Journal of ISSN: 2373-6410JNSK

Neurology & Stroke
Case Report
Volume 3 Issue 3 - 2015
A Teenager With an Acute Stroke While at School
Rodney Leacock1*, Shannon Sternberg1, Kevin Polley2, Jennifer Frederick2, Angel Rochester2, Emily Foster3, Cynthia Bishop Trout1 and Sandip Jain1
1GHS Stroke Center, Greenville Memorial Hospital, USA
2Department of Emergency Medicine, Greenville Memorial Hospital, USA
3Pediatric Neurology, GHS University Medical Grp PED NEU, USA
Received:August 18, 2015| Published: November 16, 2015
*Corresponding author: Rodney Leacock, GHS Stroke Center, 701 Grove Road, Greenville, South Carolina, USA 29605 Tel. 864-455-8848 email:
Citation: Leacock R, Sternberg S, Polley K, Frederick J, Rochester A, et al. (2015) A Teenager With an Acute Stroke While at School. J Neurol Stroke 3(3): 00093. DOI: 10.15406/jnsk.2015.03.00093

Abstract

Acute stroke in children is an uncommon occurrence. We present a 16 year old adolescent boy who developed acute left hemiparesis while at school and 911/EMS was called and received iv tpa and made an excellent recovery. We discuss potential challenges to stroke recognition and treatment in children.

Keywords: Acute stroke; Teenager; Children; Thrombolysis

Abbreviations

EMS: Emergency Medical Services; iv tpa: intravenous tissue plasminogen activator; tpa: tissue plasminogen activator; GMH: Greenville Memorial Hospital; NIHSS: National Institute of Health Stroke Scale; CT: Computerized Tomography; CTA: Computerized Tomography Angiogram; CTP: Computerized Tomography Perfusion; MRI: Magnetic Resonance Imaging; PSC: Primary Stroke Center

Introduction

Acute stroke in children is an uncommon occurrence. The reported frequency is 2.3 to 13 per 100,000 [1]. Children recognized and treated with iv tpa for acute ischemic stroke is a rare occurrence. We discuss the case of a 16 year old boy who developed acute left hemiparesis and received intravenous administration of tpa.

Recombinant tissue plasminogen activator was proven to be effective for acute ischemic stroke treatment in 1995 [2], and approved by the FDA for use in eligible patients more than 18 years old since 1996. The Brain Attack Coalition described the formation of primary stroke centers in 2000 [3], which was followed by the proposal for the formation of comprehensive stroke centers in 2005 [4], and the proposal for the formation of acute stroke ready hospitals in 2013 [5]. There are even several guidelines which address acute ischemic stroke therapy, of which the most current is from 2013 [6]. With regard to stroke in infants and children the only guideline is from 2008 [7]. The formation of the primary pediatric stroke center has only recently described [8].

Case Presentation

A 16 year old adolescent male developed acute left hemiparesis while in the school training facility during a workout. The training staff suspected that he was having a stroke and 911/EMS was called. This led to a stroke alert at Greenville Memorial Hospital (GMH). Upon arrival to the Pediatric Emergency Department (Peds ED) he was greeted by the Pediatric Emergency Medical Team. Emergency stabilization was performed. An NIHSS scale was performed by Adult Stroke Team responders.

The patient was able to recall the duration of symptoms beginning about 2 hours prior, complained of a headache and was drowsy in the Peds ED bay. The initial NIHSS was 15. Direction was provided by the Adult Stroke Team responders to obtain emergent CT head and CT angiography. Additional responders included Pediatric Neurology who basically deferred to the Stroke Team for guidance and direction in the first 24 – 48 hours.

In the CT scanner, the patient experienced nausea and vomiting was given Zofran and maintained his airway. The non-contrast head CT did not show hemorrhage and the NIHSS remained 15. We proceeded with the CTP and CTA head and neck. Cerebral ischemia was suggested by the CTP, but there were limitations with both the CTP and CTA. Initial height and weight were 190 cm and 141 kg with blood pressure 145/55 and heart rate 66.

It was concluded that the patient was having an acute ischemic stroke and thrombolysis was considered. The patient’s father was contacted and explained the diagnosis and treatment options. The benefits and risks were explained to the father questions were answered and the father verbally consented to iv rt-PA administration. The CTA head did not show a large vessel occlusion and the CTA neck was of poor quality.
Our patient had hypertension, dyslipidemia, and migraine headaches. His mother had congenital heart surgery as child. There was a paternal grandmother history of stroke.

The tpa was started at 4:22 pm which was about two hours and fifty two minutes from the onset of symptoms and was stopped at 5:20 pm. During thrombolysis administration, the patient was monitored in Adult Trauma Bay. He experienced a severe headache and the repeat emergent CT head was negative for hemorrhagic transformation. The patient was admitted to the NeuroTrauma Intensive Care Unit (NTICU) for continued post thrombolysis monitoring. By 8 am the following morning, on examination, he had mild drowsiness, mild visual impairment, mild dysarthria, left facial paresis, mild left hemiparesis with only a slight drift of the upper and lower extremities, and the NIHSS was 7. The MRI brain (Figure 1) showed a right basal ganglia infarction. Thrombolysis with tpa limited the extent of infarction as it was suspected to involve a significant portion of the right middle cerebral artery pre-treatment. Two hours after the tpa was completed, he actually improved to an NIHSS of 2 but fluctuated through the night and the following morning his NIHSS was a 7. A repeat non-contrast CT head (Figure 2) was obtained at 9:18 am without hemorrhagic or significant infarction changes.

After the NTICU course he was transferred to the Pediatric Service and followed by Pediatric Neurology. The patient regained ambulatory function. A carotid duplex was performed and less than 50% stenosis was found bilaterally. The 2D echocardiogram was interpreted as normal and without atrial septal defect. Seven days later, he was discharge to rehabilitation and his NIHSS score was 2 and the mRS=1. At a follow up office visit 3 weeks later his NIHSS was 0. No hypercoagulable disorder was found. An elevated lipoprotein A level was found and he was maintained on niacin, aspirin and topiramate.

Figure 1: MRI-DWI showing acute right head of the caudate infarction at 9:32 pm about 5 hours post tpa initiation.
Figure 2: Non contrast CT head obtained at 9:18 am the following morning about 17 hours post tpa initiation.

Discussion

This is our first administration of iv tpa for acute ischemic stroke in the pediatric population at GMH. GMH has been certified as a PSC by the Joint Commission since 2009. Our center averages about 700 adult ischemic stroke patients per year. Through ongoing participation in Get With The Guidelines-Stroke (9) [], our thrombolysis administration rate with tpa for acute ischemic stroke in adults is 28 percent and greater than 85 percent receive it in less than 60 minutes. Our pediatric stroke data is limited.

We have learned to be able to recognize acute stroke in the pediatric population can be very challenging indeed. Our patient was a 16 y.o.male who resembled an adult in many ways by height and weight. He was a football player and was under the supervision of experienced coaching and training staff who responded emergently. The EMS personnel brought the patient to GMH PedsED. There was discussion amongst all providers at GMH. In summary, the patient received the appropriate treatment and care.

Barriers to stroke recognition were his age, duration of symptoms, and uncertainty with diagnosis. Treatment delays were relying on available technology, patient stabilization, obtaining consent for treatment. Staff concerns and anxiety were raised about giving tpa to a teenage child. Intravenous thrombolytic use has not been established in pediatric patients [10]. Where to monitor the child during and after tpa administration were concerns. Fortunately reassurance was provided to all of the staff who raised questions about the process and the plan.

Reported thrombolysis rates in children are very small from 0.7-2% [1,11,12]. The challenges associated with site recruitment and patient screenings were described. Only 1 patient was enrolled out of 93 screened and 46% did have an ischemic stroke [1]. Exclusion criteria reported included moyamoya arteriopathy, anticoagulation, malignancy, recent strokes, delayed recognition and treatment times, and stroke severity NIHSS < 6 [1].

In 2009, Amlie-Lefond et al. [12] reported 15 out of 687 children enrolled in the International Pediatric Stroke Study (IPSS) received tpa 9 intravenously and 6 intra-arterially. Asymptomatic intracranial hemorrhages were reported in four patients. Two patients died and 12 of 13 had remaining neurological deficits. This is the largest reported experience with tpa administration and children.

More recently, Ladner et al. [13] reviewed 124 stroke alerts over a 42 month period from April 2011 after the formation the pediatric acute stroke team and protocols. There were 30 strokes and 21 were ischemic of which two received mechanical endovascular therapy and one received endovascular fibrinolysis. The overall benefits were up to 40% of children had a stroke or a neurological emergency. Access to MRI was readily available the majority of times.

Amlie-Lefond et al. [12] reported barriers to treatment with tpa included longer delays in making a specific diagnosis of stroke as stroke mimics are more common in children. The reason our patient received expedited care because he was in a setting around trained personnel who suspected he was having a stroke and called 911/EMS.We made every effort to adhere to current published adult guidelines for tpa administration [6] with regards to time and dosage unlike in Amlie-Lefond et al. [12] where 7 of 15 did not receive treatment according to the published guidelines [14]. Fonarow et al. [15] showed with shorter door to needle times of tpa administration in less than 60 minutes that better outcomes were achieved from a national database of 1030 Get With The Guidelines-Stroke Hospitals. It has also been shown that less than 30 percent of patients are treated within 60 minutes. Pre-notification by 911/EMSfacilitated patient preparation for the ED and Stroke Team responders. The patient outcome was directly attributable to this. EMS, hospital prenotification is associated with shorter evaluation and treatment times [15], and a greater rate of tpa administration [16].

Ways to improve the recognition of stroke in children is through the identification of predisposing risk factors like hypertension, diabetes, dyslipidemias, and obesity. Syndromes with a genetic predisposition for stroke include sickle cell disease, metabolic disorders like MELAS, hypercoagulable disorders, moyamoya disease or connective tissue disorders. Equally important is to raise community awareness through family education, teacher education, school education, and recreational and sporting event education. The most likely location for a child to have stroke other than home is at school. Although mechanisms like dissection were not identified, it is possible with football, weight training, wrestling, cheerleading or soccer.

To summarize, children can have a stroke and it is important to raise awareness about stroke recognition, treatment options, rehabilitation, secondary prevention, patient selection and eligibility, collaboration amongst participating specialties like EMS, emergency medicine, adult and pediatric neurology, radiology, and adapting stroke systems of care to include children and even potentially becoming a primary pediatric stroke center based on the criteria established by the TIPS study [1,8]. The initial steps should include the formation of a pediatric acute stroke response team and protocols, and preferable access to MRI for emergency brain imaging [1,8,13].

Despite the above mentioned barriers it is possible to achieve a good outcome using iv tpa for acute stroke in children. Individual case reports remain a significant source for outcomes in pediatric stroke care. A 15 year old boy with left hemiparesis, NIHSS was 7, was given tpa 1 hour and 43 minutes from symptom onset, and his symptoms resolved after 33 minutes [17]. Another 16 year old boy presented to the ED 1 hour after onset of symptoms, with speech impairment and right hemiparesis, NIHSS was 13, and was given iv tpa 2 hours and 40 minutes after symptom onset. 8 hours later, he had near complete resolution of symptoms with normal speech and near normal strength [18]. Tpa was administered 4 hours from symptom onset to a 16 year old girl who presented with basilar artery occlusion from a lupus anticoagulant and the NIHSS was 8. At 6 hours from symptom onset her NIHSS improved 2 [19]. To consider a child with a stroke for thrombolysis with tpa requires a more thorough assessment of history and examination, identify stroke mimics, access to advanced imaging including MRI, CTP and CTA, collaboration amongst a team of experts in stroke care, and well defined stroke protocols [7,8,12,13,17-19].

Access to endovascular therapies for acute ischemic stroke offer a more precise and directed therapeutic option which are more readily available at larger institutions [13].

References

  1. Rivkin MJ, deVeber G, Ichord RN, Kirton A, Chan AK, et al. (2015) Thrombolysis in pediatric stroke. Stroke 46(3): 880-885.
  2. (1996) Tissue plasminogen activator for acute ischemic stroke. The National Institute of Neurological Disorders and Stroke rt-PA Stroke Study Group. N Eng J Med 333(24): 1581-1588.
  3. Alberts MJ, Hademenos G, Latchaw RE, Jagoda A, Marler JR, et al. (2000) Recommendations for the establishment of primary stroke centers. JAMA 283(23): 3102-3109.
  4. Alberts MJ, Latchaw RE, Selman WR, Shephard T, Hadley MN, et al. (2005) Recommendations for comprehensive stroke centers: a consensus statement from the brain attack coalition. Stroke 36(7):1597-616.
  5. Alberts MJ, Wechsler LR, Jensen ME, Latchaw RE, Crocco TJ, et al. (2013) Formation and function of acute stroke ready hospitals within a stroke system of care recommendations from the brain attack coalition. Stroke 44(12): 3382-3393.
  6. Jauch EC, Saver JL, Adams HP, Bruno A, Connors JJ, et al. (2013) Guidelines for the early management of patients with acute ischemic stroke: a guideline for healthcare professionals from the American Heart Association/American Stroke Association. Stroke 44(3): 870-947.
  7. Roach ES, Golomb, MR, Adams R, Biller J, Daniels S, et al. (2008) Management of stroke in infants and children: a scientific statement from a Special Writing Group of the American Heart Association Stroke Council and the Council on Cardiovascular Disease in the Young. Stroke 39(9): 2644-2691.
  8. Bernard TJ, Rivkin MJ, Scholz K, deVeber G, Kirton A, et al. (2014) Emergence of the primary pediatric stroke center: impact of the thrombolysis in pediatric stroke trial. Stroke 45(7): 2018-2023.
  9. Get With The Guidelines-Stroke: American Heart Association/American Stroke Association 2015
  10. http://www.gene.com/download/pdf/activase_prescribing.pdf
  11. Alshelhlee A, Geller T, Mehta S, Storkan M, Khalili Y, et al. (2013) Thrombolysis for children with acute ischemic stroke: a perspective from the kids’ inpatient database. Pediatr Neurol 49(5): 313-318.
  12. Amlie-Lefond C, deVeber G, Chan AK, Benedict S, Bernard T, et al. (2009) Use of alteplase in childhood arterial ischaemic stroke: a multicenter, observational cohort study. Lancet Neurol 8(6): 530-536.
  13. Ladner TR, Mahdi J, Gindville MC, Gordon A, Harris ZL, et al. (2015) Pediatric acute stroke protocol activation in a children’s hospital emergency department. Stroke 46(8): 2328-2331.
  14. Adams HP, del Zoppo G, Alberts M, Furlan A, Grubb R, Brass L, et al. (2007) Guidelines for the early management of adults with ischemic stroke: a guideline from the American Heart Association/American Stroke Association Stroke Council, Clinical Cardiology Council, Cardiovascular Radiology and Intervention Council, and the Atherosclerotic Peripheral Vascular Disease and Quality of Care Outcomes in Research Interdisciplinary Working Groups: the American Academy of Neurology affirms the value of this guideline as an educational tool for neurologists. Stroke 38(5): 655-1711.
  15. Fonarow GC, Zhao X, Smith EE, Saver JL, Reeves MJ, et al. (2014) Door to needle times for tissue plasminogen activator administration and clinical outcomes in acute ischemic stroke before and after a quality improvement initiative. JAMA 311(16): 1632-1640.
  16. Mckinney JS, Mylavarapu K, Lane J, Roberts V, Ohman-Strickland P, et al. (2013) Hospital prenotification of stroke patients by emergency medical services improves stroke time targets. J Stroke Cerebrovasc Dis 22(2): 113-118.
  17. Muniz AE (2012) Thrombolytic therapy for acute stroke in a teenager. Pediatr Emerg Care 28(2): 170-173.
  18. Shuayto MI, Lopez JL, Greiner F (2006) Administration of intravenous tissue plasminogen activator in a pediatric patient with acute ischemic stroke. J Child Neurol 21(7): 604-606.
  19. Heil JW, Malinowski L, Rinderknecht A, Broderick JP, Franz D (2008) Use of intravenous tissue plasminogen activator in a 16-year-old patient with basilar occlusion. J Child Neurol 23(9): 1049-1053.
© 2014-2016 MedCrave Group, All rights reserved. No part of this content may be reproduced or transmitted in any form or by any means as per the standard guidelines of fair use.
Creative Commons License Open Access by MedCrave Group is licensed under a Creative Commons Attribution 4.0 International License.
Based on a work at http://medcraveonline.com
Best viewed in Mozilla Firefox | Google Chrome | Above IE 7.0 version | Opera |Privacy Policy