- Joined
- Apr 25, 2025
- Messages
- 16
- Reason
- DX ALS-FTD
- Diagnosis
- 03/2025
- Country
- US
- State
- IL
- City
- Chicago
This is the one post one should never want to join but glad it exists, a bit nervous to post this but here it goes. (BTW this isn’t everything regarding symptoms, tests, etc., but enough to paint the picture.)
They say hindsight is 20/20.
I’m a 52-year-old male (with a wife who I’ve known for 32 years and 5 kids, aged 25 to 9) whose life changed after contracting COVID-19 three confirmed times by PCR tests and was vaxed to the max (Moderna). What began as "Long COVID" symptoms – daytime sleepiness, brain fog, general cognitive impairment, and general weakness (in the face of maintaining bulk) without large-scale obvious wasting (mine later was determined UMN onset) – evolved into a diagnosis of frontotemporal dementia (FTD) with parkinsonism. The cramps are painful when they strike, lasting a few minutes including hands and feet "locking up," but I’ve had no numbness or chronic pain. They started to suspect an overlap syndrome (FTD-MND) somewhat early on as my progression seemed "odd" for FTD alone, but as you will see, the earlier EMGs weren’t very comprehensive and "not massively abnormal (their words not mine)" – the weird part is I have all these motor issues (UMN was the start for me, not LMN) and I still have a lot of bulk (which is starting to change). The loss of fine motor control, grip strength, and drop foot (heavily right-sided) all seemed odd in the context of FTD alone.
My diagnostic journey was a marathon, taking me through several doctors claiming expertise in Long COVID until I connected with an exceptional care team in December 2023. This team, including cognitive, movement, and neuromuscular neurologists, stopped relying on "pills" and began investigating underlying causes, such as cerebrospinal fluid (CSF) analysis for neurodegeneration. They recognized FTD with features of atypical parkinsonism, including executive dysfunction, apathy, reduced empathy, minor restful tremors, and progressive slowness in movement. CSF testing revealed borderline Alzheimer’s markers, elevated t-tau, low p-tau, significantly reduced abeta42 (<400), mildly elevated GAD65 (ruling out Stiff Person Syndrome), high protein, and other signs suggestive of neurodegeneration. Serum neurofilament light chain (NFL) levels doubled in just over six months, which my doctor said was a clear indication of neurodegeneration. SPECT scans were negative, but Levodopa eased stiffness. PET scans revealed progressive hypometabolism across brain networks, with repeat scans showing expanding affected areas, but nothing conclusive like Alzheimer’s disease or other specific conditions. (spoiler alert) My care team now suspects a TDP-43-related pathology as the common cause, ruling out progressive supranuclear palsy (PSP), corticobasal degeneration (CBD), and similar conditions based on neurological exam findings.
In June 2024, concerns about ALS prompted an EMG due to worsening movement issues. The results showed abnormalities (sporadic deltoid transients, tall motor unit potentials, and poor activation) but was ruled as isolated and potentially due to other issues, so they downplayed any ALS and suggested it was CNS-related, functional, or other causes (btw, I don’t blame anyone for the detour as hindsight is 20/20). In August 2024, I developed unstable diplopia, leading to an ER visit (not a stroke). A spinal MRI revealed C4-6 narrowing but didn’t explain my right arm and shoulder weakness or other symptoms. In October 2024, after a fall, I underwent a C5-C6 decompression as nothing else pointed to a conclusive cause, and the focus was on the obvious spinal issue, but it didn’t resolve the underlying problems, though it catalyzed further diagnostic clarity.
By late 2024, my speech and movement had deteriorated further (now termed apraxia), and I needed a walker to prevent falls. MRIs still showed no significant cerebral atrophy. The unstable diplopia, paired with these symptoms, led to a neuro-ophthalmologist who noted slow saccadic eye movements and recommended a single-fiber EMG and repetitive nerve stimulation (RNS) to rule out Myasthenia Gravis (MG). In March 2025, the single-fiber EMG revealed jitter, blocking, and motor unit instability specifically in the frontalis muscle, along with >10% RNS degradation in the arm. Three doctors made their way into the EMG room, seeking confirmation of what they were seeing, with the clinic head doc even redoing some more frontalis EMG himself (joking he was "quality control"). As the test went on, their banter started, with the head guy leaving saying, "I’m convinced," and kept downplaying MG but wouldn’t say a lot more other than, "let us put this all together and I want to see you in clinic." The report included a caveat of "NMJ disorder in the right clinical context," which I think is code for them knowing it's not MG (later confirmed) and early signs of denervation re-innervation. It was clear he knew right from the EMG, but needed additional data points to be certain. Shortly after, an in-person exam appointment appeared on my calendar, followed by a confirming phone call. For the first time, there was a lot of attention compared to a series of dead ends.
The clinic follow-up from the second EMG, involving yet another full neurological exam, happened a few weeks ago, and again, multiple doctors were there (and we aren’t talking low-level med techs). It was a scary but fun visit in the sense that the two main attendings bantered throughout, like asking me to lift my arms and close my eyes, only to hear, "See, right pronator drift," followed by, "Do it again," and, "Yep, I’m convinced." The compassion the head doc showed during the session was clear, and I felt taken care of. Findings included an upgoing Babinski reflex, right pronator drift, bilateral clonic jaw jerk, 3+ pectoral reflex, positive snout reflex, positive glabellar reflex, positive Romberg (backward), and negative Hoffman’s sign, with the right side showing more hyperreflexia than the left. Right-sided stiffness and increased tone were more pronounced than the left, with apraxic movements (slowed thought, speech, initiation, gait, and balance) and bulbar weakness. The apraxia limited the lower motor neuron (LMN) neurological exam, but my neuromuscular neurologist strongly suspected LMN involvement based on the two EMGs. When I directly asked if he thought I had ALS, he responded, "We at least know it’s not MG (albeit we tried the drug, which made things worse, btw), while we order some redo of the genetic testing. I’m less worried about debating what type of ALS this could be and more about getting you the best care – never mind the labels and timing, and let’s focus on the most important thing: you." The initial diagnosis was frontotemporal dementia with motor neuron disease (FTD-MND), with confirmed upper motor neuron (UMN) involvement, emerging LMN signs, and a strong overlap potential with amyotrophic lateral sclerosis (ALS).
Last week, I met with my cognitive neurologist, who specializes in FTD, and received a gut-punch confirmation: I have FTD-ALS. She explained that the "formal process" of diagnostic criteria, including more definitive imaging, is still required, but she was clear about the diagnosis. She noted that FTD-ALS is extremely rare, and started talking about trials as I'm about to get popular. She has only one ever had one patient with this condition and the two neuro docs (musclar and her) are going to tag team as each one understands their areas.
Just this week, I learned that the Invitae genetic testing results have been sent to my neuromuscular neurologist, though our next meeting isn’t scheduled until the end of June. However, I got a call from the Multidisciplinary Clinic (the ALS clinic), and they’ve pulled my appointment forward to Thursday – so I’m guessing we are slipstreaming into a more formal care process at this point. In reality, the ALS is the primary concern, though we need to complete the "formal" diagnostic pathways on the FTD side.
There is a lot still in flight as they are re-doing genetic testing and I’m okay with it given it pays it forward for others. The point of some of the testing doesn’t change the outcome and my wife is annoyed at all the testing still, but I want to add to the body of knowledge. The hardest moment for me came yesterday when my 12-year-old daughter was explaining to someone that dad has plaques in his brain and right now there is no cure, but she hopes they will find one someday (she ‘gets it’ but doesn’t fully understand it).
I personally don't understand all the "clarifying language around possible/probable etc but I’m currently FTD-MND with confirmed ALS (I guess because the FTD showed up first?), and the UMN was the starting point.
The bulbar progression is scary, with speech issues, mucus buildup, swallowing starting to fail, and coughing so hard it feels like I’m coughing up a lung to clear it. The cramps have now spread to my torso (abdominal muscles), the same long, painful kind. I’m also trying to describe the muscle sensation when I push too hard – it’s like a burn pain, similar to benching 200+ pounds back in the day when your arms are about to give out, knowing you’re at full tilt but can’t muster the strength to move. I’ve been told it’s bad to push this far, and the recovery time is long. It’s like an old iPhone that won’t hold a charge and drains fast. PT/OT calls it exertional myalgia with fatigue (kind of like the no pain no gain but at low levels of use), and now in the context of ALS it seems to make more sense.
I will say the doctors I have are quite direct but compassionate one of them even stopped me trying to walk out, waited with me and got me a wheelchair – while they don’t sugarcoat anything. Will update after my next "multidisp" clinic (I refuse to use the word ALS Clinic yet, and they are cool with it). We are in the process of getting a motor wheelchair (they seemed focused on getting me something for more advanced stages), and I am learning quickly that the "social worker" at the multi-clinic is probably the most important resource in the short run as she knows how to navigate the "system." - Unlike FTD, the ALS side of this is VERY VERY organized and my progression doesn't seem to surprise anyone.
We are still processing and are in the hope for the best, plan for the worst stage right now, but as I told the doctors, whatever I can do to pay this forward (genetics) other things. I'm told I'm driving my wife nuts in that I'm unmoved by all of this (as the doc tell us that's the FTD part) but I'm cared for.
I'm sure we will have a lot of questions along the way, sorry for the long note.
They say hindsight is 20/20.
I’m a 52-year-old male (with a wife who I’ve known for 32 years and 5 kids, aged 25 to 9) whose life changed after contracting COVID-19 three confirmed times by PCR tests and was vaxed to the max (Moderna). What began as "Long COVID" symptoms – daytime sleepiness, brain fog, general cognitive impairment, and general weakness (in the face of maintaining bulk) without large-scale obvious wasting (mine later was determined UMN onset) – evolved into a diagnosis of frontotemporal dementia (FTD) with parkinsonism. The cramps are painful when they strike, lasting a few minutes including hands and feet "locking up," but I’ve had no numbness or chronic pain. They started to suspect an overlap syndrome (FTD-MND) somewhat early on as my progression seemed "odd" for FTD alone, but as you will see, the earlier EMGs weren’t very comprehensive and "not massively abnormal (their words not mine)" – the weird part is I have all these motor issues (UMN was the start for me, not LMN) and I still have a lot of bulk (which is starting to change). The loss of fine motor control, grip strength, and drop foot (heavily right-sided) all seemed odd in the context of FTD alone.
My diagnostic journey was a marathon, taking me through several doctors claiming expertise in Long COVID until I connected with an exceptional care team in December 2023. This team, including cognitive, movement, and neuromuscular neurologists, stopped relying on "pills" and began investigating underlying causes, such as cerebrospinal fluid (CSF) analysis for neurodegeneration. They recognized FTD with features of atypical parkinsonism, including executive dysfunction, apathy, reduced empathy, minor restful tremors, and progressive slowness in movement. CSF testing revealed borderline Alzheimer’s markers, elevated t-tau, low p-tau, significantly reduced abeta42 (<400), mildly elevated GAD65 (ruling out Stiff Person Syndrome), high protein, and other signs suggestive of neurodegeneration. Serum neurofilament light chain (NFL) levels doubled in just over six months, which my doctor said was a clear indication of neurodegeneration. SPECT scans were negative, but Levodopa eased stiffness. PET scans revealed progressive hypometabolism across brain networks, with repeat scans showing expanding affected areas, but nothing conclusive like Alzheimer’s disease or other specific conditions. (spoiler alert) My care team now suspects a TDP-43-related pathology as the common cause, ruling out progressive supranuclear palsy (PSP), corticobasal degeneration (CBD), and similar conditions based on neurological exam findings.
In June 2024, concerns about ALS prompted an EMG due to worsening movement issues. The results showed abnormalities (sporadic deltoid transients, tall motor unit potentials, and poor activation) but was ruled as isolated and potentially due to other issues, so they downplayed any ALS and suggested it was CNS-related, functional, or other causes (btw, I don’t blame anyone for the detour as hindsight is 20/20). In August 2024, I developed unstable diplopia, leading to an ER visit (not a stroke). A spinal MRI revealed C4-6 narrowing but didn’t explain my right arm and shoulder weakness or other symptoms. In October 2024, after a fall, I underwent a C5-C6 decompression as nothing else pointed to a conclusive cause, and the focus was on the obvious spinal issue, but it didn’t resolve the underlying problems, though it catalyzed further diagnostic clarity.
By late 2024, my speech and movement had deteriorated further (now termed apraxia), and I needed a walker to prevent falls. MRIs still showed no significant cerebral atrophy. The unstable diplopia, paired with these symptoms, led to a neuro-ophthalmologist who noted slow saccadic eye movements and recommended a single-fiber EMG and repetitive nerve stimulation (RNS) to rule out Myasthenia Gravis (MG). In March 2025, the single-fiber EMG revealed jitter, blocking, and motor unit instability specifically in the frontalis muscle, along with >10% RNS degradation in the arm. Three doctors made their way into the EMG room, seeking confirmation of what they were seeing, with the clinic head doc even redoing some more frontalis EMG himself (joking he was "quality control"). As the test went on, their banter started, with the head guy leaving saying, "I’m convinced," and kept downplaying MG but wouldn’t say a lot more other than, "let us put this all together and I want to see you in clinic." The report included a caveat of "NMJ disorder in the right clinical context," which I think is code for them knowing it's not MG (later confirmed) and early signs of denervation re-innervation. It was clear he knew right from the EMG, but needed additional data points to be certain. Shortly after, an in-person exam appointment appeared on my calendar, followed by a confirming phone call. For the first time, there was a lot of attention compared to a series of dead ends.
The clinic follow-up from the second EMG, involving yet another full neurological exam, happened a few weeks ago, and again, multiple doctors were there (and we aren’t talking low-level med techs). It was a scary but fun visit in the sense that the two main attendings bantered throughout, like asking me to lift my arms and close my eyes, only to hear, "See, right pronator drift," followed by, "Do it again," and, "Yep, I’m convinced." The compassion the head doc showed during the session was clear, and I felt taken care of. Findings included an upgoing Babinski reflex, right pronator drift, bilateral clonic jaw jerk, 3+ pectoral reflex, positive snout reflex, positive glabellar reflex, positive Romberg (backward), and negative Hoffman’s sign, with the right side showing more hyperreflexia than the left. Right-sided stiffness and increased tone were more pronounced than the left, with apraxic movements (slowed thought, speech, initiation, gait, and balance) and bulbar weakness. The apraxia limited the lower motor neuron (LMN) neurological exam, but my neuromuscular neurologist strongly suspected LMN involvement based on the two EMGs. When I directly asked if he thought I had ALS, he responded, "We at least know it’s not MG (albeit we tried the drug, which made things worse, btw), while we order some redo of the genetic testing. I’m less worried about debating what type of ALS this could be and more about getting you the best care – never mind the labels and timing, and let’s focus on the most important thing: you." The initial diagnosis was frontotemporal dementia with motor neuron disease (FTD-MND), with confirmed upper motor neuron (UMN) involvement, emerging LMN signs, and a strong overlap potential with amyotrophic lateral sclerosis (ALS).
Last week, I met with my cognitive neurologist, who specializes in FTD, and received a gut-punch confirmation: I have FTD-ALS. She explained that the "formal process" of diagnostic criteria, including more definitive imaging, is still required, but she was clear about the diagnosis. She noted that FTD-ALS is extremely rare, and started talking about trials as I'm about to get popular. She has only one ever had one patient with this condition and the two neuro docs (musclar and her) are going to tag team as each one understands their areas.
Just this week, I learned that the Invitae genetic testing results have been sent to my neuromuscular neurologist, though our next meeting isn’t scheduled until the end of June. However, I got a call from the Multidisciplinary Clinic (the ALS clinic), and they’ve pulled my appointment forward to Thursday – so I’m guessing we are slipstreaming into a more formal care process at this point. In reality, the ALS is the primary concern, though we need to complete the "formal" diagnostic pathways on the FTD side.
There is a lot still in flight as they are re-doing genetic testing and I’m okay with it given it pays it forward for others. The point of some of the testing doesn’t change the outcome and my wife is annoyed at all the testing still, but I want to add to the body of knowledge. The hardest moment for me came yesterday when my 12-year-old daughter was explaining to someone that dad has plaques in his brain and right now there is no cure, but she hopes they will find one someday (she ‘gets it’ but doesn’t fully understand it).
I personally don't understand all the "clarifying language around possible/probable etc but I’m currently FTD-MND with confirmed ALS (I guess because the FTD showed up first?), and the UMN was the starting point.
The bulbar progression is scary, with speech issues, mucus buildup, swallowing starting to fail, and coughing so hard it feels like I’m coughing up a lung to clear it. The cramps have now spread to my torso (abdominal muscles), the same long, painful kind. I’m also trying to describe the muscle sensation when I push too hard – it’s like a burn pain, similar to benching 200+ pounds back in the day when your arms are about to give out, knowing you’re at full tilt but can’t muster the strength to move. I’ve been told it’s bad to push this far, and the recovery time is long. It’s like an old iPhone that won’t hold a charge and drains fast. PT/OT calls it exertional myalgia with fatigue (kind of like the no pain no gain but at low levels of use), and now in the context of ALS it seems to make more sense.
I will say the doctors I have are quite direct but compassionate one of them even stopped me trying to walk out, waited with me and got me a wheelchair – while they don’t sugarcoat anything. Will update after my next "multidisp" clinic (I refuse to use the word ALS Clinic yet, and they are cool with it). We are in the process of getting a motor wheelchair (they seemed focused on getting me something for more advanced stages), and I am learning quickly that the "social worker" at the multi-clinic is probably the most important resource in the short run as she knows how to navigate the "system." - Unlike FTD, the ALS side of this is VERY VERY organized and my progression doesn't seem to surprise anyone.
We are still processing and are in the hope for the best, plan for the worst stage right now, but as I told the doctors, whatever I can do to pay this forward (genetics) other things. I'm told I'm driving my wife nuts in that I'm unmoved by all of this (as the doc tell us that's the FTD part) but I'm cared for.
I'm sure we will have a lot of questions along the way, sorry for the long note.
