4.1 Corticosteroids

Reproductive failure and lower IVF success rates were noted in women with immune dysfunction. Immune-suppressive activity of corticosteroids was, therefore, expected to improve pregnancy outcome by reducing endometrial pro-inflammatory cytokines production and uNK cell activity [7]. The authors found that corticosteroids did not improve the clinical pregnancy rate in the study population, but subgroup analysis revealed a significantly higher pregnancy rate in the IVF, rather than ICSI group.

In a systematic review [6], there was a higher clinical pregnancy rate noted in the prednisolone group. However, data heterogeneity was substantial, thus suggesting a cautious interpretation of the results.

From various studies, significantly higher pregnancy and implantation rates were noted in women undergoing IVF, with high anticardiolipin antibody (ACA) when treated with methylprednisolone and low-dose aspirin. In presence of antithyroid antibodies (ATA) higher implantation and clinical pregnancy rates were seen in women treated with corticosteroids, aspirin and levothyroxine. In women with high uNK cells and unexplained recurrent miscarriage, live birth rates were higher in the prednisolone-treated group [8].

A number of investigators looking in to the use of steroids alone or in conjunction with other adjuvant treatments in women with positive antinuclear antibody (ANA) undergoing IVF have reported contradictory outcomes. The Cochrane review by Boomsma and colleagues (2012) [9] showed no evidence of improved clinical outcome with pre-implantation administration of glucocorticoids.

This clearly explains that steroids, in isolation or combination, are beneficial when used in targeted groups with immune dysfunction, high ACA, ATA or high uNK cells. Steroids are obviously cheap, easy to administer, widely available and have a fairly extensive history of use. The only known potential caution is the weak association with cleft palate; a threefold increase in oral clefts among offspring of women who received oral corticosteroids during pregnancy, which should be explained to the couple [10].

4.2 Intravenous Immunoglobulin (IVIg)

IVIg is a pooled blood product from numerous donors. Complications or side effects are seen in up to 35% of cases and are often related to the rate of infusion, total dose and brand of IVIg infused. Mild and transient side effects include flushing, headache, itching, low backache, nausea and fatigue. Serious and rare side effects include aseptic meningitis, severe anaphylactic reaction, acute renal failure and thrombotic events. We have previously argued that women should be provided with clear information of these side effects before embarking on the treatment [8].

Polanski et al. (2014) [6] reviewed 217 studies with high pbNK cells and identified only 3 eligible studies for analysis. The findings suggested that immune therapy for women with high pbNK cells is beneficial. Other authors found that, in women with high uNK cells and unexplained recurrent miscarriage, live birth rates were higher when IVIg was used [11]. A systematic review [12] showed significantly lower miscarriage rate, higher implantation rate, clinical pregnancy rate and live birth rate after IVIg treatment. However, the review noted numerous methodological flaws in the studies included, such as poor design, lack of randomisation, heterogeneous population, use of multiple adjuvant interventions, different doses and regimes of IVIg and lack of cost effective analysis.

4.3 Intralipid Infusion

Intralipid infusion therapy has been used for decades to correct fatty acid and calorie deficiency among those who are unable to feed orally. The intralipid infusion is an emulsion of soya bean oil, egg yolk, phospholipids, glycerin and water.

Intralipids function as immune-modulators by inhibiting pro-inflammatory factors such as TH1 cytokines [13]. It was shown that intralipid infusion could effectively suppress NK cells activity in patients with abnormal NK cytolytic activity. It is postulated that the fatty acids within the emulsion serve as ligands to activate peroxisome proliferator-activated receptors expressed by the NK cells, which would reduce NK cytotoxic activity resulting in enhanced implantation and maintenance of pregnancy [14].

A non-randomised trial showed a 46% clinical pregnancy rate with the use of 20% intralipid fat emulsion in women with recurrent implantation failure and elevated TH1 cytokine response on NK cell assay. It was noted that TH1:TH2 activity ratio decreased following treatment and this alteration in cytokine activity was deemed to be responsible for the outcome [15].

The first randomised controlled trial (RCT) with intralipid was recently presented at the ASRM Annual Meeting in Baltimore [16]. Women with repeated IVF failure and abnormal immune testing were randomised to receive intralipid or nothing. With over 100 in each group, the intralipid infusion group had significantly higher live birth rates (32%) than those who did not (12%). Given the relatively low cost and maternal-fetal safety, this type of immune therapy is likely to become more prevalent. However, caution is still necessary, not least because of the potential infection at the cannula site which has led recently to reported death [17].

4.4 Anti-tumour Necrosis Factor-Alpha

TNF-α antagonists suppress inflammatory response to tumor necrosis factor (TNF) and have been used in various autoimmune and immune-mediated conditions such as rheumatoid arthritis, ankylosing spondylitis, inflammatory bowel disease and psoriasis. Prolonged use of TNF inhibitors is associated with serious side effects such as lymphoma, demyelinating disease, congestive heart failure, induction of autoantibodies and lupus-like syndrome [18]. Direct correlation between circulating TNF-α levels and IVF outcome has yet not been fully established [8], but its use has so far been directed at women with abnormal T cell activation.

An exaggerated TH1 response is harmful to the process of embryo implantation resulting in infertility. Anti-TNF-α agents, such as Entanercept (Enbrel), Adalimumab (Humira) and Infliximab (Remicaid) were studied in infertile patients with raised TH1:TH2 cytokines ratio undergoing IVF, and a higher live birth rate was noted [19]. This treatment is however expensive and not used widely outside specialised centres.

6.1 Aspirin

Aspirin (Acetylsalicyclic acid) is a non-steroidal anti-inflammatory agent (NSAID). Daily administration of low-dose aspirin results in vasodilation and increase in the peripheral blood flow by inducing a shift from thromboxane A2 to prostacyclin [24]. Aspirin was also shown to increase uterine blood flow [25], which in turn enhances the endometrial receptivity resulting in higher embryo implantation rates. However, these findings were not shown to translate into clinical use.

Aspirin was shown to be beneficial in women with recurrent miscarriage and antiphospholipid antibody syndrome (APS) as well as in prevention of early onset pre-eclampsia (CLASP Study). The Cochrane review [26] confirmed that administration of aspirin in IVF does not improve pregnancy rates. There was no significant difference noted between aspirin and control group for the live birth rate, clinical pregnancy rate or miscarriage rate.

6.2 Heparin

Heparin is an anticoagulant. It improves implantation by regulating the endometrial receptivity and decidualisation of endometrial stromal cells by several means.

In women with thrombophilia, impaired trophoblastic invasion of maternal vessels by the syncytiotrophoblast is noted due to micro-thrombi at the site of implantation [27]. In this group of women, heparin could improve implantation, however, published studies showed contradictory findings. Significant differences in pregnancy rates were noted in women with thrombophilia receiving heparin treatment with or without low-dose aspirin and no improvement in pregnancy rates when unfractionated heparin and low-dose aspirin were used [8]. A Cochrane systematic review [28] showed a 77% increase in live birth rate, 73% in implantation rate and a 78% reduction in miscarriage rate. The same review also found a 79% increase in live birth rate in women with history of three recurrent implantation failures (RIF). Interestingly, a similar improvement was not seen when studies included only unexplained RIF.

6.3 Vasodilators

Endometrial development plays a pivotal role in successful embryo implantation. Increased endometrial blood flow and thickness are likely to improve implantation and IVF success rates. Several agents have been tried to improve sub-endometrial blood flow and increase endometrial performance during IVF treatment.

7.1 Nitroglycerine (NTG)

NTG is an NO donor. It acts as a vasodilator and relaxes the smooth muscle of the uterus. However, use of NTG three minutes before embryo transfer did not show any significant difference in the ease of transfer or the pregnancy rates [29].

7.2 β2-Adrenergic Antagonists

Selective β2-adrenergic blockers (Ritodrine, Terbutaline and Salbutamol) are known uterine smooth muscle relaxants used in obstetrics for management of pre-term labour and before external cephalic version. Administration of these agents regularly for two weeks in the luteal phase, following oocyte retrieval did not show any improvement in the implantation and pregnancy rates [30], whilst resulting in adverse side effects such as hypotension and tachycardia.