Whitney McKnight

Alcohol was involved in nearly one-quarter of all opioid pain reliever–related deaths and just over 20% of deaths related to benzodiazepines, according to a study of 2010 data released by the U.S. Food and Drug Administration and the Centers for Disease Control and Prevention.

Alcohol also was involved in nearly 20% of opioid abuse–related visits to the emergency department in that year, and over a quarter of visits for benzodiazepine drug abuse–related ones. Men were almost twice as likely as women to be admitted to the ED for alcohol/opioid abuse and slightly less than that for alcohol/benzodiazepine-related abuse.

© iStock / ThinkStockPhotos.com

Opioids such as hydrocodone mixed with acetaminophen (Vicodin) are commonly prescribed for chronic pain, while benzodiazepines such as diazepam (Valium) are often prescribed for anxiety disorders or insomnia. According to the CDC, in 2012 health care providers wrote 259 million prescriptions for painkillers or, put another way, one bottle of prescription painkillers for every adult in America. The report is based on an analysis of data reported in 2010 by 237 hospital EDs and medical examiners across 13 states to the Drug Abuse Warning Network, which is sponsored by the Substance Abuse and Mental Health Services Administration. Alcohol was involved in just over 22% of opioid and 21.4% of benzodiazepine drug-related deaths, and alcohol was involved in 18.5% of opioid and 27.2% of benzodiazepine drug abuse–related ED visits during the period reported, according to the analysis.

In all, there were 438,718 ED visits related to opioid abuse alone or in combination with other drugs: An estimated 81,365 (18.5%) of those visits involved alcohol. Another 408,021 ED visits were related to benzodiazepine abuse, alone or in combination with other drugs: Of those, 111,165 (27.2%) involved alcohol. When opioids or benzodiazepines were the only drug classes in question, alcohol was involved in 26,446 (13.8%) opioid visits and 38,244 (34.1%) benzodiazepine visits (MMWR 2014;63:881-5).

One-fifth of those admitted to the ED for opioid abuse when alcohol was involved were 30-44 years old (20.6%), and an almost equal percentage (20%) were 45-54 years old. For benzodiazepine-related events, 45- to 54-year-olds were admitted most often (31.1%). ED admissions of men for alcohol/opioid events were significantly more common than for women (22.9% and 13.5%, respectively).

Although the study did not include data on exactly how much alcohol was ingested per each reported ED visit, “these findings indicate that alcohol plays a significant role in [opioid pain reliever] and benzodiazepine abuse. Interventions to reduce the abuse of alcohol and these drugs alone and in combination are needed,” study author Christopher M. Jones, Pharm.D., of the FDA and his colleagues wrote.

The survey was conducted by the FDA and the CDC.

[email protected]

On Twitter @whitneymcknight

Alcohol was involved in nearly one-quarter of all opioid pain reliever–related deaths and just over 20% of deaths related to benzodiazepines, according to a study of 2010 data released by the U.S. Food and Drug Administration and the Centers for Disease Control and Prevention.

Alcohol also was involved in nearly 20% of opioid abuse–related visits to the emergency department in that year, and over a quarter of visits for benzodiazepine drug abuse–related ones. Men were almost twice as likely as women to be admitted to the ED for alcohol/opioid abuse and slightly less than that for alcohol/benzodiazepine-related abuse.

© iStock / ThinkStockPhotos.com

Opioids such as hydrocodone mixed with acetaminophen (Vicodin) are commonly prescribed for chronic pain, while benzodiazepines such as diazepam (Valium) are often prescribed for anxiety disorders or insomnia. According to the CDC, in 2012 health care providers wrote 259 million prescriptions for painkillers or, put another way, one bottle of prescription painkillers for every adult in America. The report is based on an analysis of data reported in 2010 by 237 hospital EDs and medical examiners across 13 states to the Drug Abuse Warning Network, which is sponsored by the Substance Abuse and Mental Health Services Administration. Alcohol was involved in just over 22% of opioid and 21.4% of benzodiazepine drug-related deaths, and alcohol was involved in 18.5% of opioid and 27.2% of benzodiazepine drug abuse–related ED visits during the period reported, according to the analysis.

In all, there were 438,718 ED visits related to opioid abuse alone or in combination with other drugs: An estimated 81,365 (18.5%) of those visits involved alcohol. Another 408,021 ED visits were related to benzodiazepine abuse, alone or in combination with other drugs: Of those, 111,165 (27.2%) involved alcohol. When opioids or benzodiazepines were the only drug classes in question, alcohol was involved in 26,446 (13.8%) opioid visits and 38,244 (34.1%) benzodiazepine visits (MMWR 2014;63:881-5).

One-fifth of those admitted to the ED for opioid abuse when alcohol was involved were 30-44 years old (20.6%), and an almost equal percentage (20%) were 45-54 years old. For benzodiazepine-related events, 45- to 54-year-olds were admitted most often (31.1%). ED admissions of men for alcohol/opioid events were significantly more common than for women (22.9% and 13.5%, respectively).

Although the study did not include data on exactly how much alcohol was ingested per each reported ED visit, “these findings indicate that alcohol plays a significant role in [opioid pain reliever] and benzodiazepine abuse. Interventions to reduce the abuse of alcohol and these drugs alone and in combination are needed,” study author Christopher M. Jones, Pharm.D., of the FDA and his colleagues wrote.

The survey was conducted by the FDA and the CDC.

[email protected]

On Twitter @whitneymcknight

Alcohol was involved in nearly one-quarter of all opioid pain reliever–related deaths and just over 20% of deaths related to benzodiazepines, according to a study of 2010 data released by the U.S. Food and Drug Administration and the Centers for Disease Control and Prevention.

Alcohol also was involved in nearly 20% of opioid abuse–related visits to the emergency department in that year, and over a quarter of visits for benzodiazepine drug abuse–related ones. Men were almost twice as likely as women to be admitted to the ED for alcohol/opioid abuse and slightly less than that for alcohol/benzodiazepine-related abuse.

© iStock / ThinkStockPhotos.com

Opioids such as hydrocodone mixed with acetaminophen (Vicodin) are commonly prescribed for chronic pain, while benzodiazepines such as diazepam (Valium) are often prescribed for anxiety disorders or insomnia. According to the CDC, in 2012 health care providers wrote 259 million prescriptions for painkillers or, put another way, one bottle of prescription painkillers for every adult in America. The report is based on an analysis of data reported in 2010 by 237 hospital EDs and medical examiners across 13 states to the Drug Abuse Warning Network, which is sponsored by the Substance Abuse and Mental Health Services Administration. Alcohol was involved in just over 22% of opioid and 21.4% of benzodiazepine drug-related deaths, and alcohol was involved in 18.5% of opioid and 27.2% of benzodiazepine drug abuse–related ED visits during the period reported, according to the analysis.

In all, there were 438,718 ED visits related to opioid abuse alone or in combination with other drugs: An estimated 81,365 (18.5%) of those visits involved alcohol. Another 408,021 ED visits were related to benzodiazepine abuse, alone or in combination with other drugs: Of those, 111,165 (27.2%) involved alcohol. When opioids or benzodiazepines were the only drug classes in question, alcohol was involved in 26,446 (13.8%) opioid visits and 38,244 (34.1%) benzodiazepine visits (MMWR 2014;63:881-5).

One-fifth of those admitted to the ED for opioid abuse when alcohol was involved were 30-44 years old (20.6%), and an almost equal percentage (20%) were 45-54 years old. For benzodiazepine-related events, 45- to 54-year-olds were admitted most often (31.1%). ED admissions of men for alcohol/opioid events were significantly more common than for women (22.9% and 13.5%, respectively).

Although the study did not include data on exactly how much alcohol was ingested per each reported ED visit, “these findings indicate that alcohol plays a significant role in [opioid pain reliever] and benzodiazepine abuse. Interventions to reduce the abuse of alcohol and these drugs alone and in combination are needed,” study author Christopher M. Jones, Pharm.D., of the FDA and his colleagues wrote.

The survey was conducted by the FDA and the CDC.

[email protected]

On Twitter @whitneymcknight

Are rheumatoid arthritis patients who are told that they meet criteria for clinical remission getting the full story?

“Despite clinical remission, histology and imaging studies documented a persistently active disease state that may benefit from more aggressive therapy.” That’s the conclusion of Dr. Allen P. Anandarajah, an immunology and rheumatology researcher at the University of Rochester (N.Y.), and his colleagues, who documented persistently active rheumatoid arthritis (RA) in more than three-quarters of 14 patients in clinical remission (J. Rheumatol. 2014 [doi:10.3899/jrheum.140411]).

The study is the latest addition to the literature demonstrating that the sensitivity of current criteria for measuring diminished disease activity in persons with RA is too low (Arthritis Rheum. 2005;52:3381-90; Ann. Rheum. Dis. 2010;69:631-7; and Semin. Arthritis Rheum. 2005;35:185-96).

“The current outcome measures fall short,” Dr. Anandarajah and his coauthors wrote. “A major gap to be addressed is accurate and reliable methods to detect active synovitis in patients deemed to be in clinical remission.”

Dr. Anandarajah and his colleagues retrospectively analyzed 15 synovial specimens from 14 patients who met 1996 revised American College of Rheumatology criteria for clinical remission from RA who had undergone orthopedic surgery. The investigators also scored histologic specimens for hyperplasia of synovial lining and stroma, as well as inflammation, lymphoid follicles, and vascularity.

The disease-modifying antirheumatic drug regimens for the patients included four on anti–tumor necrosis factor therapy (two monotherapy and two with methotrexate); four were receiving methotrexate alone; four were on combined methotrexate and hydroxychloroquine therapy; one on methotrexate and low-dose prednisone; and one on hydroxychloroquine, sulfasalazine, and low-dose prednisone.

On histology, the investigators rated disease activity as severe in four specimens, moderate in six, mild in three, and minimal in two. Three of the four specimens with minimal and mild histology were from those receiving anti-tumor necrosis factor therapy.

The investigators detected synovitis on ultrasound grayscale in 8 of 10 joints in nine patients and power Doppler signal in 6 of 10 joints. Synovitis and bone marrow edema was shown on MRI scans in six of seven patients. The authors also calculated positive, although not significant, correlations between synovitis scores on ultrasonography and histology.

Although the study was limited in that the evaluations were scored retrospectively, and the images had been obtained for reasons other than future scoring of synovitis, the authors wrote that their findings were evidence that additional prospective studies could help determine whether incorporating histologic and imaging studies into remission criteria would be beneficial.

No disclosures were reported with the study.

[email protected]

On Twitter @whitneymcknight

Are rheumatoid arthritis patients who are told that they meet criteria for clinical remission getting the full story?

“Despite clinical remission, histology and imaging studies documented a persistently active disease state that may benefit from more aggressive therapy.” That’s the conclusion of Dr. Allen P. Anandarajah, an immunology and rheumatology researcher at the University of Rochester (N.Y.), and his colleagues, who documented persistently active rheumatoid arthritis (RA) in more than three-quarters of 14 patients in clinical remission (J. Rheumatol. 2014 [doi:10.3899/jrheum.140411]).

The study is the latest addition to the literature demonstrating that the sensitivity of current criteria for measuring diminished disease activity in persons with RA is too low (Arthritis Rheum. 2005;52:3381-90; Ann. Rheum. Dis. 2010;69:631-7; and Semin. Arthritis Rheum. 2005;35:185-96).

“The current outcome measures fall short,” Dr. Anandarajah and his coauthors wrote. “A major gap to be addressed is accurate and reliable methods to detect active synovitis in patients deemed to be in clinical remission.”

Dr. Anandarajah and his colleagues retrospectively analyzed 15 synovial specimens from 14 patients who met 1996 revised American College of Rheumatology criteria for clinical remission from RA who had undergone orthopedic surgery. The investigators also scored histologic specimens for hyperplasia of synovial lining and stroma, as well as inflammation, lymphoid follicles, and vascularity.

The disease-modifying antirheumatic drug regimens for the patients included four on anti–tumor necrosis factor therapy (two monotherapy and two with methotrexate); four were receiving methotrexate alone; four were on combined methotrexate and hydroxychloroquine therapy; one on methotrexate and low-dose prednisone; and one on hydroxychloroquine, sulfasalazine, and low-dose prednisone.

On histology, the investigators rated disease activity as severe in four specimens, moderate in six, mild in three, and minimal in two. Three of the four specimens with minimal and mild histology were from those receiving anti-tumor necrosis factor therapy.

The investigators detected synovitis on ultrasound grayscale in 8 of 10 joints in nine patients and power Doppler signal in 6 of 10 joints. Synovitis and bone marrow edema was shown on MRI scans in six of seven patients. The authors also calculated positive, although not significant, correlations between synovitis scores on ultrasonography and histology.

Although the study was limited in that the evaluations were scored retrospectively, and the images had been obtained for reasons other than future scoring of synovitis, the authors wrote that their findings were evidence that additional prospective studies could help determine whether incorporating histologic and imaging studies into remission criteria would be beneficial.

No disclosures were reported with the study.

[email protected]

On Twitter @whitneymcknight

Are rheumatoid arthritis patients who are told that they meet criteria for clinical remission getting the full story?

“Despite clinical remission, histology and imaging studies documented a persistently active disease state that may benefit from more aggressive therapy.” That’s the conclusion of Dr. Allen P. Anandarajah, an immunology and rheumatology researcher at the University of Rochester (N.Y.), and his colleagues, who documented persistently active rheumatoid arthritis (RA) in more than three-quarters of 14 patients in clinical remission (J. Rheumatol. 2014 [doi:10.3899/jrheum.140411]).

The study is the latest addition to the literature demonstrating that the sensitivity of current criteria for measuring diminished disease activity in persons with RA is too low (Arthritis Rheum. 2005;52:3381-90; Ann. Rheum. Dis. 2010;69:631-7; and Semin. Arthritis Rheum. 2005;35:185-96).

“The current outcome measures fall short,” Dr. Anandarajah and his coauthors wrote. “A major gap to be addressed is accurate and reliable methods to detect active synovitis in patients deemed to be in clinical remission.”

Dr. Anandarajah and his colleagues retrospectively analyzed 15 synovial specimens from 14 patients who met 1996 revised American College of Rheumatology criteria for clinical remission from RA who had undergone orthopedic surgery. The investigators also scored histologic specimens for hyperplasia of synovial lining and stroma, as well as inflammation, lymphoid follicles, and vascularity.

The disease-modifying antirheumatic drug regimens for the patients included four on anti–tumor necrosis factor therapy (two monotherapy and two with methotrexate); four were receiving methotrexate alone; four were on combined methotrexate and hydroxychloroquine therapy; one on methotrexate and low-dose prednisone; and one on hydroxychloroquine, sulfasalazine, and low-dose prednisone.

On histology, the investigators rated disease activity as severe in four specimens, moderate in six, mild in three, and minimal in two. Three of the four specimens with minimal and mild histology were from those receiving anti-tumor necrosis factor therapy.

The investigators detected synovitis on ultrasound grayscale in 8 of 10 joints in nine patients and power Doppler signal in 6 of 10 joints. Synovitis and bone marrow edema was shown on MRI scans in six of seven patients. The authors also calculated positive, although not significant, correlations between synovitis scores on ultrasonography and histology.

Although the study was limited in that the evaluations were scored retrospectively, and the images had been obtained for reasons other than future scoring of synovitis, the authors wrote that their findings were evidence that additional prospective studies could help determine whether incorporating histologic and imaging studies into remission criteria would be beneficial.

No disclosures were reported with the study.

[email protected]

On Twitter @whitneymcknight

The best time to offer pain relief to a woman in labor is when she requests it, according to a study.

“The evidence we have does not provide a compelling reason why this [request] should be refused,” Dr. Ban Leong Sng, head of women’s anesthesia at KK Women’s and Children’s Hospital in Singapore, said in a statement, speaking about mothers who ask for an epidural early in their labor. “The right time to give the epidural is when the woman requests pain relief.”

© iStock / ThinkStockPhotos.com

Although previous studies indicated that early initiation of an epidural correlated with longer labors and increased risk of cesarean delivery, Dr. Sng and his colleagues did not find clinically significant support for this in their meta-analysis of nine randomized, controlled studies of 15,752 pregnant women who received epidural at various times during their labor. The finding appears online in the Cochrane Library.

“There is predominantly high-quality evidence that early or late initiation of epidural analgesia for labor have similar effects on all measured outcomes,” Dr. Sng and his associates wrote.

The risk ratio for cesarean delivery with early vs. late initiation of epidural was 1.02 (95% confidence interval, 0.96 to 1.08). Similarly, there was no notable difference in the risk for instrumental birth correlative to the timing of the epidural (relative risk 0.93%; 95% CI 0.86 to 1.01).

The mean difference between early or late epidural when it came to the duration of the second stage of labor was about three and a half minutes (95% CI, -6.71 to 0.27). The authors noted that there was “significant heterogeneity” in the duration of the first stage of labor, and that their data were not pooled.

As for fetal outcomes, results were similar. The differences in Apgar scores of less than 7 at 1 minute post partum in infants born to mothers who’d had early or late initiation of pain relief was negligible (RR 0.96; 95% CI 0.84 to 1.10). There also were no clinically significant differences in Apgar scores less than 7 at 5 minutes post partum (RR 0.96; 95% CI, 0.69 to 1.33).

In addition, the difference in umbilical arterial pH in infants born to mothers with early or late epidural was negligible (mean difference, 0.01; 95% CI -0.01 to 0.03).

The authors noted the studies they analyzed varied in their definition of “early” and “late” epidural; however, early initiation was typically defined as when there was cervical dilation of less than 4-5 cm. Late initiation typically was considered to be when there was cervical dilation of 4-5 cm or more. Analgesic doses also varied across the studies, as did pain relief administered before initiation of the epidural.

[email protected]

On Twitter @whitneymcknight

The best time to offer pain relief to a woman in labor is when she requests it, according to a study.

“The evidence we have does not provide a compelling reason why this [request] should be refused,” Dr. Ban Leong Sng, head of women’s anesthesia at KK Women’s and Children’s Hospital in Singapore, said in a statement, speaking about mothers who ask for an epidural early in their labor. “The right time to give the epidural is when the woman requests pain relief.”

© iStock / ThinkStockPhotos.com

Although previous studies indicated that early initiation of an epidural correlated with longer labors and increased risk of cesarean delivery, Dr. Sng and his colleagues did not find clinically significant support for this in their meta-analysis of nine randomized, controlled studies of 15,752 pregnant women who received epidural at various times during their labor. The finding appears online in the Cochrane Library.

“There is predominantly high-quality evidence that early or late initiation of epidural analgesia for labor have similar effects on all measured outcomes,” Dr. Sng and his associates wrote.

The risk ratio for cesarean delivery with early vs. late initiation of epidural was 1.02 (95% confidence interval, 0.96 to 1.08). Similarly, there was no notable difference in the risk for instrumental birth correlative to the timing of the epidural (relative risk 0.93%; 95% CI 0.86 to 1.01).

The mean difference between early or late epidural when it came to the duration of the second stage of labor was about three and a half minutes (95% CI, -6.71 to 0.27). The authors noted that there was “significant heterogeneity” in the duration of the first stage of labor, and that their data were not pooled.

As for fetal outcomes, results were similar. The differences in Apgar scores of less than 7 at 1 minute post partum in infants born to mothers who’d had early or late initiation of pain relief was negligible (RR 0.96; 95% CI 0.84 to 1.10). There also were no clinically significant differences in Apgar scores less than 7 at 5 minutes post partum (RR 0.96; 95% CI, 0.69 to 1.33).

In addition, the difference in umbilical arterial pH in infants born to mothers with early or late epidural was negligible (mean difference, 0.01; 95% CI -0.01 to 0.03).

The authors noted the studies they analyzed varied in their definition of “early” and “late” epidural; however, early initiation was typically defined as when there was cervical dilation of less than 4-5 cm. Late initiation typically was considered to be when there was cervical dilation of 4-5 cm or more. Analgesic doses also varied across the studies, as did pain relief administered before initiation of the epidural.

[email protected]

On Twitter @whitneymcknight

The best time to offer pain relief to a woman in labor is when she requests it, according to a study.

“The evidence we have does not provide a compelling reason why this [request] should be refused,” Dr. Ban Leong Sng, head of women’s anesthesia at KK Women’s and Children’s Hospital in Singapore, said in a statement, speaking about mothers who ask for an epidural early in their labor. “The right time to give the epidural is when the woman requests pain relief.”

© iStock / ThinkStockPhotos.com

Although previous studies indicated that early initiation of an epidural correlated with longer labors and increased risk of cesarean delivery, Dr. Sng and his colleagues did not find clinically significant support for this in their meta-analysis of nine randomized, controlled studies of 15,752 pregnant women who received epidural at various times during their labor. The finding appears online in the Cochrane Library.

“There is predominantly high-quality evidence that early or late initiation of epidural analgesia for labor have similar effects on all measured outcomes,” Dr. Sng and his associates wrote.

The risk ratio for cesarean delivery with early vs. late initiation of epidural was 1.02 (95% confidence interval, 0.96 to 1.08). Similarly, there was no notable difference in the risk for instrumental birth correlative to the timing of the epidural (relative risk 0.93%; 95% CI 0.86 to 1.01).

The mean difference between early or late epidural when it came to the duration of the second stage of labor was about three and a half minutes (95% CI, -6.71 to 0.27). The authors noted that there was “significant heterogeneity” in the duration of the first stage of labor, and that their data were not pooled.

As for fetal outcomes, results were similar. The differences in Apgar scores of less than 7 at 1 minute post partum in infants born to mothers who’d had early or late initiation of pain relief was negligible (RR 0.96; 95% CI 0.84 to 1.10). There also were no clinically significant differences in Apgar scores less than 7 at 5 minutes post partum (RR 0.96; 95% CI, 0.69 to 1.33).

In addition, the difference in umbilical arterial pH in infants born to mothers with early or late epidural was negligible (mean difference, 0.01; 95% CI -0.01 to 0.03).

The authors noted the studies they analyzed varied in their definition of “early” and “late” epidural; however, early initiation was typically defined as when there was cervical dilation of less than 4-5 cm. Late initiation typically was considered to be when there was cervical dilation of 4-5 cm or more. Analgesic doses also varied across the studies, as did pain relief administered before initiation of the epidural.

[email protected]

On Twitter @whitneymcknight

Patients with juvenile myoclonic epilepsy tend to have similar or better quality-of-life scores in adulthood in comparison with patients with absence epilepsy, except when there are comorbid psychiatric conditions, according to findings from a case-control study.

“In contrast to previous findings on social outcome in JME [juvenile myoclonic epilepsy], we demonstrated that the overall psychosocial outcome in the current JME patients was generally satisfying and – likewise important – did not differ from patients with absence epilepsy,” wrote the authors, including lead investigator, Dr. Martin Holtkamp, medical director at the Epilepsy Center Berlin-Brandenburg, Germany.

The findings showed that when compared with patients who had been diagnosed with childhood or juvenile absence epilepsy (AE), those with juvenile myoclonic epilepsy (JME) in their mid-40s were as likely or more likely to have a college degree, steady employment, and full integration into their social context.

“At the end of follow-up, we found only one variable to be significantly different comparing psychosocial long-term outcome in JME and AE patients,” Dr. Holtkamp and his colleagues wrote. That variable was that nearly three-quarters of JME patients had either qualified for or achieved a university education, whereas only 34.1% of AE patients had done so (P = .001).

The investigators retrospectively analyzed the records of 41 adult JME patients and 41 adult AE patients whose first treatment contact occurred at the neurology department at the Charity University Hospital Berlin between 1955 and 2000. All patients included in the study had been diagnosed with their subsyndrome of epilepsy for at least 20 years (Epilepsia 2014 Sept. 10 [doi:10.1111/epi.12751]).

Patients in each group were contacted and asked to complete a questionnaire about their education, professional situation, family and social life, as well as their psychiatric conditions and any medications used to treat them. Each group was also asked to complete the validated Quality of Life in Epilepsy Inventory 31 survey (in German).In the JME group, in which the mean age was 60.7 years (standard deviation, 13.1 years) and average time from diagnosis to follow-up was 45 years, the overall psychosocial long-term outcome was positive and quality-of-life was high when compared with controls. In the JME group, 80.5% reported never having been unemployed for more than a year, 70% reported access to higher learning, and 80% also reported their financial situation as either wealthy or sufficient. Overall, 90% of patients with JME reported they were well integrated into their social contexts.

The control group, in which the mean age was 61 years (SD, 12.9 years) and follow-up time was 45 years, also reported a 90% rate of integration into their social contexts, although only 73.2% reported never having been unemployed for more than a year, and only 75.6% reported a healthy financial situation.

Nearly a quarter of JME patients reported current or previous psychiatric comorbidity, such as depression or anxiety, compared with 22% of controls. At the time of follow-up, the JME group reported significantly more antiepileptic monotherapy (83.3%), compared with controls (48.4%, P = .004).

The investigators noted that despite its low case numbers, the study’s long follow-up time suggested that “specific neurobiologic alterations in JME, if they exist at all, do not contribute in a primary fashion to psychosocial outcome.”

Dr. Holtkamp disclosed that he has received funds from several pharmaceutical companies, including Desitin Arzneimittel, GlaxoSmithKline, UCB, and others. He is on the advisory boards of several industry entities, including Eisai and Janssen.

[email protected] 


On Twitter @whitneymcknight

Patients with juvenile myoclonic epilepsy tend to have similar or better quality-of-life scores in adulthood in comparison with patients with absence epilepsy, except when there are comorbid psychiatric conditions, according to findings from a case-control study.

“In contrast to previous findings on social outcome in JME [juvenile myoclonic epilepsy], we demonstrated that the overall psychosocial outcome in the current JME patients was generally satisfying and – likewise important – did not differ from patients with absence epilepsy,” wrote the authors, including lead investigator, Dr. Martin Holtkamp, medical director at the Epilepsy Center Berlin-Brandenburg, Germany.

The findings showed that when compared with patients who had been diagnosed with childhood or juvenile absence epilepsy (AE), those with juvenile myoclonic epilepsy (JME) in their mid-40s were as likely or more likely to have a college degree, steady employment, and full integration into their social context.

“At the end of follow-up, we found only one variable to be significantly different comparing psychosocial long-term outcome in JME and AE patients,” Dr. Holtkamp and his colleagues wrote. That variable was that nearly three-quarters of JME patients had either qualified for or achieved a university education, whereas only 34.1% of AE patients had done so (P = .001).

The investigators retrospectively analyzed the records of 41 adult JME patients and 41 adult AE patients whose first treatment contact occurred at the neurology department at the Charity University Hospital Berlin between 1955 and 2000. All patients included in the study had been diagnosed with their subsyndrome of epilepsy for at least 20 years (Epilepsia 2014 Sept. 10 [doi:10.1111/epi.12751]).

Patients in each group were contacted and asked to complete a questionnaire about their education, professional situation, family and social life, as well as their psychiatric conditions and any medications used to treat them. Each group was also asked to complete the validated Quality of Life in Epilepsy Inventory 31 survey (in German).In the JME group, in which the mean age was 60.7 years (standard deviation, 13.1 years) and average time from diagnosis to follow-up was 45 years, the overall psychosocial long-term outcome was positive and quality-of-life was high when compared with controls. In the JME group, 80.5% reported never having been unemployed for more than a year, 70% reported access to higher learning, and 80% also reported their financial situation as either wealthy or sufficient. Overall, 90% of patients with JME reported they were well integrated into their social contexts.

The control group, in which the mean age was 61 years (SD, 12.9 years) and follow-up time was 45 years, also reported a 90% rate of integration into their social contexts, although only 73.2% reported never having been unemployed for more than a year, and only 75.6% reported a healthy financial situation.

Nearly a quarter of JME patients reported current or previous psychiatric comorbidity, such as depression or anxiety, compared with 22% of controls. At the time of follow-up, the JME group reported significantly more antiepileptic monotherapy (83.3%), compared with controls (48.4%, P = .004).

The investigators noted that despite its low case numbers, the study’s long follow-up time suggested that “specific neurobiologic alterations in JME, if they exist at all, do not contribute in a primary fashion to psychosocial outcome.”

Dr. Holtkamp disclosed that he has received funds from several pharmaceutical companies, including Desitin Arzneimittel, GlaxoSmithKline, UCB, and others. He is on the advisory boards of several industry entities, including Eisai and Janssen.

[email protected] 


On Twitter @whitneymcknight

Patients with juvenile myoclonic epilepsy tend to have similar or better quality-of-life scores in adulthood in comparison with patients with absence epilepsy, except when there are comorbid psychiatric conditions, according to findings from a case-control study.

“In contrast to previous findings on social outcome in JME [juvenile myoclonic epilepsy], we demonstrated that the overall psychosocial outcome in the current JME patients was generally satisfying and – likewise important – did not differ from patients with absence epilepsy,” wrote the authors, including lead investigator, Dr. Martin Holtkamp, medical director at the Epilepsy Center Berlin-Brandenburg, Germany.

The findings showed that when compared with patients who had been diagnosed with childhood or juvenile absence epilepsy (AE), those with juvenile myoclonic epilepsy (JME) in their mid-40s were as likely or more likely to have a college degree, steady employment, and full integration into their social context.

“At the end of follow-up, we found only one variable to be significantly different comparing psychosocial long-term outcome in JME and AE patients,” Dr. Holtkamp and his colleagues wrote. That variable was that nearly three-quarters of JME patients had either qualified for or achieved a university education, whereas only 34.1% of AE patients had done so (P = .001).

The investigators retrospectively analyzed the records of 41 adult JME patients and 41 adult AE patients whose first treatment contact occurred at the neurology department at the Charity University Hospital Berlin between 1955 and 2000. All patients included in the study had been diagnosed with their subsyndrome of epilepsy for at least 20 years (Epilepsia 2014 Sept. 10 [doi:10.1111/epi.12751]).

Patients in each group were contacted and asked to complete a questionnaire about their education, professional situation, family and social life, as well as their psychiatric conditions and any medications used to treat them. Each group was also asked to complete the validated Quality of Life in Epilepsy Inventory 31 survey (in German).In the JME group, in which the mean age was 60.7 years (standard deviation, 13.1 years) and average time from diagnosis to follow-up was 45 years, the overall psychosocial long-term outcome was positive and quality-of-life was high when compared with controls. In the JME group, 80.5% reported never having been unemployed for more than a year, 70% reported access to higher learning, and 80% also reported their financial situation as either wealthy or sufficient. Overall, 90% of patients with JME reported they were well integrated into their social contexts.

The control group, in which the mean age was 61 years (SD, 12.9 years) and follow-up time was 45 years, also reported a 90% rate of integration into their social contexts, although only 73.2% reported never having been unemployed for more than a year, and only 75.6% reported a healthy financial situation.

Nearly a quarter of JME patients reported current or previous psychiatric comorbidity, such as depression or anxiety, compared with 22% of controls. At the time of follow-up, the JME group reported significantly more antiepileptic monotherapy (83.3%), compared with controls (48.4%, P = .004).

The investigators noted that despite its low case numbers, the study’s long follow-up time suggested that “specific neurobiologic alterations in JME, if they exist at all, do not contribute in a primary fashion to psychosocial outcome.”

Dr. Holtkamp disclosed that he has received funds from several pharmaceutical companies, including Desitin Arzneimittel, GlaxoSmithKline, UCB, and others. He is on the advisory boards of several industry entities, including Eisai and Janssen.

[email protected] 


On Twitter @whitneymcknight

HOLLYWOOD, FLA. – In the United States, rates of mental illness continue to increase while rates of cure do not. That’s according to a recent report on the global disease burden published in JAMA (2013;310:591-608).

For that reason, leaders in the mental health field such as Dr. Thomas Insel, director of the National Institute of Mental Health, and who is both a psychiatrist and a neuroscientist, are supporting President Barack Obama’s BRAIN Initiative. The 12-year vision with a projected $4.5 billion price tag that goal has among its aims. The hope is that the initiative will help determine biomarkers aimed at finding effective cures for a variety of mental illnesses.

After Dr. Insel spoke at the plenary session of this year’s annual meeting of the American Society of Clinical Psychopharmacology, formerly known as the New Clinical Drug Evaluation Unit meeting, he sat for an interview with this news organization.

This is part II of that interview. In this segment, Dr. Insel discusses how the BRAIN Initiative could change practice for psychiatrists and other mental health professionals. Dr. Insel also describes how he thinks the collaboration of many scientists will aid in the quest to understand the biology of the brain. In addition, he describes how funding in this new era will be determined for those interested in applying for research grants.

[email protected]

On Twitter @whitneymcknight

HOLLYWOOD, FLA. – In the United States, rates of mental illness continue to increase while rates of cure do not. That’s according to a recent report on the global disease burden published in JAMA (2013;310:591-608).

For that reason, leaders in the mental health field such as Dr. Thomas Insel, director of the National Institute of Mental Health, and who is both a psychiatrist and a neuroscientist, are supporting President Barack Obama’s BRAIN Initiative. The 12-year vision with a projected $4.5 billion price tag that goal has among its aims. The hope is that the initiative will help determine biomarkers aimed at finding effective cures for a variety of mental illnesses.

After Dr. Insel spoke at the plenary session of this year’s annual meeting of the American Society of Clinical Psychopharmacology, formerly known as the New Clinical Drug Evaluation Unit meeting, he sat for an interview with this news organization.

This is part II of that interview. In this segment, Dr. Insel discusses how the BRAIN Initiative could change practice for psychiatrists and other mental health professionals. Dr. Insel also describes how he thinks the collaboration of many scientists will aid in the quest to understand the biology of the brain. In addition, he describes how funding in this new era will be determined for those interested in applying for research grants.

[email protected]

On Twitter @whitneymcknight

HOLLYWOOD, FLA. – In the United States, rates of mental illness continue to increase while rates of cure do not. That’s according to a recent report on the global disease burden published in JAMA (2013;310:591-608).

For that reason, leaders in the mental health field such as Dr. Thomas Insel, director of the National Institute of Mental Health, and who is both a psychiatrist and a neuroscientist, are supporting President Barack Obama’s BRAIN Initiative. The 12-year vision with a projected $4.5 billion price tag that goal has among its aims. The hope is that the initiative will help determine biomarkers aimed at finding effective cures for a variety of mental illnesses.

After Dr. Insel spoke at the plenary session of this year’s annual meeting of the American Society of Clinical Psychopharmacology, formerly known as the New Clinical Drug Evaluation Unit meeting, he sat for an interview with this news organization.

This is part II of that interview. In this segment, Dr. Insel discusses how the BRAIN Initiative could change practice for psychiatrists and other mental health professionals. Dr. Insel also describes how he thinks the collaboration of many scientists will aid in the quest to understand the biology of the brain. In addition, he describes how funding in this new era will be determined for those interested in applying for research grants.

[email protected]

On Twitter @whitneymcknight

CHICAGO – Chances are good that if your patient presents with eyelid dermatitis, allergic contact with gold or nickel is the culprit.

"Gold is not thought to be easily released from jewelry, which would be the typical exposure with eyelids, unless it comes into contact with sweat, friction, or abrasives," Dr. Amber Reck Atwater told attendees of a session on facial dermatoses at the American Academy of Dermatology summer meeting.

Courtesy Wikimedia Commons/Linuxerist/Creative Commons License

However, when gold comes into contact with titanium dioxide, a common active ingredient in many cosmetics such as eye shadow, patients are at risk for eyelid irritation.

"If I am wearing a gold ring, and I put this on my eyelids using my finger, the gold will be more easily released, and I will be more likely to get a reaction on my lids," said Dr. Atwater, of the department of dermatology at Duke University, Durham, N.C.

Nickel is another leading cause of eyelid dermatitis, Dr. Atwater said. She warned of the metal’s pernicious tendency to hide in personal care products such as eyelash curlers that do not list it as an active or inactive ingredient.

A simple and relatively inexpensive dimethylglyoxime test, which Dr. Atwater said can be purchased on the consumer market, can help identify items that may contain nickel. Rub a drop of dimethylglyoxime onto an item, such as a house key, with a cotton swab. If the key turns bright pink, then you know it has nickel in it.

"So you can imagine that if I am holding my keys in my hands, I could be transferring nickel from the keys to my eyelids," said Dr. Atwater.

Other potential sources of nickel include faucets, sunglasses with metal frames, barbells, and other weight-lifting equipment.

Other common causes of eyelid dermatitis are products that contain fragrance, including balsam of Peru, neomycin (typically found in antibacterial eye drops), formaldehyde and bronopol (preservatives that are found in certain cosmetics), skin care products, and topicals.

Allergic contact dermatitis in the eyelid can present in an upper, lower, unilateral, or bilateral fashion on the eyelids alone, but typically presents in combination with dermatitis on other areas of the face, or even other areas of the body, according to Dr. Atwater.

"You should be highly suspicious that it’s contact dermatitis when you see eyelid dermatitis with other parts of the body involved," she said.

When the dermatitis presents in the eyelids alone, other factors such as seborrheic dermatitis or aspecific xerotic dermatitis could be the cause.

"Still, a good 30%-50% of our patients will have allergic contact dermatitis when we see them with eyelid dermatitis alone," Dr. Atwater said.

The eyelids are particularly susceptible to irritation in part because the skin is extremely thin – 0.55 mm – compared with other facial areas where the average skin thickness is about 2 mm, Dr. Atwater explained.

"And it’s really easy to transfer substances from our hands to our eyes. People rub their eyes and their faces a lot throughout the day," she noted.

Dr. Atwater had no financial conflicts to disclose.

[email protected]

On Twitter @whitneymcknight

CHICAGO – Chances are good that if your patient presents with eyelid dermatitis, allergic contact with gold or nickel is the culprit.

"Gold is not thought to be easily released from jewelry, which would be the typical exposure with eyelids, unless it comes into contact with sweat, friction, or abrasives," Dr. Amber Reck Atwater told attendees of a session on facial dermatoses at the American Academy of Dermatology summer meeting.

Courtesy Wikimedia Commons/Linuxerist/Creative Commons License

However, when gold comes into contact with titanium dioxide, a common active ingredient in many cosmetics such as eye shadow, patients are at risk for eyelid irritation.

"If I am wearing a gold ring, and I put this on my eyelids using my finger, the gold will be more easily released, and I will be more likely to get a reaction on my lids," said Dr. Atwater, of the department of dermatology at Duke University, Durham, N.C.

Nickel is another leading cause of eyelid dermatitis, Dr. Atwater said. She warned of the metal’s pernicious tendency to hide in personal care products such as eyelash curlers that do not list it as an active or inactive ingredient.

A simple and relatively inexpensive dimethylglyoxime test, which Dr. Atwater said can be purchased on the consumer market, can help identify items that may contain nickel. Rub a drop of dimethylglyoxime onto an item, such as a house key, with a cotton swab. If the key turns bright pink, then you know it has nickel in it.

"So you can imagine that if I am holding my keys in my hands, I could be transferring nickel from the keys to my eyelids," said Dr. Atwater.

Other potential sources of nickel include faucets, sunglasses with metal frames, barbells, and other weight-lifting equipment.

Other common causes of eyelid dermatitis are products that contain fragrance, including balsam of Peru, neomycin (typically found in antibacterial eye drops), formaldehyde and bronopol (preservatives that are found in certain cosmetics), skin care products, and topicals.

Allergic contact dermatitis in the eyelid can present in an upper, lower, unilateral, or bilateral fashion on the eyelids alone, but typically presents in combination with dermatitis on other areas of the face, or even other areas of the body, according to Dr. Atwater.

"You should be highly suspicious that it’s contact dermatitis when you see eyelid dermatitis with other parts of the body involved," she said.

When the dermatitis presents in the eyelids alone, other factors such as seborrheic dermatitis or aspecific xerotic dermatitis could be the cause.

"Still, a good 30%-50% of our patients will have allergic contact dermatitis when we see them with eyelid dermatitis alone," Dr. Atwater said.

The eyelids are particularly susceptible to irritation in part because the skin is extremely thin – 0.55 mm – compared with other facial areas where the average skin thickness is about 2 mm, Dr. Atwater explained.

"And it’s really easy to transfer substances from our hands to our eyes. People rub their eyes and their faces a lot throughout the day," she noted.

Dr. Atwater had no financial conflicts to disclose.

[email protected]

On Twitter @whitneymcknight

CHICAGO – Chances are good that if your patient presents with eyelid dermatitis, allergic contact with gold or nickel is the culprit.

"Gold is not thought to be easily released from jewelry, which would be the typical exposure with eyelids, unless it comes into contact with sweat, friction, or abrasives," Dr. Amber Reck Atwater told attendees of a session on facial dermatoses at the American Academy of Dermatology summer meeting.

Courtesy Wikimedia Commons/Linuxerist/Creative Commons License

However, when gold comes into contact with titanium dioxide, a common active ingredient in many cosmetics such as eye shadow, patients are at risk for eyelid irritation.

"If I am wearing a gold ring, and I put this on my eyelids using my finger, the gold will be more easily released, and I will be more likely to get a reaction on my lids," said Dr. Atwater, of the department of dermatology at Duke University, Durham, N.C.

Nickel is another leading cause of eyelid dermatitis, Dr. Atwater said. She warned of the metal’s pernicious tendency to hide in personal care products such as eyelash curlers that do not list it as an active or inactive ingredient.

A simple and relatively inexpensive dimethylglyoxime test, which Dr. Atwater said can be purchased on the consumer market, can help identify items that may contain nickel. Rub a drop of dimethylglyoxime onto an item, such as a house key, with a cotton swab. If the key turns bright pink, then you know it has nickel in it.

"So you can imagine that if I am holding my keys in my hands, I could be transferring nickel from the keys to my eyelids," said Dr. Atwater.

Other potential sources of nickel include faucets, sunglasses with metal frames, barbells, and other weight-lifting equipment.

Other common causes of eyelid dermatitis are products that contain fragrance, including balsam of Peru, neomycin (typically found in antibacterial eye drops), formaldehyde and bronopol (preservatives that are found in certain cosmetics), skin care products, and topicals.

Allergic contact dermatitis in the eyelid can present in an upper, lower, unilateral, or bilateral fashion on the eyelids alone, but typically presents in combination with dermatitis on other areas of the face, or even other areas of the body, according to Dr. Atwater.

"You should be highly suspicious that it’s contact dermatitis when you see eyelid dermatitis with other parts of the body involved," she said.

When the dermatitis presents in the eyelids alone, other factors such as seborrheic dermatitis or aspecific xerotic dermatitis could be the cause.

"Still, a good 30%-50% of our patients will have allergic contact dermatitis when we see them with eyelid dermatitis alone," Dr. Atwater said.

The eyelids are particularly susceptible to irritation in part because the skin is extremely thin – 0.55 mm – compared with other facial areas where the average skin thickness is about 2 mm, Dr. Atwater explained.

"And it’s really easy to transfer substances from our hands to our eyes. People rub their eyes and their faces a lot throughout the day," she noted.

Dr. Atwater had no financial conflicts to disclose.

[email protected]

On Twitter @whitneymcknight

BETHESDA, MD. – We visited the office of Dr. Steven A. Rosenberg, chief of the Surgery Branch at the National Cancer Institute, and a pioneer of adoptive cell transfer using tumor infiltrating lymphocytes (TILs) in melanoma patients. We asked for his thoughts on recently published work on TILs in breast cancer and on the future of immunotherapy for breast cancer.

He explained that the success of immunotherapy for breast cancer, he believes, lies in being able to identify the mutations driving tumor growth and manipulating the immune system to recognize those mutations. Dr. Rosenberg began studies in July to investigate this hypothesis.

Listen to the wide-ranging discussion with Dr. Rosenberg on issues from the immunogenicity of epithelial tumors to checkpoint inhibitors and the future of chemotherapy.

Dr. Rosenberg had no relevant disclosures.

[email protected]

On Twitter @whitneymcknight

BETHESDA, MD. – We visited the office of Dr. Steven A. Rosenberg, chief of the Surgery Branch at the National Cancer Institute, and a pioneer of adoptive cell transfer using tumor infiltrating lymphocytes (TILs) in melanoma patients. We asked for his thoughts on recently published work on TILs in breast cancer and on the future of immunotherapy for breast cancer.

He explained that the success of immunotherapy for breast cancer, he believes, lies in being able to identify the mutations driving tumor growth and manipulating the immune system to recognize those mutations. Dr. Rosenberg began studies in July to investigate this hypothesis.

Listen to the wide-ranging discussion with Dr. Rosenberg on issues from the immunogenicity of epithelial tumors to checkpoint inhibitors and the future of chemotherapy.

Dr. Rosenberg had no relevant disclosures.

[email protected]

On Twitter @whitneymcknight

BETHESDA, MD. – We visited the office of Dr. Steven A. Rosenberg, chief of the Surgery Branch at the National Cancer Institute, and a pioneer of adoptive cell transfer using tumor infiltrating lymphocytes (TILs) in melanoma patients. We asked for his thoughts on recently published work on TILs in breast cancer and on the future of immunotherapy for breast cancer.

He explained that the success of immunotherapy for breast cancer, he believes, lies in being able to identify the mutations driving tumor growth and manipulating the immune system to recognize those mutations. Dr. Rosenberg began studies in July to investigate this hypothesis.

Listen to the wide-ranging discussion with Dr. Rosenberg on issues from the immunogenicity of epithelial tumors to checkpoint inhibitors and the future of chemotherapy.

Dr. Rosenberg had no relevant disclosures.

[email protected]

On Twitter @whitneymcknight

Adult tertiary epilepsy centers often lack the-resources to manage young adult patients transitioning from pediatric centers, based on a study published online (Epilepsia doi.10.1111/epi.12752).

“These transitioned patients require more resources and services than other young patients with epilepsy” that are being cared for in the community, wrote the authors of the study. In addition, the researchers reported that adult neurologists, “even those specialized in epilepsy, may not feel that they are adequately prepared to diagnose and treat part of this complex population.”

For the retrospective study, Dr. Felippe Borlot, an epilepsy fellow at the University of Toronto (Canada), and his colleagues reviewed the records of all young adults, ages 18 through 25 years, with childhood-onset epilepsy seen over a 6-year period at a single adult tertiary epilepsy care site. The researchers reviewed patient demographic data, etiologies, and treatment regimens before sorting patients into two groups.

The first group of 170 patients had been referred from a pediatric epilepsy tertiary care center; the second group of 132 patients was age-matched with that group and consisted of those referred by community physicians, including pediatric neurologists, to the adult tertiary center. The mean age for Group 1 was 21.9 years and the mean age for Group 2 was 23.2 years.

The first group had earlier seizure onset, longer epilepsy duration, more symptomatic etiologies, epileptic encephalopathy, and cognitive delay (P less than .001 for all). The first group also required more care from other specialists (P = .001), as well as polytherapies (P = .003), epilepsy surgery (P less than .001), a ketogenic diet (P less than .001), and the use of a vagus nerve stimulator (P less than .001).

Patients from tertiary centers present more complex health care needs and require more resources than age-matched patients from the community, said Dr. Borlot and his co-investigators.

The researchers also surveyed 86 adult neurologists and 29 pediatric neurologists. On a scale of one (not comfortable at all) to five (very comfortable), the neurologists were asked to rate their comfort level in dealing with several types of epilepsy. The survey also addressed how the neurologists felt about treating attendant issues such as intellectual disabilities and autistic features.

Survey results, while not validated, showed that adult neurologists had less confidence diagnosing and treating more severe forms of childhood-onset epilepsies (P less than .001), as well as epilepsy associated with cognitive delay (P less than .001).

The study lacked data validating a successful transition from pediatric to adult care. Also, it did not include patients who were not assessed in the 12 months prior to the study, meaning it was not possible to determine the percentage of patients lost to follow-up. Nevertheless, the investigators concluded that the data were useful since no previous evaluation of transition of care in the epileptic setting was available.

Dr. Borlot and his co-authors concluded that transition of care for patients with epilepsy may be enhanced by efforts to “make childhood-onset epilepsies part of adult neurologists’ training and certification requirements.”

Adult tertiary epilepsy centers often lack the-resources to manage young adult patients transitioning from pediatric centers, based on a study published online (Epilepsia doi.10.1111/epi.12752).

“These transitioned patients require more resources and services than other young patients with epilepsy” that are being cared for in the community, wrote the authors of the study. In addition, the researchers reported that adult neurologists, “even those specialized in epilepsy, may not feel that they are adequately prepared to diagnose and treat part of this complex population.”

For the retrospective study, Dr. Felippe Borlot, an epilepsy fellow at the University of Toronto (Canada), and his colleagues reviewed the records of all young adults, ages 18 through 25 years, with childhood-onset epilepsy seen over a 6-year period at a single adult tertiary epilepsy care site. The researchers reviewed patient demographic data, etiologies, and treatment regimens before sorting patients into two groups.

The first group of 170 patients had been referred from a pediatric epilepsy tertiary care center; the second group of 132 patients was age-matched with that group and consisted of those referred by community physicians, including pediatric neurologists, to the adult tertiary center. The mean age for Group 1 was 21.9 years and the mean age for Group 2 was 23.2 years.

The first group had earlier seizure onset, longer epilepsy duration, more symptomatic etiologies, epileptic encephalopathy, and cognitive delay (P less than .001 for all). The first group also required more care from other specialists (P = .001), as well as polytherapies (P = .003), epilepsy surgery (P less than .001), a ketogenic diet (P less than .001), and the use of a vagus nerve stimulator (P less than .001).

Patients from tertiary centers present more complex health care needs and require more resources than age-matched patients from the community, said Dr. Borlot and his co-investigators.

The researchers also surveyed 86 adult neurologists and 29 pediatric neurologists. On a scale of one (not comfortable at all) to five (very comfortable), the neurologists were asked to rate their comfort level in dealing with several types of epilepsy. The survey also addressed how the neurologists felt about treating attendant issues such as intellectual disabilities and autistic features.

Survey results, while not validated, showed that adult neurologists had less confidence diagnosing and treating more severe forms of childhood-onset epilepsies (P less than .001), as well as epilepsy associated with cognitive delay (P less than .001).

The study lacked data validating a successful transition from pediatric to adult care. Also, it did not include patients who were not assessed in the 12 months prior to the study, meaning it was not possible to determine the percentage of patients lost to follow-up. Nevertheless, the investigators concluded that the data were useful since no previous evaluation of transition of care in the epileptic setting was available.

Dr. Borlot and his co-authors concluded that transition of care for patients with epilepsy may be enhanced by efforts to “make childhood-onset epilepsies part of adult neurologists’ training and certification requirements.”

Adult tertiary epilepsy centers often lack the-resources to manage young adult patients transitioning from pediatric centers, based on a study published online (Epilepsia doi.10.1111/epi.12752).

“These transitioned patients require more resources and services than other young patients with epilepsy” that are being cared for in the community, wrote the authors of the study. In addition, the researchers reported that adult neurologists, “even those specialized in epilepsy, may not feel that they are adequately prepared to diagnose and treat part of this complex population.”

For the retrospective study, Dr. Felippe Borlot, an epilepsy fellow at the University of Toronto (Canada), and his colleagues reviewed the records of all young adults, ages 18 through 25 years, with childhood-onset epilepsy seen over a 6-year period at a single adult tertiary epilepsy care site. The researchers reviewed patient demographic data, etiologies, and treatment regimens before sorting patients into two groups.

The first group of 170 patients had been referred from a pediatric epilepsy tertiary care center; the second group of 132 patients was age-matched with that group and consisted of those referred by community physicians, including pediatric neurologists, to the adult tertiary center. The mean age for Group 1 was 21.9 years and the mean age for Group 2 was 23.2 years.

The first group had earlier seizure onset, longer epilepsy duration, more symptomatic etiologies, epileptic encephalopathy, and cognitive delay (P less than .001 for all). The first group also required more care from other specialists (P = .001), as well as polytherapies (P = .003), epilepsy surgery (P less than .001), a ketogenic diet (P less than .001), and the use of a vagus nerve stimulator (P less than .001).

Patients from tertiary centers present more complex health care needs and require more resources than age-matched patients from the community, said Dr. Borlot and his co-investigators.

The researchers also surveyed 86 adult neurologists and 29 pediatric neurologists. On a scale of one (not comfortable at all) to five (very comfortable), the neurologists were asked to rate their comfort level in dealing with several types of epilepsy. The survey also addressed how the neurologists felt about treating attendant issues such as intellectual disabilities and autistic features.

Survey results, while not validated, showed that adult neurologists had less confidence diagnosing and treating more severe forms of childhood-onset epilepsies (P less than .001), as well as epilepsy associated with cognitive delay (P less than .001).

The study lacked data validating a successful transition from pediatric to adult care. Also, it did not include patients who were not assessed in the 12 months prior to the study, meaning it was not possible to determine the percentage of patients lost to follow-up. Nevertheless, the investigators concluded that the data were useful since no previous evaluation of transition of care in the epileptic setting was available.

Dr. Borlot and his co-authors concluded that transition of care for patients with epilepsy may be enhanced by efforts to “make childhood-onset epilepsies part of adult neurologists’ training and certification requirements.”