Female Genital Tuberculosis Among Infertile 
Women and Its Contributions to Primary and 

Secondary Infertility
A systematic review and meta-analysis

*Musa A.E. Ahmed,1,3 Abdullah A.A. Mohammed,1,4 Abiodun O. Ilesanmi,2 Christopher O. Aimakhu,2
Amel O. Bakhiet,5,6 Suad B.M. Hamad7

Sultan Qaboos University Med J, August 2022, Vol. 22, Iss. 3, pp. 314–324, Epub. 25 Aug 22
Submitted 24 jul 21
Revision Req. 31 Oct 21; Revision Recd. 22 Nov 21
Accepted 6 Jan 22

Departments of 1Reproductive Health Sciences, Pan African University Life and Earth Sciences Institute (PAULESI) and 2Obstetrics & Gynecology, College of 
Medicine, University of Ibadan, Ibadan, Nigeria; 3Department of Veterinary Surgery, Faculty of Veterinary Medicine, Al-Salam University, West Kordofan, 
Sudan; 4Department of Biomedical Sciences, Faculty of Veterinary Sciences, University of Gadarif, Gadarif, Sudan; 5Department of Pathology, College of 
Veterinary Medicine and 6The Scientific Research Deanship, College of Veterinary Medicine, Sudan University of Science & Technology, Khartoum, Sudan; 
7Department of Animal Health & Diseases Control, Ministry of Animal Recourses & Fishers, South Kordofan, Sudan
*Corresponding Author’s e-mail: musasergo@gmail.com

Tuberculosis (tb) is an infectious disease caused by Mycobacterium tuberculosis which was recently listed among the top 10 diseases 
causing death around the world. According to the 
World Health Organization (WHO), 10.0 million 
people were infected with TB and there were 1.2 million 
TB deaths in 2019.1 Two-thirds of this global burden 
was present in eight countries – India, Indonesia, 
China, the Philippines, Pakistan, Nigeria, Bangladesh 
and South Africa.1 Female genital tuberculosis (FGTB) 
is commonly secondary to pulmonary TB (PTB) or 
extrapulmonary TB (EPTB), with an incidence rate 
ranging between 9–20% and 5–13% among overall 
EPTB and PTB cases worldwide according to many 
multitask studies, respectively.2–6 Typically, FGTB is 
known as a disease of young women (20–40 years old);5,7 
it is usually diagnosed during infertility evaluations.2,8 
A previous study indicated that the infertility rates in 
women is higher compared to men.9 Moreover, 76% of 
infertile women had a history of TB;10 infertility is the 
most frequent complaint of FGTB cases which occurs 
due to irreversible damage to the fallopian tube.4,11 In 
addition to infertility, other clinical presentations of 
FGTB include pelvic pain or menstrual irregularities, 
and it remains a major health problem in low-income 
countries.8,12 Organs commonly affected by FGTB are 

the fallopian tube (90%), ovaries (10–30%), endometrium 
(50%), cervix and vagina.3,13 Infertile FGTB patients 
have been reported to have a longer duration of 
infertility compared to infertility from other sources.14 

This meta-analysis was conducted to investigate 
the prevalence of FGTB among infertile women 
of reproductive age and to evaluate the incidence 
of primary and secondary infertility among FGTB 
patients around the globe.

Methods

e l i g i b i l i t y c r i t e r i a
Studies were eligible if they characterised the 
epidemiology of FGTB among women within 
reproductive age, if the study population was infertile 
women or at least indicated a proportion of infertility 
complaints with enough explanation of epidemiology 
of FGTB, were published in English, were published 
between 1971 to 17 July, 2021 and used the diagnostic 
methods of FGTB based on the particular infertility 
centres testing protocol. Articles were excluded if they 
were characterised as only PTB or EPTB regardless of 
FGTB and if the reported prevalence of FGTB was not 
that of infertile women.

REVIEW

This work is licensed under a Creative Commons Attribution-NoDerivatives 4.0 International License.

https://doi.org/10.18295/squmj.1.2022.003

abstract: Female genital tuberculosis (FGTB) is a widespread infectious disease among young women. This 
meta-analysis aimed to investigate the prevalence of FGTB among infertile women and its contribution to primary 
and secondary infertility. PubMed, MEDLINE®, WorldCat, The Lens, direct Google search, Google Scholar and 
ResearchGate were searched from 1971 to July 17, 2021 using the following terms: “prevalence”, “epidemiology”, 
“urogenital tuberculosis”, “FGTB”, “infertile women”, “infertility complaints” and “FGTB testing methods”. Data were 
extracted and a meta-analysis was performed. A total of 42 studies were selected with a total of 30,918 infertile women. 
Of these, the pooled prevalence of FGTB was 20% (95% confidence interval: 15–25%, I2 = 99.94%) and the prevalence 
of overall infertility, primary infertility and secondary infertility among FGTB population were 88%, 66% and 34%, 
respectively. The proportion of FGTB is remarkable among infertile women globally. The biggest burden of the disease 
is present in low-income countries followed by lower-to-middle- and upper-to-middle-income countries.

Keywords: Female Genital Tuberculosis; Female Infertility; Worldwide; Prevalence of FGTB; Mycobacterium 
Tuberculosis; Infertility.

https://creativecommons.org/licenses/by-nd/4.0/


Musa A.E. Ahmed, Abdullah A.A. Mohammed, Abiodun O. Ilesanmi, Christopher O. Aimakhu, 
Amel O. Bakhiet and Suad B.M. Hamad

Review | 315

i n f o r m at i o n s o u r c e s
This study was carried out in accordance with the 
guidelines of Preferred Reporting Items for Systematic 
Reviews and Meta-Analyses (PRISMA). Several 
electronic databases such as MEDLINE® (National 
Library of Medicine, Bethesda, Maryland, USA), 
WorldCat (OCLC, Inc., Dublin, Ohio, USA), The Lens 
(Cambia, Canberra, Australia) and PubMed (National 
Library of Medicine) were used to retrieve published 
articles. In addition, other search engines were 
intensively combed through including direct Google 
search (Google LLC, Mountain View, California, USA), 
Google Scholar (Google LLC) and ResearchGate, 
in order to retrieve studies that were not indexed in 
PubMed. All mentioned databases were searched from 
their commencement for the period between 1971 to 
July 17, 2021, for human studies published in English.

s e a r c h s t r at e g y
The Boolean search terms (AND, OR) were used to 
develop the research strategy to retrieve studies from 
PubMed and WorldCat. The final search strategy 
included the use of title/abstract related to ([Female 
genital tuberculosis] OR [urogenital tuberculosis]) 
AND ([prevalence] OR [epidemiology]) AND 
([infertile women] OR [infertility]). Manual searches 
were applied in a direct Google search, Google Scholar 
and ResearchGate for the same purpose.

s t u d y s e l e c t i o n p r o c e s s
All retrieved articles were first screened by title and 
abstract followed by a full-text screening. Then, 
eligible articles were exported to the Mendeley 
citation manager software (Elsevier, Amsterdam, 
the Netherlands), Version 1.19.8, to check for 
duplicates; all duplicated articles were removed. Two 
authors (AM and MA) screened and evaluated the 
remaining studies independently by a careful reading 
of the title and abstract followed by a full-text article 
screening if the particular records mentioned the 
outcomes of the review ‘Prevalence of Female genital 
tuberculosis among infertile women’ in their titles 
and abstract. However, the screened full-text articles 
were considered for further evaluation based on the 
objectives, methods, participants and key findings. 
The two authors (MA and AM) independently 
evaluated the quality of the studies using the PRISMA 
checklist.15 Any inconsistency for the included articles 
was resolved through discussion and by consulting an 
expert. The overall study selection process is presented 
using the PRISMA statement flow diagram [Figure 1].

d ata c o l l e c t i o n p r o c e s s 
The relevant data from selected articles were 
extracted by three investigators independently (AM, 
MA and SH) using a data extraction template by 
Microsoft Office Word, Version 2016 (Microsoft 
Corp., Redmond, Washington, USA). The extracted 
information included author name, year of publication, 
reference, study country, study design/setting, sample 
size, FGTB proportion among infertile women, the 
prevalence of overall infertility, primary infertility and 
secondary infertility among FGTB cases [Table 1]. The 
data extraction accuracy was verified by comparing 
the data extraction results by a second group of 
investigators (AB, AI and CA), who independently 
extracted the data in a randomly-selected subset of 
papers (30% of the total). The extracted quantitative 
data were summarised in a Microsoft Excel sheet 
(Microsoft Corp.). Based on the aim of this study, 
which is ‘to investigate the pooled prevalence of FGTB 
among infertile women globally’, the collected data 
was divided into four subgroups according to the 
World Bank economical classification. The prevalence 
of FGTB among infertile women and prevalence of 
pooled infertility (primary and secondary) among 
FGTB cases were calculated using STATA, Version 16 
(StataCorp LP, College Station, Texas, USA).

d ata i t e m s 
The main outcome of this study was the prevalence of 
FGTB among infertile women within reproductive age 
worldwide which is measured by the direct reports from 
individual studies. Out of these, 26 studies from India, 
three studies from Nigeria and two articles each from 
Ethiopia, South Africa and Pakistan were retrieved. 
Also, only one article each was retrieved from Egypt, 
Iraq, Iran, USA, Saudi Arabia, Sudan and Yemen. To 
quantify the outcome, the investigators considered 
studies that reported the prevalence of FGTB among 
infertile women and the types of TB regarding FGTB 
among gynaecology-admitted/infertile women in 
their statistics. The result was interpreted by the 
proportions of the infertile population having any type 
of FGTB from the total population studied.

s t u d y r i s k o f b i a s a s s e s s m e n t
Inclusion criteria were appraised for all retrieved 
articles by using the title and abstract; then, full-text 
articles were screened to check the quality of each 
study before final selection. The quality assessment 
criteria for the studies included in the current meta-
analysis and systematic review is as follows: (1) the 



Female Genital Tuberculosis Among Infertile Women and Its Contributions to Primary and Secondary Infertility 
A systematic review and meta-analysis

316 | SQU Medical Journal, August 2022, Volume 22, Issue 3

diagnosis of the infertility cases were performed at 
an infertility centre with consideration that infertility 
is defined as one year without conception after 
unprotected intercourse; (2) the infertility was not 
due to the male factor; (3) the diagnosis included an 
infertile population who tested for FGTB willingly; (4) 
the diagnosis of FGTB was conducted after excluding 
the patients with confirmed FGTB; and (5) the 
sample size was representative of the population. A 
comprehensive search including electronic databases, 
grey literature and unpublished studies was done 
in order to manage and minimise the risk of bias. 
Moreover, two groups of investigators (AM, MA 
and SH) and (AB, AI and CA) used the Joanna 
Briggs Institute Quality Assessment Tool as a critical 
appraisal tool.16 The differences in the inclusion of 
the studies were resolved by consensus. The included 
studies were evaluated against each indicator of the 
tool and categorised as high-, moderate- and low-
quality. Studies with a score ≥60% were included. The 
publication bias for the included studies was checked 
by both the visual inspection of the funnel plot and the 
statistical symmetry of the funnel plot using Egger’s 
regression test.

s u m m a r y m e a s u r e s
The proportion of FGTB among infertile women and 
proportion of the type of infertility among FGTB 
patients were used to synthesise and present the 
results for the analysis. 

s y n t h e s i s m e t h o d s
The collected data were synthesised and analysed in 
STATA (StataCorp LP). The recommendations of the 
I2 statistic described by Higgins et al. (an I2 of 75/100% 

and above suggests considerable heterogeneity) were 
used to perform this meta-analysis.17 The effect size, 
with a 95% confidence interval (CI) and standard error 
(SE), was used to calculate the results of this study. The 
effect size of this study was the prevalence of FGTB 
and the prevalence of the type of infertility subgroups; 
these were calculated using the binomial distribution. 
The SE was calculated using the sample size (n) and the 
proportion of FGTB (p) using the following equation:

Any potential publication bias was checked using 
a funnel plot and Egger’s regression test. Subgroup 
analysis was applied to check the potential source of 
heterogeneity and possible source of bias. Any study 
with missing data and/or a high risk of bias was 
excluded. P values were interpreted as statistically 
significant at a value of less than 0.10. The study results 
were reported according to the PRISMA guidelines 
and the findings were presented using a narrative 
synthesis followed by a meta-analysis chart.

Results

s t u d y s e l e c t i o n 
A total of 1,203 articles/records were identified. 
Of these, 961 articles/records were removed due 
to duplication and title screening resulting in 242 
articles/records for further inspection. Subsequently, 
another 180 articles were excluded after a very careful 
screening of abstracts. Therefore, a total of 62 articles 
were eligible for full-text screening; 20 articles of 
these were excluded due to inconsistency with the 
study inclusion criteria. Finally, 42 articles fulfilled 

√P(1–P) ÷ ɳ [Equation 1]

Figure 1: Flowchart showing the selection process for articles included in the current review.



Musa A.E. Ahmed, Abdullah A.A. Mohammed, Abiodun O. Ilesanmi, Christopher O. Aimakhu, 
Amel O. Bakhiet and Suad B.M. Hamad

Review | 317

Table 1: Characteristics of studies included in the current meta-analysis4–7,10,12,19,20,23–28,38–64

Author 
and year of 
publication

Study 
design/ 
setting

World Bank 
country 
income 

classification

Country Infertile 
population

FGTB testing 
method

n (%)

Proportion 
of FGTB

Proportion of infertility among 
FGTB patient

Overall 
infertility

PI SI

Chattopadhyay 
et al.38 (1986) 

CS/HA High-income Saudi 
Arabia

945 NA 40 (4.2) NA NA NA

Tal et al.39 
(2020)

PC/HC High-income USA 323 QuantiFERON-
TB

25 (7.7) NA NA NA

Abdissa et al.4 
(2018)

CS/HA Low-income Ethiopia 152 PCR, CP, HE 8 (5.3) 5 (62.5) 4 (50) 1 (12.5)

Abebe et al.13 
(2004)

CS/HA Low-income Ethiopia 25 AFB, CP, HE, 
PCR

16 (64) NA NA NA

Ali and 
Abdallah40 
(2012)

CS/HA Low-income Sudan 2,778 HE 25 (0.9) NA NA NA

Abdelrub and 
Al Harazi41 
(2015)

P/O/HA Low-income Yemen 151 AFB, PCR, CP, 
HE

47 (31.1) NA NA NA

Nezar et al.42 
(2009)

P/O/HA Lower-middle 
income

Egypt 420 Laparoscopy, 
HE, PCR

24 (5.7) 24 (100) NA NA

Kumar et al.6 
(2008)

CS/HA Lower-middle 
income

India 285 PCR 111 (39) 111 (100) NA NA

Mohakul et al.5 
(2015)

P/HC Lower-middle 
income

India 105 PCR, 
hysteroscopy

41 (39) 41 (100) 24 (58) 17 (42)

Jindal10 (2006) R/HC Lower-middle 
income

India 2,083 LAP, AFB, HE, 
MT, ELISA

10 (7.2) 146 (97.3) 105 
(70)

41 (27.3)

Singh et al.43 
(2008

R/HC Lower-middle 
income

India 140 MH, 
laparoscopy, 
hysteroscopy

34 (48.5) NA NA NA

Sankar et al.44 
(2013)

R/HA Lower-middle 
income

India 620 AFB, PCR, CP, 
HE

158 (25.5) 151 (95.5) 119 
(78.8)

32 (21.2)

Mahajan et al.45 
(2016)

CS/HA Lower-middle 
income

India 180 PCR, CP 74 (41) NA NA NA

Sethi et al.46 
(2016)

CS/HA Lower-middle 
income

India 300 AFB, PCR, CP, 
HE

68 (22.7) NA NA NA

Chatterjee et 
al.65 (2018)

CS/HA Lower-middle 
income

India 120 PCR 2 (1.7) NA NA NA

Chowdhury et 
al.47 (2010)

CO/HA Lower-middle 
income

India 517 PCR 230 (44.5) 114 (49.7) NA NA

Saraswat et al.48 
(2010)

CS/HA Lower-middle 
income

India 125 PCR, CP 26 (20.8) NA NA NA

Malhotra et 
al.49 (2012)

O/HA Lower-middle 
income

India 555 AFB, PCR, CP 140 (25.22) NA NA NA

GajBhIye et 
al.50 (2019)

CS/O/HA Lower-middle 
income

India 50 PCR 6 (12) 5 (83.3) 4 (80) 1 (20)

Bhanothu et 
al.51 (2014)

P/CC/HA Lower-middle 
income

India 302 PCR 86 (28.47) NA NA NA

Gurjar et al.20 
(2018)

O/HA Lower-middle 
income

India 100 PCR 52 (52) NA NA NA

FGTB = female genital tuberculosis; PI = primary infertility; SI = secondary infertility; CS = cross-sectional study; HA = hospital admitted patients; NA = Not available; 
PC = prospective cohort study; HC = infertility centre admitted patient; PCR = polymerase chain reaction test; CP = culture proven; HE = histopathological examination; 
AFB = acid-fast bacilli test ; P = prospective study; O = observational study; R = retrospective study; LAP = laparotomy; MT = Mantoux test ; ELISA = enzyme-linked 
immunosorbent assay; MH = menstrual history; CC = case control study; MTD= Mycobacterium Tuberculosis Direct test ; CBNAAT = cartridge based nucleic acid 
amplification test; ZN = Ziehl-Neelsen (ZN) smear microscopy. 



Female Genital Tuberculosis Among Infertile Women and Its Contributions to Primary and Secondary Infertility 
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318 | SQU Medical Journal, August 2022, Volume 22, Issue 3

Table 1 (cont’d.): Characteristics of studies included in the current meta-analysis4–7,10,12,19,20,23–28,38–64

Author 
and year of 
publication

Study 
design/ 
setting

World Bank 
country 
income 

classification

Country Infertile 
population

FGTB testing 
method

n (%)

Proportion 
of FGTB

Proportion of infertility among 
FGTB patient

Overall 
infertility

PI SI

Patil et al.52 
(2015)

CS/HA Lower-middle 
income

India 123 Gen-Probe 
MTD test

1 (0.8) NA NA NA

Goel et al.53 
(2013)

R/HA Lower-middle 
income

India 546 PCR 20 (3.7) NA NA NA

Kamal et al.54 
(2020)

P/HA Lower-middle 
income

India 100 PCR, HE 27 (27) NA 16 
(59.4)

11 (40.6)

Kanti V et al.55 
(2021)

P/HC Lower-middle 
income

India 59 CBNAAT, HE 2 (3.4) NA 2 (100) 0

Meenu et al.56 
(2020)

CS/HA Lower-middle 
income

India 139 PCR 58 (41.7) NA NA NA

Shende et al.57 
(2017)

P/HA Lower-middle 
income

India 120 PCR 32 (27) NA NA NA

Shrivastava & 
Patel7 (2014)

P/HC Lower-middle 
income

India 218 AFB, CP, HE, 
PCR

86 (39.45) NA NA NA

Ohri et al.58 
(2016)

P/HA Lower-middle 
income

India 50 PCR 9 (18) NA 8 
(88.9)

1 (11.1)

Parikh et al.59 
(2014)

P/HA Lower-middle 
income

India 50 PCR 6 (12) NA 3 (50) 3 (50)

Gupta et al.60 
(2007)

R/HA Lower-middle 
income

India 150 AFB, MT, PCR 40 (26.7) NA 30 (75) 10 (25)

Rajaram et al.61 
(2016)

PC/HA Lower-middle 
income

India 50 HE, PCR 14 (28) NA NA NA

Ojo et al.19 
(2008)

R/HA Lower-middle 
income

Nigeria 661 AFB, HE 3 (0.45) NA 1 
(33.3)

2 (66.7)

Ojo et al.23 
(1971)

CS/HA Lower-middle 
income

Nigeria 11,896 HE 82 (0.7) NA NA NA

Emembolu28 
(1989)

R/HA Lower-middle 
income

Nigeria 114 AFB 19 (16.7) NA 9 
(47.4)

10 (52.6)

Gini and 
Ikerionwu24 
(1990)

R/HA Lower-middle 
income

Nigeria 4,700 HE 10 (0.2) NA NA NA

Shahzad62 
(2012)

R/HA Lower-middle 
income

Pakistan 150 AFB, PCR, CP 30 (20) NA 25 
(83.3)

5 (16.7)

Shaheen et al.63 
(2009)

CS/HA Lower-middle 
income

Pakistan 534 CP, AFB-ZN, 
HE

13 (2.43) 13 (100) NA NA

Khan25 (1985) R/HA Upper-middle 
income

Iran 91 LAP, HE 21 (23.08) NA 15 
(71.4)

6 (28.6)

Shallal et al.64 
(2021)

PC/HA Upper-middle 
income

Iraq 60 PCR, HE 6 (10) NA NA NA

Margolis et al.26 
(1992)

R/HA Upper-middle 
income

South 
Africa

650 CP 40 (6.15) NA 16 (40) 24 (60)

Oosthuizen et 
al.27 (1990)

CS/HA Upper-middle 
income

South 
Africa

109 CP 23 (21) NA NA NA

FGTB = female genital tuberculosis; PI = primary infertility; SI = secondary infertility; CS = cross-sectional study; HA = hospital admitted patients; NA = Not available; PC = 
prospective cohort study; HC = infertility centre admitted patient; PCR = polymerase chain reaction test; CP = culture proven; HE = histopathological examination; AFB = acid-fast 
bacilli test; P = prospective study; O = observational study; R = retrospective study; LAP = laparotomy; MT = Mantoux test; ELISA = enzyme-linked immunosorbent assay; 
MH = menstrual history; CC = case control study; MTD= Mycobacterium Tuberculosis Direct test; CBNAAT = cartridge based nucleic acid amplification test; ZN = Ziehl-
Neelsen (ZN) smear microscopy. 



Musa A.E. Ahmed, Abdullah A.A. Mohammed, Abiodun O. Ilesanmi, Christopher O. Aimakhu, 
Amel O. Bakhiet and Suad B.M. Hamad

Review | 319

the eligibility criteria (total of 30,846 participants with 
mainly infertility complaints) were included for the 
systematic review and meta-analysis [Figure 1].

s t u d y c h a r a c t e r i s t i c s
A total of 42 studies, including 30,846 participants 
were included in the quantitative analysis for this 
meta-analysis; 2 (4.8%) studies were from high-income 
countries, 4 (9.5%) from upper-middle-income 
countries, 32 (76.2%) from lower-middle-income 
countries and the remaining 4 (9.5%) were from low-
income countries. Of the included studies, 17 were 
cross-sectional studies, 13 had a prospective study 
design and 12 were retrospective studies. The majority 
of studies were in hospital-admitted patient settings 
and most used diagnostic tests (only polymerase chain 
reaction [PCR] or PCR combined with other relevant 
test methods) [Table 1].

s y n t h e s i s o f r e s u lt s
Out of the included study sample of 30,846 participants 
worldwide, there was a 20% (95% confidence interval 
[CI]: 15–25%) pooled prevalence of FGTB among 
infertile women. Residual heterogeneity was high (I2 
= 99.94, χ2 = 2553.37; P <0.001). For this analysis, the 
random effect model was employed [Figure 2].

However, out of the 42 articles, only five, 15 
and 14 articles were analysed to evaluate the pooled 
prevalence of overall infertility, primary and secondary 
infertility among FGTB patients, respectively; this 
resulted in a pooled prevalence rate of 88% (95% CI: 
74–100%, I2 = 99.91), 66% (95% CI: 56–76%, I2 = 99.23) 
and 34% (95% CI: 24–43%, I2 = 98.04) and P <0.001 
each [Table 2]. In addition, the random effect model 
was applied because the heterogeneity was high with 
P <0.001. The publication bias was checked using the 
funnel plot of the forest plot and the plot was visually 
symmetric with Egger’s test (P = 0.25). 

Due to the very high heterogeneity level 
presented in FGTB among infertile women in this 
analysis, a two-subgroup analysis was performed to 
check the effect of the study’s publication year and 
the World Bank Economical Country Classification 
on the pooled prevalence of FGTB among the infertile 
population [Table 3]. The included studies were divided 
as per the particular country’s classification (i.e. high-
income, upper-middle-income, lower-middle-income 
and low-income groups). The analysed data showed 
that the lowest income countries have a higher pooled 
prevalence of FGTB; conversely, the highest income 
countries have a lower pooled prevalence of FGTB 
among infertile women. The results showed pooled 
proportions of 5.7% (I2 = 78.56%), 14% (I2 = 86.91%), 

21% (I2 = 99.95%) and 24% (I2 = 99.48%) for high-
income, upper-middle-income, lower-middle-income 
and low-income countries, respectively [Table 2].

To evaluate the effect of the study’s publication 
year on the pooled prevalence of FGTB among infertile 
women, the included articles were divided into three 
groups. The results indicated a 10%, 23% and 22% 
pooled prevalence of FGTB among infertile women 
for the period before 2000, between 2001 to 2010 and 
between 2011 to 2021 of this study’s publication year 
subgroups, respectively [Table 2]. 

Discussion

Although men significantly have the bigger burden of 
TB compared to women, in 2018, the WHO estimated 
that 3.2 million women were infected with TB and the 
disease is accompanied with severe consequences, 
especially in women of reproductive age.18 Although 
FGTB rarely occurs in developed countries,3 it 
represents an important cause of infertility in 
developing countries especially in countries with high 
TB-incidence rates.18 

Recently, many published studies have invest- 
igated the prevalence of FGTB among infertile women 
of reproductive age which shows that the lowest 
prevalence was 0.45% in Nigeria and the highest 
prevalence was 52% in India.19,20 Worldwide, the 
prevalence was 24.2% in the first-published meta-
analysis and systematic review in 2016.21 The current 
study’s finding shows this prevalence to be slightly less 
at 20%. This outcome is due to the relative progress 
in the availability of more sensitive TB diagnosis 
methods such as GeneXpert and PCR in developing 
countries. Moreover, there is a relative increase in the 
number of TB healthcare services and many countries 
have adopted the WHO’s End TB Strategy around the 
globe.22

In the current comprehensive research, the 
prevalence of FGTB among infertile women progr- 
essively increased over time from 10%, 23% and 22% 
in the period before 2000, between 2001 to 2010 and 
between 2011 to 2021, respectively. This may be due 
to the differences in the diagnostic methods used for 
FGTB which have changed over time. Surprisingly, 
the researchers noted that the PCR test was not used 
in studies published in the period before 2000 while 
the same diagnosis method was used by 70% and 
80.8% studies for the period between 2001 to 2010 
and 2011 to 2021, respectively. The utilised diagnostic 
methods in the analysed data were histopathological 
examination,23–25 culture,26,27 acid-fast bacilli test and 
laparotomy.25,28 According to the literature, there is 



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A systematic review and meta-analysis

320 | SQU Medical Journal, August 2022, Volume 22, Issue 3

Author and year of publication Effect size 
(95% CI)

Weight 
in %

Ojo et al.23 (1971) 0.01 (0.01–0.01) 2.49

Gini and Ikerionwu24 (1990) 0.00 (0.00–0.00) 2.49

Emembolu28 (1989) 0.17 (0.10–0.24) 2.37

Khan25 (1985) 0.23 (0.14–0.32) 2.31

Margolis et al.26 (1992) 0.05 (0.04–0.08) 2.48

Oosthuizen et al.27 (1990) 0.21 (0.13–0.29) 2.36

Chattopadhyay et al.38 (1986) 0.04 (0.03–0.05) 2.48

Ali and Abdallah40 (2012) 0.01 (0.01–0.01) 2.49

Abebe et al.13 (2004) 0.54 (0.45–0.83) 1.82

Jindal10 (2006) 0.07 (0.05–0.08) 2.49

Shaheen et al.63 (2009) 0.02 (0.01–0.04) 2.48

Ojo et al.19 (2008) 0.00 (-0.00–0.01) 2.49

Gupta et al.60 (2007) 0.27 (0.20–0.34) 2.37

Singh et al.43 (2008) 0.48 (0.40–0.57) 2.32

Nezar et al.42 (2009) 0.05 (0.03–0.08) 2.48

Kumar et al.6 (2008) 0.39 (0.33–0.45) 2.41

Chowdhury et al.47 (2010) 0.45 (0.40–0.49) 2.44

Saraswat et al.48 (2010) 0.21 (0.14–0.28) 2.36

Abdissa et al.4 (2018) 0.05 (0.02–0.09) 2.46

Abdelrub and Al Harazi41 (2015) 0.31 (0.24–0.38) 2.36

Mohakul et al.5 (2015) 0.39 (0.30–0.48) 2.28

Shahzad62 (2012) 0.20 (0.14–0.25) 2.39

Sankar et al.44 (2013) 0.25 (0.22–0.29) 2.46

Goel et al.53 (2013) 0.04 (0.02–0.05) 2.48

Malhotra et al.49 (2012) 0.25 (0.22–0.29) 2.46

Patil et al.52 (2015) 0.01 (-0.01–0.02) 2.48

Shrivastava and Patel7 (2014) 0.39 (0.33–0.45) 2.38

Parikh KP et al.59 (2014) 0.12 (0.03–0.21) 2.30

Bhanothu et al.51 (2014) 0.28 (0.23–0.34) 2.42

Mahajan et al.45 (2016) 0.41 (0.34–0.48) 2.36

Sethi et al.46 (2016) 0.23 (0.18–0.27) 2.43

GajBhIye et al.50 (2019) 0.12 (0.03–0.21) 2.30

Kamal et al.54 (2020) 0.27 (0.18–0.36) 2.31

Shende et al.57 (2017) 0.27 (0.19–0.35) 2.34

Ohri et al.58 (2016) 0.18 (0.07–0.29) 2.23

Chatterjee et al.65 (2018) 0.02 (-0.01–0.04) 2.48

Gurjar et al.20 (2018) 0.52 (0.42–0.52) 2.26

Kanti et al.55 (2021) 0.03 (-0.01–0.08) 2.43

Meenu et al.56 (2020) 0.42 (0.34–0.50) 2.33

Rajaramet al.61 (2016) 0.28 (0.15–0.40) 2.14

Shallal et al.64 (2021) 0.10 (0.02–0.18) 2.36

Tal et al.39 (2020) 0.08 (0.05–0.11) 2.47

Overall 0.20 (0.15–0.25)

Heterogeneity: τ2 = 0.02, I2 = 99.94%, H2 = 1745.13

Test of θ1 = θ1: Q(41) = 2553.37; P = 0.00
Test of θ = θ: z = 7.94; P = 0.00

Figure 2: Forest plot (random-effects model) showing the pooled prevalence of female genital tuberculosis among 
infertile women.4–7,10,13,19,20,23–28,38–65
CI = confidence interval. 



Musa A.E. Ahmed, Abdullah A.A. Mohammed, Abiodun O. Ilesanmi, Christopher O. Aimakhu, 
Amel O. Bakhiet and Suad B.M. Hamad

Review | 321

no gold-standard test for FGTB as this depends on 
the facilities’ test protocol. However, different FGTB 
testing methods have been providing various results of 
the disease rate among infertile women.20 The increase 
of the prevalence of FGTB among infertile women is 
due to the previously mentioned reasons, including 
utilisation of modern TB diagnosis methods and 
adopting the WHO’s End TB Strategy.18 Furthermore, 
the global funds on TB control have substantially 
increased in recent decades.29 

The present study reveals that the prevalence 
of FGTB is inversely proportional to the economic 
situation of the country. The lowest prevalence was 
5.7% in the high-income countries while the highest 
prevalence was 24% in the low-income countries. 
The upper-middle-income and lower-middle-income 
countries showed 14% and 22%, respectively. Although, 
there was no published data to describe the rate of 
FGTB among infertile women in different countries 
based on their economic status, other studies have 
shown that FGTB is associated with PTB and EPTB 
as secondary infections.2,3 This outcome may be due 
to the delay of TB diagnosis and other sociocultural 
reasons. In line with this, Getnet et al. reported that 
42% of PTB diagnoses were delayed for a varied period 

of time (a month to a year) in low-income and middle-
income countries’ setting.30 Furthermore, MacPherson 
et al. indicated that 4–38% of TB-patients were lost to 
follow-up for treatment in the same setting.31 In the 
Middle East and North Africa, factors such as being 
female and having a low income per capita is relatively 
reflected in the delay of TB diagnosis;32 although, the 
proportions are 1.24% and 1.26%, respectively, it has 
considerable impact on FGTB incidence. In addition, 
the high incidence of FGTB in low- and middle-
income settings is due to factors such as the higher 
rate of losses to follow-up with TB or EPTB treatment 
and the relatively negative experiences of TB patients 
and their level of satisfaction with their healthcare 
system.33,34 Moreover, poverty and the high cost of the 
accurate diagnosis of FGTB in developing countries 
have a largely negative effect on FGTB control and 
treatment.35,36 In accordance with this, Cazabon et 
al. reported that 32% and 46% of TB patients had 
a negative experience and were dissatisfied with 
healthcare providers and TB services, respectively.34 

The findings of the current study reveal that the 
pooled prevalence of infertility among overall FGTB-
patients was very high (88%). Of this, the pooled 
prevalence of primary infertility was higher than 

Table 2: Pooled prevalence of infertility among female genital tuberculosis (FGTB) patients, pooled proportion of FGTB 
among infertile women based on the World Bank country economic classification and subgroup analysis of FGTB among 
infertile women based on year of publication*

Subgroup classification Subgroup Number 
of studies

Total 
number 

of 
patients

FGTB 
proportion 

in % 
(95% CI)

Infertility 
proportion 

in % 
(95% CI)

Heterogeneity

I2 in % P value

Type of infertility (among FGTB 
patients)

Pooled 
infertility

5 430 - 88 (74–100) 99.912 >0.001

Primary 
infertility

15 560 - 66 (56–76) 99.226 >0.001

Secondary 
infertility

14 558 - 34 (24–43) 98.039 >0.001

World Bank country economic 
classification (among infertile 
patients)

High 
income

2 1268 5.7 (2.3-9.1) - 78.56 >.001

Upper-
middle 
income 

4 910 14 (6–23) - 86.91 >0.001

Lower-
middle 
income 

32 25,562 21 (15–27) - 99.95 >0.001

Low 
income 

4 3,106 24 (3–52) - 99.48 0.084

Year of publication
(among infertile patients)

<2000 7 18,530 10 (3–17) - 99.96 <0.001

2001–2010 11 7,718 23 (10–36) - 99.93 <0.001

2011–2021 24 4,623 22 (16–27) 97.98 <0.001

FGTB = female genital tuberculosis; CI = confidence interval.
*Out of 42 studies 34 were analysed for type of infertility (subgroup among FGTB patients) and the remaining studies were excluded as there was no 
mention of the prevalence of infertility, primary infertility or secondary infertility.



Female Genital Tuberculosis Among Infertile Women and Its Contributions to Primary and Secondary Infertility 
A systematic review and meta-analysis

322 | SQU Medical Journal, August 2022, Volume 22, Issue 3

that of secondary infertility among FGTB patients. 
Although these results are in agreement with other 
meta-analysis findings done by Chaman-Ara et al. 
(who reported 70.7%, 75.7% and 24.3% for infertility 
among FGTB patients, primary infertility and 
secondary infertility, respectively), the present study 
showed a slight increase in the pooled prevalence 
infertility and secondary infertility incidence among 
FGTB patients. On the other hand, the rate of primary 
infertility decreased over time.37 

To achieve the WHO End TB Strategy goal to 
eliminate catastrophic costs for TB-affected households 
by 2030 as Sustainable Development Goal target, a 
more thorough clinical investigation should be admin- 
istrated at the level of TB and infertility clinics, 
particularly in low- and lower-income settings.18

This review is subject to certain limitations. 
Articles published in languages other than English 
were excluded and the study population included 
only infertile women of reproductive age. Some grey 
literature may have also been missed. During the data 
collection process, no published studies investigating 
the incidence of FGTB among infertile women from 
the continents of Australia, Europe or South America 
were found. The likelihood for publication bias is high.

Conclusion

The results of this meta-analysis found that the pooled 
prevalence of FGTB among infertile women is 20%, 
and the pooled prevalence of overall infertility, primary 
infertility and secondary infertility among FGTB 
patients globally is 88%, 66% and 34%, respectively. 
In the last two decades, the FGTB incidence rate was 
increasing gradually. The biggest burden of FGTB 
is reported in the low- and lower-middle-income 
countries with a pooled prevalence of 46% globally.

a c k n o w l e d g e m e n t s

The authors would like to thank the Pan African 
University, Institute Life and Earth Sciences (Including 
Health and Agriculture), the African Union for 
financial support and University of Ibadan for hosting 
this Ph.D. programme. 

a u t h o r s’ c o n t r i b u t i o n s
MA, AM, AI, CA, AB and SH conceived and designed 
the review. MA, AM and SH carried out the draft 
of the manuscript and MA is the guarantor of the 
review. MA, AM, AI, CA, AB and SH developed the 
search strings. MA, AM and SH screened, evaluated 
and selected the studies as well as extracted the data. 
AI, CA and AB evaluated the quality of the studies. 

MA and AM carried out the statistical analysis and 
interpretation. MA, AM, AI, CA, AB and SH rigorously 
reviewed the manuscript. All authors approved the 
final version of the manuscript. 

References
1. World Health Organization. Global tuberculosis report 2020. 

From: https://www.who.int/publications/i/item/9789240013131

2. Grace GA, Devaleenal DB, Natrajan M. Genital tuberculosis 
in females. Indian J Med Res 2017; 145:425–36. https://doi.
org/10.4103/ijmr.IJMR_1550_15.

3. Parvez R, Sugunan AP, Vijayachari P, Burma SP, Mandal A, 
Saha MK, et al. Prevalence of female genital tuberculosis, its 
risk factors and associated clinical features among the women 
of Andaman Islands, India: A community-based study. Public 
Health 2017; 148:56–62. https://doi.org/10.1016/j.puhe.2017.03.001.

4. Abdissa S, Abebe T, Ameni G, Teklu S, Bekuretsion Y, Abebe M, 
et al. Endometrial tuberculosis among patients undergoing 
endometrial biopsy at Tikur Anbesa specialized hospital, Addis 
Ababa, Ethiopia. BMC Infect Dis 2018; 18:1–8. https://doi.
org/10.1186/s12879-018-3202-x.

5. Mohakul SK, Beela VRK, Tiru P. Hysteroscopy findings and its 
correlation with latent endometrial tuberculosis in infertility. 
Gynecological Surgery 2015; 12:31–9. https://doi.org/10.1007/
s10397-014-0865-1.

6. Kumar P, Shah NP, Singhal A, Chauhan DS, Katoch VM, Mittal S, 
et al. Association of tuberculous endometritis with infertility 
and other gynecological complaints of women in India. J Clin 
Microbiol 2008; 46:4068–70. https://doi.org/10.1128/JCM.01162-08.

7. Shrivastava G, Patel K. Genital tuberculosis: Evaluating 
microscopy, culture, histopathology and PCR for diagnosis all 
play their role. Int J Curr Microbiol App Sci 2014; 3:439–45.

8. Fatima T, Hasan R, Malik FR, Ahmed I, Bartlett LA, Gravett MG, 
et al. Female genital tuberculosis in Pakistan – A retrospective 
review of 10-year laboratory data and analysis of 32 cases. Int 
J Mycobacteriol 2021; 10:66–70. https://doi.org/10.4103/ijmy.
ijmy_6_21.

9. A AA, Ahmed M, Oladokun A. Prevalence of infertility in 
Sudan: A systematic review and meta-analysis. Qatar Med J 
2021; 2021:47. https://doi.org/10.5339/qmj.2021.47.

10. Jindal UN. An algorithmic approach to female genital tuber- 
culosis causing infertility. The Int J Tuberc Lung Dis 2006; 
10:1045–50.

11. Namavar Jahromi B, Parsanezhad ME, Ghane-Shirazi R. Female 
genital tuberculosis and infertility. Int J Gynaecol Obstet 2001; 
75:269–72. https://doi.org/10.1016/s0020-7292(01)00494-5.

12. Bhanothu V, Theophilus JP, Reddy PK, Rozati R. Occurrence 
of female genital tuberculosis among infertile women: a study 
from a tertiary maternal health care research centre in South 
India. Europ Eur J Clin Microbiol Infect Dis 2014; 33:1937–49. 
https://doi.org/10.1007/s10096-014-2164-1.

13. Abebe M, Lakew M, Kidane D, Lakew Z, Kiros K, Harboe, et al. 
Female genital tuberculosis in Ethiopia. Int J Gynaecol Obstet 
2004; 84:241–6. https://doi.org/10.1016/j.ijgo.2003.11.002.

14. Dai W, Ma L, Cao Y, Wu D, Yu T, Zhai J. In vitro fertilization 
outcome in women with endometrial tuberculosis and tubal 
tuberculosis. Gynecol Endocrinol 2020; 36:819–823. https://
doi.org/10.1080/09513590.2019.1702639.

15. Liberati A, Altman DG, Tetzlaff J, Mulrow C, Gøtzsche PC, 
Ioannidis JP, et al. The PRISMA statement for reporting systematic 
reviews and meta-analyses of studies that evaluate health care 
interventions: Explanation and elaboration. J Clin Epidemiol 
2009; 62:e1–34. https://doi.org/10.1016/j.jclinepi.2009.06.006.

https://doi.org/10.4103/ijmr.IJMR_1550_15
https://doi.org/10.4103/ijmr.IJMR_1550_15
https://doi.org/10.1016/j.puhe.2017.03.001
https://doi.org/10.1186/s12879-018-3202-x
https://doi.org/10.1186/s12879-018-3202-x
https://doi.org/10.1007/s10397-014-0865-1
https://doi.org/10.1007/s10397-014-0865-1
https://doi.org/10.1128/JCM.01162-08
https://doi.org/10.4103/ijmy.ijmy_6_21
https://doi.org/10.4103/ijmy.ijmy_6_21
https://doi.org/10.5339/qmj.2021.47
https://doi.org/10.1016/s0020-7292(01)00494-5
https://doi.org/10.1007/s10096-014-2164-1
https://doi.org/10.1016/j.ijgo.2003.11.002
https://doi.org/10.1080/09513590.2019.1702639
https://doi.org/10.1080/09513590.2019.1702639
https://doi.org/10.1016/j.jclinepi.2009.06.006


Musa A.E. Ahmed, Abdullah A.A. Mohammed, Abiodun O. Ilesanmi, Christopher O. Aimakhu, 
Amel O. Bakhiet and Suad B.M. Hamad

Review | 323

16. Porritt K, Gomersall J, Lockwood. Study selection and critical 
appraisal: the steps following the literature search in a systematic 
review. CJAJN 2014; 114:47–52. https://doi.org/10.1097/01.
NAJ.0000450430.97383.64.

17. Higgins JPT, Thompson SG, Deeks JJ, Altman DG. Measuring 
inconsistency in knowledgebases. BMJ 2003; 327:557–60. 
https://doi.org/10.1136/bmj.327.7414.557.

18. World Health Organization. Global tuberculosis report 2018. 
From: https://www.who.int/publications/i/item/9789241565646

19. Ojo BA, Akanbi AA, Odimayo MS, Jimoh AK. Endometrial 
tuberculosis in the Nigerian middle belt: An eight-year review. 
Trop Doc 2008; 38:3–4. https://doi.org/10.1258/td.2007.052090.

20. Gurjar K, Meena KL, Rajoria L, Sharma N. Comparison of 
diagnostic efficacy of USG, Tuberculin test, Nucleic acid 
amplification test (PCR) & histopathology for diagnosis of 
genital tuberculosis in infertile women, assuming culture as 
gold standard. IMJH 2018; 4:138–43.

21. Chaman-Ara K, Bahrami MA, Bahrami E, Bahrami S, Bahrami MN, 
Moosazadeh M, et al. Prevalence of genital tuberculosis among 
infertile women: A systematic review and meta-analysis. Int J 
Med Res Health Sci 2016; 5:208–15. 

22. World Health Organization. Framework for implementing the 
“End TB Strategy” in the African Region 2016 - 2020. From: 
https://www.afro.who.int/publications/framework-implem 
enting-end-tb-strategy-african-region-2016-2020

23. Ojo OA, Onifade A, Akande EO, Bannerman RH. The pattern of 
female genital tuberculosis in Ibadan. Isr J Med Sci 1971; 7:280–7.

24. Gini PC, Ikerionwu SE. Incidental tuberculous endometritis 
in premenstrual curettings from infertile women in Eastern 
Nigeria. Int J Gynaecol Obstet 1990 ;31:141–4. https://doi.
org/10.1016/0020-7292(90)90711-s.

25. Khan SM. Incidence of genital tuberculosis in infertile women. 
J Pak Med Assoc 1985; 35:280–1. 

26. Margolis K, Wranz PA, Kruger TF, Joubert JJ, Odendaal HJ. 
Genital tuberculosis at Tygerberg Hospital--prevalence, clinical 
presentation and diagnosis. S Afr Med J 1992; 81:12–15.

27. Oosthuizen AP, Wessels PH, Hefer JN. Tuberculosis of the 
female genital tract in patients attending an infertility clinic. S 
Afr Med J 1990; 77:562–4.

28. Emembolu JO. Endometrial flora of infertile women in Zaria, 
Northern Nigeria. Int J Gynecol Obstet 1989; 30:155–9. https://
doi.org/10.1016/0020-7292(89)90310-x.

29. Floyd K, Fitzpatrick C, Pantoja A, Raviglione M. Domestic 
and donor financing for tuberculosis care and control in low-
income and middle-income countries: an analysis of trends, 
2002–11, and requirements to meet 2015 targets. Lancet 
Glob Health 2013; 1:e105–15. https://doi.org/10.1016/S2214-
109X(13)70032-9.

30. Getnet F, Demissie M, Assefa N, Mengistie B, Worku A. Delay 
in diagnosis of pulmonary tuberculosis in low-and middle-
income settings: Systematic review and meta-analysis. BMC 
Pulm Med 2017; 17:1–15. https://doi.org/10.1186/s12890-017-
0551-y.

31. MacPherson P, Houben RMGJ, Glynn JR, Corbett EL, Kranzer K. 
Pre-treatment loss to follow-up in tuberculosis patients in low- 
and lower-middle-income countries and high-burden countries 
A systematic review and meta-analysis. Bull World Health Organ 
2013; 92:126–38. https://doi.org/10.2471/BLT.13.124800.

32. Eltayeb D, Pietersen E, Engel M, Abdullahi L. Factors associated 
with tuberculosis diagnosis and treatment delays in Middle East 
and North Africa: A systematic review. East Mediterr Health J 
2020; 26:477–86. https://doi.org/10.26719/2020.26.4.477.

33. Ade S, Harries AD, Trébucq A, Ade G, Agodokpessi G, 
Adjonou C, et al. National profile and treatment outcomes of 
patients with extrapulmonary tuberculosis in Bénin. PLoS One 
2014; 9:e95603. https://doi.org/10.1371/journal.pone.0095603.

34. Cazabon D, Pande T, Sen P, Daftary A, Arsenault C, Bhatnagar H, 
et al. User experience and patient satisfaction with tuberculosis 
care in low-and middle-income countries: a systematic review. 
J Clin Tuberc Other Mycobact Dis 2020; 19:100154. https://doi.
org/10.1016/j.jctube.2020.100154.

35. Lu C, Liu Q, Sarma A, Fitzpatrick C, Falzon D, Mitnick CD. A 
systematic review of reported cost for smear and culture tests 
during multidrug-resistant tuberculosis treatment. PLoS One 
2013; 8:e56074. https://doi.org/10.1371/journal.pone.0056074.

36. Lund C, De Silva M, Plagerson S, Cooper S, Chisholm D, Das J, 
et al. Poverty and mental disorders: Breaking the cycle in low-
income and middle-income countries. Lancet 2011; 378:1502–14. 
https://doi.org/10.1016/S0140-6736(11)60754-X.

37. Chaman-Ara K, Bahrami MA, Moosazadeh M, Bahrami E. 
Prevalence of infertility in women with genital tuberculosis: 
a systematic review and meta-analysis. IJBS 2017; 11:21–7. 
https://doi.org/10.15562/ijbs.v11i1.133.

38. Chattopadhyay SK, Sengupta BS, Edrees YB, Al-Meshari AA. 
The pattern of female genital tuberculosis in Riyadh, Saudi 
Arabia. Br J Obstet Gynaecol 1986; 93:367–71. 

39. Tal R, Lawal T, Granger E, Simoni M, Hui P, Buza N, et al. 
Genital tuberculosis screening at an academic fertility center 
in the United States. Am J Obstet Gynecol 2020; 223:737.e1-10. 
https://doi.org/10.1016/j.ajog.2020.05.045.

40. Ali AA, Abdallah TM. Clinical presentation and epidemiology 
of female genital tuberculosis in eastern Sudan. Int J 
Gynaecol Obstet 2012; 118:236–8. https://doi.org/10.1016/j.
ijgo.2012.04.005.

41. Abdelrub AS, Al Harazi AH. Genital tuberculosis is common 
among females with tubal factor infertility: Observational study. 
Alexandria J Med 2015; 51:321–4. https://doi.org/10.1016/j.
ajme.2014.11.004.

42. Nezar M, Goda H, El-Negery M, El-Saied M, Wahab AA, Badawy AM. 
Genital tract tuberculosis among infertile women: an old 
problem revisited. Arch Gynecol Obstet 2009; 280:787–91. 
https://doi.org/10.1007/s00404-009-1000-9.

43. Singh N, Sumana G, Mittal S. Genital tuberculosis: A leading 
cause for infertility in women seeking assisted conception in 
North India. Arch Gynecol Obstet 2008; 278:325–7. https://
doi.org/10.1007/s00404-008-0590-y.

44.  Sankar MM, Kumar P, Munawwar A, Kumar M, Singh J, Singh A, 
et al. Usefulness of multiplex PCR in the diagnosis of genital 
tuberculosis in females with infertility. Eur J Clin Microbiol 
Infect Dis 2013; 32:399–405. https://doi.org/10.1007/s10096-
012-1755-y.

45. Mahajan N, Naidu P, Kaur SD. Insight into the diagnosis and 
management of subclinical genital tuberculosis in women 
with infertility. J Hum Reprod Sci 2016; 9:135–44. https://doi.
org/10.4103/0974-1208.192043.

46. Sethi S, Dhaliwal L, Dey P, Kaur H, Yadav R. Loop-mediated 
isothermal amplification assay for detection of Mycobacterium 
tuberculosis complex in infertile women. Indian J Med Micro- 
biol 2016; 34:322–7. https://doi.org/10.4103/0255-0857.188323.

47. Chowdhury RG, Paine SK, Bhattacharjee B, Chatterjee S. 
Infestation of endometrium by mycobacterium tuberculosis 
bacilli-cause of reproductive failure. Al Ameen J Med Sci 2010; 
3:322–31. 

48. Saraswat P, Swarankar ML, Bhandari A, Soni RR. Detection of 
active female genital tuberculosis by molecular method. Int J 
Pharma Bio Sci 2010; 1:328–34. 

49. Malhotra B, Sinha P, Hooja S, Vyas L. Rapid diagnosis of 
genital tuberculosis by real time polymerase chain reaction. 
J South Asian Feder Obst Gynae 2012; 4:39–42. https://doi.
org/10.5005/jp-journals-10006-1170. 

50. GajBhIye SB, Bhakre JB, Damle AS. Assessment of Endometrial 
Specimens for Tubercular Infection among Infertile Women 
using DNA-PCR. J Clin Diagnostic Res 2019; 13:DC01–5. 
https://doi.org/10.7860/JCDR/2019/42587.13208.

https://doi.org/10.1097/01.NAJ.0000450430.97383.64
https://doi.org/10.1097/01.NAJ.0000450430.97383.64
https://doi.org/10.1136/bmj.327.7414.557
https://doi.org/10.1258/td.2007.052090
https://doi.org/10.1016/0020-7292(90)90711-s
https://doi.org/10.1016/0020-7292(90)90711-s
https://doi.org/10.1016/0020-7292(89)90310-x
https://doi.org/10.1016/0020-7292(89)90310-x
https://doi.org/10.1016/S2214-109X(13)70032-9
https://doi.org/10.1016/S2214-109X(13)70032-9
https://doi.org/10.1186/s12890-017-0551-y
https://doi.org/10.1186/s12890-017-0551-y
https://doi.org/10.2471/BLT.13.124800
https://doi.org/10.26719/2020.26.4.477
https://doi.org/10.1371/journal.pone.0095603
https://doi.org/10.1016/j.jctube.2020.100154
https://doi.org/10.1016/j.jctube.2020.100154
https://doi.org/10.1371/journal.pone.0056074
https://doi.org/10.1016/S0140-6736(11)60754-X
https://doi.org/10.15562/ijbs.v11i1.133
https://doi.org/10.1016/j.ajog.2020.05.045
https://doi.org/10.1016/j.ijgo.2012.04.005
https://doi.org/10.1016/j.ijgo.2012.04.005
https://doi.org/10.1016/j.ajme.2014.11.004
https://doi.org/10.1016/j.ajme.2014.11.004
https://doi.org/10.1007/s00404-009-1000-9
https://doi.org/10.1007/s00404-008-0590-y
https://doi.org/10.1007/s00404-008-0590-y
https://doi.org/10.1007/s10096-012-1755-y
https://doi.org/10.1007/s10096-012-1755-y
https://doi.org/10.4103/0974-1208.192043
https://doi.org/10.4103/0974-1208.192043
https://doi.org/10.4103/0255-0857.188323
https://doi.org/10.5005/jp-journals-10006-1170
https://doi.org/10.5005/jp-journals-10006-1170
https://doi.org/10.7860/JCDR/2019/42587.13208


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324 | SQU Medical Journal, August 2022, Volume 22, Issue 3

51. Bhanothu V, Theophilus JP, Rozati R. Use of endo-ovarian 
tissue biopsy and pelvic aspirated fluid for the diagnosis of 
female genital tuberculosis by conventional versus molecular 
methods. PLoS One 2014; 9:e98005. https://doi.org/10.1371/
journal.pone.0098005. 

52. Patil AD, Shinde SK, Sachdeva GM, Pasi AR, Chitlange SM, 
Chandhiok N, et al. Is testing of menstrual blood justifiable 
for diagfnosis of endometrial tuberoculosis among infertile 
women. Ind J Obstet Gynecol Res 2015; 2:103–7. 

53. Goel G, Khatuja R, Radhakrishnan G, Agarwal R, Agarwal S, 
Kaur I. Role of newer methods of diagnosing genital tuberculosis 
in infertile women. Indian J Pathol Microbiol 2013; 56:155–7. 
https://doi.org/10.4103/0377-4929.118670.

54. Kamal S, Singh V, Singh S. A clinical study of association of 
genital tuberculosis with infertility in a tertiary centre of Jhark- 
hand, India. Int J Reproduction, Contraception, Obstet Gyne 2020; 
9:120–6. https://doi.org/10.18203/2320-1770.ijrcog20196008.

55. Kanti V, Seth S, Gupta S, Verma V, Singh A, Maurya G, et al. 
Comparison of the Efficacy of the Cartridge-Based Nucleic 
Amplification (CBNAAT)/Xpert Test and Histology of Genital 
Tissues in Diagnosing Female Genital Tuberculosis. Cureus 
2021; 13:e15000. https://doi.org/10.7759/cureus.15000.

56. Meenu S, Ramalingam S, Sairam T, Appinabhavi A, Panicker S, 
Oommen S, et al. Comparison of Polymerase Chain Reaction 
(PCR), Microbiological and Histopathological Observations in 
the Diagnosis of Endometrial Tuberculosis. J Obstet Gynaecol 
India 2020; 70:510–15. https://doi.org/10.1007/s13224-020-01367-9.

57. Shende P, Valecha SM, Gandhewar M, Dhingra D. Genital 
tuberculosis and infertility. Int J Reprod Contracept Obstet 
Gynecol 2017; 6:3514–18.

58. Ohri S, Patil SK, Patil A, Patil Y, Kshirsagar NS. Study of genital 
tuberculosis in infertile women. Age 2016; 21:F1–3.

59. Parikh KP, Deshpande HG, Madkar CS, Jethani S. Study to find 
out the incidence of Genital Tuberculosis as a cause for female 
infertility in Semi-Urban population. J Evol Med Dent Sci 2014; 
3:3223–7. https://doi.org/10.14260/jemds/2014/2271.

60. Gupta N, Sharma JB, Mittal S, Singh N, Misra R, Kukreja M. 
Genital tuberculosis in Indian infertility patients. Int J 
Gynaecol Obstet 2007; 97:135–8. https://doi.org/10.1016/j.
ijgo.2006.12.018.

61. Rajaram S, Gupta P, Gupta B, Kaur IR, Goel N. Laparoscopy 
in the diagnosis of tuberculosis in chronic pelvic pain. Int 
J Mycobacteriol 2016; 5:318–23. https://doi.org/10.1016/j.
ijmyco.2016.06.016.

62. Shahzad S. Investigation of the prevalence of female genital 
tract tuberculosis and its relation to female infertility: An 
observational analytical study. Iran J Reprod Med 2012; 
10:581–8. 

63. Shaheen R, Subhan F, Tahir F. Epidemiology of genital 
tuberculosis in infertile population. J Pak Med Assoc 2006; 
56:306–9. 

64. Shallal MM, Al-Asadi FAS, Mizaal MI. Detection of 
Endometrial TB in Patients with AUB using PCR Method of 
Assessment of Menstrual Blood Flow of Iraqi Females. Indian J 
Forensic Med Toxicol 2021; 15:1225. https://doi.org/10.37506/
ijfmt.v15i1.13584.

65. Chatterjee T., Basak AK. Mycobacterium tuberculosis and 
non-tubercular mycobacterium infection in women with 
unexplained infertility from eastern India. Int J Reprod Biomed 
2018; 16:557–62.

https://doi.org/10.1371/journal.pone.0098005
https://doi.org/10.1371/journal.pone.0098005
https://doi.org/10.4103/0377-4929.118670
https://doi.org/10.18203/2320-1770.ijrcog20196008
https://doi.org/10.7759/cureus.15000
https://doi.org/10.1007/s13224-020-01367-9
https://doi.org/10.14260/jemds/2014/2271
https://doi.org/10.1016/j.ijgo.2006.12.018
https://doi.org/10.1016/j.ijgo.2006.12.018
https://doi.org/10.1016/j.ijmyco.2016.06.016
https://doi.org/10.1016/j.ijmyco.2016.06.016
https://doi.org/10.37506/ijfmt.v15i1.13584
https://doi.org/10.37506/ijfmt.v15i1.13584