Recent eLetters

Charlotte K Russell - Research Associate, Department of Anthropology, Durham University

Helen L Ball - Professor of Anthropology, Department of Anthropology, Durham University; Director of the Parent-Infant Sleep Lab

Dear Editor,

This publication analyses SIDS-risks associated with bed-sharing under different circumstances using data from five historical SIDS studies. Unlike previous analyses of these data, this analysis includes data on feeding type. It promises, at last, to enable those of us working with parents and the staff who support them to be able to answer complicated but commonly asked questions about SIDS, and allow parents to make informed decisions about any potential risk associated with their personal and cultural infant care beliefs and behaviours.

Because this analysis is based on old data, however, it can only inform us as to the risks as they existed 15-26 years ago: knowledge both of bed-sharing behaviour and safety issues not considered here have advanced considerably in the intervening period. The authors present analysis of a dataset in which 'safer' bed-sharing is considered as distinct from bed-sharing in conjunction with known hazards (that is, breastfeeding infants bed-sharing in the absence of smoking, alcohol, drugs and sofa-sharing). Babies were categorized as bed-sharing if they were found dead in the parental bed, or woke up in the parental bed in the morning following the 'index night' (deviating from the original analyses which used many different definitions for 'bed-sharing'). This definition under-estimates the number of 'control' babies who bed-shared as some infants bed-share for a portion of the night and are placed in a cot following the last feed, so would not wake up in the parents' bed (and would be classed here as 'room-sharers'), however babies who die would not be returned to the cot. 'Accidental' (and consequently unplanned) bed- sharing is therefore also likely to be overrepresented in the SIDS group (Ball 2012). Both factors would inflate the risk associated with bed- sharing.

The authors predict a SIDS-rate of approximately 1 per 10,000 babies for room-sharers, and 2 per 10,000 babies for bed-sharers. The current rate of SIDS in UK is 1/3000, or 3.4/10,000, which means that both sleep locations for breastfed infants of non-smoking parents in the absence of alcohol experience very few SIDS deaths. It is curious, therefore, that the authors focus attention only to this small difference in predicted SIDS rates for breastfed babies of non-smoking parents who bed-share compared to room-sharing-while ignoring the hugely inflated risks associated with hazardous bed-sharing environments. It appears as though the authors choose to target breastfeeding mothers in this way as they are a sub-group with strong opinions about the benefits of bed-sharing, even though the infants of these mothers contribute negligibly to UK SIDS rates.

The recommendations of the authors that parents are advised to 'simply avoid bedsharing' indicates a worrying lack of cultural awareness or sensitivity to childrearing beliefs of different groups of parents on the part of these SIDS researchers. Such a recommendation does not allow parents, especially those whose infants are at low risk for SIDS (healthy term births, breastfed, not exposed to parental smoking or alcohol consumption), to make an informed choice to bed-share or not. While single message recommendations may have been appropriate and effective in previous campaigns targeting simple infant care practices such as supine vs. prone sleep position, they are inappropriate and ineffective for addressing infant care issues involving relational behaviours and cultural beliefs (Ball and Volpe 2012). Closing down all discussion of the reasons why parents might bed-share with their infant by issuing a dogmatic recommendation inhibits health professionals from raising the topic, causes parents to lie about their behavior, and stifles the provision of information about hazardous sleeping environments and the degrees of risk involved (Fetherston and Leach, 2013).

We argue that SIDS is not the only issue that must be taken into consideration when considering parent-infant bed-sharing, and that risk minimization, involving parent education and facilitating informed choice, is a more logical and ethical approach to the bed-sharing issue, than one focusing on risk elimination.

References:

Ball, H. L. (2012). Sleeping with the baby. IBFAN Breastfeeding Briefs, No. 53, September 2012.

Ball, H. L., & Volpe, L. E. (2013). Sudden Infant Death Syndrome (SIDS) risk reduction and infant sleep location - moving the discussion forward. Social Science & Medicine, 79, 84-91.

Fetherston C.M., & Leach, J.S. (2012) Analysis of the ethical issues in the breastfeeding and bedsharing debate. Breastfeeding Review, 20(3): 7-17.

Conflict of Interest:

Ball and Russell run the Infant Sleep Information Source (ISIS), an online source of infant sleep research information for parents and health professionals (www.isisonline.org.uk). They do so as part of their academic outreach activities and do not receive any income from the project.

Dear Editor: By design, incomplete examinations provide data that lead to superficial correlations, erroneous inferences, and poor public health policy. Schmidt et al.1, provide an exemplar of this increasingly frequent event. Physical inactivity is a leading cause of death worldwide as well as a principal underlying pathology in most major causes of morbidity and mortality.2 Inactivity affects cardiovascular disease3,4, cancer5, obesity 6,7 and type 2 diabetes.8 Importantly, studies that purport to examine associations between BMI-defined obesity and chronic non-communicable diseases without examining physical activity are by design rendering their conclusions irrelevant by ignoring a major causal factor in their analyses. We have published numerous papers showing that obese individuals who are moderately fit, as assessed by a maximal treadmill test have substantially lower death rates during follow-up than people who are normal weight and unfit.9 We contend that one cannot study the health effects of obesity and diet without properly measuring physical activity or fitness and incorporating them into the analyses. We think because Schmidt et al.,1 explicitly acknowledge the importance of "exercise" when counseling patients on risk management, they should acknowledge that their failure to include physical activity in the analyses does little to advance the science of disease management.

1.Schmidt M, et al. BMJ open. 2013;3(4). 2.Lee IM, et al. Lancet. Jul 21 2012;380(9838):219-229. 3.Archer E, Blair SN. Prog Cardiovasc Dis. May-Jun 2011;53(6):387-396. 4.Blair SN, et al. JAMA. 1995;273(14):1093-1098. 5.Lee CD, et al. Ann Epidemiol. Oct 2011;21(10):749-754. 6.Hankinson AL., et al. JAMA. 2010;304(23):2603-2610. 7.Donnelly JE., et al. Arch Intern Med. 2003;163(11):1343-1350. 8.LaMonte MJ. et al. J Appl Physiol. Sep 2005;99(3):1205-1213. 9.Sui X., et al. JAMA. Dec 5 2007;298(21):2507-2516.

Conflict of Interest:

None declared

In the UK, the rate of maternal request caesareans is also higher in private hospitals, and up until November 2011 (when NICE guidance[1] on Caesarean Section changed) maternal request was not on its own supported as an indication for CS in public (NHS) hospitals; therefore many women, who could afford to, paid for their maternal request caesarean privately.

Unfortunately, despite the fact that NICE guidance now supports maternal request following an individual's risk and benefit consultation (and the offer of counseling in cases of tokophobia), a blanket refusal of maternal request still occurs in many NHS hospitals.

This is largely because UK maternity recommendations push for caesarean rate reduction and an increase in what is ideologically described as 'normal birth',[2] which is obviously a very difficult environment for women who want a caesarean to actually have a caesarean.

While it is not my intention to suggest that maternity care in the private sector is necessarily better than the public sector, or in any way to advocate that a planned caesarean is the best birth plan for all women, I do believe it's worth noting the findings of two Australian research papers in this context.

First, a survey of four public hospitals that found one in three women (33%) identified a traumatic birthing event and reported the presence of at least three trauma symptoms,[3] and second, a survey of 78 women who had requested and planned a cesarean birth in private maternity hospitals, which found the women were highly satisfied with their delivery. On a scale from 1 (totally unsatisfied) to 10 (completely satisfied), the mean score was a significantly high 9.25.[4]

Perhaps maternal request is contributing to rising caesarean rates more than has been traditionally considered, and because private health care offers women a greater freedom of maternal autonomy over how they give birth, maternal request rates can be seen most clearly there.

Finally, it is worth considering obstetricians' attitudes to risks associated with macrosomic babies, as this may be contributing to increased rates of caesarean births too. Research carried out in 2001 in Australia and New Zealand found that the proportion of doctors who would choose a caesarean rose from 11% to 26% if the baby was believed to weigh 8.8 pounds, and as high as 55% if 9.9 pounds or more, mainly due to fear of fecal and urinary incontinence. If these concerns are more readily communicated to women in the private sector, then this may influence women's final birth plan choice, and in an environment of increased maternal weight and birth weights at full term, again, it could very well be a significant factor.

References [1] National Institute for Clinical Excellence. Caesarean Section CG132 Guideline. [2] New RCOG guidance urges CCGs to increase births without epidurals and reduce caesarean rates to 20% August 24, 2012 electivecesarean.com [and] Making sense of commissioning Maternity Services in England - some issues for Clinical Commissioning Groups to consider. August 14, 2012 RCOG [3] D. K. Creedy, i. M. Shochet, and J. horsfall, "Childbirth and the Development of Acute trauma Symptoms: incidence and Contributing Factors," Birth 27, no. 2 (June 2000): 104-11. [4] Stephen Robson et al., "Elective Caesarean Delivery at Maternal request: A Preliminary Study of Motivations influencing Women's Decision Making," Australian and New Zealand Journal of Obstetrics and Gynaecology 48, no. 4 (August 2008): 415-20. [5] R. land et al., "Personal Preferences of Obstetricians towards Childbirth," Australian and New Zealand Journal of Obstetrics and Gynaecology 41, no. 3 (August 2001): 249-52.

Conflict of Interest:

Co-author of Choosing Cesarean, A Natural Birth Plan

Dr. Pantzaris and colleagues (1) have recently performed a study on a dietary intervention consisting of omga-3, omega-6 and vitamin A and -E in various formulations in relapsing-remitting multiple sclerosis (RR-MS). The authors suggested that a special combination of omega-3, omega-6 and fat soluble vitamins could have profound effects on magnetic resonance (MR) disease activity and disease progression. The main problem in intervention studies, where different compounds and interventions are combined, is to determine which substance actually had a therapeutic effect. There have been a number of both randomised controlled trials and cohort studies published on dietary intervention in MS, which could have helped to explain the findings in this study (for two excellent reviews, see Geldern et al. (2) and Farinotti et al (3)). Unfortunately, these studies have not been cited or discussed in the article. We think these newly published data should be taken into account when interpreting their results, as this will be of great importance for future larger randomised controlled clinical trials.

As one of their findings, the authors suggest that omega-3 intervention, in the form of eicosapentaenoic acid (EPA) and docosahexaenoic acid (DHA), could have therapeutic effects in MS. Although omega-3 has a theoretic anti-inflammatory effect, recently performed RCTs have not detected any positive effects on relapse-rate (4, 5) or MRI activity (6). Further, experimental studies in different animal models for MS have indicated conflicting results, with most studies actually reporting a negative effect of omega-3 intervention (7). Thus, there seems to be little rationale for choosing EPA and DHA as interventional substances. The fact that the authors did not detect any positive effect in treatment arm A, where these substances were given, further suggests that EPA and DHA did not have any treatment effect in this study either.

The authors also gave the patients in two of the experimental groups omega-6 fatty acids in the form of gamma-linoleic acid (GLA) and linoleic acid. Some studies have indicated a possibly reduced relapse severity and lower increase in disability in those receiving GLA than placebo (8), but the results are difficult to interpret because of lacking information on dropouts and patient characteristics. One recently published Cochrane review, based on all published studies on omega-3 and omega-6 supplementation, concluded that PUFA supplementation seemed to have no effect on disease progression (3). Although it is possible that the omega- 6 supplementation given to the MS-patients in two of the treatment groups could have had a beneficial effect on MRI disease activity, this seems less likely, as both group A and B also received the same dosage of omega- 6 supplementation.

Recently performed cohort-studies indicate that both vitamin A and E could have important disease modifying effects in MS (9, 10). Further, both vitamins have biological properties and have demonstrated positive effects in animal models for MS, which make them interesting candidates for future intervention studies (11). In one cohort study, where patients were followed for two years, we found that each 1 ?mol/L increase in serum -retinol reduced the odds ratio for new T1 gadolinium enhanced lesions by 49%, new T2 lesions by 42%, and combined unique activity by 46% in simultaneous MRI scans (9). We were also able to control for serum-levels of EPA, DHA and 25-hydroxyvitamin D, and found that they did not affect this association. Also higher serum levels of Retinol Binding Protein (a surrogate marker for vitamin A) has recently been demonstrated to be associated with decreased MS risk (OR=0.38) (12). In Pantzaris' and colleagues study (1), vitamin A was given to the patients in intervention group A and B, but the amount was rather moderate (0.6 mg), which is below the recommended dietary allowance for men and women of 0.9 and 0.7 mg, respectively. For vitamin E, we have demonstrated that during interferon beta (IFNB) treatment, each 10 ?mol/L increase in alpha-tocopherol reduced the odds ratio for simultaneous new T2 lesions by 36.8%, and for combined unique activity by 35.4% (10). As for vitamin A, we were also in this study able to control for serum-levels of EPA, DHA and 25-hydroxyvitamin D, without detecting any interaction. Since the patients in group B received both vitamin A and high dose vitamin E, this combination seems to be the most plausible explanation for the positive effect in this study, and not EPA and DHA, which were also given to the treatment arm where no effect was detected.

The authors of the present study reported a dropout rate of 49%, making it difficult to draw firm conclusions about their results. As most patients discontinued because of unpleasant taste and smell of the interventional treatment with fatty oils, we would suggest that future studies could primarily aim at detecting a possible protective effect of vitamin A and E treatment. This would probably greatly influence the compliance in future studies. The biological rationale for choosing these substances are stronger than for the PUFA-supplementation, which based on what we know from previous studies, probably have no beneficial effects in MS (3).

References: 1 Pantzaris MC, Loukaides GN, Ntzani EE, Patrikios IS. A novel oral nutraceutical formula of omega-3 and omega-6 fatty acids with vitamins (PLP10) in relapsing remitting multiple sclerosis: a randomised, double- blind, placebo-controlled proof-of-concept clinical trial. BMJ Open. 2013; 3 (4).

2 Geldern G, Mowry EM. The influence of nutitional factors on the prognosis of multiple sclerosis. Nature Reviews Neurology. 2012; 8, 678- 689

3 Farinotti M, Vacchi L, Simi S, Di Pietrantonj C, Brait L, Filippini G.Dietary interventions for multiple sclerosis. Cochrane Database Syst Rev. 2012; 12: CD004192.

4 Bates D, Cartlidge NE, French JM, et al. A double-blind controlled trial of long chain n-3 polyunsaturated fatty acids in the treatment of multiple sclerosis. J Neurol Neurosurg Psychiatry. 1989; 52 : 18-22.

5 Weinstock-Guttman B, Baier M, Park Y, et al. Low fat dietary intervention with omega-3 fatty acid supplementation in multiple sclerosis patients. Prostaglandins Leukot Essent Fatty Acids. 2005; 73: 397-404.

6 Torkildsen O, Wergeland S, Bakke S, Beieske AG, Bjerve K, Bjornar? B, Bjorn? IK, Bru A, Dalene F, Eikeland R, Henriksen OA, Hovdal H, Kierulf H, Kleveland G, Kristensen T, Lilleaas F, Midgard R, Olsen IC, Pedersen T, Schepel J, Myhr KM. Omega-3 Fatty Acid Treatment in Multiple Sclerosis (OFAMS study): a randomised, double-blind, placebo-controlled trial. Archives of Neurology. 2012; 69: 1044-1051.

7 Wergeland S, Torkildsen O, Myhr KM, Bo L. Polyunsatturated fatty acids in multiple sclerosis therapy. Acta Neuroligca Scandinavica Suppl. 2012: 195; 70-75.

8 Dworkin, R. H., Bates, D., Millar, J. H. D. & Paty, D. W. Linoleic acid and multiple sclerosis: a reanalysis of three double-blind trials. Neurology. 1984; 34, 1441-1445.

9 Loken-Amsrud KI, Myhr KM, Bakke SJ, Beiske AG, Bjerve KS, Bjornar? BT, Hovdal H, Lilleaas F, Midgard R, Pedersen T, ?altyt? Benth J, Torkildsen O, Wergeland S, Holmoy T. Retinol levels are associated with MRI disease activity in multiple sclerosis. Multiple Sclerosis. . 2013; 19: 451-457.

10 Loken-Amsrud KI, Myhr KM, Bakke SJ, Beiske AG, Bjerve KS, Bjornar? BT, Hovdal H, Lille?s F, Midgard R, Pedersen T, ?altyt? Benth J, Torkildsen O, Wergeland S, Holmoy T. Alpha-tocopherol levels are associated with MRI outcomes in multiple sclerosis. PloS one. 2013;8:e54417.

11 Torkildsen O, Loken-Amsrud KI, Wergeland S, Myhr KM, Holmoy T. Fat soluble vitamins as modulators of disease activity in multiple sclerosis. Acta Neurologica Scandinavica Suppl. 2013; 196: 16-23.

12 Salzer J, Hallmans G, Nystrom M, Stenlund H, Wadell G, Sundstrom P. Vitamin A and systemic inflammation as protective factors in multiple sclerosis. Multiple Sclerosis. 2013; Jan 18. [Epub ahead of print].

Conflict of Interest:

None declared

This is excellent work, and something most of us, i would like to think,know for a very long time!

Time pressures is the single most important factor, aside from lack of knowledge and skills, that results in acts of commission or omission, sometimes with harm ensuing. Something akin to "system error"

A GMC backed study recently suggested, due to time pressures, GPs find it difficult to achieve the requisite amount of CPD. And then there was the major study on prescribing errors in primary care recently and an important theme there was time pressures disabling GPs from getting it right all the time. The RCGP, unless i am wrong, has called for extension of the consultation time from 10 to 15minutes- i agree.

Can you imagine, comparing us to other professionals like Lawyers or others, which reasonable man on the Clapham Omnibus would consider 10 minutes as anywhere satisfactory for a proper holistic safe consultation? When patients are told they only have 10 minutes they are often shocked to hear this.

Whereas one can appreciate that to get through the workload in ones day,short consultations time are the only way round that, i would argue the end does not justify the means however way you look at it.

Conflict of Interest:

None declared