Mana S, Martinot MLP, Martinot JL (2010) Brain Imaging Findings in Children and Adolescents with Mental Disorders: A Cross-sectional Review J Eurpsy 25: 345-354
  8. 8.0 8.1 8.2 8.3 Wagner KD, Redden L, Kowatch RA, Willens T, Segal S, et al. (2009) A double-blind, randomized, placebo-controlled trial of divalproex extended-release in the treatment of bipolar disorder in children and adolescents J Am Acad Child Adolesc Psychiatry 48: 519-532
  9. Pavuluri MN, Passarotti AM, Parnes SA, Fitzgerald JM, Sweeney JA (2010) A Pharmacological Functional Magnetic resonance imaging Study Probing the Interface of Cognitive and Emotional Brain Systems in Pediatric Bipolar Disorder J Child Adol Psychop 20: 395-406
  10. Moreno C, Gonzaol L, Blanco C, Huiping J, Schmidt AB, et al. (2007) National Trends in the Outpatient Diagnosis and Treatment of Bipolar Disorder in Youth Arch Gen Psychiatry 64: 1032-1039
  11. 11.0 11.1 Wozniak J, Biederman J, Mick E, Waxmonsky J, Hantsoo L et al. (2007) Omega-3 fatty acid monotherapy for pediatric bipolar disorder: A prospective open-label trial J Euro Neuro17: 440-447
  12. 12.0 12.1 Rucklidge JJ, Gately D, Kaplan BJ (2010) Database Analysis of Children and Adolescents with Bipolar Disorder Consuming a Micronutrient Formula BMC Psychiatry 10: 74-88


Jessica Kelly 01:03, 23 March 2011 (UTC)