TUBERCOLOSI DIAGNOSI E TERAPIA.pdf

Transcript

Anais Brasileiros de Dermatologia 2022;97(2):129---144

Anais Brasileiros de
Dermatologia
www.anaisdedermatologia.org.br

CONTINUING MEDICAL EDUCATION

Cutaneous tuberculosis: epidemiological, clinical,
diagnostic and therapeutic update!
Arival Cardoso de Brito ∗ , Clivia Maria Moraes de Oliveira ,
Deborah Aben-Athar Unger , Maraya de Jesus Semblano Bittencourt
A Exogenous cutaneous tuberculosis
Tuberculous chancre and Tuberculosis verrucosa cutis

Dermatology Service, Universidade Federal do Pará, Belém, PA, Brazil B. Endogenous cutaneous tuberculosis
a) Bycontiguityorautoinoculation(Scrofuloderma,ori-
ficial tuberculosis and some cases of lupus vulgaris)
b) By hematogenic dissemination (Lupus vulgaris,
Received 20 April 2021; accepted 26 July 2021 tuberculous gumma and acute miliary tuberculosis)
Available online 4 January 2022 C. Tuberculids
- Papulonecrotic tuberculid
- Lichen scrofulosorum

D. Cutaneous tuberculosis secondary to BCG vaccination
Abstract Tuberculosis is certainly one of the diseases considered to be ancient on planet
KEYWORDS Earth. The etiological agent of tuberculosis is Mycobacterium tuberculosis. This terrible bac-
Epidemiology; terial infection still results in severe socioeconomic consequences to date, and its complete
Mycobacterium eradication represents a great challenge. It constitutes one of the most important public health
tuberculosis; problems in developing countries. According to the World Health Organization, this infection
Pathogenesis, results in more than 4,000 deaths daily worldwide, with 10.4 million being affected annually
homeopathic; and 1.5 million deaths from TB every year. With the emergence of the HIV/AIDS pandemic,
Tuberculosis; the disease became the main cause of morbidity and mortality in patients infected with the
Tuberculosis, human immunodeficiency virus. Cutaneous tuberculosis is a rare infection that represents 1% to
cutaneous 1.5% of extrapulmonary tuberculosis, whose etiological agents are Mycobacterium tuberculosis,
Mycobacterium bovis, and the attenuated form of the bacillus Calmette-Guérin (BCG vaccine).
Cutaneous tuberculosis can be exogenous; endogenous: caused by contiguity or autoinocula-
tion and by hematogenous spread; induced by the Calmette-Guérin bacillus and manifest as
a tuberculid. The diagnosis of the infection is carried out through the direct test, culture,
histopathology, tuberculin skin test, polymerase chain reaction, interferon-gamma release
assay, and genotyping. Drugs used comprise isoniazid, rifampicin, pyrazinamide and ethambutol.
© 2021 Sociedade Brasileira de Dermatologia. Published by Elsevier España, S.L.U. This is an
open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).

Introduction

Tuberculosis (TB) is an ancient, cosmopolitan infectious dis-
ease caused by Mycobacterium tuberculosis that occurs with
greater incidence in developing countries, constituting one
! Study conducted at the Dermatology Service, Universidade Fe- of the most serious public health problems, a constant threat
deral do Pará, Belém, PA, Brazil. to health, which incapacitates and causes the death of a
∗ Corresponding author. large number of people. TB is considered by the World
E-mail: [email protected] (A.C. Brito). Health Organization (WHO) as a worldwide disease with

https://doi.org/10.1016/j.abd.2021.07.004
0365-0596/© 2021 Sociedade Brasileira de Dermatologia. Published by Elsevier España, S.L.U. This is an open access article under the CC
BY license (http://creativecommons.org/licenses/by/4.0/).
 A.C. Brito, C.M. Oliveira, D.A. Unger et al.

more than 4,000 deaths daily, 10.4 million infected indi- Etiology and pathogenesis
viduals annually, and 1.5 million deaths from this infection
every year. With the emergence of the HIV/AIDS pandemic, Mycobacterium tuberculosis was identified and isolated by
the disease is the leading cause of morbidity and mortal- Robert Koch in 1882. It is an obligate intracellular, aero-
ity in patients infected with the Human Immunodeficiency bic, straight or slightly curved, immobile, non-sporulating
Virus (HIV).1---3 In 2018, 484,000 cases of rifampicin-resistant pathogen, measuring 1 to 10 !m long and 0.2 to 0.6 !m wide,
tuberculosis were registered worldwide, of which 78% were an acid-fast bacillus (AFB), with the ability to survive and
multidrug-resistant TB (MDR-TB).1---8 multiply inside macrophages. Its genome consists of approx-
China, India and Indonesia account for 45% of TB cases imately 4,000 genes, of which about 200 are responsible for
worldwide.1,2,9 Regarding the Southeast Asia and regions of encoding enzymes for fatty-acid metabolism, and another
Africa, its mortality rate represents 85% of all deaths due to 170 encode families of proteins related to antigenicity, some
tuberculosis.1,2,9---11 related to the metabolism of the bacillus and constituents
In 2018, the disease caused 4,490 deaths in Brazil. In of the cell wall --- lipids, proteins, carbohydrates --- however,
2019, 73,864 new cases of TB were registered in Brazil --- most genes play an important role in the invasion of the
an incidence of 35.0 cases/100,000 inhabitants. In Brazil, immune system.10,11,13,17,18 The high concentration of lipids
an enormous increase in new cases of TB-HIV coinfection on the cell wall is responsible for the resistance/survival of
was detected between 2010 and 2018.3---5 The risk of acquir- the microorganism; nevertheless, it shows sensitivity to heat
ing TB depends on the coexistence of conditioning factors and ultraviolet radiation.9---11,18
such as genetic factors, age, sex, malnutrition, alcoholism, Tuberculosis research has played an important role in the
smoking status, environmental factors, the immune system birth of immunology field of studies; however, the relation-
status of each individual --- the increased use of immunosup- ship between the two has been ambivalent from the start.19
pressive drugs for the treatment of autoimmune diseases, Chen et al. propose that: ‘‘proteins are the most impor-
neoplasms, transplant recipients --- development of MDR-TB, tant antigens of M. tuberculosis and can induce T-cell
HIV infection, previous pulmonary disease, in addition to immune responses and other allergic reactions, includ-
other comorbidities.1---10 ing late-onset hyperreactive cell immune responses. The
Studies have reported that the immunosuppressive condi- caseous necrosis that occurs in the disease is induced by
tion, determined by HIV/AIDS infection, predisposes to the lipoids.’’9
contagion and illness of afected individuals. The chance that The T-cell immune response act in the host defense
infection with the bacillus will develop into tuberculosis in mechanism against bacteria, dendritic cells, activated
immunocompetent individuals is 10% over one’s lifetime, macrophages, which phagocytose and destroy the mycobac-
whereas it may reach 10% each year in those infected with terium, for antigen presentation to lymphocytes, in which a
HIV.12 series of biological events are processed, highlighting the
Extrapulmonary TB represents 20% of the cases of the important protective function of CD4+ and CD8+ T lym-
disease, which includes pleural TB, osteoarticular TB, phocytes, which secrete cytokines to eliminate the bacillus
genitourinary TB, ocular TB, abdominal TB, breast TB, tuber- of Koch (BK).9,13,15 According to Sehgal et al.19 one can
culous meningitis, and pericarditis, cutaneous tuberculosis, consider the spectral concept in cutaneous tuberculosis,
among other affected organs.9,11,13,14 based on bacteriological, histopathological and immunolog-
Cutaneous tuberculosis (CTB) is a rare form of mycobac- ical parameters, similarly to what is described in leprosy
teriosis that accounts for 1% to 2% of all forms of and pulmonary tuberculosis. At one end, lupus vulgaris, with
extrapulmonary tuberculosis.9 The main etiological agent active cell immunity and apparently normal immunoglobu-
is Mycobacterium tuberculosis and occasionally Mycobac- lin, and at the other end, scrofuloderma, with less active cell
terium bovis and the bacillus Calmette-Guérin (BCG vaccine, immunity and increased humoral response, evidenced by
an attenuated strain of M. bovis).3,8---11,15 elevated serum levels of immunoglobulins and reduced C3.20
In 1826, Théophile Laënnec (1781---1826), the inventor of T-cells are responsible for the polarization of the dis-
the stethoscope (1819), described the first case of CTB in the ease in the host since they can restrain M. tuberculosis,
world that killed Laënnec himself. Robert Koch (1843---1910) developing the paucibacillary form or, through immunologi-
identified and isolated M. tuberculosis only in 1882.7---9,13 cal suppression, allow the survival of the pathogen, leading
It is important to emphasize that there are infections to the multibacillary form. The Th1 and Th17 pathways
that are not caused by the Mycobacterium tuberculosis are the main effectors involved in the pathogenesis of TB,
complex and by Mycobacterium leprae and Mycobac- mediating protection against the etiological agent. The reg-
terium lepromatosis, but produced by non-tuberculous or ulatory T (Treg) cells subgroup also plays an important role
atypical mycobacteria (NTM), among which the following in the process, as it maintains the cell-mediated immunity
stand out: Mycobacterium avium complex (MAC), Mycobac- effector cells in homeostasis.20---22 The most important com-
terium ulcerans, Mycobacterium marinum, Mycobacterium ponent of the defense against TB through the Th1 pathway
haemophilum, Mycobacterium fortuitum, Mycobacterium is the production of the cytokine IFN-", which activates
chelonae, Mycobacterium kansasii, Mycobacterium absces- macrophages and stimulates phagocytosis, phagosome mat-
sus, Mycobacterium scrofulaceum, Mycobacterium simiae, uration, production of reactive nitrogen intermediates and
Mycobacterium malmoense, Mycobacterium xenopi.7---11,13 antigen presentation. Although IFN-" is one of the most
CTB is prevalent in young adults, particularly women, important cytokines for the protective response against M.
tuberculosis verrucosa cutis predominates in males, and ery- tuberculosis, it is not enough to control the pathogen.23---25
thema induratum of Bazin in females.8---11,16 The Th17 cells produce IL-17, which plays a major protec-

130

IL-17 is mostly associated with induction of proinflammatory programs
TH1 IFNg MACROFAGI FAGOCITOSI associated with chemokine secretion and neutrophil recruitment, early
recruitment of neutrophils to Mtb lungs is associated with early
granuloma formation.In addition, neutrophils and macrophages
cooperate for efficient mycobacterial killin
 Anais Brasileiros de Dermatologia 2022;97(2):129---144

tive role in TB, observed through the survival of neutrophils d) Tuberculids: papulonecrotic tuberculid; lichenoid tuber-
in the early stages of infections, providing control of the culid (lichen scrofulosorum)
bacterial load.26---30 e) Facultative tuberculids: erythema induratum of Bazin -
The suppressive mediation of Treg cells occurs mainly nodular vasculitis.
through the secretion of the immunosuppressive cytokine
TGF-#, which has an anti-inflammatory effect.31---33 In
patients with cutaneous tuberculosis, Treg cells produce a Tuberculous chancre
significant amount of TGF-#, which plays an important role
in CD4+, CD25+ Treg expansion and also inhibits Th17 cell Tuberculous chancre (TC) or primary inoculation tuberculo-
polarization.22 sis results from the direct penetration of M. tuberculosis
The main target of M. tuberculosis in the human species into the skin and/or mucous membranes through trauma,
is the lungs; however, all organs and systems of the host wounds, preexisting dermatosis, surgical procedures with
can be infected by the microorganism. Most of the infec- contaminated material in people who do not have innate
tions occur through the airways and 80% of TB clinical forms or adaptive immunity to M tuberculosis. Individuals also
are pulmonary.7---11,15,17 Skin integrity is very effective in acquire the disease through mouth-to-mouth breathing,
preventing BK entry, but solutions of continuity of the muco- circumcision, injections with contaminated hypodermic
cutaneous integument will favor infection of the host by the needles, after tattooing procedures, piercings, at insulin
BK and, therefore, cutaneous and/or mucosal tuberculous application sites. Infection of the oral mucosa by M. bovis
manifestations. 7,8,11,17 can occur by ingestion of unpasteurized milk and by dental
extraction. It is the most common form in children; how-
ever, adolescents and young adults can also be infected in
Clinical manifestations and classification this way.7---11,13,34

The clinical manifestations of CTB polymorphism can be
explained by factors such as the pathogenicity of the bacte- Clinical manifestations
rial strain, the host immune status, previous treatment, or LESIONE ULCERATA+LINFONODALE
local factors, including proximity to lymph nodes.8---11,17 TC manifests two to four weeks after infection as a papule,
The polymorphous lesions of CTB include papules, nod- infiltrated plaque or nodule that develops into an ulcera-
ules, infiltrated plaques, ulcers, gummas, verrucous lesions. tive lesion located more frequently on the face (including
Their differential diagnosis is mandatory with other diseases the conjunctiva), upper limbs (mostly the hands) and lower
of similar clinical expression. This lesion polymorphism has limbs. The ulcer is painless, shallow, with a granular back-
led to the proposition of several complex and controversial ground, an infiltrated base that can reach a few centimeters
classifications. in diameter, and is difficult to heal. After two to eight
The bacterial load is the basis for a proposed classifica- weeks, lymphangitis and regional lymph node disease ensue,
tion for the disease, which is analogous to the Ridley and constituting the primary tuberculous complex in the skin,
Jopling classification for leprosy and includes: similar to the Ghon complex of the lung.7 The lymph nodes
may liquefy, ulcerate and eliminate necrotic/necropurulent
a) The multibacillary form --- low immunity to BK, including material. Paronychia resulting from infection of the fingers
tuberculous chancre, tuberculosis orificialis, scrofulo- by the bacillus is not so rare.7
derma, acute miliary tuberculosis, and tuberculous
gumma. Histopathology
b) The paucibacillary form --- high immunity to M. tubercu-
losis, including verrucous tuberculosis, lupus vulgaris and An acute inflammatory infiltrate of neutrophils can be seen
tuberculids. at the beginning of the infectious process, followed a few
weeks later by granuloma organization, associated with
The classification for TB based on more robust criteria caseous necrosis and the presence of numerous acid fast
--- pathogenesis, anatomopathological analysis, immune sys- bacilli (AFB), demonstrated by Fite-Faraco or Ziehl-Neelsen
tem, clinical picture --- accepted worldwide by those who stains.
study mycobacteriosis will be adopted in this work:7---9,11,16,17

a) Exogenous cutaneous tuberculosis: tuberculous chancre
Diagnosis
and tuberculosis verrucosa cutis.
b) Endogenous cutaneous tuberculosis: Laboratory confirmation of the etiological agent by direct
screening and culture for AFB, PPD (purified protein deriva-
tive), histopathological analysis, interferon-gamma release
Contiguity or self-inoculation (scrofuloderma, tuberculo-
assay (IGRA) and polymerase chain reaction (PCR) for BK.
sis orificialis and some cases of lupus vulgaris);
Hematogenous spread (lupus vulgaris, gummatous tuber-
culosis and acute miliary tuberculosis). Differential diagnosis

c) Cutaneous tuberculosis caused by bacillus of Calmette- It must be established with NTM, syphilis, bartonellosis,
Guerin (BCG vaccine); post-vaccination lupus vulgaris. sporotrichosis, and leishmaniasis.

131

LA BASE DELL’ULCERA, CHE E’ INDOLORE, SI
INFILTRA SEMPRE PIU’ E QUINDI L’ULCERA
DIVENTA DURA. LA LINFOADENOPATIA PUO’
ANDARE INCONTRO A FISTOLIZZAZIONE
 A.C. Brito, C.M. Oliveira, D.A. Unger et al.

PLACCA IPERKERATOSICA
ESTENS.CENTRIFUGA
FOCI DI SECREZ.PURULENTA

Figure 1 (A), Tuberculosis verrucosa cutis (TVC): verrucous plaque with centrifugal expansion on the left arm. (B), TVC: epidermis
with focal hyperplasia and dermis showing granulomatous inflammation involving follicular structures and vessels, (Hematoxylin &
eosin, ×40).

Tuberculosis verrucosa cutis cosis, Tuberculosis (other forms), NTM, verrucous lesions,
carcinoma, keratoacanthoma, bromoderma, iododerma,
Tuberculosis verrucosa cutis results from the exogenous hypertrophic lichen planus.
inoculation in individuals previously infected with BK, with
high immunity to the microorganism. It is the most common
paucibacillary variant in healthcare professionals --- physi- Scrofuloderma
cians, pathologists, veterinarians, biomedical technicians,
nurses, autopsy technicians --- in farmers, butchers and is Scrofuloderma or tuberculosis cutis colliquative is the most
unusual in people with other activities (Fig. 1A).7---11 frequent form of TB in developing countries, being prevalent
in children and young adults, but it also affects the elderly.
Clinical manifestations Depending on the host’s immune system and other condition-
ing factors, it can affect the host in both the multibacillary
Initially, the lesion is a papule/papulo-pustule with an ery- and paucibacillary clinical forms.
thematous halo or a nodule with hyperkeratosis on the
surface, developing into a verrucous plaque with centrifugal
growth, sharp edges, and the presence of purulent secretion Clinical manifestations
foci. The lesion is usually single, preferably located on the
hands, but other areas of the skin may be involved, such as M. tuberculosis infection develops in lymph nodes, bones,
the lower limbs, particularly in children.7,8,13,16,17 This lesion joints, as tuberculous epididymitis, or orchiepididymitis,
eventually progresses to spontaneous healing with atrophic and the overlying skin is affected through contiguity by the
scarring. mycobacteria. The coexistence of pulmonary TB is seen in
most cases of scrofuloderma.7---9,11,16,17
The initial lesion is a subcutaneous nodule --- single or
Histopathology
multiple --- initially firm, which progressively increases in
size. After several weeks, it softens, ruptures, resulting in
Hyperkeratotic pseudoepitheliomatous hyperplasia is
fistulas and ulceration, with the elimination of necrotic or
observed and, a lymphocytic inflammatory infiltrate,
necro-purulent material. They are known as cold abscesses.
neutrophil abscesses in association with epithelioid cell
The cervical, axillary, supraclavicular, and inguinal lymph
granulomas, Langhans-type multinucleated cells, and
node chains are most frequently involved in this form of
caseous necrosis are seen in the dermis. AFB are scarce or
tuberculosis (Figs. 2A and 2B)
difficult to identify (Fig. 1B).

Diagnosis Histopathology

Clinical suspicion is confirmed through bacilloscopy, culture, The epidermis is atrophic or ulcerated, depending on the
IGRA, PPD, PCR, or histopathology. biopsied lesion. The dermis and subcutaneous tissue show
caseous necrosis, surrounded by macrophage granulomas,
Differential diagnosis Langhans-type multinucleated giant cells and a small num-
ber of lymphocytes. AFB are scarce. In most cases, M.
It includes the verrucous syndrome (PLECT) --- (Paracoc- tuberculosis is difficult to demonstrate by special stains
cidioidomycosis, Leishmaniasis, Sporotrichosis, Chromomy- (Fig. 2C).

132 scrofuloderma (tubercolosi cutanea colliquativa)

è il prototipo dell’affezione cutanea per
contiguità, derivante da una tubercolosi
linfonodale, osteoarticolare o più raramente
epididimale
 Anais Brasileiros de Dermatologia 2022;97(2):129---144

Figure 2 (A), Scrofuloderma --- nodules/gummas and ulcerations on the cervical and right mastoid regions associated with lymph
node tuberculosis. (B), Scrofuloderma --- infiltrated and ulcerated lesions on the right clavicular region. (C), Scrofuloderma ---
caseation necrosis surrounded by granulomatous inflammation with a palisade of macrophages and Langhans-type multinucleated
giant cells, (Hematoxylin & eosin, ×40).

Figure 3 (A), Tuberculosis orificialis (tuberculosis cutis orificialis) --- Ulcerovegetating lesion affecting the labia majora and minora.
(B), TB orificialis --- ulcerated epidermis and massive dermal granulomatous inflammatory infiltrate, (Hematoxylin & eosin, ×40).
(C), TB orificialis --- granuloma associated with caseation necrosis, (Hematoxylin & eosin, ×200). Pictures by: Dr. Maraya Bittencourt.

133
 A.C. Brito, C.M. Oliveira, D.A. Unger et al.

Diagnosis Diagnosis

Clinical findings are complemented by laboratory tests: PPD Clinical aspect of the lesions, complementary exams, inves-
(strong reactor), culture in specific media, histopathology, tigation of TB in other organs, especially in the lungs.
IGRA, PCR for BK.
Differential diagnosis
Differential diagnosis
Consider recurrent aphthous stomatitis, syphilis, and other
The following should be considered: paracoccidioidomyco- sexually transmitted infections with a clinical ulcerative
sis, actinomycosis, sporotrichosis, syphilitic gumma, NTM, characteristic, deep mycoses, and malignant neoplasms,
hidradenitis suppurativa. especially squamous cell carcinoma.35

Tuberculosis orificalis Lupus vulgaris

Tuberculosis orificalis (TO), also known as acute tuberculous Lupus vulgaris (LV) is a type of endogenous, chronic cuta-
ulcer and ulcerative cutaneous and mucosal tuberculo- neous tuberculosis, caused by contiguity or self-inoculation
sis, results from self-inoculation of M. tuberculosis in the (some cases) and by hematogenous or lymphatic spread, in
mucosa and periorificial skin in individuals with low immu- individuals with high or moderate immunity to M. tuber-
nity and tuberculosis in internal organs --- lungs, urogenital, culosis, who are tuberculin-positive, with paucibacillary
gastrointestinal, in addition to other activity foci. This rare disease, which has a higher prevalence in females than in
form of TB has a higher incidence in the elderly, who males, affecting any age group. The infection occurs from a
usually have an immunological deficiency and non-reactive tuberculosis focus of pulmonary, osteoarticular, lymph node
PPD.7---9,11,16---18,35,36 origin, or from other organs. It can exceptionally develop
Considering the multiple differential diagnoses that gen- after BCG vaccination.11---13,16,18,36
ital ulcers raise with other diseases that manifest with APPLE JELLY
ATROPHIC CENTER
this type of lesion - viral, bacterial, fungal infections, Clinical manifestations ULCERATION
pre-cancerous, neoplastic lesions, and other causes - it is
essential to carefully investigate for an accurate diagnosis.37 LV is manifested by the presence of an erythematous-
Genital tuberculosis occurs more frequently in old, post- brownish papule or nodule with a smooth or keratotic
menopausal women, almost always related to an active surface, a gelatinous consistency that, on diascopy, looks
or reactivated tuberculous focus, with a predominance of like ‘‘apple jelly’’.
lesions in the fallopian tubes, in the endometrium, and The lesion is usually single; however, it can be multiple.
rarely in the vulvovaginal region. However, the develop- Its preferred location is on the face --- nose, malar regions,
ment of a painful ulcer of tuberculous etiology on the left chin, ears --- but other regions can be affected, such as
labia majora in a 14-year-old virgin female is an exceptional the cervical area, upper and lower limbs. The initial lesion
report in the literature.37 The record is a warning to include progresses to a plaque with centrifugal expansion, with an
TO among the proposed diagnoses, even when it appears in atrophic center that can ulcerate (Figs. 4A and 4B).
adolescents who have not yet started sexual activity. Published case reports with different types of LV lesions
have resulted in variants, as follows: psoriasiform, eczema-
Clinical manifestations tous, annular, ulcerative, vegetating, hypertrophic, and
scarring plaques.9,38 the ulcerative and vegetating muti-
The sites most often affected by mycobacterioses are lating variants cause severe deformities in the affected
the oral cavity, external genitalia, Fallopian tubes, sites.7---9,13,17
endometrium, anal/perianal regions (Fig. 3A). The mucosa can be compromised by direct inoculation
Oral cavity lesions can extend contiguously to the phar- of m. tuberculosis or from the expansion of a skin lesion.
ynx and larynx in the form of very painful ulcerations. The Malignant degeneration --- squamous cell carcinoma, sarco-
disease starts as a yellowish erythematous papule or nodule, mas, Hodgkin’s lymphoma --- has been reported in patients
progressing to painful ulceration with irregular edges, infil- with long-term LV.7,35,39
trated base, with no tendency to scarring, causing marked The disease has a chronic course and, if left untreated,
oropharyngeal dysphagia. will cause deformities due to the destruction of structures
in the affected anatomical sites. Spontaneous healing of LV
Histopathology is very difficult, but can occur after several years, leaving
an atrophic or deforming scar.
Ulceration of the lining epithelium and dermis and granu-
lomas with caseation necrosis ---- there are numerous AFB, Histopathology
demonstrated by special stains (Figs. 3B and 3C).
The epidermis may present with atrophy, acanthosis, pseu-
doepitheliomatous hyperplasia, or ulceration. In the dermis,

134

lesione rilevata e molle, giallastra o rossastra, chiamata lupoma, che evolve lentamente in una placca rosso
violacea, a bordi irregolari e policiclici, a superficie cheratosica, che può raggiungere dimensioni notevoli, con
graduale infossamento e cicatrizzazione della zona centrale e progressiva espansione dei margini. Alla
vitropressione si osserva una colorazione giallastra (“a marmellata di mele”) alla periferia della lesione.
L’estensione agli orifizi è responsabile di mutilazioni, atresie ed ectropion. In assenza di trattamento, l’evoluzione è
lenta e mal definita. La lesione può essere complicata tardivamente da un carcinoma spinocellulare.
 Anais Brasileiros de Dermatologia 2022;97(2):129---144

Figure 4 (A), Lupus vulgaris --- infiltrated, eroded lesion, with sharp edges, in the right masseteric region. (B), Lupus vulgaris
--- extensive plaque covered with papules/nodules, scarring areas, with sharp raised edges on the right gluteal region. (C), Lupus
vulgaris --- the dermis shows granulomatous inflammation with foci of caseous necrosis, (Hematoxylin & eosin, ×40).

Figure 5 (A), Gummatous TB --- irregular ulcer with sharp edges on the cervical region. (B), Gummatous TB --- granuloma consisting
of lymphocytes, macrophages and multinucleated giant cells, (Hematoxylin & eosin, ×100).

tuberculoid granulomas containing Langhans-type multin- Differential diagnosis
ucleated giant cells and surrounded by lymphocytes can
be observed. Caseation necrosis is minor and sometimes The following should be included: lupus erythematosus,
absent. AFB is difficult to identify or absent (Fig. 4C). sarcoidosis, cutaneous pseudolymphoma, leishmaniasis, lep-
rosy, tertiary syphilis, paracoccidioidomycosis, and diseases
with similar clinical expression.

Diagnosis
Acute miliary tuberculosis
The diagnosis is carried out through the clinical appearance
and diascopy of skin lesions, strong reactive PPD, culture in Acute miliary tuberculosis or disseminated cutaneous tuber-
specific media, histopathological analysis, IGRA, PCR for M. culosis occurs by hematogenous spread of the active focus
tuberculosis. of BK from visceral tuberculosis, commonly from the lungs.

135
 LA GOMMA E’ IL NODULO CHE SI ULCERA, LO SCRUFULODERMA I NODULI CHE FISTOLIZZANO

A.C. Brito, C.M. Oliveira, D.A. Unger et al.

The higher prevalence is observed in childhood, in patients Histopathology
immunosuppressed by HIV infection, undergoing chemother-
apy, using immunosuppressants for autoimmune disease, and AFB is evidenced in areas of massive caseation necrosis.
in transplant recipients. It represents a rare form of TB, Tuberculous panniculitis cases reveal granulomas with mult-
however, with risk of death for this group of patients. Coin- inucleated giant cells, and AFB are demonstrated by special
fection with HIV in patients with a CD4 cell count < 100/!L staining (Fig. 6B).
has contributed to the increase in the number of cases of
this clinical form of tuberculosis.8---12
Diagnosis

Clinical manifestations PAPULE VESCICOLE CROSTE
The diagnosis is attained through the clinical aspect of the
lesions and laboratory support: bacilloscopy and culture for
The lesions are polymorphic, including papules, vesicles, AFB, anatomopathological analysis, PPD, IGRA, PCR.
pustules, nodules, with preferential distribution in the upper
and lower limbs, and trunk, but they can be disseminated,
usually asymmetric. Whitlow abscesses and ulcerations have Differential diagnosis
been recorded in the literature.7---9
The following should be considered: panniculitis of other
etiologies, NTM, deep mycoses (especially sporotrichosis),
Histopathology syphilis.

The histomorphological picture of the initial lesions shows
areas of necrosis and neutrophilic abscesses. As the lesions Cutaneous tuberculosis after BCG vaccination
progress, the presence of histiocytes and the formation (Bacillus Calmette-Guerin)
of granulomas in the periphery of the infiltrate can be
observed. Numerous AFB can be identified in neutrophilic The BCG vaccine was developed by Albert Léon C. Calmette
abscesses, as well as vascular thrombi. and Jean M. Camille Guérin and used for the first time in
1921. It must be applied after birth until before the age of
five, aiming to protect the individual against tuberculosis
Diagnosis by preventing the primary infection caused by M. tubercu-
losis from progressing, especially into severe forms of the
It is based on the dermatological lesions, general physical disease --- meningoencephalitis and miliary tuberculosis. Vac-
examination, bacilloscopy, culture in specific media, anato- cine protection is low in adults.17,41 The main hypothesis
mopathological analysis, IGRA, PCR, diagnostic imaging. is that BCG induces effector memory T cells that will pro-
tect the individual for 10 to 15 years. Another factor would
be that the protective effect of the vaccine would suffer
Differential diagnosis geographic variation.42
Approximately 12 vaccines against TB are under devel-
The following should be considered: NTM, secondary opment: recombinant BCG (rBCG), Mycobacterium vaccae,
acneiform syphilis, deep mycoses, sarcoidosis, drug reac- protein vaccines with adjuvants, viral vector vaccines, DNA
tions. vaccines, RNA-based vaccines, and others.13,42
Adverse effects occur with any vaccine used in the world,
and the BCG vaccine is no exception. The most frequently
Gummatous tuberculosis detected adverse effects of the BCG vaccine include: sub-
cutaneous cold abscess; suppurated regional lymph node
Gummatous tuberculosis (GT) or metastatic tuberculous disease; ulceration with a diameter > 1 cm; keloid-type
abscesses is a type of CTB caused by the hematoge- scars; Koch’s phenomenon; lupus vulgaris lesions (at or near
nous spread of M. tuberculosis originating from a primary the vaccine site), scrofuloderma, tuberculid-like lesions;
tuberculous focus.7---9,11,13,18 GT has a higher incidence in osteoarthritis. Exceptionally, generalized lesions affecting
immunosuppressed individuals and in children and adoles- other organs have been recorded (Fig. 7).41,42
cents with malnutrition (Figs. 5A and 5B).7---9,17

Tuberculids
Clinical manifestations
Most recent studies do not consider tuberculids as authentic
The initial lesions are firm nodules, progressing to abscesses forms of CTB, but rather a heterogeneous group of clinical
and later ulceration, draining necrotic material, located on entities that result from the host’s hypersensitivity response
the trunk and on the upper and lower limbs. Some lesions to M. tuberculosis. Bacilloscopy is usually negative for AFB
mimic those seen in scrofuloderma. Tuberculous gumma in skin lesions.
with a sporotrichoid appearance has been the subject of The main forms are papulonecrotic tuberculid, lichen
several published studies that emphasize the difficulty in scrofulosorum (lichenoid tuberculid), and erythema indura-
conclusively diagnosing these cases (Fig. 6A).7---11,16,40 tum of Bazin - nodular vasculitis.

136

QUINDI LO SCRUFOLODERMA E’ IL PROTOTIPO DELLA CONTIGUITA’. LA GOMMA LO E’ DELLA DIFFUSIONE
EMATOGENA
 Anais Brasileiros de Dermatologia 2022;97(2):129---144

Figure 6 (A), Sporotrichoid gummatous TB --- ulcerated lesions along the upper limb. (B), Sporotrichoid gummatous TB - numerous
resistant acid-fast bacilli (AFB) in the infiltrate on Fite-Faraco staining. Pictures by: Dr. Deborah Unger.

Papulonecrotic tuberculid Its association with pulmonary, extrapulmonary, tuber-
culous mesenteric lymphadenopathy with reactive PPD has
Papulonecrotic tuberculid (PNT) is currently a rare form of been reported.44 Evidence of the presence of AFB is diffi-
the disease in industrialized countries; however, it is still cult to attain or it is absent in skin lesions. However, there
common in developing countries with a high prevalence of are several studies that have identified the presence of M.
tuberculosis. Children, adolescents, and young adults are tuberculosis DNA by PCR in 50% of PNT lesions.7,11,45 Pos-
the main victims of this tuberculid variant.13,17,18,43 itive cultures for the microorganism are also reported in

137

PAPULE DERMICHE , POI PUSTOLE NECROTICHE CON CICATRICI ATROFICHE VARIOLIFORMI
 PAPULE LICHENOIDI IN PLACCHE PERIFOLLICOLARI, GIALLE O ROSSO BRUNASTRE

A.C. Brito, C.M. Oliveira, D.A. Unger et al.

Lichenoid tuberculid or lichen scrofulosorum

It is characterized by lichenoid papules in individuals highly
sensitized to M. tuberculosis and/or its proteins. It is fre-
quently associated with tuberculosis in the pleura, lungs,
osteoarticular areas, lymph nodes, and other organs. Chil-
dren and adolescents are the most frequently affected
groups, usually from a tuberculous focus.16,17,36,46 Some stud-
ies show the occurrence of this tuberculid post-vaccination
with BCG, as well as infections by NTM, among which the
M. avium-intracellulare complex stands out. However, M.
tuberculosis DNA has been previously demonstrated by PCR
in some cases.7,14,45

Clinical manifestations

Asymptomatic lichenoid papular eruption, with greater
concentration on the trunk. There are follicular and/or
Figure 7 Post-BCG TVC --- disseminated annular lesions on the
perifollicular papules, isolated or coalescent, forming
trunk and upper limbs.
plaques with slight scaling on the surface. Spontaneous or
treatment-specific resolution may occur.46

skin lesions.45 The association of PNT with discoid lupus
erythematosus, erythema nodosum, and arthritis have been Histopathology
reported in the literature.13,43
The upper dermis reveals a granulomatous inflammatory
infiltrate consisting of epithelioid cells, associated with a
Clinical manifestations LESIONI A STAMPO small number of giant Langhans cells and scarce lympho-
cytes, affecting hair follicles and sweat glands. In other
This is a skin eruption that usually occurs in recurrent areas of the dermis, the lymphocytic inflammatory infiltrate
outbreaks of erythematous papules that progress with cen- is perivascular, with a low density. Absence of M. tuberculo-
tral necrosis and ulceration covered by crusts --- called sis on special staining of the biopsy material and in cultures
punched-out lesions. The distribution of lesions is symmet- for AFB. In some studies, the presence of M. tuberculosis
ric, preferably on the extension surfaces of the upper limbs has been demonstrated by PCR.45
(including hands), lower limbs, and the trunk. After treat-
ment or spontaneous resolution, varioliform scars are the Differential diagnosis
result (Figs. 8A and 8B).
It necessarily includes lichen planus, lichen nitidus, sec-
ondary lichenoid syphilis, papular sarcoidosis.
Histopathology

Ulcerated epidermis and dermis with an area of wedge-
Erythema induratum of Bazin and nodular
shaped necrosis and dense granulomatous chronic inflam- vasculitis
matory infiltrate with few multinucleated giant cells in the
surrounding connective tissue. Necrosis may affect hair folli- Ernest Bazin, a French dermatologist, was the first to
cles and granulomatous vasculitis is the alteration detected describe this form of tuberculid in 1861, which was named
in some cases (Fig. 8C). after him.7---11,17,47
Erythema induratum of Bazin (EIB) and nodular vasculitis
(NV) are diseases included in the category of lobular pan-
Diagnosis niculitis, whose clinical manifestations predominate in the
lower limbs. The identification of M. tuberculosis DNA by
The diagnosis is attained through the clinical picture PCR in skin lesions in some cases confirms the tuberculous
and complementary exams: reactive PPD, histopathological etiology. The term nodular vasculitis or erythema induratum
analysis and PCR for AFB. of Whitfield should be reserved for indurated erythema not
associated with tuberculosis.47,48

Differential diagnosis Epidemiology

The following should be considered: pityriasis lichenoides EIB and NV predominate in young and middle-aged females;
et varioliformis acuta, leukocytoclastic vasculitis, secondary however, males can be affected, as well as any ethnic group.
syphilis, prurigos. Countries with a high incidence of tuberculosis have a higher

138
 Anais Brasileiros de Dermatologia 2022;97(2):129---144

Figure 8 (A), Papulonecrotic tuberculid --- ‘‘punched-out’’ lesions on the lower limbs. (B), Papulonecrotic tuberculid --- papuloery-
thematous and papulocrustous lesions in the lower limbs. (C), Papulonecrotic tuberculid --- thinning of the epidermis and granulomas
with caseation necrosis in the underlying dermis, (Hematoxylin & eosin, ×20).

prevalence of these diseases and venous insufficiency is a Nodular vasculitis has been associated with several dis-
frequent association. This variant is very rarely observed in eases: hepatitis B and C, rheumatoid arthritis, ulcerative
children, although there are several case reports from South colitis, Crohn’s disease, leukemia, hypothyroidism. Some
Africa and Pakistan. A case of EIB due to BCG vaccination has drugs are also associated with NV --- propylthiouracil, and
been recorded.13,17 etanercept.13,16

Clinical manifestations
Pathogenesis
They are characterized by erythematous or erythematous-
Tuberculosis-associated EIB is observed in populations with violaceous, painful, isolated, or clustered nodules forming
a prevalence of mycobacterioses. In patients with a clinical a nodular plaque, which progresses into an ulcer that drains
picture of EIB/NV, in which the agent responsible for the skin necrotic or necro-purulent material. The preferential loca-
lesions is not identified through histopathology and culture, tion of the lesions is on the posterior surface of the lower
it is mandatory to use PCR and specific primers for an accu- limbs (calf); however, other places can be affected: upper
rate diagnosis. It is considered that most cases of EIB are limbs, face, gluteal regions, thighs, and feet. The ulcer has
a type IV cell-mediated hypersensitivity reaction, consider- sharp, raised edges, an hemorrhagic background, crusts and
ing that T lymphocytes, macrophages, and Langerhans cells an infiltrated base. Regression of the lesion with scarring
participate in the process. Studies have shown a strongly and subsequent recurrence is observed in most cases. Reac-
reactive PPD in these cases and high positivity on the IGRA tive PPD is observed in patients with a tuberculous focus
test for M. tuberculosis. (Fig. 9A).

139
 A.C. Brito, C.M. Oliveira, D.A. Unger et al.

Figure 9 (A), Erythema induratum of Bazin --- erythematous-violaceous infiltrated nodule on the posterior aspect of the lower
limb. (B), Erythema induratum of Bazin --- Lobular granulomatous panniculitis. (C), Erythema induratum of Bazin: Strong reaction to
PPD skin test.

Histopathology Diagnosis

An incisional biopsy is recommended to include as It is based on the clinical manifestations and complementary
much of the adipose tissue as possible, especially to tests: positive PPD, histopathological analysis, and PCR for
analyze the involvement of the adipose lobe present M. tuberculosis DNA (Fig. 9C).
in the material. Punch biopsies cannot obtain enough
adipose tissue for a more accurate histopathological anal-
Differential diagnosis
ysis.
Microscopic findings in EIB/NV are lobular or mixed
It should include erythema nodosum, pancreatic panniculi-
septal/lobular granulomatous panniculitis, with an inflam-
tis, lipodermatosclerosis (sclerosing panniculitis), panniculi-
matory infiltrate consisting of lymphocytes, epithelioid
tis caused by alpha-1 antitrypsin deficiency, other types of
histiocytes, plasmocytes, and Langhans-type multinucle-
vasculitis, especially cutaneous polyarteritis nodosa, sar-
ated giant cells. Other identified histological alterations
coidosis, and subcutaneous Sweet syndrome.
include adiponecrosis, areas of caseation necrosis, and
vasculitis compromising adipose tissue arteries and veins.
Fibrosis is observed in lesions with a long-term evolu- Diagnosis of cutaneous tuberculosis
tion. In general, AFB are not identified on special stains
(Fig. 9B). Mycobacterium tuberculosis direct test or bacilloscopy aims
to detect the microorganism in smears of biological material

140
 Anais Brasileiros de Dermatologia 2022;97(2):129---144

stained by special techniques, with the Ziehl-Neelsen tech- In CTB, the biological material to be analyzed can be
nique being the most often employed in laboratories. There fresh tissue or embedded in paraffin. The general sensitivity
is low positivity for BK, 50 kg of body
diagnosis. RIPE
weight); isoniazid (300 mg/day), pyrazinamide (1,500 to
The tuberculin test is an intradermal inoculation of
2,000 mg/day); ethambutol (750 mg/day for < 50 kg body
0.1 mL, equivalent to 2TU (tuberculin unit) of a purified
weight and 1,000 mg/day for > 50 kg body weight).
protein derivative of M. tuberculosis (PPD-RT23, in Brazil)
Doses for children: rifampicin (10---20 mg/kg daily), iso-
on the anterior surface of the left forearm to assess the
niazid (10---15 mg/kg daily), and pyrazinamide (30---40 mg/kg
patient’s cell immune response. The reading is carried out
daily).
48 to 72 and up to 96 hours after the application, which
Doses of drugs used in the maintenance phase: rifampicin
is performed with a specific millimeter ruler to measure
(600 mg/day for adults and 10 mg/kg daily for children)
the largest cross-sectional diameter of the induration. The
and isoniazid (600 mg/day for adults and 10 mg/kg daily for
patient is considered to be infected with BK when the
children).36
patient has an induration ≥ 5 mm (Fig. 9).
Surgical excision may be considered in refractory lesions
to correct deformities in recalcitrant cases.50
Interferon-gamma release assay Tuberculid treatment follows the same regimens recom-
mended for true TB. For EIB, a longer period of treatment is
The IGRA test is used to identify individuals with latent M. recommended, such as the proposed maintenance of iso-
tuberculosis infection (LTBI); to identify individuals more niazid for up to two years.50 Dapsone, potassium iodide,
likely to have LTBI and/or higher risk of becoming ill; to and doxycycline have been reported as adjunctive treat-
indicate the correct treatment; to notify patients who will ments to treat inflammation in EIB, whereas corticosteroids
be treated for LTBI and to monitor the treatment of these or tuberculin protein at different dilutions are occasionally
patients. used for desensitization.50 The treatment of lupus vulgaris
One should consider that PPD has limitations, including with isoniazid alone has resulted in high cure rates.51
cross-reaction with NTM and with BCG vaccine; false- Some studies have reported an eventual paradoxical skin
negative results in immunocompromised patients (e.g., HIV reaction in patients undergoing regular treatment for TB,
positive); the possibility of error in the test induration particularly in anergic patients treated for miliary TB. Weeks
measurement; the need for two or three readings after or months after starting the polychemotherapy, purulent
48---72---96 hours. swollen skin lesions appear, whose culture for M. tubercu-
The target population of this test is HIV-positive patients, losis is generally positive, representing an immunological
patients with renal failure undergoing hemodialysis, and phenomenon (and not bacterial resistance) that responds
patients with rheumatoid arthritis and psoriasis on immuno- well to continued treatment. 7
biological therapy.
Immunobiologicals and latent tuberculosis
Tests available in Brazil: QuantiFERON-TB Gold
Plus® (QTF-G) and T-SPOT.TB In immunocompetent individuals, the host’s natural defense
system controls the initial infection caused by M. tuber-
The PPD and IGRA tests must be used simultaneously to culosis; the carrier remains asymptomatic and develops
detect LTBI. Note that these tests cannot differentiate LTBI latent tuberculosis. However, in the presence of dis-
from active infection. eases or medications that lead to immunosuppression,
Polymerase chain reaction (PCR) is a molecular technique such as immunobiologicals, latent tuberculosis can be
that attains amplification of specific sequences of DNA and reactivated.52,53
RNA nucleic acids. It is an important tool in the genotyping Significant advances in the understanding of the
of pathogens, in atypical lymphoid infiltrates of T cells, in pathogenesis of immune-mediated diseases allowed the
the investigation of malignant neoplasm translocations, in development of new drugs called immunobiologicals, which
addition to other clinical entities. revolutionized the therapeutic approach to several diseases,

141

2 RIPE
4 RI
 A.C. Brito, C.M. Oliveira, D.A. Unger et al.

such as psoriasis. In particular, the introduction of tumor that ‘‘the subject be made available for public consultation,
necrosis factor-alpha inhibitors (anti-TNF$) constituted one with a preliminary recommendation in favor of the incor-
of the most revolutionary advances in the treatment of this poration of rifapentine (Priftin® ) into the SUS, to be used
group of diseases, as they were the first target in treat- together with isoniazid in the 3HP regimen, for the treat-
ment. In addition to the observed efficacy, one of the great ment of individuals with latent Mycobacterium tuberculosis
advantages of these agents is their safety profile in rela- infection (LTBI).61
tion to the absence of toxicity in target organs, such as
nephro- or hepatotoxicity, characteristic of conventional
systemic treatments. However, as the blocking occurs in the Financial support
initial phase of the immunological cascade, this therapeu-
tic class leads to a broader immune suppression, which is None declared.
not as selective and, therefore, does not have such a strong
immunological safety profile.54 Authors’ contributions
TNF-$ is a cytokine that plays a central role in the estab-
lishment and maintenance of the inflammatory response
Arival Cardoso de Brito: Approval of the final version of
against infections, being crucial for the formation of granu-
the manuscript; design and planning of the study; draft-
lomas, which represent an essential defense function against
ing and editing of the manuscript; effective participation
intracellular pathogens such as mycobacteria. Anti-TNF-$
in research orientation; intellectual participation in the
therapy compromises the physiological immunoinflamma-
propaedeutic and/or therapeutic conduct of the studied
tory responses mediated by TNF-$ and may alter the
cases; critical review of the literature; critical review of
formation and maintenance of granulomas, leading to TB
the manuscript.
reactivation or spread.55
Clivia Maria Moraes de Oliveira: Approval of the final ver-
In patients receiving anti-TNF-$ treatment, the relative
sion of the manuscript; design and planning of the study;
risk of TB infection ranges from 1.5% to 17%, being higher
drafting and editing of the manuscript; effective partici-
with anti-TNF-$ monoclonal antibody therapy (adalimumab
pation in research orientation; intellectual participation in
and infliximab) than with therapy with soluble TNF-$ recep-
the propaedeutic and/or therapeutic conduct of the studied
tor (etanercept).56,57
cases; critical review of the literature; critical review of the
In an attempt to better seek the specific target to be
manuscript.
blocked in the treatment of autoimmune diseases, anti-
Deborah Aben-Athar Unger: Approval of the final ver-
interleukin immunobiologicals emerged, which are more
sion of the manuscript; design and planning of the study;
selective and, therefore, have a much better safety profile.
drafting and editing of the manuscript; effective partici-
It is possible that blocking anti-IL does not carry the same
pation in research orientation; intellectual participation in
risk of TB reactivation as TNF-$ inhibitors.58 Th17-related
the propaedeutic and/or therapeutic conduct of the studied
cytokines seem to contribute to immunological protection
cases; critical review of the literature; critical review of the
against primary M. tuberculosis infection, and their expres-
manuscript.
sion levels decrease in patients with TB.58
Maraya de Jesus Semblano Bittencourt: Approval of the
Despite the effect on the defense mechanism against M.
final version of the manuscript; design and planning of the
tuberculosis infection of IL-17 and IL-23, the available safety
study; drafting and editing of the manuscript; effective par-
data on anti-IL-17 and anti-IL-23 immunobiologicals demon-
ticipation in research orientation; intellectual participation
strate that this effect may be lower than expected, and this
in the propaedeutic and/or therapeutic conduct of the stud-
may constitute an advantage of this group of immunobio-
ied cases; critical review of the literature; critical review of
logicals in relation to anti-TNF and anti-IL 12/23. However,
the manuscript.
further studies on the safety of anti-interleukin immunobi-
ologicals are needed to further elucidate the issue.59
It is recommended by international guidelines that prior Conflicts of interest
to treatment with immunobiological drugs, a careful TB
investigation should be carried out.58 The investigation None declared.
should be performed with the simultaneous use of PPD and
IGRA and chest radiography (PA and profile), performed
periodically.59 References
Although PPD is a test to assess personal exposure to
TB, in patients with psoriasis there is a possibility of false- 1. who.int [Internet]. Genebra: World Health Organization;
positive results due to pathergy. A decreased response to c2021. Who operational handbook on tuberculosis: module 1:
PPD occurs during treatment with methotrexate, making it prevention: tuberculosis preventive treatment. Available from:
difficult to interpret the result.60 file:///C:/Users/estagio.comunicacao/Downloads/978924000
In Brazil, two therapeutic regimens are recommended for 2906-eng.pdf.
2. who.int [Internet]. Genebra: World Health Orga-
the treatment of latent TB: one with isoniazid, at a dose of
nization; c2021 [cited 2020 Jan 01]. Global
300 mg/day for nine months and the other with rifampicin Tuberculosis Report 2019; [about 2]. Available from:
600 mg/day, for four months.58 https://www.who.int/teams/global-tuberculosis-programme/
The members of the National Commission for the Incor- tb-reports/global-report-2019.
poration of Technologies in the Unified Health System 3. aids.gov [Internet]. Brasil: Ministério da Saúde. Secre-
(CONITEC), at the 86th meeting (March 5, 2020), decided taria de Vigilância em Saúde. Boletim Epidemiológico

142
 Anais Brasileiros de Dermatologia 2022;97(2):129---144

HIV/Aids 2019. [cited 2020 Fev 15]. Available from: 24. Flynn JL, Chan J, Lin PL. Macrophages and control of gran-
http://www.aids.gov.br/pt-br. ulomatous inflammation in tuberculosis. Mucosal Immunol.
4. aids.gov [Internet]. Brasil: Ministério da Saúde. Secretaria 2011;4:271---8.
de Vigilância em Saúde. Departamento de Vigilância das 25. Ma J, Chen T, Mandelin J, Ceponis A, Miller NE, Hukkanen M,
Doenças Transmissíveis. Manual de Recomendações para et al. Regulation of macrophage activation. Cell Mol Life Sci.
o Controle da Tuberculose no Brasil. Brasília: Ministério 2003;60:2334---46.
da Saúde [cited 2020 Fev 15]. Available from: http:// 26. Torrado E, Cooper AM. Células IL-17 and Th17 cells in tubercu-
bvsms.saude.gov.br/bvs/publicacoes/manual recomendacoes losis. Cytokine Growth Factor Rev. 2010;21:455---62.
controle tuberculose brasil 2 ed.pd. 27. Umemura M, Yahagi A, Hamada S, Begum MD, Watanabe
5. gov.br [Internet]. Brasil: Ministério da Saúde. Secretaria H, Kawakami K, et al. IL-17-mediated regulation of innate
de Vigilância em Saúde. Boletim Epidemiológico. Tubercu- and acquired immune response against pulmonary Mycobac-
lose. Brasília: Número Especial Mar. 2021. Available from: terium bovis bacille Calmette-Guerin infection. J Immunol.
https://www.gov.br/saude/pt-br/media/pdf/2021/marco/24/ 2007;178:3786---96.
boletim-tuberculose-2021 24.03#: :text=Em%202020%2C%20o 28. Hu S, He W, Du X, Yang J, Wen Q, Zhong XP, et al. IL-17
%20Brasil%20registrou,%C3%B3bitos%20por%20100%20mil% Production of Neutrophils Enhances Antibacteria Ability but
20habitantes. Promotes Arthritis Development During Mycobacterium tuber-
6. Soares VM, Almeida IN, Figueredo LJA, Haddad JPA, Oliveira culosis Infection. EBioMedicine. 2017;23:88---99.
CSF, Carvalho WS, et al. Factors associated with tuberculosis 29. Jurado JO, Pasquinelli V, Alvarez IB, Peña D, Rovetta AI,
and multidrug-resistant tuberculosis in patients treated at a Tateosian NL, et al. IL-17 and IFN-" expression in lymphocytes
tertiary referral hospital in the state of Minas Gerais, Brazil. from patients with active tuberculosis correlates with the sever-
J Bras Pneumol. 2020;46, 20180386. ity of the disease. J Leukoc Biol. 2012;91:991---1002.
7. Hill MK, Sanders CV. Cutaneous tuberculosis. Microbiol Spectr. 30. Crome SQ, Wang AY, Levings MK. Translational mini-review series
2017;5. on Th17 cells: function and regulation of human T helper 17 cells
8. Zyl L, Plessis J, Viljoen J. Cutaneous tuberculosis overview and in health and disease. Clin Exp Immunol. 2009;159:109---19.
current treatment regimens. Tuberculosis. 2015;95:629---38. 31. Saini C, Ramesh V, Nath I. Increase in CD4 + CD25 + FOXP3 +
9. Chen Q, Chen W, Hao F. Cutaneous tuberculosis: A great imita- TGF-#-secreting T cells in anergic patients with lepromatous
tor. Clin Dermatol. 2019;37:192---9. leprosy. PLoS Negl Trop Dis. 2014;8:2639.
10. Franco-Paredes C, Marcos LA, Henao-Martínez AF, Rodríguez- 32. Belkaid Y, Rouse BT. Natural regulatory T cells in infectious dis-
Morales AJ, Villamil-Gómez WE, Gotuzzo E, et al. Cutaneous ease. Nat Immunol. 2005;6:353---60.
Mycobacterial Infections. Clin Microbiol Rev. 2018;32, 00069-18. 33. Li MO, Wan YY, Sanjabi S, Robertson AK, Flavell RA. Transforming
11. Khadka P, Koirala S, Thapaliya J. Cutaneous Tuberculosis: Clin- growth factor-beta regulation of immune responses. Annu Rev
icopathologic Arrays and Diagnostic Challenges. Dermatol Res Immunol. 2006;24:99---146.
and Pract. 2018;2018, 7201973. 34. Chakraborty PP, Chakraborty M, Dasgupta S. Primary Mycobac-
12. Tshisevhe V, Mbelle N, Peters RPH. Cutaneous tuberculosis in terium tuberculosis infection over insulin injection site. BMJ
HIV-infected individuals: lessons learnt from a case series. S Af Case Rep. 2016;2016.
J HIV Med. 2019;20:1---3. 35. Santos JB, Figueiredo AR, Ferraz CE, Oliveira MH, Silva
13. Sethi A. Tuberculosis and Infections with atypical mycobacte- PG, Medeiros VLS. Cutaneous tuberculosis: epidemiologic,
ria. In: Kang S, Amagai M, Bruckner AL, Enk’s AH, Margolis DJ, etiopathogenic and clinical aspects----part I. An Bras Dermatol.
McMichael AJ, et al., editors. Fitzpatrick’s Dermatology. 9th ed. 2014;89:219---28.
New York: McGraw-Hill; 2019. p. 2859---69. 36. Ljubenovic MS, Ljubenovic DB, Binic II, Jankovic AS, Jancic SA.
14. Mehta PK, Raj A, Singh N, Khuller GK. Diagnosis of extra- Cutaneous tuberculosis and squamous cell carcinoma. An Bras
pulmonary tuberculosis by PCR. FEMS Immunol Med Mic. Dermatol. 2011;86:541---4.
2012;66:20---36. 37. Sharma C, Shekhar S, Sharma V, Sharma M, Aggarwal T. J Pediatr
15. Silva JRL. Novos Aspectos da Patogenia da Tuberculose. Pulmão Adolesc Gynecol. 2012;25:123---4.
RJ. 2012;21:10---4. 38. Padmavathy L, Rao LL, Ethirajan N, Dhanlaklshmi M. Psoriasi-
16. Ramarao S, Greene JN, Casanas BC, Carrington ML, Rice J, forme lupus vulgaris. Indian J Tuberc. 2008;55:97---9.
Kass J. Cutaneous manifestations of tuberculosis. Infect Dis Clin 39. Ezzedine K, Simonart T, Malvy D, Burgoin C, Noel JC. Cuta-
Pract. 2012;20:376---83. neous verrucous carcinoma arising in lupus vulgaris. J Dermatol.
17. Sethuraman G, Ramesh V. Cutaneous tuberculosis in children. 2012;39:505---7.
Pediatr Dermatol. 2013;30:7---16. 40. Hadj I, Meziane M, Mikou O, Inani K, Harmouch T, Mernissi FZ.
18. Charifa A, Mangat R, Oakley AM. Cutaneous Tubercu- Tuberculous gummas with sporotrichoid pattern in a 57-year-
losis. In: StatPearls [Internet]. Treasure Island (FL): old female: A case report and review of the literature. Int J
StatPearls Publishing; 2020. Jan-. Available from: Mycobacteriol. 2014;3:66---70.
https://www.ncbi.nlm.nih.gov/books/NBK482220/ 41. bvsms.saúde [Internet]. Brasil: Biblioteca Virtual da
19. Sehgal VN, Bhattacharya SN, Jain S, Logani K. Cutaneous tuber- Saúde: Ministério da Saúde; c1998. Secretaria de Vig-
culosis: the evolving scenario. Int J Dermatol. 1994;33:97---104. ilância em Saúde. Departamento de Vigilância das
20. Sehgal VN, Wagh SA. Cutaneous tuberculosis. Current concepts. Doenças Transmissíveis. Brasília: Manual de vigilân-
Int J Dermatol. 1990;29:237---52. cia epidemiológica de eventos adversos pós-vacinação.
21. Kaufmann SHE. Tuberculosis: back on the’ ’’immunologists’ 2014. 3rd ed; p. 1-254 [about 2 screens] Available from:
agenda. Immunity. 2006;24:351---7. https://bvsms.saude.gov.br/bvs/publicacoes/manual vigila
22. Saini C, Kumar P, Tarique M, Sharma A, Ramesh V. Regulatory ncia epidemiologica eventos adversos pos vacinacao.pdf.
T cells antagonize proinflammatory response of IL-17 during 42. Zhu B, Dockrell HM, Ottenhoff THM, Evans TG, Zhang Y.
cutaneous tuberculosis. J Inflamm Res. 2018;28:377---88. Tuberculosis vaccines: oportunities and challenges. Respirology.
23. Weiss G, Schaible UE. Mecanismos de defesa dos 2018;23:359---68.
macrófagos contra bactérias intracelulares. Immunol Rev. 43. Jordaan HF, Niekerk DJV, Louw M. Papulonecrotic tuberculid.
2015;264:182---220. A clinical, histopathological and immunohistochemical study of
15 patients. Am J Dermatopathol. 1994;16:474---85.

143
 A.C. Brito, C.M. Oliveira, D.A. Unger et al.

44. Bae SH, Yun SJ, Lee JB, Kim SJ, Lee SC, Won YH. Papu- with latent tuberculosis infection requiring biologic therapy in
lonecrotic Tuberculid: A Rare Skin Manifestation in a Child with rheumatology and dermatology clinical practice. Autoimmun
Mesenteric Tuberculous Lymphadenopathy. Acta Derm Venereol. Rev. 2015;14:503---9.
2017;97:137---8. 54. Mahe E, Descamps V. Anti-TNF alpha en dermatology. Ann Der-
45. Agarwal P, Singh EN, Agarwal US, Meena R, Purohit S, Kumar matol Venereol. 2002;129:1374---9.
S. The role of DNA polymerase chain reaction, culture and 55. Xie X, Li F, Chen JW, Wang J. Risk of tuberculosis infection in
histopathology in the diagnosis of cutaneous tuberculosis. Int anti-TNF-$ biological therapy: from bench to bedside. J Micro-
J Dermatol. 2017;56:1119---24. biol Immunol Infect. 2014;47:268---74.
46. Camacho D, Pielasinski U, Revelles JM, Górgolas M, Manzarbeitia 56. Erkens CGM, Kamphorst M, Abubakar I, Bothamley GH, Chem-
F, Kutzner HM, et al. Lichen scrofulosorum mimicking lichen tob D, Haas W, et al. Tuberculosis contact investigation in
planus. Am J Dermatopathol. 2011;33:186---91. low prevalence countries: a European consensus. Eur Respir J.
47. Lake EP, Worobec SM, Aronson IK. Subcutaneous tissue Disor- 2010;36:925---49.
ders. Panniculitis. Erythema induratum and Nodular vasculitis. 57. Brassard P, Kezouh A, Suissa S. Antirheumatic drugs
In: Kang S, Amagai M, Bruckner AL, Enk’s AH, Margolis DJ, and risk of tuburculosis. Clin Infect Dis. 2006;43:
McMichael AJ, et al., editors. Fitzpatrick’s Dermatology. 9rd ed. 717---22.
New York: McGraw-Hill; 2019. p. 1251---62. 58. Nogueira M, Warren RB, Torres T. Risk of tuberculosis reacti-
48. Varas P, Antúnez-Lay A, Bernucci JM, Cossio L, González S, Eymin vation with interleukin (IL)-17 and IL-23 inhibitors in psoriasis
G. Erythema nodosum: Analysis of 91 hospitalized patients. Rev - time for a paradigm change. J Eur Acad Dermatol Venereol.
Med Chile. 2016;144:162---8. 2021;35:824---34.
49. Patil K, Bagade S, Bonde S, Sharma S, Saraogi G. Recent 59. Shen H, Chen ZW. The crucial roles of Th17-related
therapeutic approaches for the management of tubercu- cytokines/signal pathways in M. tuberculosis infection. Cell Mol
losis: Challenges and opportunities. Biomed Pharmacother. Immunol. 2018;15:216---25.
2018;99:735---45. 60. Sivamani RK, Goodarzi H, Garcia MS, Raychaudhuri SP, Wehrli
50. Dias MFRG, Bernardes Filho F, Quaresma MV, Nascimento LV, LN, Ono Y, et al. Biologic therapies in the treatment of psoria-
Nery JAC, Azulay DR. Update on cutaneous tuberculosis. An Bras sis: a comprehensive, evidence-based basic science and clinical
Dermatol. 2014;89:925---38. review and a practical guide to tuberculosis monitoring. Clin
51. Brück C, Westbeck-Carlsson M. Treatment of lupus vulgaris with Rev Allergy Immunol. 2013;44:121---40.
INH exclusively. Acta Derm Venereol. 1964;44:223---5. 61. conitec.gov [Internet]. Brasil: Comissão Nacional de
52. Souto A, Maneiro JR, Salgado E, Carmona L, Gomez-Reino JJ. Incorporação de Tecnologias no Sistema Único de Saúde;
Risk of tuberculosis in patients with chronic immune-mediated c2016-2021. Relatório de Recomendação: Rifapentina +
inflammatory diseases treated with biologics and tofacitinib: isoniazida para o tratamento da Infecção Latente pelo
a systematic review and meta-analysis of randomized con- Mycobacterium Tuberculosis (ILTB); [about 2 screens].
trolled trials and long-term extension studies. Rheumatology. Available from: http://conitec.gov.br/images/Consultas/
2014;53:1872---85. Relatorios/2020/Relatorio Rifapentina Isoniazida ILTB CP 14
53. Cantini F, Nannini C, Niccoli L, Iannone F, Delogu G, Gar- 2020.pdf.
laschi G, et al. Guidance for the management of patients

144