Therapeutic potential of interferon-gamma in tuberculosis


doi: http://dx.doi.org/10.5599/admet.1078   63 

ADMET & DMPK 10(1) (2022) 63-73; doi: https://doi.org/10.5599/admet.1078  

 
Open Access : ISSN : 1848-7718  

http://www.pub.iapchem.org/ojs/index.php/admet/index   

Review 

Therapeutic potential of interferon-gamma in tuberculosis 

Svetlana A. Berns
1
, Julia A. Isakova

2 
and Polina I. Pekhtereva

3, 
* 

1
Federal State Institution National Medical Research Center for therapy and Preventive Medicine of the Ministry of 

Healthcare of the Russian Federation, svberns@yandex.ru  
2
SPP  “Pharmaclon”  Ltd., Moscow, Russia, julia.is.alex@gmail.com  

3
SPP  “Pharmaclon”  Ltd., Moscow, Russia, pekhterevapolina@gmail.com  

*Corresponding Author: Polina I. Pekhtereva; E-mail: pekhterevapolina@gmail.com; Tel.: +7-909-675-9643 

Received: August 11, 2021; Revised: November 27, 2021; Published: January 14, 2021  

 

Abstract 

Tuberculosis is one of the critical health problems worldwide. The search for ways to improve the results 
of tuberculosis treatment and overcome drug resistance lies in understanding the pathogenesis of the 
development of the infectious process. The interferon system, particularly the role of interferon-gamma, 
has been identified as the main link in the immune response in tuberculosis. The clinical efficacy of 
interferon-gamma has been studied and evaluated in clinical trials since the end of the last century. There 
was obtained evidence of the clinical efficacy of interferon-gamma as part of complex therapy. Recent 
experimental data make it possible to consider interferon-gamma as a promising therapeutic option for 
the treatment of multidrug-resistant tuberculosis as part of complex therapy worthy of further studies. 

©2021 by the authors. This article is an open-access article distributed under the terms and conditions of the Creative Commons 
Attribution license (http://creativecommons.org/licenses/by/4.0/). 

Keywords 

Interferon gamma; MRD-TB; immunotherapy; IFN-γ; complex treatment. 

 

Introduction 

The problem of resistance of microorganisms to antimicrobial drugs and, consequently, issues related to 

the ineffectiveness of treatment remain one of the most urgent in medicine. The World Health 

Organization (WHO) developed and published in 2001 the WHO Global Strategy for Containing 

Antimicrobial Resistance, which recommends considering this problem as one of the priorities of national 

health systems [1]. The significance of the problem of antibiotic resistance is determined by the widespread 

prevalence of resistant microorganisms in inpatient departments and the wide access to drugs used for the 

treatment of multi-resistant strains [2]. A decrease in the effectiveness of therapy ultimately requires the 

use of more expensive drugs and an increase in the duration of treatment, which leads to hospitalization 

time increase, economic losses, and mortality risk [3]. 

Tuberculosis (TB) is a socially significant disease and the deadliest infection, continuing to be the most 

pressing challenge for the healthcare system around the world. According to WHO, TB is the ninth leading 

cause of death in the world, having been the leading cause of death from any single infectious agent, ahead 

of Human Immunodeficiency Virus (HIV) / Acquired Immunodeficiency Syndrome (AIDS), till 2020, when 

http://dx.doi.org/10.5599/admet.1078
https://doi.org/10.5599/admet.1078
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mailto:svberns@yandex.ru
mailto:julia.is.alex@gmail.com
mailto:pekhterevapolina@gmail.com
mailto:pekhterevapolina@gmail.com
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64  

COVID-19 occupied this place [4]. In 2019, WHO estimates that 1.21 million HIV-negative people died from 

TB (less than 1.7 million deaths in 2000), and 208,000 deaths were reported among HIV-positive people [5]. 

Thus, global TB deaths have been reduced by 35 % from 2015 to 2020. The incidence of TB has decreased 

by 20 % over the same period. In this way, there are notable successes in the fight against this infectious 

disease, but so far, not enough to achieve the global goals set by the WHO [5]. 

Most TB deaths can be prevented with early diagnosis and appropriate treatment. Millions of people are 

diagnosed and successfully treated with TB each year, but there are still significant gaps in the detection 

and therapy of the disease. The situation may be aggravated by the epidemic threat of COVID-19, in 

particular, due to the redistribution of human, financial, and other resources not in favour of diagnosis and 

treatment of tuberculosis. The number of medical institutions providing inpatient and outpatient care for 

TB patients has decreased, and there are overlaps in data collection and reporting [5]. 

In conditions of unstable drug supply, underdeveloped infrastructure, and limited resources [6], the 

threat of drug-resistant TB remains. According to WHO estimates, in 2019, in the world, 3.3 % (95 % 

confidence interval (CI): 2.3–4.3 %) of newly diagnosed TB cases and 18 % (95 % CI: 9.7–27 %) of previously 

treated patients have been identified as resistant to rifampicin (RR-TB), the most effective first-line drug, or 

multidrug-resistant TB (MDR-TB). Among them, 20.1 % (95 % CI: 15.5-25.0 %) were also resistant to 

fluoroquinolones, the drugs of choice in establishing resistance to rifampicin or isoniazid. It is alarming that 

about half of these cases are registered in India, China and the Russian Federation [5]. 

The problem of overcoming drug resistance to TB is also complicated because chemotherapy itself has 

an antimicrobial effect and suppresses the immune system's activity and can aggravate the patient's 

immunological reactivity. Impaired immune response in TB patients can be corrected by immunotherapy. 

The correction of the immune status in MDR-TB patients is of particular importance because these patients 

initially have a worse prognosis and a more severe course of the disease [7]. 

In such conditions, the possibility of adjuvant immunotherapy, which can change the course of the 

disease and alleviate the patient's condition, gains a special role. One of the ways of such therapy is to 

regulate the body's immune response. 

Features of the formation of the immune response in bacterial infection 

Returning to the pathophysiological background of the immune response in bacterial infection, it is 

known that when the pathogen enters the human body for the first time, the innate and adaptive immune 

response mechanisms get activated [8]. In case of repeated exposure to the same pathogen, i. e. upon 

reinfection, the removal of the pathogen can occur at a higher rate due to protective immunity and 

immunological memory [9]. 

The important role of interferons (IFNs) in the implementation of the immune response process was 

proven back long ago [10,11]. The search for new ways to overcome drug resistance in patients with MDR-

TB aimed at the role of IFN as an immunomodulator in the complex therapy of TB. The IFN system includes 

the IFN cytokines themselves, transcriptional activators and repressors, cellular receptors and enzyme 

systems activated by them. IFNs increase the resistance of cells to infectious agents and propagate signals 

to other cells that have not previously had contact with either the antigen or IFN. All IFNs are divided into 3 

types: IFN of type I (-α, -β, -κ, -ε, -ω, -τ) [12], type II (-γ) [13] and type III (-λ1-4, -£1-3) [14]. 

At an early stage of infection (several hours), IFNs of types I and II are produced as the first line of 

immune defense in order to attract the largest number of dendritic cells and macrophages to the site of 

injury, which trigger active phagocytosis and inactivate the pathogen. However, if there is a defect in the 



ADMET & DMPK 10(1) (2022) 63-73 Therapeutic potential of interferon-gamma in tuberculosis 

doi: http://dx.doi.org/10.5599/admet.1078 65 

immune mechanism, attracted macrophages can promote infection, providing the microorganism with a 

target for intracellular growth and spread [15,16]. In this case, type I IFNs can contribute to the 

development of TB by inducing IL-10 and deactivating macrophages [17,18]. The immune defense of the 

first level will be broken and the cellular response to the antigen blocked. As a result, a latent form of TB 

may develop [19]. 

The optimal immune response is formed in a few days after infection. CD4+ and CD8+ effector T cells are 

directed to the affected area and start inducing type II IFN, strongly shifting the balance towards this class 

of cytokines [15] and reducing the risk of developing an active TB process [20]. It was found that CD4+ 

lymphocyte count below 100 cells/mm3 before treatment significantly increases the likelihood of an 

unfavourable outcome of generalized tuberculosis in HIV patients [21]. 

At least 10 genes are known to be associated with increased susceptibility to mycobacterial infection 

[22]. First of all, these are genes encoding IFN-γ and its receptors, as well as cellular factors STAT1 [23] and 

NFκB [24], directly related to the mechanism of IFN-γ action on the cell: antigen recognition, the realization 

of an innate immune response, and oxidative properties of macrophages [25], and necessary for protection 

against TB [26] and other infectious diseases, since they determine nonspecific pathways of action on the 

pathogen (Figure 1). 

 

Figure 1. Mechanism of IFN-γ action via the immune cells 

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Disseminated forms of infections in children often arise due to congenital defects in the structure of the 

IFN-γ protein [27]. The deficiency of genes encoding protein chains of receptors is one of the most common 

mutations that cause increased susceptibility to mycobacterial infection. The IFNγR1 gene accounts for 39 

% of mutations [28]. For reasons still unclear, IFNγR2 deficiency is much less common [29]. In patients with 

complete deficiencies of any of these genes, there is an absence or incomplete formation of granulomas 

and diffusely loaded macrophages [30]. 

Features of the formation of bacterial resistance 

The main mechanisms of the resistance development include genetic changes that ensure the "removal 

of the effect" of the antibiotic (change in the target, metabolism, method of removing the antibiotic from 

the cell), as well as the isolation of the microorganism from the drug (intracellular localization, biofilm 

formation) [31]. In the case of M. tuberculosis, the microorganism forms resistance due to the hydrophobic 

cell wall, β-lactamases, and mutations in the bacterial genes [7]. 

The immune system ensures the elimination of the pathogen primarily due to the strength of the 

cellular immunity by activating the phagocytosis. 

It was shown that IFN-γ could affect each of the main aspects of the phagocytes activation, thereby 

playing an important role in the immune response [32-34]: 

 activates macrophages, attracts them to the site of infection; 

 induces the release of nitric oxide; 

 serves as the only inducer in the cell of the synthesis of proteins of the second class 

histocompatibility complex (MHC class II) - an antigen-presenting complex for extracellular 

pathogens. 

The primary feature of the functioning of phagocytes, which ensures the relationship of nonspecific and 

specific immunity, is the performance of the role of antigen-presenting cells. Antigen-presenting cells are 

located on the main routes of entry of antigens into the body (in the skin and the mucous membranes), 

from where, after capturing antigens, they migrate to the peripheral organs of the immune system, where 

they present antigens to lymphocytes. Phagocytes are the cells that directly kill bacteria through 

phagocytosis ("eating" them) and play one of the leading roles in the body's first immune response to 

bacterial infection. Hereditary and acquired disorders of phagocytosis can lead to severe pathologies of the 

functioning of the immune system [35]. 

Mechanisms of action of phagocytes: 

 a phagocyte cell carries receptors on its surface that recognize an infectious agent (for example, the 

cell wall of a bacterium). When a phagocyte comes into contact with a bacterium, receptors on its 

surface bind to it, leading to the bacterium's absorption by the phagocyte. 

 Release of reactive oxygen species and nitric oxide by phagocytes cause oxidative stress that 

destroys bacteria; 

 Stimulation of other cells of the immune system through "antigen presentation" is a process in 

which phagocytes place fragments of pathogen proteins on the surface of their cells, thereby 

presenting these fragments to other cells of the immune system, developing an antigen-specific 

immune response [8,35-37]. 

It is important to note that at an early stage of infection, IFNs of types I and II are produced in equal 

concentrations, and IFNs of type I are able to reduce the expression of the major histocompatibility 



ADMET & DMPK 10(1) (2022) 63-73 Therapeutic potential of interferon-gamma in tuberculosis 

doi: http://dx.doi.org/10.5599/admet.1078 67 

complex (MHC or MHC) of class II on antigen-presenting cells, induced by IFN of type II, preventing it action 

[38]. 

Thus, during the development of a bacterial infection, the effects of IFN-γ provide a relationship 

between the two most important links of the immune response of a macroorganism, enhancing the 

antigen-dependent immune response and stimulating the work of phagocytes. 

An additional factor affecting the course of a bacterial infection is the ability of bacteria to inhibit the 

synthesis of pro-inflammatory cytokines. It has been shown that some microorganisms can specifically 

repress the synthesis of endogenous IFN-γ [39]. In a study by Fortes et al., it was demonstrated that 

patients infected with an antibiotic-resistant strain of Mycobacterium tuberculosis have a reduced level of 

endogenous IFN-γ compared to normal patients [40]. It has also been shown that the use of beta-lactam 

antibiotics can decrease the level of endogenous IFN-γ [41]. 

Thus, the IFN system and directly IFN-γ are key regulators of the body's immune response to the 

infection caused by TB. Therefore, additional exposure to exogenous IFN-γ can play the role of an inducer 

of the immune system under conditions of a reduced response to antibiotics and correct the endogenous 

cytokine deficiency. 

Despite all the attractiveness of the idea, unfortunately, interest in the development has not yet been 

represented by widely deployed large-scale clinical trials (except for diagnostics use research). This is 

probably due to the limited number of medical products based on interferon-gamma presented on the 

world market. Nevertheless, in our view, the diagnostic and clinical value of the molecule will undoubtedly 

gain momentum in the nearest future. 

Clinical efficacy of interferon-gamma in the treatment of tuberculosis 

On the open resource https://clinicaltrials.gov/ 99 clinical trials with keywords “interferon-gamma” and 

“tuberculosis” were found, 15 of which are in active status, 64 are completed, 20 are cancelled or have an 

unknown status. Out of 64 completed studies, 16 studies have published results. Current research is mainly 

concerned with the diagnostic use of the interferon-gamma secretion test to assess the immune status of 

the body [42]. 

The therapeutic activity of IFN-γ against TB and MDR-TB has been intensively studied since the end of 

the last century; a number of clinical studies have demonstrated the effectiveness of IFN-γ against TB, 

including MDR-TB [43-49]. 

A meta-analysis that pooled data from 9 clinical trials showed a statistically significant effect for IFN-γ as 

an adjunct drug for TB [43]. The studies of nebulized IFN-γ showed statistically significant benefits as a 

result of negative sputum conversion and chest radiographs: the pooled relative risk (RR) for conversion 

was 1.97 (95 % confidence interval (CI) 1.20-3.24, p = 0.008) after 1 month of treatment, 1.74 (95 % CI 1.30-

2.34, p = 0.0002) after 2 months of treatment, 1.53 (95 % CI 1.16-2.01, p = 0.003) after 3 months of 

treatment, 1.57 (95 % CI 1.20-2.06, p = 0.001) after 6 months of treatment, and 1.55 (95 % CI 1.17-2.05, p = 

0.002) at the end of treatment; the pooled RR for chest radiographs was 1.38 (95 % CI 1.10–1.17, p = 0.006) 

at the end of treatment [44]. A randomized controlled trial with aerosol and subcutaneous injected IFN-γ 

showed a significant reduction in fever symptoms, wheezing and night sweats compared with the control 

group after one month of treatment [46]. For intramuscularly administered IFN-γ, the meta-analysis 

included three studies that showed significant improvement in negative sputum conversion after two 

months of treatment [43]. Intramuscular injection of IFN-γ also showed a beneficial effect in treating 

pulmonary MDR-TB [45]. The authors concluded that adjuvant therapy with IFN-γ, especially in an aerosol 

form, may be beneficial for TB patients. 

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The results of another randomized clinical trial published in 2016 also confirmed the high clinical efficacy 

of IFN-γ as part of the complex therapy for TB. This study evaluated the clinical efficacy of IFN-γ in the 

intensive phase of complex treatment of newly diagnosed patients with destructive pulmonary TB with 

bacterial excretion. The dynamics of laboratory and immunological parameters were also assessed. The 

study included 60 patients (the study group included 30 newly diagnosed patients who received 500,000 IU 

of IFN-γ intramuscularly every other day, for a month in addition to standard therapy; control group - 30 

patients who received only standard therapy). The predominant clinical form was infiltrative, diagnosed in 

80 % of patients in both groups (p> 0.05). Clinical efficacy was assessed in patients who received IFN-γ after 

two months of the intensive phase of treatment. According to the results of a control X-ray examination, 

cavities in the lungs closed in 23 % of cases, and by four months, this indicator was 50 %. While in patients 

in the control group, the closure of cavities in the lungs was 10 %, in the study group, this indicator was 

three times higher (37 %) (p <0.05). Abacillation occurred in 90 % of patients receiving IFN-γ. A month later, 

the normalization of indicators of the clinical analysis of blood occurred in 70 % of patients. In the group of 

patients who additionally received IFN-γ, the number of CD4+ lymphocytes increased to 41 %, exceeding 

the initial level by 1.7 times (p <0.001). The authors of the study concluded that the addition of 

immunomodulatory therapy is a significant addition to anti-TB drugs in terms of pathogenesis. The use of 

IFN-γ in the complex treatment of patients with destructive pulmonary TB with bacterial excretion has 

shown its high efficiency in the intensive phase of chemotherapy, accompanied by an increase in patients' 

quality of life. The results of the study indicate a significant improvement in the quality of life based on the 

assessment according to the methodology recommended by the WHO. After complex treatment, when 

studying the quality of life of patients in the main group, there was a positive trend in aspects 

characterizing social relationships and the psychological sphere, as well as reflecting the physical and 

mental health of the patient. It should be noted that the addition of IFN-γ to anti-tuberculosis therapy was 

not accompanied by a significant increase in the number of adverse reactions (20 % vs. 17 % in the control 

group) (p> 0.05). All adverse reactions were removable and stopped by pathogenetic methods of 

concomitant treatment [48]. 

One more clinical example was published in the scientific literature about the experience of IFN-γ 

medical use in MDR-TB. The treatment of MDR-TB of the brain in a patient with acute lymphocytic 

leukemia, after five months of adjuvant therapy using subcutaneously injected IFN-γ, showed a positive 

trend with the achievement of complete remission after 12 months of therapy [47].  

In another study evaluating the effects of IFN-γ in MDR-TB, it was found for resistant forms of TB that 

there is an increase in the basal and IL12/IL27-induced secretion of IFN-γ by blood lymphocytes in vitro, 

with the maximum severity of changes in the disseminated form of the disease. Hypersecretion of IFN-γ in 

vitro is associated with a low content of CD3-IFN-γ+ lymphocytes and an increase in the proportion of CD3-

IFN-γ+ against the background of general T-lymphocytopenia [50]. 

A recent study to assess the effects of IFN-γ on macrophage activity in overcoming MDR-TB drug 

resistance demonstrated the high efficacy of IFN-γ as an adjuvant therapy for MDR-TB. The authors of the 

study draw encouraging conclusions about the prospect of using IFN-γ as a part of adjuvant therapy for 

MDR-TB. It increases the activity of macrophages against Mycobacterium tuberculosis and improves the 

activity of macrophages treatment outcomes in patients with poor response to therapy [7]. 

The use of exogenous IFN-γ in adjuvant therapy, especially in the case of diseases caused by 

microorganisms resistant to antibiotics, can have a significant effect on the course of the disease and 

accelerate the patient's recovery, contributing to earlier abacillation of sputum. 



ADMET & DMPK 10(1) (2022) 63-73 Therapeutic potential of interferon-gamma in tuberculosis 

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Assessment of the economic feasibility of using interferon-gamma in the treatment of tuberculosis 
(experience of the Russian Federation) 

As a socially significant disease, TB poses a significant social and economic burden on the healthcare 

system around the world [51]. The economic burden of TB is conditioned by several components: direct 

economic losses associated with medical costs and indirect economic losses of the country's gross domestic 

product due to the loss of “human capital”. The costs of drug therapy account for more than half of the 

direct medical costs of TB treatment [52]. In this regard, when adding new drugs to TB treatment regimens, 

not only clinical indicators of the effectiveness of therapy should be taken into account, but also their 

impact on the health economics. Assessment of health technologies when deciding on the inclusion of 

medicines in the drug supply system is a mandatory component of health systems in all countries of the 

world, regardless of economic development, morbidity and mortality. In the Russian study published in 

2018 [53] on the assessment of the cost-effectiveness for IFN-γ, a positive impact on the budget from the 

use of IFN-γ as a part of complex TB therapy was demonstrated due to reducing the duration of 

hospitalization. As a result of the behavioural pharmacoeconomic analysis, it was shown that IFN-γ 

contributed to an increase of the duration of quality life by 2.1 QALY, and its use will be accompanied by 

savings in the budget of the Russian Federation in the amount of up to 27 % of funds for the treatment of 

this group of patients [53]. 

Results and Discussion 

Analysis of data from preclinical and clinical studies shows that the inflammatory cytokine IFN-γ 

occupies an important place in the pathogenesis of bacterial infections, including TB. 

The significance and potential of the use of interferons are discussed in all areas of phthisiology: 

diagnosis, therapy, and prevention of TB [54]. For instance, the main alternative to tuberculin skin test 

widely used for diagnostic purposes is IFN-γ release assays (IGRA) test. It measures the ex vivo production 

of IFN-γ from T-cells stimulated with the TB-specific antigens. The test doesn’t have cross-reactivity to BCG 

and nontuberculous mycobacteria showing higher specificity keeping the same level of sensitivity [55-57].  

Preclinical data confirm the enhancement of the cellular component of immunity when using IFN-γ in 

combination with the recombinant BCG vaccine (Bacillus Calmette - Guérin (BCG)) [58]. The use of IFN-γ as 

a means of preventing infection, as well as the transition of the latent phase of TB to the active form, 

requires the study of this agent in clinical trials of vaccines and other therapeutic drugs [20]. 

The greatest amount of evidence and data today is obtained in the direction of the use of IFN-γ as a 

therapeutic option in the complex therapy of pulmonary TB. It has been shown that IFN-γ plays a significant 

role in the pathogenesis of TB [15,59], is a marker of type 1 Th-helper lymphocytes [55], and is considered a 

key immunomodulatory agent for the maintenance adjuvant therapy of TB patients. 

Many factors play a role in the infectious process and outcomes of TB, but the most important of them 

is the activity of the body's immune system and its ability to resist infection. The human immune system is 

able to control it. Weakness of the immune response is the main condition for the development of the 

disease and subsequently for the prolonged course of the infectious process against the background of 

antibiotic therapy. In patients with immunodeficiency, the treatment of the disease is always difficult, even 

with maximum doses of drugs as part of complex antibiotic therapy [6]. In conditions of bacterial resistance 

to antibiotics, the role of the immune response in the fight against infection and the stress on the immune 

system increases dramatically. S.H. Kaufman et al., in their review published in 2014 in the Lancet [60], 

focused on host-directed therapies defining such strategy “especially beneficial for patients with multidrug-

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70  

resistant tuberculosis”. The use of traditional anti-tuberculosis drugs only is no more a sufficient tactic to 

achieve the target [60].  

Conclusions 

Understanding the pathogenesis of the development of the infectious process and the role of IFN-γ in 

the activation of the immune system in TB, made it possible to identify IFN-γ as a promising therapeutic 

option for improving treatment results and overcoming the development of bacterial resistance. The 

clinical efficacy of IFN-γ against TB has been studied in clinical trials for over 20 years. The clinical 

experience and medical application of IFN-γ accumulated in the course of long research allow us to 

recommend it as a safe and effective therapeutic agent in a complex, comprehensive TB treatment, not 

only from the standpoint of evidence-based medicine but also from the point of view of health economics. 

For the full disclosure of the therapeutic potential of IFN-γ in overcoming multidrug resistance of TB, 

further study of its effectiveness in controlled clinical trials is necessary. 

Conflict of interest: The authors declare that they have no competing interests. 

References 

[1] World Health Organization. WHO Global Strategy for Containment of Antimicrobial Resistance. 
Geneva, 2001. WHO/CDS/CSR/DRS/2001.2. https://www.who.int/drugresistance/WHO%20Global-
%20Strategy%20-%20Executive%20Summary%20-%20English%20version.pdf?ua=1.  

[2] J.P. Cegielski, T. Dalton, M. Yagui M, et al. Extensive drug resistance acquired during treatment of 
multidrug-resistant tuberculosis. Clinical Infectious Diseases 59(8) (2014) 1049-1063. https://doi.-
org/10.1093/cid/ciu572.  

[3] A.V. Dehnich. Antibiotic resistance: problems and solutions. Materials of the IX National Congress on 
Cystic Fibrosis "Cystic Fibrosis in Children and Adults - 2009», CJSC « Reklamno-izdatel'skaja gruppa 
MegaPro», 2009, стр. 34-35. 

[4] Johns Hopkins University. Corona Virus Resource Center. 2020. Available from: https://coronavirus.-
jhu.edu/map.html.  

[5] WHO, Global tuberculosis report, 2020, https://apps.who.int/iris/bitstream/handle/10665/-
336069/9789240013131-eng.pdf.  

[6] A.K. Azad, W. Sadee, and L. S. Schlesinger. Innate immune gene polymorphisms in tuberculosis. 
Infection and Immunity 80(10) (2012) 3343–3359. https://doi.org/10.1128/IAI.00443-12. 

[7] T.A. Khan, H. Mazhar, Sh. Saleha, H.N. Tipu, N. Muhammad, M.N. Abbas. Interferon-gamma improves 
macrophages function against m. tuberculosis in multidrug-resistant tuberculosis patients. 
Chemotherapy Research and Practice (2016) 7295390. https://doi.org/10.1155/2016/7295390.  

[8] C.A. Jr. Janeway, P. Travers, M. Walport, et al. Immunobiology: The Immune System in Health and 
Disease. 5th edition. New York: Garland Science (2001).  

[9] R.J. Meshkova. Immunization Guidelines for Physicians. Smolensk State Medical Academy (1998). 

[10] S. Sharma, M. Bose. Role of cytokines in immune response to pulmonary tuberculosis. Asian Pac J 
Allergy Immunol. 19(3) (2001) 213-219.  

[11] J. Parkin, B. Cohen. An overview of the immune system. Lancet 357(9270) (2001) 1777–1789. 
https://doi.org/10.1016/S0140-6736(00)04904-7.  

[12] J. Piehler, C. Thomas, K.C. Garcia, G. Schreiber. Structural and dynamic determinants of type I 
interferon receptor assembly and their functional interpretation. Immunological Reviews 250 (2012) 
317–334. https://doi.org/10.1111/imr.12001.  

[13] J. Ye, J.R. Ortaldo, K. Conlon, R. Winkler-Pickett, H.A. Young. Cellular and molecular mechanisms of 
IFN-gamma production induced by IL-2 and IL-12 in a human NK cell line. Journal of Leukocyte 
Biology 58(2) (1995) 225–233. https://doi.org/10.1002/jlb.58.2.225.  

https://www.who.int/drugresistance/WHO%20Global%20Strategy%20-%20Executive%20Summary%20-%20English%20version.pdf?ua=1
https://www.who.int/drugresistance/WHO%20Global%20Strategy%20-%20Executive%20Summary%20-%20English%20version.pdf?ua=1
https://doi.org/10.1093/cid/ciu572
https://doi.org/10.1093/cid/ciu572
https://coronavirus.jhu.edu/map.html
https://coronavirus.jhu.edu/map.html
https://apps.who.int/iris/bitstream/handle/10665/336069/9789240013131-eng.pdf
https://apps.who.int/iris/bitstream/handle/10665/336069/9789240013131-eng.pdf
https://doi.org/10.1128/IAI.00443-12
https://doi.org/10.1155/2016/7295390
https://www.ncbi.nlm.nih.gov/pubmed/?term=Sharma%20S%5BAuthor%5D&cauthor=true&cauthor_uid=11826917
https://www.ncbi.nlm.nih.gov/pubmed/?term=Bose%20M%5BAuthor%5D&cauthor=true&cauthor_uid=11826917
https://www.ncbi.nlm.nih.gov/pubmed/11826917
https://www.ncbi.nlm.nih.gov/pubmed/11826917
https://doi.org/10.1016/S0140-6736(00)04904-7
https://doi.org/10.1111/imr.12001
https://doi.org/10.1002/jlb.58.2.225


ADMET & DMPK 10(1) (2022) 63-73 Therapeutic potential of interferon-gamma in tuberculosis 

doi: http://dx.doi.org/10.5599/admet.1078 71 

[14] H. Bierne, L. Travier, T. Mahlakõiv, et al. Activation of type III interferon genes by pathogenic bacteria 
in infected epithelial cells and mouse placenta. PloS One 7(6) (2012) e39080. https://doi.org/10.-
1371/journal.pone.0039080.  

[15] L. Desvignes, A.J. Wolf, J.D. Ernst. Dynamic roles of type I and type II interferons in early infection 
with Mycobacterium tuberculosis. Journal of Immunology. 188(12) (2012) 6205–6215. 
https://doi.org/10.4049/jimmunol.1200255.  

[16] S.V. Jamwal, P. Mehrotra, A. Singh, Z. Siddiqui, A. Basu, K.V. Rao. Mycobacterial escape from 
macrophage phagosomes to the cytoplasm represents an alternate adaptation mechanism. Scientific 

Reports 6 (2016) 23089. https://doi.org/10.1038/srep23089.  

[17] T.N. Ottenhoff, R.H. Dass, N. Yang, et al. Genome-wide expression profiling identifies type 1 
interferon response pathways in active tuberculosis. PloS One 7(9) (2012) e45839. 
https://doi.org/10.1371/journal.pone.0045839 

[18] M. Travar, M. Petkovic, A. Verhaz. Type I, II, and III interferons: regulating immunity to 
Mycobacterium tuberculosis infection. Archivum Immunologiae et Therapiae Experimentalis 
(Warsz) 64(1) (2016) 19–31. doi: https://doi.org/10.1007/s00005-015-0365-7.  

[19] M.A. Huaman, D. Henson, P.L. Rondan, et al. Latent tuberculosis infection is associated with 
increased unstimulated levels of interferon-gamma in Lima, Peru. PloS One 13(9) (2018) e0202191. 
https://doi.org/10.1371/journal.pone.0202191.  

[20] E. Petruccioli, T.J. Scriba, L. Petrone, et al. Correlates of tuberculosis risk: predictive biomarkers for 
progression to active tuberculosis. The European respiratory journal 48(6) (2016) 1751-1763. 
https://doi.org/10.1183/13993003.01012-2016.  

[21] V.N. Zimina, I.A. Vasilieva, A.V. Kravchenko, F.A. Batyrov. Generalized tuberculosis in HIV-infected 
patients with AIDS. Journal of the International AIDS Society 13(4) (2010) P195. 
https://doi.org/10.1186/1758-2652-13-S4-P195.  

[22] E. van de Vosse, M.A. Hoeve, T.N. Ottenhoff. Human genetics of intracellular infectious diseases: 
molecular and cellular immunity against mycobacteria and salmonellae. Lancet Infect. Dis. 4 (2004) 
739–749. https://doi.org/10.1016/S1473-3099(04)01203-4.  

[23] L.C. Platanias. Mechanisms of type-I- and type-II-interferon-mediated signalling. Nature Reviews. 
Immunology 5(5) (2005) 375–386. https://doi.org/10.1038/nri1604.  

[24] B.H. Salt, J.E. Niemela, R. Pandey, E.P. Hanson, R.P. Deering, R. Quinones, A. Jain, J.S. Orange, E.W. 
Gelfand. IKBKG (nuclear factor-kappa B essential modulator) mutation can be associated with 
opportunistic infection without impairing Toll-like receptor function. The Journal of allergy and 
clinical immunology 121 (2008) 976–982. https://doi.org/10.1016/j.jaci.2007.11.014. 

[25] J. Bustamante, A.A. Arias, G. Vogt, C. Picard, L.B. Galicia, et al. Germline CYBB mutations that 
selectively affect macrophages in kindreds with X-linked predisposition to tuberculous mycobacterial 
disease. Nature immunology 12 (2011) 213–221. https://doi.org/10.1038/ni.1992.        

[26] J.D. Ernst. The immunological life cycle of tuberculosis. Nature Reviews Immunology 12 (2012) 581–
591. https://doi.org/10.1038/nri3259.  

[27] O. Filipe-Santos, J. Bustamante, A. Chapgier, G. Vogt, L. de Beaucoudrey, J. Feinberg, E. Jouanguy, S. 
Boisson-Dupuis, C. Fieschi, C. Picard, J.L. Casanova. Inborn errors of IL-12/23- and IFN-γ-mediated 
immunity: molecular, cellular, and clinical features. Seminars in immunology 18 (2006) 347–361. 
https://doi.org/10.1016/j.smim.2006.07.010.   

[28] S. Al-Muhsen, J.L. Casanova. The genetic heterogeneity of mendelian susceptibility to mycobacterial 
diseases. Journal of allergy and clinical immunology 122 (2008) 1043–1051. https://doi.org/10.1016/-
j.jaci.2008.10.037.  

[29] S.D. Rosenzweig, S.E. Dorman, G. Uzel, S. Shaw, A. Scurlock, M.R. Brown, R.H. Buckley, S.M. Holland. 
A novel mutation in IFN-γ Receptor 2 with dominant negative activity: biological consequences of 
homozygous and heterozygous states. Journal of immunology 173 (2004) 4000–4008. https://doi.-
org/10.4049/jimmunol.173.6.4000.  

http://dx.doi.org/10.5599/admet.1078
https://doi.org/10.1371/journal.pone.0039080
https://doi.org/10.1371/journal.pone.0039080
https://doi.org/10.4049/jimmunol.1200255
https://dx.doi.org/10.1038%2Fsrep23089
https://doi.org/10.1371/journal.pone.0045839
https://doi.org/10.1007/s00005-015-0365-7
https://doi.org/10.1371/journal.pone.0202191
https://doi.org/10.1183/13993003.01012-2016
https://doi.org/10.1186/1758-2652-13-S4-P195
https://doi.org/10.1016/S1473-3099(04)01203-4
https://doi.org/10.1038/nri1604
https://doi.org/10.1016/j.jaci.2007.11.014
https://doi.org/10.1038/ni.1992
https://doi.org/10.1038/ni.1992
https://doi.org/10.1038/nri3259
https://doi.org/10.1016/j.smim.2006.07.010
https://doi.org/10.1016/j.jaci.2008.10.037
https://doi.org/10.1016/j.jaci.2008.10.037
https://doi.org/10.4049/jimmunol.173.6.4000
https://doi.org/10.4049/jimmunol.173.6.4000


Svetlana A. Berns et al.   ADMET & DMPK 10(1) (2022) 63-73 

72  

[30] J.F. Emile, N. Patey, F. Altare, S. Lamhamedi, E. Jouanguy, F. Boman, J. Quillard, M. Lecomte-Houcke, 
O. Verola, J.F. Mousnier, F. Dijoud, S. Blanche, A. Fischer, N. Brousse, J.L. Casanova. Correlation of 
granuloma structure with clinical outcome defines two types of idiopathic disseminated BCG 
infection. J Pathol. 181 (1997) 25–30. https://doi.org/10.1002/(SICI)1096-9896(199701)181:1<25::-
AID-PATH747>3.0.CO;2-Z .  

[31] S.N. Kozlov, R.S. Kozlov. Modern antimicrobial chemotherapy. A guide for doctors. 3rd edition revised 
and enlarged. Medicinskoe informacionnoe agentstvo (2017) 400 с. 

[32] T. Eddens, J.K. Kolls. Host defenses against bacterial lower respiratory tract infection. Curr. Opin. 
Immunol. 24(4) (2012) 424–430. https://doi.org/10.1016/j.coi.2012.07.005.   

[33] C.V. Harding, W.H. Boom. Regulation of antigen presentation by Mycobacterium tuberculosis: a role 
for Toll-like receptors. Nat. Rev. Microbiol. 8 (2010) 296–307. https://doi.org/10.1038/nrmicro2321.  

[34] A. Razaghi, L. Owens, K. Heimann. Review of the recombinant human interferon gamma as an 
immunotherapeutic: Impacts of production platforms and glycosylation. Journal of Biotechnology 240 
(2016) 48–60. https://doi.org/10.1016/j.jbiotec.2016.10.022.  

[35] F.C. Fang. Antimicrobial reactive oxygen and nitrogen species: concepts and controversies. Nat. Rev. 
Microbiol. 2(10) (2004) 820-32. https://doi.org/10.1038/nrmicro1004.  

[36] E. Pashkov, A. Karaulov, S. Bykov, M. Korn, A. Bykov, A. Vorob'ev, V. Zverev. Atlas of Medical 
Microbiology, Virology and Immunology. M.: Medicinskoe informacionnoe agentstvo (2008) 272 с. 

[37] R.S. Orlov, A.D. Nozdrachev. Normal physiology: textbook. - second edition, revised and enlarged M. 
GJeOTAR-Media (2010) 832 p. 

[38] E.L. Lousberg, C.K. Fraser, M.G. Tovey, K.R. Diener, J.D. Hayball. Type I interferons mediate the innate 
cytokine response to recombinant Fowlpox virus but not the induction of plasmacytoid dendritic cell-
dependent adaptive immunity. Journal of Virology 84(13) (2010) 6549–6563. https://doi.org/10.-
1128/JVI.02618-09.  

[39] P.O. Pinheiro, E.B. Oliveira, G. Santos, G.M. Sperandio da Silva, B.J. Andrade Silva, R.M.B. Teles, A. 
Milagres, E.N. Sarno, M.P. Dalcolmo, E.P. Sampaio. Different immunosuppressive mechanisms in 
multi-drug-resistant tuberculosis and non-tuberculous mycobacteria patients. Clinical and 
experimental immunology 171(2) (2013) 210–219. https://doi.org/10.1111/cei.12007.  

[40] A. Fortes, K. Pereira, P.R.Z. Antas, C.L.M.C. Franken, M. Dalcolmo, M.M. Ribeiro-Carvalho, K.S. Cunha, 
A. Geluk, A. Kritski, A. Kolk, P. Klatser, E.N. Sarno, T.H.M. Ottenhoff, E.P. Sampaio. Detection of in 
vitro interferon-γ and serum tumour necrosis factor-α in multidrug-resistant tuberculosis patients. 
Clinical and experimental immunology 141(3) (2005) 541–548. https://doi.org/10.1111/j.1365-
2249.2005.02872.x.   

[41] B.M. Brooks, C.A. Hart, J.W. Coleman. 2005. Differential effects of beta-lactams on human IFN-
gamma activity. The Journal of antimicrobial chemotherapy 56(6) (2005) 1122-1125. 
https://doi.org/10.1093/jac/dki373.  

[42] https://clinicaltrials.gov (date accessed 10.06.2021).  

[43] X.F. Gao, Z.W. Yang, J. Li. Adjunctive therapy with interferon-gamma for the treatment of pulmonary 
tuberculosis: a systematic review. International Journal of Infectious Diseases 15 (2011) e594–e600. 
https://doi.org/10.1016/j.ijid.2011.05.002. 

[44] R. Condos, W. N. Rom, and N. W. Schluger. Treatment of multidrug-resistant pulmonary tuberculosis 
with interferon-gamma via aerosol. Lancet 349(9064) (1997) 1513–1515. https://doi.org/10.1016/-
S0140-6736(96)12273-X   

[45] R. Suarez-Mendez, I. García-García, N. Fernández-Olivera et al. Adjuvant interferon gamma in 
patients with drug resistant pulmonary tuberculosis: a pilot study. BMC Infectious Diseases 4 (2004) 
44. https://doi.org/10.1186/1471-2334-4-44.  

[46] S. K. Park, S. Cho, I. H. Lee et al. Subcutaneously administered interferon-gamma for the treatment of 
multidrugresistant pulmonary tuberculosis. International Journal of Infectious Diseases 11(5) (2007) 
434–440. https://doi.org/10.1016/j.ijid.2006.12.004.  

https://doi.org/10.1002/(sici)1096-9896(199701)181:1%3c25::aid-path747%3e3.0.co;2-z
https://doi.org/10.1002/(sici)1096-9896(199701)181:1%3c25::aid-path747%3e3.0.co;2-z
https://doi.org/10.1016/j.coi.2012.07.005
https://doi.org/10.1038/nrmicro2321
https://doi.org/10.1016/j.jbiotec.2016.10.022
https://doi.org/10.1038/nrmicro1004
https://doi.org/10.1128/JVI.02618-09
https://doi.org/10.1128/JVI.02618-09
https://doi.org/10.1111/cei.12007
https://doi.org/10.1111/j.1365-2249.2005.02872.x
https://doi.org/10.1111/j.1365-2249.2005.02872.x
https://doi.org/10.1093/jac/dki373
https://clinicaltrials.gov/
https://doi.org/10.1016/j.ijid.2011.05.002
https://doi.org/10.1016/S0140-6736(96)12273-X
https://doi.org/10.1016/S0140-6736(96)12273-X
https://doi.org/10.1186/1471-2334-4-44
https://doi.org/10.1016/j.ijid.2006.12.004


ADMET & DMPK 10(1) (2022) 63-73 Therapeutic potential of interferon-gamma in tuberculosis 

doi: http://dx.doi.org/10.5599/admet.1078 73 

[47] I. Raad, R. Hachem, N. Leeds, R. Sawaya, Z. Salem, and S. Atweh. Use of adjunctive treatment with 
interferon-gamma in an immunocompromised patient who had refractory multidrug-resistant 
tuberculosis of the brain. Clinical Infectious Diseases 22(3) 1996 572–574. https://doi.org/10.1093/-
clinids/22.3.572.  

[48] A.A. Maslennikov, N.I. Obolonkova. Efficiency of Ingaron in the treatment of patients with destructive 
pulmonary bacteriologicaly proven tuberculosis. Research result. Medicine and pharmacy series 1(7) 
2016. https://doi.org/10.18413/2313-8955-2016-2-1-10-16.   

[49] R. Dawson, R. Condos, D. Tse, et al. Immunomodulation with recombinant interferon-gamma1b in 
pulmonary tuberculosis. PloS one 4(9) (2009) e6984. https://doi.org/10.1371/journal.pone.0006984.  

[50] M.S. Pisarenko. Pecularities of IFN-g secretion in drug-resistant pulmonary tuberculosis. Fundamental 
research 9 (2013) 444-447. 

[51] I.A. Vasilyeva, E.M. Belilovsky, S.E. Borisov, S.A. Sterlikov. Incidence, mortality and prevalence as 
indicators of tuberculosis burden in WHO regions, countries of the world and the Russian Federation. 
Part 2. Tuberculosis mortality. Tuberculosis and Lung Diseases 95(7) (2017) 8-16. 
https://doi.org/10.21292/2075-1230-2017-95-6-9-21.  

[52] T. Tanimura, E. Jaramillo, D. Weil, M. Raviglione, K. Lönnroth. Financial burden for tuberculosis 
patients in low- and middle-income countries: a systematic review. The European Respiratory Journal 
43(6) (2014) 1763-1775. https://doi.org/10.1183/09031936.00193413.  

[53] S.L. Plavinskiy, P.I. Shabalkin. Evaluation of the clinical and economic effectiveness of interferon-
gamma in the treatment of tuberculosis. Epidemiology and Infectious Diseases. Russian journal 22(6) 

(2017) 276-280. https://doi.org/10.17816/EID40981.  

[54] K.L. Chin, F.Z. Anis, M.E. Sarmiento, M.N. Norazmi, A. Acosta. Role of Interferons in the Development 
of Diagnostics, Vaccines, and Therapy for Tuberculosis. Journal of immunology research 2017 (2017) 
5212910. https://doi.org/10.1155/2017/5212910.  

[55] S. Anderson, V. Ansdell, P.M. Arguin, et al.. The Travel and Tropical Medicine Manual (Fifth Edition). 
Elsevier (2017) 646p. https://doi.org/10.1016/B978-0-323-37506-1.00061-1.  

[56] P. C. Hopewell, M. Kato-Maeda, J. D. Ernst. Murray and Nadel's Textbook of Respiratory Medicine 
(Sixth Edition). Elsevier (2016). https://doi.org/10.1016/B978-1-4557-3383-5.00035-X.  

[57] T. Togun, B. Kampmann, M. Pai. Diagnosis of Childhood Tuberculosis, Reference Module in 
Biomedical Sciences. Elsevier (2017). https://doi.org/10.1016/B978-0-12-801238-3.64157-0.  

[58] Y. Xu, B. Zhu, Q. Wang, et al. Recombinant BCG coexpressing Ag85B, ESAT-6 and mouse-IFN-gamma 
confers effective protection against Mycobacterium tuberculosis in C57BL/6 mice. FEMS Immunology 
and Medical Microbiology 51(3) (2007) 480–487. https://doi.org/10.1111/j.1574-695X.2007.00322.x.  

[59] G. C. K. W. Koh, M.F. Schreiber, R. Bautista, et al. Host responses to melioidosis and tuberculosis are 
both dominated by interferon-mediated signaling. PloS One 8(1) (2013) e54961. https://doi.org/10.-
1371/journal.pone.0054961.  

[60] S.H. Kaufmann, C. Lange, M. Rao, et al. Progress in tuberculosis vaccine development and host-
directed therapies – a state of the art review. The Lancet. Respiratory medicine 2(4) (2014) 301-320. 
https://doi.org/10.1016/S2213-2600(14)70033-5.  

 

 

 

 

 

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http://dx.doi.org/10.5599/admet.1078
https://doi.org/10.1093/clinids/22.3.572
https://doi.org/10.1093/clinids/22.3.572
https://doi.org/10.18413/2313-8955-2016-2-1-10-16
https://doi.org/10.1371/journal.pone.0006984
https://doi.org/10.21292/2075-1230-2017-95-6-9-21
https://doi.org/10.1183/09031936.00193413
http://www.medlit.ru/journalsview/infections/main/
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http://www.medlit.ru/journalsview/infections/view/journal/en/2017/issue-6/
https://doi.org/10.17816/EID40981
https://doi.org/10.1155/2017/5212910
https://www.sciencedirect.com/book/9780323375061/the-travel-and-tropical-medicine-manual
https://doi.org/10.1016/B978-0-323-37506-1.00061-1
https://doi.org/10.1016/B978-1-4557-3383-5.00035-X
https://doi.org/10.1016/B978-0-12-801238-3.64157-0
https://doi.org/10.1111/j.1574-695X.2007.00322.x
https://doi.org/10.1371/journal.pone.0054961
https://doi.org/10.1371/journal.pone.0054961
https://doi.org/10.1016/S2213-2600(14)70033-5
http://creativecommons.org/licenses/by/3.0/