To carry out a full STI risk assessment for each individual, we need their complete medical history, which includes sociodemographic, clinical and behavioural variables. The patient should be interviewed alone and we need to create a suitable atmosphere of trust, guaranteeing confidentiality and explaining the reasons for asking about sexual practices. Questions should be concise, open and respectful, without making assumptions about sexual practices and avoiding judging the person.9

The patient should first of all be asked about the reason for consulting: specific symptoms of STI, whether genital (urethral/vaginal discharge), non-genital (anorectal, oropharyngeal, skin-related) or nonspecific (fever, malaise, weight loss, etc.); date of onset of symptoms; and time since he/she last had unprotected sex.4,10

In many cases, STIs are asymptomatic and do not even show clinical signs. In addition to a physical examination, it is therefore essential to identify sexual practices and the pattern of condom use. This helps us determine the individual risk for each patient, make an effective early clinical diagnosis of the STI and provide personalised advice on prevention.

Using a structured questionnaire is highly recommended, including at least the five variables recommended for assessing the risk of STI, the “five P” rule: Partners, Sexual Practices, Prevention of Pregnancy, Protection against STIs and Past STIs.4

Partners, Practices, Prevention of Pregnancy, Protection against STIs, Past STIs

Partners:

• •

  Who are you having sex with, men, women or transgender people?

• •

  How many sexual partners have you had in the last two months?

• •

  How many sexual partners have you had in the last 12 months?

• •

  Do you think any of your sexual partners in the last 12 months might have had sex with anybody else?

Practices:

• •

  Have you had vaginal sex?

• •

  Have you had insertive or receptive anal sex?

• •

  Have you had oral sex?

• •

  If the answer is yes, “Do you use condoms: never, sometimes or always?”

Prevention of pregnancy:

• •

  What methods of contraception do you use?

Protection against STIs:

• •

  How do you protect yourself from STIs and HIV?

Past history of STIs:

• •

  Have you ever had an STI?

• •

  Have any of your partners ever had an STI?

Additional questions to identify HIV and viral hepatitis risk include:

• •

  Have you ever injected drugs?

• •

  Have you ever exchanged sex for money or drugs?

• •

  Have you ever shared sex toys?

• 1)

  Sociodemographic variables: gender, age, country of origin, level of education.

• 2)

  Behaviour indicators:

  • •

    Sexual partners: age of first sexual relations; number of sexual partners in the last year and throughout life; gender of sexual partners (male, female, transgender); practices prostitution or is a client of prostitutes.

  • •

    Sexual practices: type of sex (oral, anal, vaginal); use of condoms in each activity; time since last unprotected sex; shared use of sex toys, fisting and use of apps to find sexual partners.

  • •

    Use of substances of abuse: consumption of excess alcohol and/or drugs for sex; unprotected sexual practices under the effect of said substances; routes of drug administration (oral, nasal, parenteral, etc.); shared use of material for drug use; and participation in chemsex sessions.11

• 3)

  Clinical indicators: known drug allergies; STI history; vaccinations; other relevant medical history; and concomitant medication.

In both symptomatic and asymptomatic patients, a full clinical examination should be carried out, with special emphasis on the patient's symptoms and sexual practices. Particular attention should be paid to internal genitalia (vagina, cervix) and external genitalia (vulva, penis, testicles), oropharynx, perianal and rectal region, skin and lymphadenopathy.

• 1)

  Skin and mucous membranes: they should be examined for lesions compatible with primary or secondary syphilis or other skin/mucous membrane manifestations associated with HIV infection or other STIs.

• 2)

  Genital: inspection of external genitalia (vulva, penis, testicles). Characteristics of urethral or vaginal discharge: purulent, haemorrhagic, mucous. Palpation of the testicles and epididymis, considering size, shape and sensitivity. Cervical/vaginal examination with speculum, assessing the characteristics of vaginal discharge, cervical erythema or secretions and the presence of any lesions.

• 3)

  Anal/rectal: external inspection of the anal region, observing for possible HPV, herpes, syphilis or chlamydia lesions. Internal assessment: proctoscopy should be performed with anal speculum and cold light lamp to assess for secretions and lesions in the rectal mucosa. Visualisation of the anal canal while extracting the speculum.

• 4)

  Lymphadenopathy: axillary, inguinal, lateral/cervical, submandibular and supraclavicular.

Depending on the clinical symptoms, exploratory signs, sexual practices and any sharing of sex toys or materials for drug use, the following should be requested: serology for syphilis, HIV, HAV, HBV, HCV, urethral, cervical/vaginal, rectal or pharyngeal secretions, study of genital or extragenital ulcers and anal and/or cervical cytology with HPV detection.

In summary, to ensure effective early diagnosis and the correct treatment for the STI, diagnostic tests need to be guided by the clinical and behavioural indicators of each individual. Additionally in patients diagnosed with an STI, screening for other STIs is recommended, along with tracing of sexual contacts in the previous few months, in order to interrupt the chain of transmission and prevent reinfection of the patient.

The use of suitable microbiological tests is key to effective management of STIs. They are necessary for the diagnosis itself, screening in high-risk groups, monitoring of treatment, epidemiological surveillance, the study of antibiotic sensitivity, and research.

The spectrum of diagnostic tests in microbiology used in STI ranges from direct microscopy, culture, antigen detection and serology, to the detection of genomic material. Apart from culture, all of the above could be considered as rapid diagnostic tests. Significant advances have been made in the different methods, primarily in the area of molecular biology (MB), providing greater efficiency and a shorter response time.

The collection, transport and processing of samples are critical factors in the diagnostic effectiveness of microbiological techniques. The type of samples needed will depend on sexual practices. A genital sample should always be taken, and oropharyngeal and/or rectal swabs if the patient has had oral and/or anal sex. Table 1 shows the best sample to collect according to the aetiology and signs and symptoms.

Samples should be taken before starting antibiotic therapy and avoiding contact with disinfectants and antiseptics. They should be collected in the appropriate container, in a sufficient volume according to the test to be requested, and suitably identified. The techniques can give false negative results if sample collection and transport guidelines are not followed.12

The most effective diagnostic techniques for studying the different microorganisms involved in STIs are shown in Table 2.

Microscopy techniques are a quick, simple and economical but observer-dependent tool. In the case of Neisseria gonorrhoeae (N. gonorrhoeae), Gram staining has high sensitivity (≥95%) and specificity in the diagnosis of symptomatic urethritis in men, but lower for other sites (endocervical or rectal secretions) and is not recommended in pharyngeal secretions. Dark-field microscopy examination of genital chancres provides an immediate result for the diagnosis of syphilis, but there are some limitations: it has to be analysed immediately after collection and requires experience in microscopy to minimise false negative results. This test is not recommended in mouth ulcers because saprophytic spirochetes may be visualised. Wet mount microscopic examination for the detection of Trichomonas vaginalis (T. vaginalis) is easy, quick and low cost, but, although it does have a specificity of 98%, it has low, observer-dependent sensitivity (62–92%). Microscopic diagnosis is essential for other protozoa of intestinal origin (Giardia, Entamoeba sp.) in cases of gastrointestinal symptoms related to the type of sexual practices, in particular in the male homosexual population, in view of the fact that the route of transmission is faecal-oral.13

Culture is indicated fundamentally for the isolation of N. gonorrhoeae from genital samples using selective culture media (Thayer-Martin agar). It is the recommended technique because of its sensitivity, specificity and suitability for multiple types of samples. Sensitivity to antibiotics and epidemiological studies can also be determined with culture; important nowadays because of the worrying increase in resistance. Culture of T. vaginalis is easy and inexpensive to perform, although it does require an incubation time of several days.

The MB methods used in clinical microbiology laboratories for the study of STIs are mainly gene amplification techniques based on the polymerase chain reaction. They are rapid, automated tests with high sensitivity and specificity which can be used to detect virtually all microorganisms and to measure viral load (HIV and hepatitis). Some of the polymerase chain reaction techniques are able to detect several STI-causing microorganisms in the same reaction, as well as determine the mechanisms of resistance to certain antibiotics (Mycoplasma genitalium [M. genitalium] – macrolides and quinolones). As a result of technological advances, rapid, easy-to-use molecular diagnostic options are becoming commercially available. They are still expensive, but the speed in obtaining diagnoses probably makes up for the high cost.

Serology is the technique used in the screening and/or diagnosis of Treponema pallidum (T. pallidum), HIV and hepatitis virus (A, B and C) infections. In the case of syphilis, treponemal tests (determination of specific antibodies) are used for screening/diagnosis and non-treponemal tests (determination of non-specific antibodies) to determine the status of the infection (active or inactive) and treatment follow-up. In all cases, there is evidence that immunochromatography (HIV, syphilis and hepatitis) and agglutination (RPR syphilis) are very useful for a rapid diagnosis.

There is a need for microbiological diagnostics to be decentralised to a certain extent nowadays in order to provide a faster response and allow earlier, targeted treatment. The WHO defines rapid or “point of care” (PoC) diagnostic tests as those which are: “Affordable, Sensitive, Specific, User-friendly, Rapid and robust, Equipment-free and Deliverable to end-users” (ASSURED).

The management of STIs is made easier and more effective by access to a rapid diagnosis, as the patient can often be dealt with in a single consultation.14 The rapid tests also enable patients to receive early, specific treatment, avoiding unnecessary and inadequate antibiotic therapy and minimising the chain of transmission, which helps prevent new cases. Qualitative studies also affirm the need for diagnostic tests in PoC format perceived by the end users and healthcare professionals.15

Moreover, the increase in the incidence of STIs is saturating the classic healthcare dynamic, making it necessary for us to adapt to a new scenario. The emergence of new rapid access circuits closer to users with self-collection of samples and PoC tests can complement diagnosis in centralised and specialised laboratories.16,17 These models have focused more on the screening of asymptomatic users, but may also be useful in cases with symptoms. Table 3 shows the potential benefits and drawbacks of diagnosis in hospital-based laboratories versus PoC centres.

Of the tests mentioned in the previous section, we would consider microscopy, antigen/antibody detection and some MB techniques, to a greater or lesser degree, as suitable candidates for use as PoC tests. Table 4 shows a summary of the tests available by aetiological agent. All have the possibility of being implemented, in STI consultations or 24-h laboratories according to the context, to facilitate the diagnosis of STIs, whether in symptomatic cases or for screening at-risk populations.

Being diagnosed with a sexually transmitted infection can provoke a great deal of stress and generate anxiety. One of a doctor's jobs is to advise and inform the patient. They therefore need to provide information about the infection, while providing reassurance to reduce the patients unease and ensure good adherence to treatment. After giving the diagnosis, the doctor needs to inform the patient about the nature of the aetiological agent, possible methods of transmission (risk associated with each method) and the natural history of the infection if not treated. Additionally, to ensure good adherence to treatment, it is best to inform the patient about both the efficacy of the treatment and any adverse effects that may occur while they are taking it. The importance of refraining from sex (abstinence) during the treatment should also be stressed to avoid further transmission to sexual partners. Lastly, the opportunity should be taken at each medical consultation for an STI to emphasise the different STI prevention measures, and allow sufficient time to resolve any uncertainties the patient may have.18

Contact tracing (CT) is defined as the identification and tracing of sexual partners (“contacts”) of a person diagnosed with an STI (“index case”) to provide them with information and an early diagnosis and treatment (if required). Treating contacts prior to confirming the infection with laboratory tests is known as “epidemiological treatment”.27 In general terms, and in the absence of medical contraindication, the regime for epidemiological treatment is simply the treatment of choice for each STI.

CT is not mandatory and must be carried out in compliance with EU laws and in accordance with the declaration of human rights. The most common reasons for the index case refusing to become involved in CT are being scared, worrying about loss of confidentiality and failure to accept the diagnosis. Therefore, the healthcare professional responsible for the CT must be able to show empathy and create a confidential, trusting atmosphere in order to carry the process through.

CT has many aims and benefits for both the index case and the contacts:

• •

  Interruption of the chain of transmission.

• •

  Prevention of reinfection of the index case by their sexual partners in the case of curable STIs.

• •

  Increased diagnosis of asymptomatic infections, preventing the development of symptoms or long-term complications.

CT also helps bring new users to STI clinics, creating the opportunity to further promote prevention measures, provide more people with sex and health education and carry out screening for other STIs. It also has benefits for public health, by shortening the period of transmissibility among contacts and reducing asymptomatic cases in the general population.

How far back to trace contacts depends on each STI. Table 6 sets out information for the main STIs in which CT is recommended along with the need for epidemiological treatment.

Despite international efforts and preventative measures already in place, there has not been a significant decrease in new cases of HIV in the last decade. In 2017, there were 1,800,000 new infections worldwide.28 In the West, figures are particularly significant among MSM and transgender women, with these groups now having the highest rates of new infections (53% of new infections in the EU/EEA in 2016 for which the method of transmission was known were in MSM).29 A new approach to prevention has therefore been required to try to make progress towards eradicating the epidemic.

PrEP prophylaxis is an additional HIV prevention measure, complementary to all the other measures used up to now (condom use, population screening and early diagnosis, health education, undetectability of people living with HIV). PrEP consists of the administration of emtricitabine (FTC) 200mg/tenofovir (TDF) 300mg in a single tablet to people who are HIV-negative but at high risk of acquiring HIV. The prophylaxis is given as part of a comprehensive programme including periodic STI and HIV screening, ongoing medical advice and health education and promotion of other preventive measures, without which the efficacy of the prophylaxis would be reduced.

The recommendations in Spain for PrEP have been established for individuals whose characteristics mean they belong to a high-risk group with an HIV incidence of two cases/100 person-years or higher; falling into this category are MSM and transgender women who also meet any of the following criteria30:

• •

  Multiple sexual partners

• •

  Anal sex without a condom

• •

  Recreational substance abuse

• •

  Diagnosis of a bacterial STI

• •

  Having required post-exposure prophylaxis.

The effectiveness of PrEP has been demonstrated in numerous different clinical trials.30 In the Ipergay and PROUD studies conducted in MSM, an 86% reduction was found in the risk of acquiring HIV. In later studies such as the follow-up cohort of the Ipergay study, even higher effectiveness was demonstrated, with a 97% risk reduction. The high efficacy of this measure has been found to be closely linked to adherence. In the cohort study conducted with the users previously included in the ATN 082, iPrex and US Safety Study trials, in users with adherence levels of four or more tablets per week, the incidence of HIV was found to be 0/100 person-years.31 There are two ways to take PrEP: one tablet a day; or dosing related to having sex, consisting of taking two tablets before exposure and then one tablet a day for two days after the last exposure.

The continued use of FTC/TDF can lead to various adverse effects, although they are reversible. Self-limiting nausea and gastrointestinal discomfort has been reported in clinical trials in the first few weeks. The use of tenofovir disoproxil fumarate (TDF) is associated with renal toxicity and decreased bone mineral density, although these disorders are reversible. The introduction of PrEP has raised concerns about compensatory behavioural changes (increased high-risk sex) in the population and a consequent increase in STIs. In the studies carried out to date, although the incidence has been high, which is not surprising given the high-risk criteria of the users, there has been no significant increase in the number of STIs.32,33

Post-exposure prophylaxis (PEP) after risky sexual behaviour (RSB) consists of the administration of antiretroviral therapy (ART) at an early stage for a limited period of 28 days to prevent HIV infection. There are few efficacy data regarding PEP as, for ethical reasons, it is not feasible to carry out clinical trials. However, PEP efficacy has been demonstrated in animal studies and observational studies.34

For PEP to be adequately prescribed, the risk after sexual exposure has to first be assessed and will be affected by multiple factors:

• -

  Sexual practices: Receptive anal sex without a condom is considered to be the practice with greatest risk, followed by insertive anal sex, receptive vaginal sex and insertive vaginal sex. Oral sex is considered to be low or minimal risk.35

• -

  Serological status of the source. If the source is known to be HIV+, a high viral load increases the chances of infection, while people with undetectable viral load do not transmit HIV. We also have to take into account the presence of resistance mutations in the virus which may result in modification of the ART regimen. Where HIV status is unknown, the possibility of the source belonging to a population with a higher prevalence of HIV has to be taken into account. Having an STI also increases the risk.

• -

  Host susceptibility. The presence of breaks in the genital mucosa due to STI, traumatic sex or host disease can enhance the risk of acquiring HIV. Circumcision decreases the likelihood in heterosexual males.

The risk of infection can be calculated by multiplying the risk of the source being HIV+ (from the estimated prevalence) by the risk according to sexual practices. PEP is indicated at risks greater than 1/1000 and should be considered when risk is from 1/1000 to 1/10,000.35Table 7 shows a summary of the recommendations for the administration of PEP, although the indication should always be agreed with the user once risks and benefits have been assessed.

Taking PEP is extremely stressful for users as they have to come to terms with the possibility that they may have been infected with HIV. Psychological support therefore needs to be provided, and the importance of adherence to ART and medical follow-up should be emphasised. It is also an opportunity to provide sex education and assess the indication for PrEP.

The ART regimen indicated at present is the combination of two NRTI (emtricitabine/tenofovir) and an integrase inhibitor. This regimen has been shown to have good tolerance and few adverse effects. However, a good medical history must be taken to avoid interactions or undesirable effects. For example, in the case of elvitegravir, combination with cobicistat (cytochrome P450 inhibitor) can lead to interactions with concomitant medication or the use of recreational substances.36

PEP has to be started within the first 72h of exposure and ideally within the first 24h. The established duration is 28 days. A general analysis (complete blood count and basic biochemistry) should be carried out at the beginning as well as STI screening. It is recommended that screening for STI and HIV serology be repeated at 4 and 12 weeks. In the event of HIV infection, the user should be referred to a specialist to continue the treatment and perform a full assessment.