Anthrax natural history, complications and prognosis

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: João André Alves Silva, M.D. [2]

Overview

Natural History

Cutaneous Anthrax

Day 0

  • There is entry of the infecting B. anthracis (usually as spores) through a skin lesion (cut, abrasion, etc.) or (possibly as vegetative forms or vegetative forms and spores) by means of a fly-bite.

Days 2-3

Days 3–4

  • A ring of vesicles develops around the papule. Vesicular fluid may be exuded. Unless the patient was treated, capsulated B. anthracis can be identified in appropriately stained smears of this fluid, and the bacterium can be isolated by culture.
  • Marked edema starts to develop.
  • Unless there is secondary infection, there is no pus and pathognomonically the lesion itself is not painful, although painful lymphadenitis may occur in the regional lymph nodes and a feeling of pressure may result from the edema.
  • The lesion is usually 1–3 cm in diameter and remains round and regular. Occasionally a lesion may be larger and irregularly shaped.[1]

Days 5–7

  • The original papule ulcerates to form the characteristic eschar. Topical swabs will not pick up B. anthracis. Detection in smears or by culture requires lifting the edge of the eschar with tweezers (this gives no pain unless there is secondary infection) and obtaining fluid from underneath. The fluid will probably be sterile if the patient has been treated with an antibiotic.
  • Edema extends some distance from the lesion.
  • Systemic symptoms are low-grade fever, malaise, and headache.
  • If the cutaneous reaction is more severe, especially if located on the face, neck, or chest, clinical symptoms may be more severe with more extensive edema extending from the lesion, toxamia, a change in mental status, high fever, hypotension, regional lymphadenomegaly and the patient unable to eat or drink.
  • Tracheotomy is a life-saving procedure in patients having a cutaneous lesion on the face or neck with an extensive edema leading to compression on the trachea. This clinical manifestation is very dangerous.[1]

Day 10

  • The eschar begins to resolve; resolution takes several weeks and is not hastened by treatment.
  • Clinicians unaware of this suffer from concern that the treatment has been ineffective. A small proportion of untreated cases develop sepsis or meningitis with hyperacute symptoms.

Time to Resolution

  • Time to resolution will depend on the size, location and local severity of the lesion.
  • The initial crust separates several weeks after onset, with subsequent healing by granulation. Sometimes the separation of the crust is delayed and the lesion may become secondarily infected. In this situation, the crust should be excised surgically.
  • Lesions characterized by “malignant edema” can be expected to take months to heal.
  • Very large lesions may require skin grafts, and lesions in locations such as the eyelid may require surgical intervention due to scarring.[1]

Inhalation Anthrax

Initial Phase

  • Symptoms prior to the onset of the final hyperacute phase are nonspecific, and suspicion of anthrax depends on the knowledge of the patient’s history. The mild initial phase of nonspecific symptoms is followed by the sudden development of dyspnea, cyanosis, disorientation with coma, and death.
  • The typical clinical course of this form of the disease is consistent with the lesion development within the mediastinal lymph nodes before the development of bacteraemia. The assault on the lung appears to be two-pronged. In the initial phase, the blockade of the lymphatic vessels develops, in association with symptoms such as a sensation of tightness of the chest. Lymphatic stasis is associated with edema, which may be apparent above the thoracic inlet, and pleural effusion. Histological sections of the lung may reveal bacilli within the lymphatic vessels. In the acute phase, damage associated with septicemia occurs.[1]
  • Lymphatic stasis resulting from the damaged lymph nodes leads to dilatation of pulmonary lymphatics which originate in the pleura and drain towards the hilum, following interlobular septa in association with blood vessels. The stasis manifests as an early onset pleural effusion and peripheral infiltrates, representing thickened bronchovascular bundles, detectable on chest X-ray. These findings mark fully developed initial stage illness.

Acute Phase

  • Ultimately, the bacteria escape from the damaged lymph nodes and invade the blood stream via the thoracic duct. Once the bacteremia and associated toxemia reach a critical level, the severe symptoms characteristic of the acute phase illness are manifest. During the acute phase illness, damage of the lung tissue becomes apparent on X-ray. This damage results from the action of anthrax toxin on the endothelium of the lung’s capillary bed. Primary damage of the lung is not normally a feature of the initial phase illness and primary pulmonary infection is an uncommon presentation.[1]

Ingestion Anthrax

Oropharyngeal anthrax

  • The oral lesion is generally 2–3 cm in diameter and covered with a grey pseudomembrane surrounded by extensive edema.
  • When the lesion is localized on tonsils, the affected tonsil is also intensely edematous and covered with a grey or white pseudomembrane. Tonsil lesions may be ulcerated.
  • The lesion and extensive edema may lead to airway obstruction. In this situation, tracheotomy is frequently required. Even with treatment, mortality can be high.[1]

Gastrointestinal Anthrax

  • The character of the lesion is generally ulcerative, usually multiple and superficial, surrounded by edema. These lesions may bleed, hemorrhage may be massive and fatal, in some cases with stomach infection. Intestinal lesions may also lead to hemorrhage, obstruction, perforation or any combination of these. Some cases are complicated with massive ascites and this leads to shock and death.
  • Pathological examination of intestinal anthrax shows mucosal ulceration with edema, and enlarged and hemorrhagic regional lymph nodes. Necrosis is sometimes present.
  • The infection may also be disseminated, and sepsis with pulmonary or meningeal involvement may result.[1]
  • In these instances, patients will probably not seek medical treatment and, if they do, intestinal anthrax may not be considered in differential diagnosis. In some cases, approximately 24 hours later the symptoms may become severe and include acute diarrhea, nausea, vomiting, and abdominal pain.
  • With progression of the illness, abdominal pain, hematemesis, bloody diarrhea, massive ascites and signs of suggestive acute abdomen (rapid increase in abdominal girth and paroxysms of abdominal pain) appear. Toxemia, sepsis and shock may develop, followed by death.
  • The time from onset of symptoms to death has most frequently varied from 2 to 5 days
  • The incubation period is typically 1 - 6 days, although it may be as long as 10 days
  • There is evidence that not all untreated cases end in toxemia, sepsis and death and that, after the initial symptoms, recovery occurs.

Complications

Cutaneous Anthrax

  • Skin lesions may become scarred. Very large lesions may require skin grafts, and lesions in locations such as the eyelid may require surgical intervention due to scarring.

Gastrointestinal Anthrax=

Complications

Prognosis

The anthrax prognosis will depend on a number of factors, including:

Any form of anthrax is treatable if the diagnosis is made early enough and with the appropriate supportive therapy. The pulmonary anthrax is the one with highest mortality rate (45%).[2] Mortality rate for other forms is 40%[3] for the gastrointestinal type, 28%[4] for the injection type and less than 2% for the cutaneous type.[5]

In the non-cutaneneous forms, a correct early diagnosis is harder to reach, so these are associated with particularly high mortality.

Following recovery, resolution of small- to medium-size cutaneous lesions is generally complete with minimal scarring. With larger lesions, or lesions on mobile areas carring and contractures may require surgical correction to return normal functioning and large cutaneous defects may require skin grafting.

References

  1. 1.0 1.1 1.2 1.3 1.4 1.5 1.6 "Anthrax in Humans and Animals" (PDF).
  2. Barakat LA, Quentzel HL, Jernigan JA, Kirschke DL, Griffith K, Spear SM; et al. (2002). "Fatal inhalational anthrax in a 94-year-old Connecticut woman". JAMA. 287 (7): 863–8. PMID 11851578.
  3. Beatty ME, Ashford DA, Griffin PM, Tauxe RV, Sobel J (2003). "Gastrointestinal anthrax: review of the literature". Arch Intern Med. 163 (20): 2527–31. doi:10.1001/archinte.163.20.2527. PMID 14609791.
  4. "An Outbreak of Anthrax Among Drug Users in Scotland, December 2009 to December 2010" (PDF).
  5. "Centers for Disease Control and Prevention Expert Panel Meetings on Prevention and Treatment of Anthrax in Adults".