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Antibiotics & Lyme: Everything You Need to Know

https://www.bca-clinic.de/en/antibiotics-and-lyme-disease-everything-you-need-to-know/

Antibiotics And Lyme Disease: Everything You Need To Know

25. March 2019 in BCA-clinic

Antibiotics are often the default treatment path for many doctors when it comes to Lyme disease. However, they are not always effective. Lyme disease is a complicated disorder that we don’t yet fully understand. Yes, antibiotics work to a certain degree, but in some cases they don’t fully eradicate the disease, leading to years of debilitating symptoms for patients. So when are antibiotics effective, which types are effective, and in cases where they fail to get rid of the Lyme bacteria, what happens? These aren’t easy questions to answer, as much Lyme disease knowledge is still murky at best. However, it’s important to try to understand exactly how antibiotics and Lyme disease work in tandem.

Firstly, let’s look at when they are effective. Lyme disease can be broadly split into two stages: acute and chronic. Acute Lyme lasts for a few weeks, and is easily identifiable by the presence of a bullseye rash. This distinctive Lyme symptom is present in the majority of cases in the initial stages of the disease, and is one of the best indicators available to doctors and patients alike. If the condition is presented to a medical professional in the acute stages, Lyme disease can almost always be eradicated by antibiotics. Successful treatment is usually achieved by a short course of oral antibiotics, namely doxycycline or amoxicillin. However, if this acute stage of the disease is missed and it progresses to the chronic stage, antibiotics alone will not be enough to fight off the disorder.

*Many doctors prescribe antibiotics for patients who have a diagnosis of Lyme disease.*

Chronic Lyme disease is a much more diverse and complicated condition than acute Lyme. This is because inflammation also plays a significant role in the symptoms. Many doctors follow the traditional line of thinking that Lyme, being caused by the presence of bacteria, can be treated successfully using synthetic microbes (i.e. antibiotics), like many other conditions and diseases. While this reasoning may be structurally sound, it doesn’t take into account the body’s own reaction to the bacteria, and how that can kickstart a whole set of new and debilitating symptoms. On top of that, individuals will have different reactions to the borrelia bacteria, depending on their constitution. Lyme disease is not a one-size-fits-all condition like the flu, which has very little variance in its symptoms on a person-to-person level.

The symptoms of chronic Lyme vary wildly, but usually include joint pain, muscle pain, aches, soreness and a chronic sense of fatigue. All these symptoms are a result of the immune system’s response to the bacteria. For some reason, the immune system goes into overdrive when faced with a long-term borrelia infection, resulting in severely debilitating symptoms, even when the actual presence of the bacteria may be minimal. Obviously, antibiotics administered at this point will have zero effect on inflammation symptoms, as they are the body’s own doing. Yet Lyme-illiterate doctors will often insist on antibiotics as the only treatment path for chronic Lyme disease, if they believe the diagnosis at all (chronic Lyme is still not officially recognised by the CDC).

Treating chronic Lyme requires a more nuanced touch. The medical staff at BCA-clinic in Augsburg, Germany, have been experts in Lyme disease for a long time. Their approach to treatment is designed to tackle both the inflammation and infection symptoms of the disease. The first thing to do is test the patient to see what the ratio of inflammation and infection actually is. Some people might have a lot of inflammation and only traces of a bacterial infection, while some others might have the complete opposite. Successful Lyme disease treatment constitutes knowing the difference between the two, and responding accordingly. Antibiotics are only half of the approach here, as they solely deal with infection. For the inflammatory symptoms, herbal supplements and diet adjustments are necessary.

*Antibiotics can be helpful in fighting chronic Lyme, but they really only deal with the infection side of the disease, not the inflammation.*

Borrelia bacteria have been proven to be surprisingly resistant to antibiotic treatment. If they are left in the system, they can adapt to survive the natural immune response, as well as tolerating various forms of common antibiotic. Borrelia exists in two separate forms: the spirochete and the ‘cell wall’ variant, sometimes known as the ‘cyst’ form. Under stress, the spirochete will adapt to the cyst form, making it much more resistant to antibiotics. It is likely that the majority of chronic Lyme sufferers have both borrelia forms present in their systems at any given time. Therefore, it is crucial to combine antibiotics in order to attack the bacteria from all angles. This requires an experienced medical professional who is well-versed in Lyme; unfortunately, many doctors are not.

It’s important to back up any heavy antibiotic use with a probiotic, in order to keep your gut healthy. Knowing how long to stay on a course of a particular antibiotic is also necessary. If you suspect you have chronic Lyme disease, getting help from an expert in the field should be paramount. The disease can affect people for many years, and is very hard to treat if you don’t know what you’re doing. While antibiotics are an important component, they are not totally reliable in every case. When it comes to chronic Lyme, they should be used as part of a broader treatment process.

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**Comment**

A few points:

There is legitimate science behind antibiotics killing pathogens which is why it is a “default.”
The jury’s really still out on whether or not acute cases are “cured” by short-term antibiotics. According to Microbiologist Tom Greer, treatment failures have been documented since the beginning. Who’s to say a person treated early doesn’t go on to develop arthritis or even mental illness and never connects the dots to a past Lyme/MSIDS infection? The M.D. who wrote this thinks we should be concerned: https://madisonarealymesupportgroup.com/2017/06/10/the-coming-pandemic-of-lyme-dementia/
There are various reasons why antibiotics sometimes do not work. Until this is teased out, there is a lot that remains unknown. We know the organisms are stealthy and evade treatment, and I don’t believe that’s just in the case of antibiotics. Also, there are nuances with antibiotic treatment that most doctors aren’t privy to. For more on this see: https://madisonarealymesupportgroup.com/2016/02/13/lyme-disease-treatment/. Also, for an informative video by Dr. Burrascano, a well known and experienced Lyme literate doctor, see: https://www.ilads.org/dr-burrascano-happy-holidays/?. Drug blood levels are crucial and need to be addressed. I highlight the 40 minute video where he discusses treatment nuances here: https://madisonarealymesupportgroup.com/2019/02/22/why-mainstream-lyme-msids-research-remains-in-the-dark-ages/. I’ve seen a lot of patients through the years and the ones that do the poorest are those that have tried alternative things for years, unwilling to even try antibiotics, and those who have used antibiotics indiscriminately. What I mean by that is they’ve been given the CDC mono-therapy of doxycycline for long periods of time without consideration of and treatment for the various forms of Lyme or coinfections. Doxy, while a great front-line drug that works against many of the pathogens will not work against some – like Babesia for instance. Also, in my opinion, there are some doctors who have not taken a holistic approach and have neglected key aspects of treatment like detoxification and gut health. To steal a quote from Dr. Burrascano, “Now is the time for pristine health habits.” This illness will test your metal in every way, shape, and form. Learn ALL you can to improve your immune system, but let me be clear – antibiotics DO kill things. It’s proven. Lyme/MSIDS finds and uses your weaknesses against you. The best thing you can do is find out and address your weaknesses.
If you study the Lyme organism, you realize that it is pleomorphic and certain antibiotics (doxycycline) will only address certain forms – potentially leaving other forms to emerge later. This is a real concern. I think it folly to use the mono-therapy on anyone – acute or chronic. Researcher Eva Sapi has shown that high doses of doxy actually throws the spirochete into the non-cell wall form: https://www.dovepress.com/evaluation-of-in-vitro-antibiotic-susceptibility-of-different-morpholo-peer-reviewed-article-IDR. My main concern is the potential for this to be happening to folks treated early with only doxy. While this author states there are only 2 forms of the bacteria, there are actually 4 and effective treatment takes this into account:
Once infected, a person should be on the look-out for future symptoms and work with an experienced practitioner that understands the nature of the organisms involved.
What IS murky is the Bull’s-eye rash criteria that’s been used for decades keeping thousands from a proper diagnosis. The percentage who gets it varies wildly (27-80%) clearly demonstrating the need for better markers. While those who DO have the rash HAVE Lyme disease, those who DON’T – CAN ALSO HAVE Lyme disease. I can’t be any clearer.
Some antibiotics DO address inflammation: https://madisonarealymesupportgroup.com/2017/06/04/minocycline-for-ms-and-much-more/. Mino was one of the most effective drugs for me as it crosses the blood/brain barrier, kills pathogens AND addresses inflammation. Another thing that really has been a game-changer for me is MSM: https://madisonarealymesupportgroup.com/2018/03/02/dmso-msm-for-lyme-msids/. Interesting note: MSM did nothing while I was in full-fledged treatment. It was only AFTER treatment that this seemed to help. I noticed a 70% reduction in pain within a week and had nearly none in a month’s time. Also, consider systemic enzymes for their anti-inflammatory properties: https://madisonarealymesupportgroup.com/2016/04/22/systemic-enzymes/. Interestingly, these also only worked after treatment for me. Also consider LDN & CBD oil: https://madisonarealymesupportgroup.com/2016/12/18/ldn/, https://madisonarealymesupportgroup.com/2019/02/10/the-endocannabinoid-system-and-the-important-role-it-plays-in-human-health/
In sum, treating this complex illness will be one of the most challenging things you’ve ever done. Partner with an experienced practitioner and learn all you can. Bring ideas to the table if you feel them worth consideration. Feeling overwhelmed is part of this process but if you learn one thing every day by the end of the year, you’ve learned 365 new things! Keep an open mind and talk to others. While what they’ve done may or may not work for you, you’ve learned something that may help someone else, and develop the attitude that you are willing to try everything and the kitchen sink if it works.

Chin up. You can do this!

Category:

Activism, Gut Health, Inflammation, Lyme, Treatment

AutismOne 2019 Chicago Conference in May – Dr. Brown Speaking

conf-2019

Register here: https://autismone.ticketspice.com/autism-one-2019-conference

The most rewarding educational and networking experience you can have at any autism conference! An exceptional value as you gather new hope, answers, help, and direction.

New to the autism diagnosis? Come hear the “Newly Diagnosed” track just for you!
Yearning to learn more? Hear the “Biomedical Research and Treatments” track!

This conference will help you answer and understand important concepts:

Recovery from autism is possible and children get better!
There are medical comorbidities of autism that, when treated, allow the child to enjoy improved learning and behavior.

On the autism journey a little while? Come hear the latest research and healing information!
Medical professional? Hear renowned researchers present the latest cutting-edge autism research.

Conference track highlights include:

Membrane Medicine track
PANDAS/PANS track (pediatric autoimmune neuropsychiatric disorders associated with streptococcal infections and pediatric acute-onset neuropsychiatric syndrome)
4th Annual International HPV Vaccine Education Symposium
Focus for Health Advocacy Training track
Chiropractic Pediatric Continuing Education Credit Program with Emphasis on Autism
Endocannabinoid Medicine track
ADHD (attention-deficit/hyperactivity disorder) track
Culinary Day: Culinary Day on a Budget
And a special surprise panel that illuminates the bigger picture that affects your family’s world

The AutismOne 2019 Conference will be held May 22-26, 2019, at the Loews Chicago O’Hare Hotel in Rosemont, IL.

“AutismOne always has the cutting-edge information years ahead of any other autism conference. You hear it first at AutismOne.” ~Janet Cakir, PhD

CONFERENCE SCHEDULE-AT-A-GLANCE

WEDNESDAY, MAY 22, LECTURES:
1:30PM-6:00PM

THURSDAY, MAY 23, LECTURES, MOVIES, PANELS:
8:30AM-10:15PM

FRIDAY, MAY 24, LECTURES AND PANELS:
8:30AM-5:45PM

SATURDAY, MAY 25, LECTURES AND PANELS:
8:30AM-7:00PM

SUNDAY, MAY 26, LECTURES:
8:45AM-1:30PM

See list of speakers: https://autismoneconference.com/conference_speakers.html Erica Linn, MSN & Dr. Greg Brown MD from Serenity Health in Wisconsin will be speakers at the conference. Dr. Brown treats children and adults with Lyme/MSIDS as well as PANS/PANDAS. He’s stated that up to 80% of his autistic and PANS/PANDAS patients are infected with Lyme/MSIDS.

For more on that connection: https://madisonarealymesupportgroup.com/2017/10/01/panspandas-steroids-autoimmune-disease-lymemsids-the-need-for-medical-collaboration/

https://madisonarealymesupportgroup.com/2017/10/08/misdiagnosed-how-children-with-treatable-medical-issues-are-mistakenly-labeled-as-mentally-ill/

https://madisonarealymesupportgroup.com/2017/06/30/child-with-lymemsidspans-told-by-doctors-she-made-it-all-up/

https://madisonarealymesupportgroup.com/2017/10/09/today-is-panspandas-awareness-day/ Trifiletti officially diagnosed Carson with PANS, not PANDAS, due to the active co-infections found in his blood work: mycoplasma, the bacteria that causes pneumonia; coxsackie — the virus causing Hand, Foot and Mouth disease; streptococcus, the bacteria causing strep throat; bartonella and babesia — a bacteria and parasite related to Lyme disease; and yeast, Melissa Spears said.

Instead of attacking these infections, Carson’s antibodies were instead going after his brain.

https://madisonarealymesupportgroup.com/2018/03/14/dr-frid-children-lyme/

Category:

Activism, Autism, Inflammation, Lyme, Psychological Aspects, Treatment

Innovative “Alternative” Therapies for Chronic Lyme Disease

https://restorativemedicine.org/wp-content/uploads/2017/01/4Holtorf_-Lyme-CFS.pdf (Slides Found in link)

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Innovative “Alternative” Therapies for Chronic Lyme Disease

Kent Holtorf, M.D.

Holtorf Medical Group National Academy of Hypothyroidism Kholt@holtorfmed.com

Category:

Inflammation, Lyme, Pain Management, Sleep, Supplements, Treatment

Sjogren’s Syndrome: Clinical Benefits of Low-dose Naltrexone Therapy

https://ldnresearchtrust.org/sites/default/files/sjogrens%20publication.pdf

Sjogren’s Syndrome: Clinical Benefits of Low-dose Naltrexone Therapy

Scott Zashin 1

1. Rheumatology, University of Texas Southwest Medical Center, Dallas, USA Corresponding author: Scott Zashin, szashin823@aol.com

Abstract

Sjogren’s Syndrome is a chronic autoimmune disorder that causes the inflammation of the lacrimal and salivary glands, resulting in dryness of the eyes and mouth. In addition, fatigue and musculoskeletal pain, often described as aching, is very common. Treatment directed toward alleviating the fatigue and pain associated with Sjogren’s is currently very limited. This report describes a case of a 47-year-old female with suspected Sjogren’s based on long-standing dry eyes, dry mouth, joint pain, fatigue, elevated measures of inflammation, and a positive rheumatoid factor. She failed standard therapy but improved clinically with low-dose naltrexone therapy.

Introduction

Low-dose naltrexone (LDN) is a unique compound that has pain-relieving and anti- inflammatory properties. Limited studies have shown benefit in helping relieve the pain in patients with fibromyalgia and improving disease activity in autoimmune conditions such as inflammatory bowel disease and multiple sclerosis. As a result, it seems reasonable that the medication might be useful in Sjogren’s Syndrome, an autoimmune condition that is associated with pain and inflammation.

Case Presentation

A 47-year-old female was diagnosed with Sjogren’s Syndrome six years ago by another rheumatologist, based on her history of eye and mouth dryness. She was found to have a negative rheumatoid factor at that time, but her sedimentation rate by modified Westergren (erythrocyte sedimentation rate, ESR) was recorded as low as 48 and as high as 61 (normal: less than 20 mm/h). Her C-reactive protein (CRP) was 1.74 (normal less than 0.80 mg/dl). Two years ago, she saw a second rheumatologist who agreed with the diagnosis of Sjogren’s Syndrome. At that time, her rheumatoid factor was now elevated at 69 IU/ml (normal: less than 14 IU/m/). Her antinuclear antibody (ANA) and Sjogren antibodies (SS-A and SS-B) were absent. Her anti-CCP antibody and 14.3.3 ETA protein were normal. Her ESR was 48 and her CRP was 1.42. Past medical history included a diagnosis of fibromyalgia. She also had a history of breast cancer that had been in remission for 20 years, a generalized seizure disorder, and elevated liver tests with normal biopsy. Additional medical issues included symptoms of neuropathy, anxiety, and depression. A prior sleep study did not reveal evidence of sleep apnea. She first came to see this author 18 months ago, seeking another opinion, with complaints of fatigue, severe musculoskeletal pain, as well as dryness of her eyes and mouth.

Her daily medications to help with her symptoms of Sjogren’s Syndrome and fibromyalgia included Lexapro, Restasis, meloxicam 15 mg, vitamin D3, magnesium, tramadol 100 mg daily prn, salagen 5 mg tid prn, and hydroxychloroquine 400 mg daily. Her exam demonstrated widespread trigger points affecting both sides of her body, above and below her waist. Her blood work was remarkable for an ESR of 37 and a CRP of 0.77. Her alanine aminotransferase (ALT) was 40 U/L (normal 6-29 U/L).

She elected to try low-dose naltrexone (LDN), which was compounded using a short-acting filler and started at 1.5 mg daily with instructions to increase the medication weekly by 1.5 mg. She came back to see me two weeks after starting the medication and was taking 3 mg daily. She stated that she felt terrific. Her lab was remarkable for a normal ESR of 25 and a CRP of 2.33. Her ALT was normal.

She was seen in follow-up 16 months ago and remained on 3 mg of naltrexone. She felt well but complained of neuropathic pain. Her ESR was now 20. CRP was not ordered. Her ALT was 31 U/L. She was seen in follow-up 14 months ago and remained on 3 mg of naltrexone and continued to feel well without stiffness or pain. She noted that, previously, it would take her all day to feel better. Her ESR remained at 20 and CRP was only minimally increased at 0.87.

She was then seen in follow-up 11 months ago with complaints of increased achiness. She had widespread tender points. She was given a short course of corticosteroids with symptomatic improvement in place of meloxicam. Naltrexone was increased on that visit to 4.5 mg. On the day of that visit, her ESR was 40 and CRP was 25.7 ( current normal value less than 8 mg/L). She was again seen in follow-up nine months ago, doing well on 4.5 mg of naltrexone. Hydroxychloroquine was discontinued a few weeks earlier due to a prolonged QTc interval. Her ESR was back down to 20 and CRP was down to 10.9.

Overall, the patient noted significant clinical benefit with her fatigue and pain within two weeks of starting low-dose naltrexone but no significant change in her dry eyes or mouth. She continues to do well on low-dose naltrexone four months after stopping hydroxychloroquine due to the electrocardiogram (EKG) abnormalities. While her symptoms improved, what is most interesting about this case is that her clinical improvement was associated with an improvement in her inflammatory markers.

Discussion

In the initial pilot study that used low-dose naltrexone in the treatment of fibromyalgia, the baseline sedimentation rate was a significant predictor of clinical response to LDN [1]. It was of interest to note that this patient’s dramatic clinical response to LDN correlated with an improvement in her ESR. It is postulated that low-dose naltrexone has a beneficial effect on the immune system due to the following mechanisms.

Low-dose naltrexone blocks mu-, delta-, and other opioid receptors. These receptors are present in the cells of the immune system. This inhibition may result in an upregulation of endorphins, which in addition to decreasing pain, may have a beneficial effect on the immune abnormalities by suppressing cell growth [2].

Low-dose naltrexone inhibits microglia activity. Microglia are immune cells in the central nervous system that, when stimulated, produce inflammatory products that may be associated with pain, fatigue, cognitive dysfunction (brain fog) sleep, and mood disorders. Low-dose naltrexone inhibits toll-like receptors that are found in microglia cells. As a result, the production of inflammatory substances declines with resulting symptomatic improvement [3- 4]. The inhibition of these toll-like receptors has been postulated to be responsible for the effectiveness of hydroxychloroquine, a standard therapy in diseases such as Sjogren’s Syndrome and systemic lupus.

Overall, LDN is well-tolerated. The 50 mg standard dose of naltrexone is Food and Drug Administration (FDA) approved in the treatment of alcohol dependence and for inhibiting the effects of opioids. Low-dose naltrexone is sometimes used to help alleviate the symptoms of patients with chronic conditions, including fibromyalgia [1], Crohn’s disease [5-6], and multiple sclerosis [7]. The use of LDN at this low dose and for these indications is considered “off-label” use. In other words, it has not undergone the rigorous testing needed to get the approval of the FDA. Side effects include but are not limited to vivid dreams (most patients take the medication in the evening, but morning dosing of the medication may help with this issue). Patients may experience a reduction in pain relief from narcotics for at least six to 24 hours after taking low-dose naltrexone. In addition, low-dose naltrexone should not be used in patients who are currently receiving opioid analgesics due to the possibility of acute opioid withdrawal. The medication should be avoided until it is felt that the narcotics are out of the patient’s system. Those patients taking thyroid replacement may require a lower amount of thyroid medication so periodic monitoring is indicated. The elevation of liver enzymes is a potential risk with naltrexone treatment but is not felt to be common with low-dose therapy. Other potential side effects may include but are not limited to gastrointestinal disturbances, such as stomach cramps and diarrhea, agitation, anxiety, flu-like symptoms, and headaches. The drug should be compounded with short-acting fillers, so calcium carbonate should be avoided. The most common starting dose is 0.5 mg daily in the evening and increased weekly up to a target dose of 4.5 mg. The drug can be started at higher doses. The drug should be stopped at a minimum of 24 hours prior to the time narcotics may be needed for pain relief for a scheduled surgical procedure. In my practice, I will ask patients to temporarily discontinue low-dose naltrexone 72 hours in advance of taking narcotics if the patient is new to therapy, to ensure pain relief [8-11].

Conclusions

Based on a Medline review, this is the first peer-reviewed case report of a patient with Sjogren’s Syndrome who was treated with low-dose naltrexone and obtained clinical benefits. As a result of this case, further study is needed to determine if low-dose naltrexone will subsequently prove to be a useful medication for treating Sjogren’s Syndrome.

Additional Information

Disclosures

Human subjects: Consent was obtained by all participants in this study. Conf licts of interest: In compliance with the ICMJE uniform disclosure form, all authors declare the following: Payment/services info: All authors have declared that no financial support was received from any organization for the submitted work. Financial relationships: All authors have declared that they have no financial relationships at present or within the previous three years with any organizations that might have an interest in the submitted work. Other relationships: I prescribe low dose naltrexone to patients in my medical practice.

References

Younger J, Mackey S: Fibromyalgia symptoms are reduced by low-dose naltrexone: a pilot study. Pain Med. 2009, 10:663-672. 10.1111/j.1526-4637.2009.00613.x
Wang D, Sun X, Sadee W: Different effects of opioid antagonists on μ-, δ-, and κ-opioid receptors with and without agonist pretreatment. J Pharmacol Exp Ther. 2007, 321:544-552.10.1124/jpet.106.118810
Younger J, Parkitny L, McLain D: The use of low-dose naltrexone (LDN) as a novel anti-inflammatory treatment for chronic pain. Clin Rheumatol. 2014, 33:451-459. 10.1007/s10067-014-2517-2
Watkins LR, Hutchinson MF, Ledeboer A, Wieseler-Frank J, Milligan ED, Maier SF: Glia as the ‘bad guys”: implications for improving clinical pain control and the clinical utility of opioids. Brain Behav Immun. 2007, 21:131-146. 10.1016/j.bbi.2006.10.011
Smith JP, Stock H, Bigaman S, Mauger D, Rogosnitzky M, Zagon I: Low-dose naltrexone therapy improves active Crohn’s disease. Am J Gastroenterol. 2007, 102:820-828.
Raknes G, Simonsen P, Smabrekke L: The effect of low-dose naltrexone on medication in inflammatory bowel disease: a quasi experimental before-and-after prescription database study. J Crohns Colitis. 2018, 12:677-686.
Gironi M, Martinelli-Boneschi F, Sacerdote P, et al.: A pilot trial of low-dose naltrexone in primary progressive multiple sclerosis. Mult Scler. 2008, 14:1076-1083.10.1177/1352458508095828
Low dose naltrexone. (2018). Accessed: 2018: http://www.lowdosenaltrexone.org/.
LDN Research Trust. (2018). Accessed: 2018: https://www.ldnresearchtrust.org/.
Dickson, Windham, Smith, et al.: The LDN Book . Linda Elsegood (ed): Chelsea Green Publishing, White River Junction, VT; 2016.
Moore E, Wilkinson S: The Promise of Low Dose Naltrexone Therapy. McFarland & Company Inc, Jefferson NC; 2009

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For an overview of Sjogren’s: https://www.hopkinsrheumatology.org/rheumtv/sjogrens-syndrome-disease-overview/ (3 Min Video) Please notice symptoms are quite similar to Lyme/MSIDS.

Sjögren’s Syndrome is an autoimmune disease that is found primarily in women, where inflammation at the salivary and lacrimal glands causes dryness of the eyes and mouth. However, it’s also a systemic disease that affects the entire body, producing joint pain and fatigue, and damaging internal organs. As many as four million Americans suffer from Sjögren’s Syndrome, which often overlaps with other rheumatic diseases making it very common to misdiagnose or overlook. Unfortunately, many patients are not diagnosed on time, which makes it much more difficult to treat. In this video, the Director of the Jerome L. Greene Sjögren’s Syndrome Center, Dr. Alan Baer, discusses the symptoms and problems that many patients with Sjögren’s Syndrome face.

If you search the internet with the words Lyme & Sjogren’s, tons of blogs will pop up with people with both. There isn’t much if any science on the two, however. This is another problem with research in Lyme-land – nobody is studying the effects of Lyme triggering or in conjunction with other syndromes within the body. A big problem.

Excerpt from The Lyme Book: http://www.lymebook.com/beg_signs_symptoms.pdf

Lyme disease can trigger autoimmunity, so some people will present with rheumatoid arthritis, lupus, Sjogren’s, Hashimoto’s thyroiditis or any number of autoimmune diseases. It may not be that these diagnoses are incorrect; it may just be that the Lyme infection has unbalanced the immune system sufficiently to trigger the autoimmune mechanism. Where there is autoimmune disease with sufficient evidence of Lyme disease (either through lab work or clinically), treating the Lyme will often improve, if not eliminate, the autoimmunity.

The key concept to grasp here is that of underlying cause. Western medicine has somehow distanced itself from the quest for discovery of the underlying cause of illness. As is the case with bromyalgia or chronicfatigue syndrome, the diagnosis describes a set of symptoms but does not explain why they occur.

For more: https://madisonarealymesupportgroup.com/2016/12/18/ldn/

https://madisonarealymesupportgroup.com/2018/10/30/ldn-an-overview-of-clinical-applications/

https://madisonarealymesupportgroup.com/2017/06/12/ldn-reduced-pro-inflammatory-cytokines-in-fm-after-eight-weeks/

https://madisonarealymesupportgroup.com/2018/05/18/bullseye-low-dose-naltrexone-lyme-disease-documentary/ Very informative documentary put out by the LDN Research Trust on Lyme/MSIDS. Dr. Horowitz, Dr. Toups, Dr. Schweig, Dr. Windham, Dr. Holtorf, & Dr. Schwarzback, speak on everything from testing, to diet, to inflammation, and how LDN can help Lyme/MSIDS patients.

https://madisonarealymesupportgroup.com/2018/07/16/low-dose-naltrexone-for-lyme-living-with-lyme-podcast/

https://madisonarealymesupportgroup.com/2019/01/16/ldn-cbd/

Category:

Activism, Inflammation, Pain Management, research, Treatment

What Does it Mean to Herx?

https://globallymealliance.org/what-does-it-mean-to-herx/?

MyLymeLife_2-4

by Jennifer Crystal

Sometimes when I’m describing tick-borne illness, I feel like I’m speaking a foreign language.

Most people have heard of Lyme disease—though too many mistakenly call it “Lyme’s” when there is actually no possessive form. I often get blank stares when I use words like babesia, ehrlichia, and bartonella. Another term that confuses people, even those who have been diagnosed with Lyme, is Jarisch-Herxheimer reaction, more commonly referred to as a “Herx”.

A what? Bear with me.

Discovered by dermatologists Adolf Jarisch and Karl Herxheimer in their studies of syphilis—another illness like Lyme whose bacterium is a spirochete, meaning having a spiral shape—a Jarisch-Herxheimer reaction is an adverse response to toxins released by bacteria killed by antibiotics. In the case of Lyme disease, antibiotics sometimes kill spirochetes faster than the body can eliminate them. This means the patient is stuck with a backlog of dead bacteria which takes time to expel. The buildup of this toxic waste can make the patient feel much worse before it makes them feel better; their symptoms increase until their bodies can expel the dead spirochetes.

That’s one explanation of a Herxheimer reaction, but what does it feel like to actually have one?

When I started taking intravenous antibiotics, the first six weeks were awful. I’d expected the medicine to slowly clear up my symptoms the way antibiotics work, for example, on a sinus infection or simple bronchitis. But within a week of beginning treatment, I started feeling worse than I ever had before. My fatigue was as intense as it was when I first took ill. I felt a pulling sensation in my limbs stronger than I’d ever had before. I couldn’t find a comfortable position in bed because of all the the pains in my joints. Usually easy tasks like brushing my hair and washing dishes felt like workouts. My sleep became so heavy that my blood stopped circulating properly, and my limbs felt weighted. I wondered how I could still be alive when my body seemed so lifeless.

“This is great news,” my doctor said, paradoxically. “It means the medicine is working. Stay the course.”

My doctor said I was Herxing, meaning that the antibiotics were doing exactly what they were supposed to do.

“Once your body gets rid of that build up of dead bacteria, you’ll start to feel better.”

You may wonder how the bacteria gets eliminated. Some of it, especially the toxins from the parasitic tick-borne co-infection babesia, is sweated out. I’d wake two or three times a night completely soaked from head to toe, as if I’d just showered. The sweat felt slimy on my body, like a lotion or oil. I often had to change pajamas and sometimes even the sheets of my bed in the middle of the night.

But most dead spirochetes are eliminated as you might imagine: through the stool. I’d sit up in bed and suddenly feel a great urge for the bathroom. Once there, I’d barely get my nightgown raised and underwear down before my bowels exploded. The release came with the rush of diarrhea but the consistency was of foam noodles snaking out of me in long tubes. The toilet filled so quickly that I had to flush before continuing to go. The toilet steamed with hot dung the color of dead, hardened manure. The smell made me gag.

During my most intense Herxes, I ran to the bathroom upwards of ten times a day. I had to make sure to drink lots of electrolyte-enhanced water, to combat the dehydration brought on by night sweats and frequent elimination. I ate bananas to keep up my potassium levels. I spent a lot of time sleeping, or trying to sleep. During these periods my neurological symptoms would also worsen, because dead spirochetes were piling in my central nervous system, which for me meant insomnia or even hallucinatory nightmares.

The span of a Herx differs by patient. It depends on how you respond to treatment. How much bacteria do you have in your body to start with? Moreover, how quickly can your body detox? For me, a Herx could last anywhere from a couple days to a couple weeks. Then, I’d get a reprieve for a week or two, and then the cycle would start all over. Each time, the Herxheimer reaction was a little less intense, but shorter. You might feel like you’re dying when you’re having one, but in fact it’s actually the bacteria that is dying, and that’s really a good thing.

You can’t control how well your body will respond to antibiotics, but you can help the detox process. There are many theories on how to do so. Some Lyme Literate Medical Doctors (LLMDs) use actual detox protocols. What helped me the most was electrolyte- augmented water, decaffeinated green tea, and lemon juice. Talk to your LLMD about how you can best support your body during a detox, so that your Herxes aren’t so bad. And when you do have a Herx and someone asks, “What’s that?” just show them this article.

Opinions expressed by contributors are their own.

Jennifer Crystal is a writer and educator in Boston. She has written a memoir about her journey with chronic tick borne illness, for which she is seeking representation. Contact her at:

lymewarriorjennifercrystal@gmail.com.

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**Comment**

One of the hardest things to understand about this complex disease(es) is that you feel a whole lot worse before you feel better and this can take considerable time. Managing the herx is a challenging job. Many find sauna’s to be of great help. I also found drinking lemon water, green tea, MSM, and taking enzymes helpful. As Dr. Burrascano says, “Now is the time for pristine health habits.”

For more: https://madisonarealymesupportgroup.com/2015/08/15/herxheimer-die-off-reaction-explained/

https://www.lymedisease.org/lymesci-herxing/

https://madisonarealymesupportgroup.com/2019/01/26/lyme-herxheimer-reactions-dr-rawls/

https://madisonarealymesupportgroup.com/2015/12/06/tips-for-newbies/

Enzymes: https://madisonarealymesupportgroup.com/2016/04/22/systemic-enzymes/

https://madisonarealymesupportgroup.com/2018/03/05/how-proteolytic-enzymes-may-help-lyme-msids/

https://madisonarealymesupportgroup.com/2018/10/24/herbs-habits-to-revive-your-gut/

MSM – another detoxifier, gut support, & inflammation & pain reducer: https://madisonarealymesupportgroup.com/2018/03/02/dmso-msm-for-lyme-msids/

Category:

Detoxing, diet and nutrition, Gut Health, Herbs, Inflammation, Lyme, Treatment