Learning how to not be "RASH"! My pemphigus/pemphigoid story-

How skin falls apart: The pathology of autoimmune skin disease is revealed at the nanoscale - UoB study of pemphigoid rashes discovered new details of how autoantibodies destroy healthy cells in skin! 

This information provides new insights into autoimmune mechanisms in general and could help develop and screen treatments for patients suffering from all autoimmune diseases, estimated to affect 5-10 percent of the U.S. population.

The study of pemphigoid rashes is of interest to people like me, who get these types of rashes-here's a pic of me with one-

My Pemphigoid Rash

It hurt, felt like my skin was pulling, then it seeped clear white blood cells.  I could actually smell them!  (Yuk, right?)  It took quite a while to heal completely.  It took about 5 months to completely heal.  It did not leave any discolored skin. I used betamethazone to heal it.  A stronger type of steroid cream &/or a steroid shot right into the rash would have probably healed it faster, but I didn't know that then.  I had this rash Feb 2013. It popped in right after a radiofrequency ablation to my cervical spine for cervical spondylitis & radiculopathy right at the shot site!  Imagine that-Lupus stopping by to say hello just because I had a shot there-(how nice....NOT!  lol)
I've only had one pemphigoid type rash since, and it was a small one.  Since being treated for lupus with Cellcept (mycophenalate) my rashes (discoid, pemphigoid, porphyria, urticaria) have all been minimal.  Much less severe!!!  Of course now I stay in as much as possible, it's the only real way to minimize the rashes.  Don't go out during the day!
Here's some info on Pemphigoid Rashes!

Definition

Pemphigoid is a group of subepidermal, blistering autoimmune diseases that primarily affect the skin, especially the lower abdomen, groin, and flexor surfaces of the extremities. Here, autoantibodies (anti-BPA-2 and anti-BPA-1) are directed against the basal layer of the epidermis and mucosa.
The condition tends to persist for months or years with periods of exacerbation and remission. Localized variants of the condition have been reported, most often limited to the lower extremities and usually affecting women.

Types

There are two predominant types of pemphigoid: mucous membrane pemphigoid (MMP) also called cicatricial pemphigoid, and bullous pemphigoid (BP) (g). Pathogenesis and management are quite different for these conditions. Scar formation in mucous membrane pemphigoid can lead to major disability (g).

Pemphigoid gestationis

Pemphigoid gestationis (PG) is a rare autoimmune bullous dermatosis of pregnancy. The disease was originally named herpes gestationis on the basis of the morphological herpetiform feature of the blisters, but this term is a misnomer because PG is not related to or associated with any active or prior herpes virus infection (h). PG typically manifests during late pregnancy, with an abrupt onset of extremely pruritic urticarial papules and blisters on the abdomen and trunk, but lesions may appear any time during pregnancy, and dramatic flares can occur at or immediately after delivery. PG usually resolves spontaneously within weeks to months after delivery.

Epidemiology

Bullous Pemphigoid:

• BP is the most frequent blistering disease of the skin (and mucosa) affecting typically the elderly (>65 years) (k), but can occur at any age and in any race.
• Overall incidence: ± 7-10 new cases per million inhabitants per year.
• After the age of 70 incidence significantly increases.
• Relative risk for patients > 90 y have a 300-fold higher than those < 60 y.
• Women and men equally afflicted.
• Precipitating factors include trauma, burns, ionizing radiation, ultraviolet light, and certain drugs such as neuroleptics and diuretics, particularly lasix (furosemide), thiazides, and aldosterone antagonists.
• Correlations between BP flare activity and recurrence of underlying cancer suggest such an association in some patients.
• Even without therapy, BP can be self-limited, resolving after a period of many months to years, but is still a serious condition especially in the elderly.
• (j) 1-y survival probability may be as high as 88.96% (standard error 5.21%), with a 95% confidence interval (75.6%, 94.2%) but other analyses have documented 1 year mortalities of as much as 25-30% in moderate to severe pemphigus even on therapy (hh).
• Genetics
  • Genetic predisposition, but not hereditary

Pemphigoid Gestationis:

• Is a condition of pregnancy (childbearing age women).
• In the United States, PG has an estimated prevalence of 1 case in 50,000-60,000 pregnancies.
• No increase in fetal or maternal mortality has been demonstrated, although a greater prevalence of premature and small-for-gestational-age (SGA) babies is associated with PG.
• Patients with PG have a higher relative prevalence of other autoimmune diseases, including Hashimoto thyroiditis, Graves disease, and pernicious anemia.

Histology

The earliest lesion of BP is a blister arising in the lamina lucida, between the basal membrane of keratinocytes and the lamina densa. This is associated with loss of anchoring filaments and hemidesmosomes. Histologically, there is a superficial inflammatory cell infiltrate and a subepidermal blister without necrotic keratinocytes. The infiltrate consists of lymphocytes and histiocytes and is particularly rich in eosinophils. There is no scarring.
Approximately 70% to 80% of patients with active BP have circulating antibodies to one or more basement membrane zone antigens.

• Autoantibodies to BP180 (and BP230).
• BP180 and BP230 are two components of hemidesmosomes, junctional adhesion complexes.
• T cell autoreactive response to BP180 and BP230 regulate autoantibody production (l).
• On direct immunofluorescence, the antibodies are deposited in a thin linear pattern; and on immune electron microscopy, they are present in the lamina lucida. (By contrast, the antibodies to basement membrane zone antigens that are present in cutaneous lupus erythematosus are deposited in a granular pattern).

Clinical Features

Pemphigoid

Bullous Pemphigoid (BP) is subepidermal blistering autoimmune disease primarily affects the skin, especially the lower abdomen, groin, and flexor surfaces of the extremities. Mucous membrane involvement is seen in 10%-40% of patients. The disease tends to persist for months or years with periods of exacerbation and remission.
The spectrum of presentations is extremely broad (l), but typically there is an itchy eruption with widespread blistering, and tense vesicles and bulla (blisters), with clear fluid (can be hemorrhagic) on apparently normal or slightly erythematous skin.
Lesions normally appear on the torso and flexures, particularly on the inner thighs. Blisters can range in size from a few millimeters to several centimeters, and although. pruritic, typically heal without scarring.
Sometimes erosions and crusting is seen. Also itchy bumps (papules) and crusts (plaques) can be seen with an annular or figurate pattern. A characteristic feature is that multiple bullae usually arise from large (palm-sized or larger), irregular, urticarial plaques. (r) Mucosal (oral, ocular, genital) involvement is also sometimes present, but ocular involvement, is rare. (s) BP can be difficult to diagnose in its ‘non-blistering’ stage, when just itchy, red, elevated patches are visible. Erosions are much less common than in pemphigus, and the Nikolsky sign is negative.
BP is characterized by spontaneous remissions followed by flares in disease activity that can persist for years. Even without therapy, BP is often self-limited, resolving after a period of many months to years, but may become very extensive.
Localized variants of the disease have been reported, most often limited to the lower extremities and usually affecting women. One such variant, localized vulvar pemphigoid, reported in girls aged 6 months to 8 years, presents with recurrent vulvar vesicles and ulcerations that do not result in scarring (t)
Bullous pemphigoid is distinguished from other blistering skin diseases, such as linear IgA dermatosis, epidermolysis bullosa acquisita, and cicatricial pemphigoid, by the following 4 clinical items (it can also be distinguished by biopsy and certain immunological tests) (u)

• Absence of atrophic scars;
• Absence of head and neck involvement;
• Relative absence of mucosal involvement.

Mucous membrane pemphigoid

Mucous membrane pemphigoid (MMP) is a chronic autoimmune disorder characterized by blistering lesions that primarily affect the various mucous membranes of the body, but also affects the skin (MMP is now the preferred term for lesions only involving the mucosa) (v). It is also known as Cicatricial Pemphigoid (CP), as it is often scarring.
The mucous membranes of the mouth and eyes are most often affected, but those of the nose, throat, genitalia, and anus may also be affected. The symptoms of MMP vary among affected individuals depending upon the specific site(s) involved and the progression of the disease. Disease onset is usually between 40 and 70 years and oral lesions are seen as the initial manifestation of the disease in about two thirds of the cases. Blistering lesions eventually heal, sometimes with scarring. Progressive scarring may potentially lead to serious complications affecting the eyes and throat.
There is no racial or ethnic predilection although most studies have demonstrated a female to male ratio of approximately 2:1 (w). The diagnosis of MMP is mainly based on history, clinical examination and biopsy of the lesions.

More on Pemphigoid Rashes from the Pemphigus & Pemphigoid Foundation HERE!

MORE HERE from the University of Buffalo-

Pemphigus Erythematosus or AKA lupus discoid rash with weeping

First my rash.  I saw my rheumie and he said something about it being pemphigus.  I thought it was just subacute cutaneous lupus.  (in addition to my SLE)  Btw I am very confused about lupus rashes, lol. 

Here is a pic of the rash and then another pic of it healing five days later.  It itched, it seeped it was in a circle with dark edges.  It hurt and pulled the little hairs on my neck.  I"d wake up with my long hair stuck to my neck.  Really gross stuff.  I had one like this on my chest (left me discolored but not scarred) and one on my face and one on my head.  (see my rashes page).

The various types of pemphigus include pemphigus erythematosus, pemphigoid, pemphigus vegetans, pemphigus vulgaris, and pemphigus foliaceus.

Pemphigus erythematosus, also known as Senear-Usher syndrome, is an overlap syndrome with features of lupus erythematosus (LE) and pemphigus foliaceus. Pemphigus is demonstrated by acantholysis and immunoglobulin deposits in the interkeratinocyte substance (see the image below).
Direct immunofluorescence microscopy performed on epithelial biopsy specimen obtained from a patient with pemphigus vulgaris detects immunoglobulin G deposits at the epithelial cell surfaces. 

 The lupus component of pemphigus erythematosus is demonstrated by circulating antinuclear antibodies (ANA) and sometimes by immunoglobulin and complement deposits at the dermoepidermal junction
For a thorough description and introduction to the possible causes of pemphigus, see the article "Pemphigus: An Acronym for a Disease with Multiple Causes ", published by the International Pemphigus Society.^[1] 

 

Ode to Decompression Surgery

There once was a girl with a whole lot of curl

and feet that just weren't right   

so one day she did scream

to her docs it would seem   

she really just wanted a fight.    

Then one kind ole doc  

looked at his clock  

and said we'll set up a room where we'll serve                

and we'll cut out your bad nerve...   

and take your pain all away.     

In other words my nerve entrapment in my right foot hasn't stopped for FOUR agonizing days and is sucking the life out of me so my neuro and pain doc r trying to get me admitted for surgery.      ........and thats that!                          

Crumbling and Grumbling (my teeth, that is! lol)

Hi guys!  I'm doing good, coming out of the lupus funk I've been in (tired and cranky, lol) but my back teeth on the top are crumbling.  Falling apart and falling out.  I had a gap back there where my filling fell out (was there about 30 yrs or more I guess) and it was getting worse and worse over the last 6 months but now the  tooth next to it is chipping (crumbling) away.  I've never had much trouble with my teeth till now so I'm a little nervous.  At least it's in the back.

Anyone else have problems with their teeth?  Is it from lupus?  I know gums are connective tissue, but I also know not everything is because of lupus (unless it's my fault of course and then I can freely blame lupus, hahahaha)  I know many lupies have problems with teeth and their gums from Sjogren's and dry mouth.  I'll keep posting as I go, time to go see a dentist, YUK!  

Here's some info I found about teeth:

The accumulation of dental plaque and tartar is usually what causes gingivitis, and it's almost always the result of inadequate brushing and flossing.
If poor oral hygiene promotes the overgrowth of bacterial plaque, changes in the composition of the plaque occur. The bacterial balance shifts over to gram negative anaerobic bacteria, which are responsible for inflammatory diseases.

The bacteria also invade the crevices between the gum and tooth (sulcus) and infect the periodontal tissues. These bacteria that form dental plaque and tartar release toxins that stimulate the body's immune system to over produce powerful infection-fighting factors called cytokines.

The immune factors of the body, in their effort to fight the infection, attack the person's own infected cells and periodontal tissues. This way, the supporting tissues of the teeth - gums, connective tissue and alveolar bone - are destroyed.

25% of lupus patients develop Sjogrens Syndrome which is characterized by autoimmune attack on the tear producing lacrimal glands in the eye and the saliva producing glands in the mouth which results in a sensation of dry eyes, sometimes accompanied by a feeling of sand, grit or gravel in the eyes, and dry mouth. The reduction in saliva production is unhealthy and can promote dental decay as saliva has the function normally of cleaning teeth and also provides antibodies which can protect from bacterial damage to teeth and gums. Persons with this condition need excellent dental hygiene, should avoid smoking, receive frequent dental cleaning and checkups and can use sugar free lozenges to promote residual saliva production. There are two prescription medications that can be used, salagen/pilocarpine and evoxax that promote saliva formation.

Lupus and related conditions can cause the gums to recede, making them more vulnerable to infection and potentially exposing the lower parts of teeth which aren"t covered by thick protective enamel. For this reason, lupus patients should take extra care of their gums and, if possible, use an antibacterial mouthwash twice a day. A dentist may be able to cover exposed areas of lower tooth with artificial enamel. A patient in this situation should also avoid sugary fizzy drinks and acidic fruit or drinks which are especially damaging to vulnerable areas of the tooth.