Friday, December 11, 2020

Knocking on Wood...

Well I haven't posted an update since April when I started the Clobazam, so this one is a bit lengthy (sorry). 

I started on a very low dose, just 5mg. That's about as tiny as you can get--I even had to cut the pills in half, since usually you get 10mg. It seemed to be helping and I was doing well for awhile. I had 0 partials in May, only 3 in June, 1 in July, and 0 in August. So I thought it was really helping. That was a really good stretch.

Then suddenly BAM out of nowhere, on September 5-6 I had this massive, intense cluster. I had 6 partials on Sept 5 and 2 on Sept 6. I've never had 6 in one day, and they were incredibly intense, to the point that I was worried some of them might generalize. I had to sit down for a couple of them in case I might pass out. The last time I had a cluster this intense was back in March 2018 when the walk-in clinic doctor had put me on antibiotics (which of course is how I learned that I shouldn't use antibiotics...). 

So I was running the checklist in my head... had I missed any medications? Sleep deprivation? Alcohol? Virus? Of course I was having headaches and severe fatigue and feeling like crap, but was that because I was sick or because of all the partials? I couldn't think of anything. But here's one thing: any kind of imbalance or stressor on the body, including illness, can trigger something like this. So I went and got a covid test. 

Now, covid does not have a direct relationship with seizures, but as I said, any kind of illness or stressor can trigger seizures and I couldn't think of anything else, so I figured it was worth checking. But the test came back negative. 

To this day I have no idea what triggered it, and it went away on its own. 

The next time I spoke with my neuro, I told him about this. We agreed to increase the Clobazam to 10mg and see what happens. 

I had been functioning with 5mg just fine, but as I said in my previous post, Clobazam is essentially a sedative, and doubling the dose has impacted me pretty significantly. I am soooooooooooo sleepy. Some days I'm ok, but other days I just want to sleep allllll day. It doesn't help that I have a crazy sleep schedule because of teaching at 3am every day. But even when I get 8 or 9 hours of sleep in a day, I just want to keep sleeping more. It has gotten a little better as I've adapted, but not really. I need a nap most days just to feel ok. 

With that said, I would rather be sleepy than have seizures. The increase seems to be working (knock wood). As of today, I have broken my record. Zero symptoms for 3 months and 5 days. Cross your fingers that the streak continues. 

On a different note, I've been both amused and annoyed lately at some people's misguided paranoia about the side effects of the covid vaccine. If they could only see the list of side effects from the three different medications that I take. Combine all three meds and it's amazing that I can function at all. Luckily, the actual side effects that I experience out of the potential side effects are relatively manageable. Here is what I actually experience on a regular basis from each med:

Topiramate: electrolyte imbalance (causes tingling in my hands, feet, head, etc.), hair loss, and memory/cognition/attention issues. Sometimes I feel like I have ADHD. I drink an electrolyte supplement daily to help with that part (yay nuun!). 

Lacosamide: mainly headaches. Usually one day per week I get intense headaches for no apparent reason.

Clobazam: oh so sleepy!!! Sinus/nasal issues. And constipation (sorry TMI).

And guess what? All of that is worthwhile to stave off the seizures and keep my brain healthy. But if things continue to go well, then I want to see about a small decrease in the Topiramate. 

I'm waiting for the Province to release the list of underlying conditions which qualify for early vaccination. If I qualify, I will be getting the vaccination as soon as I qualify... the last thing I need is that damn virus. 

Wednesday, April 29, 2020

Clobazam

This update is a little late.

I had my spring "appointment" on March 26, but it was over the phone instead of in person, because of Covid.

For the past year and a half, we have been playing with the dosages of Topiramate and Lacosamide, moving each one up and down in the hopes that that would do the trick. Not only has it not worked, but in the most recent six month period I was having more episodes.

On top of that, the increase to the max dose (400mg) of Topiramate resulted in some pretty heavy depression. I wasn't sure at first what was causing it because I'd never had trouble with the Topiramate at the lower doses, but I couldn't pinpoint another cause. The only other time I had felt that terrible was when I was on the higher doses of Keppra. So it had to be the increased dose of Topiramate.

So I told the neuro that not only was the current mix not working for my partials but the increased Topiramate was making me depressed, and of course he said that that was not going to work! So we reduced the Topiramate back to a dose that is ok for me. And then it was time to introduce a third med. Yay.

The reason for adding a third med instead of changing them altogether is that each of these meds comes from a different class, and they all work on the brain in different ways. Or so I'm told. To be honest I don't know enough about how they operate, but the idea is that if I am handling the ones I'm on, I'll stay on those ones because they are doing good things, and then add one that is going to do more good things in a different way, and hopefully between all three of them I can get it all under control. Anyway....

Introducing: Clobazam.

This one is a "benzo", and it's one of the "bad" ones that in theory you don't want to be on long-term. They can be addictive and not so great for you in the long run. It's actually a tranquilizer. But my dose is very low (just 5mg once a day, at night time).

And lo and behold.... I have not had ANY symptoms since starting it. Five weeks and counting. My record is about three months, so I'm not getting too excited yet. We'll see....


Tuesday, September 17, 2019

Fall Update, Part B

Dr Mary Glen
This morning I had another doctor appointment, but for something un-brain-related. Doesn't matter what for, but the point was that I saw Dr. Mary Glen. She is now working at my regular clinic, alongside my regular GP.

She introduced herself and I said, "Actually, we've met before." She didn't remember, and I hadn't expected her to.

I told her that four years ago, she was the doctor at the walk-in clinic when I first went to talk about the strange deja vu symptoms I was having. She's the one who sent me to my first neurologist.

I told her thank you for taking me seriously, for listening and not dismissing me. I've heard some horror stories from people who have experienced the opposite from other doctors.

It's been a hell of a journey since then, but I'm still incredibly grateful for her.

On sleep, and feeling rested. 
This morning I was thinking about the fact that I am a good sleeper now. It's so weird. For 16 years I was chronically sleep-deprived. I know now that it was from extremely low iron. Then when my epilepsy started my iron was (finally) checked and was brought up to normal levels through supplements, but then I was on stupid seizure meds that made me so exhausted that the sleep didn't help. I still felt insanely tired all the time. Even when I slept and slept, I was tired.

Now--ever since I switched from Keppra to Vimpat--I sleep 7 or 8 hours, and I wake up in the morning... and... I feel good. I feel rested. I still tire out by about dinner time, but that's probably because of my brain and my meds, and that's ok.

It took me awhile to notice, and I still think it's strange. But it's also pretty cool. I'll take it.


Monday, September 16, 2019

Fall Update

Saw Dr Kula today for my six month appointment.

I last saw him in March, when we increased the Lacosamide. At that time, he also had sent me for an ECG because the Lacosamide is a sodium channel blocker and can impact the heart. My ECG showed "first degree AV block", which is just a borderline abnormality, most likely caused by the med and not a huge concern. According to this page, "In general, a 1st degree AV block is a benign finding that does not require any treatment, however it may be an indicator of higher degree AV block in the future."

Anyway, because the Lacosamide increase made zero difference in the number of partials I've been having over the last six months, we're decreasing it back down to 200mg per day rather than 300mg per day anyway. I will have another ECG in a month to see if my results go back to normal.

Instead, we are going to increase the Topiramate from 300mg to 400mg.
I suggested this and had already read that 400mg is the max dose.

He said we are on the same page, and throughout the appointment kept saying that I am a star patient and should be a neurologist because everything I suggested was exactly what he was going to suggest himself, lol. He also loves that I keep track of every partial, and that I do my own research and reading. He said I am the ideal patient.

I asked about the long term effects of the medications. I've asked both him and my old neuro this before but I always want reassurance and he told me again that the long term effects are nothing to worry about.

I also told him that I'm actually really worried about my brain, looking into the future. Alzheimer's and dementia run in my family, particularly in the women. Between that and the damage that the seizures are probably doing, I am worried that I am going to lose my faculties early. He said to focus on what I can control: diet, exercise, taking care of myself. Basically, he said, "keep doing what you're doing." I was worried that he would be dismissive of my concern but he wasn't at all, thankfully.  He also told me that partial seizures have a far smaller impact on my brain than generalized seizures do, so I have the "good" kind of seizures, as far as that goes.

 He also said that just because Alzheimer's runs in the family, I don't necessarily have the gene. Also, he said that we will likely have medical treatment for it within the next 10 years(!).

If the Topiramate increase doesn't do the trick, then we may add a third medication in the spring. Next appointment is six months from now.

Now to get through the increase... this is the one that makes me feel drugged. I will probably wait until the weekend and take Monday off as a sick day. Monday is the four year anniversary of my partials starting, and I always take a self-care day that day anyway.

Monday, March 11, 2019

Spring Update

Well, not too much to tell here. I was hoping for something more exciting. I saw my neuro today and got my test results. I'll do this in bullet points because it's all over the place:

  • My EEG showed some spikes in the "anterior right temporal lobe", which we already knew because the EEG tech told me this and I told you in the previous blog post.
  • My new, high-res MRI still did not show anything!! 
  • I asked if this means we can't do anything except medicate... does this mean I am not a surgery candidate?? I was reading recently about a cool new tech called laser ablation surgery where they just zap the bad cells from your brain and you're done. He said I could still be a surgery candidate if I really want to pursue it, but it requires a lot more testing and that testing is extensive and invasive (like staying in the hospital for a week or more, etc.). They usually only do that for serious cases that are not responsive to meds, but if I really pushed it they could look at it. I said we could leave it on the backburner for now since my meds are doing ok and I'm not in a place in my life right now where I want to put myself through that... but maybe another time. 
  • We are increasing the Lacosamide, at my request, since I have been doing well with it (no side effects) and I want to try to get to 100% control where I am not having any partial seizures or anything else going on. Keeping the Topiramate dosage the same. He wants me to go for an ECG in a few weeks because the increased dosage on the Lacosamide can sometimes have an impact on the heart(!). 
  • I asked about long term effects of both meds, including memory loss, etc. He said both are fine, as far as we know. He said that people who report memory loss or other effects with the Topiramate report it in the short term and I would have noticed it already; i.e., it's not a long-term effect so if I haven't noticed it in the past two years already, it's not going to happen. So that's good. 
  • Today is the 2 year anniversary since my last generalized seizure!
  • Turns out that since I last filled my Lacosamide prescription, a generic version has been released in Canada. There was no generic version before (and there still isn't in the US), which meant it was massively expensive. I'm covered under Fair Pharmacare because of the type of medications and the cost of them, but going generic is still helpful for the portion that I do have to pay. The non-generic Vimpat costs around $300/month vs. $100 for the generic, and then I still have to add my Topiramate on top of it. Thankfully, Fair Pharmacare covers the bulk of it, so my actual cost now is around $66/month. Thank the gods for socialized health care!!! 
When I think about where I was at two years ago... or even one year ago, I feel a lot of gratitude and hope. I'm in a vastly different and better place mentally, physically and emotionally. I look back at my blog posts and remember how exhausted and sad and hopeless I felt, and I can't describe how much better I feel now. I still have off days and weeks of course, and I don't expect that that's going to go away, but overall it's like night and day. So good. :)  

Thursday, November 29, 2018

Yay Coffee, Yay Sleep!

Wow, what a week!

A month ago, when I met my new neurologist, he told me that he would be putting in requisitions for a new MRI and a sleep-deprived EEG. But there are wait-lists for both, so I was not expecting either one to happen any time soon.

Monday, I got the call for the sleep-deprived EEG. Already. She asked if I could come in Thursday. Yes, but... so soon?? Suddenly I didn't feel ready. She gave me all the instructions: St Pauls Hospital, Thursday morning. Allowed 4 hours of sleep. Hair must be completely dry. Take meds as normal. No caffeine after 3pm Wednesday. Light breakfast. Comfortable clothing. Here's how you find us... I'm writing all this down and I feel my anxiety level rising before the phone call is even finished.

I'm not usually someone who is prone to high levels of anxiety, but that day it was through the roof. Here's why:

I've spent the last three years doing everything in my power to NOT have seizures. Also, my previous EEG came out clear. But now, I had to try to turn everything around in a three day period and shift the balance so that I would have some activity on Thursday--just enough to show something on the EEG, within that one-hour window while I was hooked up to the machine. But I did not want to shift it so much that I would end up giving myself a generalized seizure.

Adding to the anxiety was transportation. I was thinking worst case scenario. If I did happen to trigger a generalized seizure due to the sleep deprivation, etc, and I was on public transit, what was going to happen? Should I take a cab? Thank goodness for Michelle and her hubby Gary, who offered to drive me to the hospital--that took a giant load off my mind!

So, how to shift the balance?

Since I was tapering off of the Keppra anyway and nearly finished with it, I stopped taking it immediately. I was down to 500mg and figured that bit of withdrawal might give a response. Sure enough, I started feeling a response over Tuesday and Wednesday (the anxiety may have contributed as well). I also stopped my Progesterone cream for those few days. Brainstormed a few other things like THC and antibiotics, but those were less practical so I didn't do them. Ultimately, I had to face the fact that I could not control the result no matter how badly I wanted to.

Wednesday night came and my plan was to sleep 1:30 to 5:30, but my fear was that I wouldn't sleep at all since I often don't if I'm anxious about something. Luckily I did sort of sleep those four hours, though I did wake up three times in that timeframe. Up, walked the dog, ready to go by the time Michelle and Gary arrived. In the car, Michelle gave me a good luck coin from Japan. :) Arrived at the hospital early enough to spend some time fretting about the test and wishing I could have some coffee. Checked in, met my EEG technician, who was very friendly and talkative. She asked me a bunch of questions about my meds, history, etc. Then she started raving about my new neurologist. Apparently he is one of the best. She said they all love him and he is very involved and compassionate. She said that he will be down at the hospital himself by tomorrow, looking at the results in person, and that most doctors don't do that (!). That was really encouraging and good to hear.

Then she hooked me up. So for those who aren't familiar with the process, they stick a couple dozen electrodes all over your head (also one on your left cheek for your eye and one on your chest for your heart). The glue they use is very sticky and nasty so that you have to wash your hair after. The electrodes pick up the electrical signals from your brain and a few are picking up muscle activity. Feeds it all to a computer. So from her computer she could see when I opened and closed my eyes, when I twitched a facial muscle, or when my ears moved, etc. It's wild. But she could also see the electrical activity in my brain, which of course is why we were there. Then they put you through some activities to try to encourage seizure activity. So the first thing she had me do was heavy breathing for 3 minutes, like hyperventilation (those of you following on facebook may have seen the comments about sometimes getting partials when I'm running). Then after that she had me relax and actually left me alone with a white noise machine for awhile in the hopes that I would doze off. This is because some people have seizures when they're asleep, or just on the verge of falling asleep (I don't tend to, but many do). Then after that, she flashed a series of bright lights in my eyes with varying patterns and speeds. Many people with epilepsy are light sensitive, apparently because the optical nerve is the only nerve that runs through the entire brain (or so my previous EEG technician told me).

Through all of this, I felt NO activity, no partials, nothing. When she was done and was taking off the electrodes, I was discouraged. I told her that I hadn't felt anything.

Then she said the magic words: No worries. We got lots.

Wait, what? You did?

She had told me beforehand that they could catch activity even if I didn't feel anything, but I wasn't really sure how much. But yep, she said that she had all sorts of "big puppies" she called them, "epileptic discharges, clear as day". She offered to show me what it looked like on the computer. She showed me the normal waves, just little squiggly waves, and then she scrolled over to one of the "big puppies", and there it was... big, jagged, pointy, mountainous line that then returned to the little squiggly lines. She explained to me how she could see from that one spot--which lasted just a fraction of a second--where in my brain my seizures are originating (called the focal point), and where in the brain they're spreading. She said it's like throwing a pebble in a pond. You have the spot the pebble lands, and then the ripples go out from there. The focal point is where the pebble lands, and she can tell that from the lines on the computer where all the ripples are(!). She moved on to another one and it showed the same thing. So my discharges are happening in the same place. Some people have multiple focal points but from a cursory glance it looks like I have just one.

She gave me a little diagram and showed me where my focal point is, where the red star is:

That is the front of my right temporal lobe. We've always known it was temporal lobe from my symptoms, and I've always thought it was my right lobe, but this confirms it.

Having a single focal point is good for a specific reason (and here is where she told me something she is not supposed to tell me, so pretend she didn't tell me this... I'm just making this part up on my own... ;). There's a possibility that it's being caused by a specific thing, as in scar tissue, and if that's the case there's a possibility that it could be removed through surgery. This is still a long shot and would need to be confirmed by further testing but it's the first time that the idea of being a surgery candidate has entered my mind--primarily because my first MRI showed nothing.

Some of you might think that the idea of opening up my head and removing a piece of my brain is not good news. But it is. Success rates with this kind of surgery are good, and the people with epilepsy who I've talked to who have had it are really happy with their results. In many cases it stops the seizures altogether and some people are med-free afterwards.

I'm not saying this is the road I'll go down. But an MRI has already been ordered for me on a stronger machine than my first one. If it were to show scarring in the same spot as my focal point, there's a chance I could be a candidate for surgery, and if my neuro were to recommend it I would consider it.

If not, then I continue on the same path, and we are at least better informed now.

In any case, this is all good news! I am happy with today's results. The sleep deprivation was worthwhile, and I was really glad to come home and sleep and drink coffee! :)

HUUUUGEEEE thank you to everyone who helped me this week with your moral support. Those of you who offered to be available in case of emergency, those who kept me company late at night, everyone who checked in on me, offered support on facebook and in texts, offered rides, and everything else. It means a lot, and I love you all. I'm going to kick back for the rest of the day. :)

Monday, October 22, 2018

New Neurologist, New Tests, New Medication

Well I met my new neurologist today, finally!
And I already like him better than my old one.
First, instead of staring at a computer screen for the entire appointment like most doctors do (including my old neuro), he asked me to tell him my story, and he faced me and took notes and asked a lot of questions about my experience. This is completely different from my old neuro. Dr K asked more questions in this one appointment than my old neuro did in three years.

I told him that I want off of the Keppra because it makes me exhausted and depressed, but that I'm happy with the Topamax. He said no problem. He said we will try one called Vimpat. It's a relatively new one on the market but does not have the mood side effects like the other ones I've been on in the past, and I also shouldn't have the big physical reactions as well. He said most likely I will just get some dizziness in the beginning but that will go away. The other big thing with this med is that it's expensive but he's going to put in the paperwork to get it covered under Fair Pharmacare for me since I qualify for that, having already tried four other meds and failed. So I can't start it right away, until that is cleared (it will be a few days to get that processed, apparently).

He is also going to send me for more testing. He wants me to do a sleep-deprived EEG. My previous EEG was just the short, regular one. This one will be sleep-deprived (meaning I have to stay up all night the night before). He's also going to send me for another MRI, but with a more powerful machine than the one I had before at the Lionsgate Hospital; this one can pick up stuff that the other one might have missed. So if there are anomalies or scar tissue or whatever in my brain that was too small for the other MRI, this one could catch it. I'll be on a wait list for those tests so they may be a few months.

Now for the bad news. He told me that every time I change my meds, I have to stop driving for three months. I didn't believe this because no other doctor has ever told me this, and I've had several different doctors change my meds (not just my old neuro, but hospital neurologists as well--none of them ever told me to stop driving each time!). He said it's the law, and actually showed me the page on the BC provincial website. So why is this the first time I've heard this??

Of course that's not what I want to hear... but I want off the Keppra more than I want/need to drive, so I'll go with it. Also I'm not working right now so it's not the end of the world. I can go back to transit/foot for awhile.

In any case, I'm not starting the new med until the Fair Pharmacare thing gets processed, so in the meantime I'll stock up on groceries and any other running around I need to do. :P