So, a few months ago, I came across an epilepsy diagnosis that literally gave me goose bumps. As I read through all the information I could find, I couldn't believe how much it sounded like Hannah. I called Hannah's genetics doctor and he agreed that it was definitley worth testing. drum roll please....... R (20) Epilepsy Syndrome (or ring 20)..... There is a foundation set up to share awareness about this diagnosis...
http://www.ring20.org/r20syndrome/index.aspx
Ring chromosome 20 epilepsy syndrome, also known as r(20) syndrome, is a rare chromosomal anomaly resulting from a break on each arm of chromosome 20 resulting in ring formation. In r(20) syndrome, the breakpoint of most patients is in the p13q13.33 region of chromosome 20. This syndrome is characterized by medically intractable epilepsy, nocturnal subtle seizures, behavioral problems and mild mental impairment. Unlike other chromosomal aberrations, dysmorphism (major or minor congenital malformation) is rarely reported.
Epilepsy is a constant feature of this syndrome and in many cases is intractable and drug resistant. Seizures are often complex partial in type and reported as episodes of altered consciousness with staring, oral automatisms, unspecified automatic behavior, focal motor symptomsand/or head turning. Subtle nocturnal behavioral changes such as stretching, rubbing and turning have been observed which resemble normal arousal behavior. In addition, subtle nocturnal seizures (SNS) and subtle nocturnal frontal lobe seizures (SNFLS) are also reported Seizures are often difficult to control with antiepileptic medications.
Today was our genetics appointment. I have been very reserved because I don't want to get my hopes up of after almost 10 years, to finally have an answer. I went to the appointment loaded with my information all about it. We work with a wonderful resident who was very attentive and felt like it was a very good thing to test for.
Diagnosis of ring chromosome 20 syndrome can be made by recognition of certain characteristic clinical features; however, definitive diagnosis requires chromosomal testing of the affected person's cells. This is most easily done by looking at the chromosome pattern (karyotype) in blood cells but any other tissue including skin could be examined. Since chromosomal analysis or karyotype testing is not a routine investigation when epilepsy first presents, the diagnosis of r(20) syndrome may be delayed or go unrecognized. In other words, some people with difficult to control epilepsy may have a ring chromosome 20 but be unaware of it. Almost all parents of individuals with r(20) syndrome have no evidence of r(20) syndrome in their own blood chromosome analysis. A few individuals, typically relatives of affected patients , have been found to have a ring chromosome 20 without any evidence of symptoms. Why these people are protected against development of epilepsy remains unknown. Neuroimaging studies and metabolic studies are unrevealing in this disorder
So, we have already done the chromosome array test. It showed normal chromosomes. But the following is what really caught my attention.....
Since chromosomal analysis or karyotype testing is not a routine investigation when epilepsy first presents, the diagnosis of r(20) syndrome may be delayed or go unrecognized.
Please note:
1) We have seen the ring 20 in as few as 5% of cells, and we recommend requesting a screen for chromosomal mosaicism.
2) Newer array technology will NOT detect the ring chromosome and we recommend standard metaphase chromosome analysis.
We ask that you please consider chromosomal analysis if you have a patient (age 0-17) with the following symptoms:
predominantly complex partial seizures
medically refractory epilepsy with no etiology identified
Lennox-Gastaut-like features with no etiology identified
frequent subtle nocturnal seizures (SNS) and/or subtle nocturnal frontal lobe seizures (SNFL)
EEG showing prolonged high voltage frontally dominant slowing intermixed with spikes or sharp waves
EEG showing overlapping features of continuous slow spike and wave discharges in sleep (CSWS) and electrical status epilepticus in sleep (ESES)
normal childhood development until onset of epilepsy
lack of dysmorphism or other congenital malformations
cognitive impairment/learning difficulties/mild retardation
WOW!!! There is still hope. This abnormal ring can be found in less than 5% of the cells. So, after much discussion today, we did a skin biopsy on Hannah. They said the skin cells would be the best modality to test. Before the test, the attending came in. He agreed to do the test but, started to poo poo it. I think he wanted me to know it was really a long shot. He said he thought it was less than 1% chance of showing this mosaic ring. He said they very rarely test for mosaic chromosomes (exactly why R (20) in underdiagnosed!!) Okay, so he deflated me, but I am still hopeful. After all, Hannah has NEVER done anything by the book.
Hannah did FANTASTIC with the biopsy. I could not have be more proud of her. They put numbing cream on her arm, waited 20 minutes (thank God for the new DS game she got for her birthday), and then they retrieved a chunk of her skin. She didn't even flinch! (must have really been numb). I think I flinched for her..... She is so brave.
So, now we wait..... 2-3 weeks. I am still hopeful.....
Wednesday, February 3, 2010
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Beautiful Hannah...
How this journey started....
Hannah was born prematurely at 34 weeks gestation. She was a relatively healthy preemie; initially having difficulty maintaining body temperature and needing to grow. She weighed 4 pounds 9 ounces at birth. When she was four months old she began to drool, non stop. We were told the first year she was "teething." At 18 months old, we really started searching for reasons of why her shirt was always soaking wet. We saw various specialists who always sent us to another specialist, saying "everything looks okay." She spent years in oral motor/feeding therapy to help her not to drool. It wasn't until she was four years old and in preschool that we started to get some answers. Her preschool teacher commented one day that she wasn't reponding when her name was called. I took this information to her pediatrician who then orderd an EEG, "just to rule it out." Much to our shock and amazement, the results showed, she was having seizures. That is the day our journey REALLY began. Once she began taking seizure medication the drooling almost stopped completely. (She will still drool to this day when she is having seizure activity). Since then, it has been a roller coaster; countless medications and medication changes. She has never really reponded well to any medication.
About two years after she was diagnosed with epilepsy, the doctors noticed that her blood pressure was running high. After many tests, she was diagnosed with hypertension. We still are not sure why, but her cardiologist feels her blood vessels are thicker than normal.
About this same time, we also began looking into why Hannah was such a horrible sleeper. She would thrash, talk, move every which way, during her sleep. The sleep studies revealed that she has alveolar hypoventilation sydrome, which means she has too much carbon dioxide in her system when she sleeps. To help this, she wears a BI-PAP at night. This has been monumental in giving her more effective and quality of sleep.
Every day is a challenge for Hannah and our family as a whole. Blitzen has been an absolutely wonderful addition. She calms herself sometimes just by petting and loving on him. He has been trained in behavior disruptions and will sometimes be able to stop a meltdown from getting out of control.
It has been extra hard on the whole family since daddy is deployed to Iraq. He has been gone since January 09 and will gone until Jan 2010. We get to talk with him by phone and on the web cam; which is nice, but not the same!! Blitzen has helped to make his absence go just a little smoother....
About two years after she was diagnosed with epilepsy, the doctors noticed that her blood pressure was running high. After many tests, she was diagnosed with hypertension. We still are not sure why, but her cardiologist feels her blood vessels are thicker than normal.
About this same time, we also began looking into why Hannah was such a horrible sleeper. She would thrash, talk, move every which way, during her sleep. The sleep studies revealed that she has alveolar hypoventilation sydrome, which means she has too much carbon dioxide in her system when she sleeps. To help this, she wears a BI-PAP at night. This has been monumental in giving her more effective and quality of sleep.
Every day is a challenge for Hannah and our family as a whole. Blitzen has been an absolutely wonderful addition. She calms herself sometimes just by petting and loving on him. He has been trained in behavior disruptions and will sometimes be able to stop a meltdown from getting out of control.
It has been extra hard on the whole family since daddy is deployed to Iraq. He has been gone since January 09 and will gone until Jan 2010. We get to talk with him by phone and on the web cam; which is nice, but not the same!! Blitzen has helped to make his absence go just a little smoother....
3 comments:
*fingers crossed*
You know...I really think the doctors do not know how to relate to us with this stuff. Because it's not their child...it's more their puzzle...they can't wrap their minds around why finding answers are so important to us. And it's not like I've really thought up a great answer to the "why" anyway. I need to know because I'm a MOM. That's my answer.
Anyway...now we wait.
xoxo
...danielle
Wow Marcia, I just read the blog about the R20 chromosome. I hope that the results will be revealing.
Here is a link to more information about the genetics of Ring Chromosome 20 Syndrome that was prepared by our genetic counselor and which has links to some useful resources for those dealing with this condition: http://www.accessdna.com/condition/Ring_Chromosome_20_Syndrome/798. There is also a phone number listed if you need to speak to a genetic counselor by phone. I hope it helps. Thanks, AccessDNA
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