References
1 Bonita R. Epidemiology of stroke. Lancet 1992; 339:
342–344.
2 Bath PMW. Treating acute ischaemic stroke. Br Med J
1995; 311: 139–140.
3 The International Stroke Trial (IST): a randomised trial
of aspirin, subcutaneous heparin, both or neither among
19435 patients wit...
Stroke is th e th ird m ost com m on cau se of d eath in com e w as looked at as a m ajor en d -p oin t. In th e IST
th e West an d th e com m on est cau se of ad u lt d is- 6-m on th ou tcom e figu res (Figu re 1), th ere w ere on ly
ability. 1 Un fortu n ately, efficaciou s treatm en ts h ave 1.3% m ore p eop le in d ep en d en t in th e asp irin grou p
rem ain ed elu sive 2 u n til recen tly. A n atu ral startin g com p ared w ith th e n on -asp irin grou p . Con trasts can
p oin t for d evelop in g treatm en ts for acu te isch aem ic be m ad e h ere w ith th e NINDS rt-PA 5 stu d y w h ere
stroke h as been to assess su ccessfu l th erap ies for th rom bolysis w as sh ow n to be associated w ith a 11–
an oth er vascu lar con d ition , m yocard ial in farction , 13% im p rovem en t in th e best clin ical ou tcom e w ith
in p articu lar asp irin , h ep arin an d th rom bolysis. a sim ilar n on -sign ifican t im p rovem en t in m ortality.
Th e qu estion w h eth er asp irin is first, ben eficial So it w ou ld seem th at rt-PA is u n d en iably m ore
an d secon d , safe in th e acu te stages of stroke h as effective. How ever, in favou r of asp irin is th e fact
been ad d ressed in tw o recen t m egatrials: th e In ter- th at on ly a sm all p rop ortion (,10% ) of p atien ts
n ation al Stroke Trial (IST)3 an d th e Ch in ese Acu te p resen tin g w ith isch aem ic stroke w ou ld satisfy cri-
Stroke Trial (CAST).4 Th e IST also looked at tw o teria for th e u se of th rom bolysis, com p ared w ith
d oses of su bcu tan eou s u n fraction ated h ep arin ; a asp irin w h ich cou ld be given to m ost (.90% ).6
‘ven ou s’ d ose of 5000 IU b.d . an d an ‘arterial’ d ose At first glan ce it w ou ld seem th at h ep arin w ou ld
of 12 500 IU b.d . Both trials h ad arou n d 20 000 h ave n o role in th e acu te treatm en t of stroke. In th e
p atien ts. IST h ad a 2×3 factorial d esign an d alth ou gh IST p rim ary ou tcom e m easu res (Table 1), th e sm all
ran d om ised w as n ot p lacebo-con trolled or blin d . acu te m ortality ben efit w as n ot reflected at 6 m on th s
CAST w as a p lacebo-con trolled an d d ou ble-blin d
trial of asp irin alon e. Table 1 Su m m ary of th e m ain trial ou tcom es, % even ts p re-
Th e asp irin resu lts from th e tw o trials w ere very ven ted . (All th e d ata is com bin ed in on e table bearin g in m in d
sim ilar (Table 1). Wh en takin g th e p rim ary ou tcom e d ifferen ces in treatm en t p eriod an d sp ecified ou tcom es in IST
m easu res, early d eath , an d later d eath or d ep en - an d CAST)
d en cy, th ere is a tren d tow ard m ortality red u ction
IS T CA S T
in th e acu te stages (ju st statistically sign ifican t in
CAST), an d a sm all ben efit is also seen in th e later
A sp vs N o Hep vs N o A sp vs N o
en d -p oin ts. How ever, it is on ly by com bin in g th e
trials an d th e early en d -p oin t w ith early recu rren t Prim ary ou tcom es
n on -fatal stroke th at a reason ably con vin cin g stat-
Death early 0.4 0.3 0.54
istical resu lt is obtain ed . By d oin g th is an absolu te 2 w eeks (IST) NS NS 2P = 0.04
red u ction (AR) in early d eath an d n on -fatal stroke 4 w eeks (CAST)
by 0.9% (2P = 0.001) an d late d eath an d d ep en d en cy
Death / Dep en d en ce 1.3 0 1.14
by 1.3% (2P = 0.01) is seen . By far th e m ost strikin g 6 m on th s (IST) NS NS NS
resu lt to com e from th ese trials is th e red u ction in Disch arge (CAST)
early recu rren t isch aem ic stroke w ith asp irin , an d
p resu m ably a large p art of th e later m ortality an d S econ d ary ou tcom es
d ep en d en cy ben efit w as d u e to th is. Th e acu te u se Recu rren t Isch aem ic 1.1 0.9 0.47
of asp irin can be recom m en d ed on th is basis, m ore Stroke 2P , 0.001 2P , 0.01 2P = 0.01
so th an for th e acu te treatm en t of th e in itial cere- Haem orrh agic −0.1 −0.8 −0.21
bral in farction . Stroke NS 2P , 0.00001 NS
Th is con clu sion w ou ld also ap p ly if a good ou t- All 0.9 0.2 0.16
2P , 0.001 NS NS
Corresp on d en ce: Dr Roh an Path an sali, Clin ical Research Fellow , Tran sfu sed or fatal 2P , 0.001 2P , 0.00001 2P = 0
Kin gs College Hosp ital, Bessem er Road , Lon d on , UK extracran ial bleed
Received an d accep ted 1 October 1997
The benefits of buying summaries with Stuvia:
Guaranteed quality through customer reviews
Stuvia customers have reviewed more than 700,000 summaries. This how you know that you are buying the best documents.
Quick and easy check-out
You can quickly pay through credit card or Stuvia-credit for the summaries. There is no membership needed.
Focus on what matters
Your fellow students write the study notes themselves, which is why the documents are always reliable and up-to-date. This ensures you quickly get to the core!
Frequently asked questions
What do I get when I buy this document?
You get a PDF, available immediately after your purchase. The purchased document is accessible anytime, anywhere and indefinitely through your profile.
Satisfaction guarantee: how does it work?
Our satisfaction guarantee ensures that you always find a study document that suits you well. You fill out a form, and our customer service team takes care of the rest.
Who am I buying these notes from?
Stuvia is a marketplace, so you are not buying this document from us, but from seller StudyCenter1. Stuvia facilitates payment to the seller.
Will I be stuck with a subscription?
No, you only buy these notes for $11.49. You're not tied to anything after your purchase.