Porphyria
Porphyria
Porphyria
Porphyrias are a group of inherited or acquired disorders of certain enzymes in the heme
biosynthetic pathway (also called porphyrin pathway). They are broadly classified as acute
(hepatic) porphyrias and cutaneous (erythropoietic) porphyrias, based on the site of the
overproduction and accumulation of the porphyrins (or their chemical precursors). They manifest
with either neurological complications or skin problems (or occasionally both). A clinically
induced and histologically identical condition is called pseudoporphyria. Pseudoporphyria is
characterized by normal serum and urine porphyrin levels.
The term derives from the Greek πορφύρα, porphyra, meaning "purple pigment". The name is
likely to have been a reference to the purple discolouration of feces and urine in patients during
an attack.[1] Although original descriptions are attributed to Hippocrates, the disease was first
explained biochemically by Dr Felix Hoppe-Seyler in 1874,[2] and acute porphyrias were
described by the Dutch physician Prof B.J. Stokvis in 1889.[1][3]
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The acute, or hepatic, porphyrias primarily affect the nervous system, resulting in abdominal
pain, vomiting, acute neuropathy, muscle weakness, seizures, and mental disturbances, including
hallucinations, depression, anxiety, and paranoia. Cardiac arrhythmias and tachycardia (fast heart
rate) may develop as the autonomic nervous system is affected. Pain can be severe and can, in
some cases, be both acute and chronic in nature. Constipation is frequently present, as the
nervous system of the gut is affected, but diarrhea can also occur.
Given the many presentations and the relatively uncommon occurrence of porphyria, the patient
may initially be suspected to have other, unrelated conditions. For instance, the polyneuropathy
of acute porphyria may be mistaken for Guillain-Barré syndrome, and porphyria testing is
commonly recommended in those scenarios.[4] Systemic lupus erythematosus features
photosensitivity and pain attacks and shares various other symptoms with porphyria.[5]
Not all porphyrias are genetic, and patients with liver disease who develop porphyria as a result
of liver dysfunction may exhibit other signs of their condition, such as jaundice.
Patients with acute porphyria (AIP, HCP, VP) are at increased risk over their life for
hepatocellular carcinoma (primary liver cancer) and may require monitoring. Other typical risk
factors for liver cancer need not be present.
The cutaneous, or erythropoietic, porphyrias primarily affect the skin, causing photosensitivity
(photodermatitis), blisters, necrosis of the skin and gums, itching, and swelling, and increased
hair growth on areas such as the forehead. Often there is no abdominal pain, distinguishing it
from other porphyrias.
In some forms of porphyria, accumulated heme precursors excreted in the urine may cause
various changes in color, after exposure to sunlight, to a dark reddish or dark brown color. Even
a purple hue or red urine may be seen.
[edit] Diagnosis
[edit] Porphyrin studies
Porphyria is diagnosed through spectroscopy and biochemical analysis of blood, urine, and stool.
[6]
In general, urine estimation of porphobilinogen (PBG) is the first step if acute porphyria is
suspected. As a result of feedback, the decreased production of heme leads to increased
production of precursors, PBG being one of the first substances in the porphyrin synthesis
pathway.[7] In nearly all cases of acute porphyria syndromes, urinary PBG is markedly elevated
except for the very rare ALA dehydratase deficiency or in patients with symptoms due to
hereditary tyrosinemia type I.[citation needed] In cases of mercury- or arsenic poisoning-induced
porphyria, other changes in porphyrin profiles appear, most notably elevations of uroporphyrins I
& III, coproporphyrins I & III and pre-coproporphyrin.[8]
Repeat testing during an attack and subsequent attacks may be necessary in order to detect a
porphyria, as levels may be normal or near-normal between attacks. The urine screening test has
been known to fail in the initial stages of a severe life threatening attack of acute intermittent
porphyria.[citation needed]
The bulk (up to 90%) of the genetic carriers of the more common, dominantly inherited acute
hepatic porphyrias (acute intermittent porphyria, hereditary coproporphyria, variegate porphyria)
have been noted in DNA tests to be latent for classic symptoms and may require DNA or enzyme
testing. The exception to this may be latent post-puberty genetic carriers of hereditary
coproporphyria.[citation needed]
As most porphyrias are rare conditions, general hospital labs typically do not have the expertise,
technology or staff time to perform porphyria testing. In general, testing involves sending
samples of blood, stool and urine to a reference laboratory.[6] All samples to detect porphyrins
must be handled properly. Samples should be taken during an acute attack, otherwise a false
negative result may occur. Samples must be protected from light and either refrigerated or
preserved.[6]
If all the porphyrin studies are negative, one has to consider pseudoporphyria. A careful
medication review often will find the inciting cause of pseudoporphyria.
Further diagnostic tests of affected organs may be required, such as nerve conduction studies for
neuropathy or an ultrasound of the liver. Basic biochemical tests may assist in identifying liver
disease, hepatocellular carcinoma, and other organ problems.
[edit] Pathogenesis
In humans, porphyrins are the main precursors of heme, an essential constituent of hemoglobin,
myoglobin, catalase, peroxidase, respiratory and P450 liver cytochromes.
Heme synthesis—note that some reactions occur in the cytoplasm and some in the
mitochondrion (yellow)
Deficiency in the enzymes of the porphyrin pathway leads to insufficient production of heme.
Heme function plays a central role in cellular metabolism. This is not the main problem in the
porphyrias; most heme synthesis enzymes—even dysfunctional enzymes—have enough residual
activity to assist in heme biosynthesis. The principal problem in these deficiencies is the
accumulation of porphyrins, the heme precursors, which are toxic to tissue in high
concentrations. The chemical properties of these intermediates determine the location of
accumulation, whether they induce photosensitivity, and whether the intermediate is excreted (in
the urine or feces).
There are eight enzymes in the heme biosynthetic pathway, four of which—the first one and the
last three—are in the mitochondria, while the other four are in the cytosol. Defects in any of
these can lead to some form of porphyria.
The hepatic porphyrias are characterized by acute neurological attacks (seizures, psychosis,
extreme back and abdominal pain and an acute polyneuropathy), while the erythropoietic forms
present with skin problems, usually a light-sensitive blistering rash and increased hair growth.
Variegate porphyria (also porphyria variegata or mixed porphyria), which results from a partial
deficiency in PROTO oxidase, manifests itself with skin lesions similar to those of porphyria
cutanea tarda combined with acute neurologic attacks. All other porphyrias are either skin- or
nerve-predominant.
[edit] Subtypes
X-linked
δ-aminolevulinate
Mitochondrion sideroblastic Erythropoietic X-linked
(ALA) synthase
anemia (XLSA)
Doss
δ-aminolevulinate porphyria/ALA Autosomal Abdominal pain,
Cytosol Hepatic
(ALA) dehydratase dehydratase recessive [9] neuropathy[9]
deficiency
Severe
photosensitivity
with erythema,
Congenital
uroporphyrinogen Autosomal swelling and
Cytosol erythropoietic Erythropoietic
(URO) synthase recessive [9] blistering.
porphyria (CEP)
Hemolytic
anemia,
splenomegaly[9]
Photosensitivity,
Hereditary
coproporphyrinogen Autosomal neurologic
Mitochondrion coproporphyria Hepatic
(COPRO) oxidase dominant [9] symptoms,
(HCP)
colic[9]
Photosensitivity,
neurologic
protoporphyrinogen Variegate Autosomal
Mitochondrion Mixed symptoms,
(PROTO) oxidase porphyria (VP) dominant [9]
developmental
delay
Photosensitivity
with skin
Erythropoietic
Autosomal lesions.
Ferrochelatase Mitochondrion protoporphyria Erythropoietic
dominant [9] Gallstones, mild
(EPP)
liver
dysfunction[9]
Transient
Purpuric skin
erythroporphyri
lesions[10]:526
a of infancy
[edit] Treatment
[edit] Acute porphyria
Often, empirical treatment is required if the diagnostic suspicion of a porphyria is high since
acute attacks can be fatal. A high-carbohydrate diet is typically recommended; in severe attacks,
a glucose 10% infusion is commenced, which may aid in recovery.
Hematin and haem arginate are the drugs of choice in acute porphyria, in the United States and
the United Kingdom, respectively. These drugs need to be given very early in an attack to be
effective; effectiveness varies amongst individuals. They are not curative drugs but can shorten
attacks and reduce the intensity of an attack. Side effects are rare but can be serious. These
heme-like substances theoretically inhibit ALA synthase and hence the accumulation of toxic
precursors. In the United Kingdom, supplies of this drug are maintained at two national centers.
In the United States, one company manufactures Panhematin for infusion.
Haem Arginate (NormoSang) is used during crises but also in preventive treatment to avoid
crises, one treatment every 10 days
Any sign of low blood sodium (hyponatremia) or weakness should be treated with the addition of
hematin or heme arginate or even Tin Mesoporphyrin as these are signs of impending syndrome
of inappropriate antidiuretic hormone (SIADH) or peripheral nervous system involvement that
may be localized or severe progressing to bulbar paresis and respiratory paralysis.[citation needed]
Precipitating factors
If drugs or hormones have caused the attack, discontinuing the offending substances is essential.
Infection is one of the top causes of attacks and requires vigorous treatment.
Symptom control
Pain is severe, frequently out of proportion to physical signs and often requires the use of opiates
to reduce it to tolerable levels. Pain should be treated early as medically possible due to its
severity. Nausea can be severe; it may respond to phenothiazine drugs but is sometimes
intractable. Hot water baths/showers may lessen nausea temporarily, though caution should be
used to avoid burns or falls.
Early identification
Patients with a history of acute porphyria and even genetic carriers are recommended to wear an
alert bracelet or other identification at all times in case they develop severe symptoms or in case
of accidents where there is a potential for drug exposure, as a result of which they are unable to
explain to healthcare professionals about their condition and the fact that some drugs are
absolutely contraindicated.
Neurologic and psychiatric issues
Patients who experience frequent attacks can develop chronic neuropathic pain in extremities as
well as chronic pain in the gut. Gut dysmotility, ileus, intussusception, hypoganglionosis,
encopresis in children and intestinal pseudo-obstruction have been associated with porphyrias.
This is thought to be due to axonal nerve deterioration in affected areas of the nervous system
and vagal nerve dysfunction.
In these cases treatment with long-acting opioids may be indicated. Some cases of chronic pain
can be difficult to manage and may require treatment using multiple modalities. Opioid
dependence may develop.
Depression often accompanies the disease and is best dealt with by treating the offending
symptoms and if needed the judicious use of anti-depressants. Some psychotropic drugs are
porphyrinogenic, limiting the pharmacotherapeutic scope.
Seizures
Seizures often accompany this disease. Most seizure medications exacerbate this condition.
Treatment can be problematic: barbiturates especially must be avoided. Some benzodiazepines
are safe and, when used in conjunction with newer anti-seizure medications such as gabapentin,
offer a possible regime for seizure control.
Magnesium sulfate and bromides have also been used in porphyria seizures, however,
development of status epilepticus in porphyria may not respond to magnesium alone. The
addition of hematin or heme arginate has been used during status epilepticus.[citation needed]
Some liver diseases may cause porphyria even in the absence of genetic predisposition. These
include hemochromatosis and hepatitis C. Treatment of iron overload may be required.
Hormone treatment
Hormonal fluctuations that contribute to cyclical attacks in women have been treated with oral
contraceptives and luteinizing hormones to shut down menstrual cycles. However, oral
contraceptives have also triggered photosensitivity and withdrawal of oral contraceptives has
triggered attacks. Androgens and fertility hormones have also triggered attacks.
These are associated with accumulation of porphyrins in erythrocytes and are rare. The rarest is
Congenital erythropoetic porphyria (C.E.P) otherwise known as Gunther's disease. The signs
may present from birth and include severe photosensitivity, brown teeth that fluoresce in
ultraviolet light due to deposition of type one porphyrins and later hypertrichosis. Haemolytic
anaemia usually develops. Pharmaceutical-grade beta carotene may be used in its treatment.[11] A
bone marrow transplant has also been successful in curing CEP in a few cases, although long
term results are not yet available.[12]
The pain, burning, swelling and itching that occur in erythropoietic porphyrias generally require
avoidance of bright sunlight. Most kinds of sunscreen are not effective, but SPF-rated long-
sleeve shirts, hats, bandanas and gloves can help. Chloroquine may be used to increase porphyrin
secretion in some EPs.[6] Blood transfusion is occasionally used to suppress innate heme
production.
The links between porphyrias and mental illness have been noted for decades. In the early 1950s
patients with porphyrias (occasionally referred to as "Porphyric Hemophilia"[13]) and severe
symptoms of depression or catatonia were treated with electroshock.
Porphyria has been suggested as an explanation for the origin of vampire and werewolf legends,
based upon certain perceived similarities between the condition and the folklore.
In January 1964, L. Illis' 1963 paper, "On Porphyria and the Aetiology of Werwolves", was
published in Proceedings of the Royal Society of Medicine. Later, Nancy Garden argued for a
connection between porphyria and the vampire belief in her 1973 book, Vampires. In 1985,
biochemist David Dolphin's paper for the American Association for the Advancement of
Science, "Porphyria, Vampires, and Werewolves: The Aetiology of European Metamorphosis
Legends", gained widespread media coverage, thus popularizing the connection.
The theory has since faced heavy criticism, especially for the stigma it has placed on its
sufferers. Norine Dresser's American Vampires: Fans, Victims, Practitioners (1989) treats the
matter with more depth.
The theory also operates on a highly-flawed premise, mainly in regard to a perceived harmful
effect sunlight had on vampires. But this is a much more recent innovation in vampire lore: its
origin is from 1922, with the release of vampire movie, Nosferatu, eine Symphonie des Grauens.
[citation needed]
There are about eight different types of porphyria, four of these types of porphyria can
sometimes cause sensitivity to light: Erythropoietic Protoporphyria (EPP) or Protoporphyria,
Congenital Erythropoietic Porphyria (C.E.P.), Porphyria Cutanea Tarda (PCT) and Variegate
Porphyria.
[edit] Notable cases
The insanity exhibited by King George III evidenced in the regency crisis of 1788 has inspired
several attempts at retrospective diagnosis. The first, written in 1855, thirty-five years after his
death, concluded he suffered from acute mania. M. Guttmacher, in 1941, suggested manic-
depressive psychosis as a more likely diagnosis. The first suggestion that a physical illness was
the cause of King George's mental derangements came in 1966, in a paper "The Insanity of King
George III: A Classic Case of Porphyria",[14] with a follow-up in 1968, "Porphyria in the Royal
Houses of Stuart, Hanover and Prussia".[15] The papers, by a mother/son psychiatrist team, were
written as though the case for porphyria had been proven, but the response demonstrated that
many, including those more intimately familiar with actual manifestations of porphyria, were
unconvinced. Many psychiatrists disagreed with Hunter's diagnosis, suggesting bipolar disorder
as far more probable. The theory is treated in Purple Secret,[16] which documents the ultimately
unsuccessful search for genetic evidence of porphyria in the remains of royals suspected to suffer
from it.[17] In 2005 it was suggested that arsenic (which is known to be porphyrogenic) given to
George III with antimony may have caused his porphyria.[18] Despite the lack of direct evidence,
the notion that George III (and other members of the royal family) suffered from porphyria has
achieved such popularity that many forget that it is merely a hypothesis. In 2010 an exhaustive
analysis of historical records revealed that the porphyria claim was based on spurious and
selective interpretation of contemporary medical and historical sources.[19]
The insanity of George III is the basis of the plot in The Madness of King George, a 1994 British
film based upon the 1991 Alan Bennett play, The Madness of George III. The closing credits of
the film include the comment that the illness suffered by King George has been attributed to
porphyria and that it is hereditary. Among other descendants of George III theorised by the
authors of Purple Secret to suffering from porphyria (based upon analysis of their extensive and
detailed medical correspondence) were his great-great-granddaughter Princess Charlotte of
Prussia (Kaiser Wilhelm II's eldest sister) and her daughter Princess Feodora of Saxe-Meiningen.
They had more success in being able to uncover reliable evidence that George III's great-great-
great-grandson Prince William of Gloucester was reliably diagnosed with variegate porphyria.
It is believed that Mary Stuart, Queen of Scots – King George III's great-great-great-great-great-
grandmother – also suffered from acute intermittent porphyria, although this is subject to much
debate. It is assumed she inherited the disorder, if indeed she had it, from her father, James V of
Scotland; both father and daughter endured well-documented attacks that some believe fall
within the constellation of symptoms of porphyria.
Vlad III the Impaler was also said to had suffered from Acute Porphyria, which may have started
the notion that Vampires were, "allergic to the light of day."[citation needed]
Other commentators have suggested that Vincent van Gogh may have suffered from acute
intermittent porphyria.[20] It has also been imagined that King Nebuchadnezzar of Babylon
suffered from some form of porphyria (cf. Daniel 4).[21] However, the symptoms of the various
porphyrias are so extensive that a wide constellation of symptoms can be attributed to one or
more of them.[citation needed]
The poet Robert Browning, also, notoriously wrote a poem called "Porphyria's Lover", which
aside from a literal interpretation of the word also compares love itself to a form of disorder.
Paula Frías Allende, the daughter of the Chilean novelist Isabel Allende, fell into a porphyria-
induced coma in 1991 which inspired Isabel Allende to write the autobiographical book Paula,
dedicated to her daughter.
Julia Gnuse, regarded as the most tattooed woman in the world, got hers to hide scars from
porphyria cutanea tarda (PCT).