Philip Morris
Source of Funding and Outcome of Clinical Trials
Fields
- Author
- Davidson, R.A.
- Area
- WORLDWIDE REG AFFAIRS/LIBRARY
- Type
- PSCI, PUBLICATION SCIENTIFIC
- BIBL, BIBLIOGRAPHY
- CHAR, CHART, GRAPH, TABLE, MAPS
- BIBL, BIBLIOGRAPHY
- Attachment
- 2048252199/2048252525
- 2048252446/2048252450
- Named Organization
- NIH, Natl Inst of Health
- Named Person
- Caranasos, G.
- Davidson, R.A.
- Lea, E.
- Smith, S.
- Davidson, R.A.
- Document File
- 2048252198/2048252525/Bero Barnes (Ciar)
- Request
- Stmn/R1-048
- Litigation
- Stmn/Produced
- Author (Organization)
- Univ of Fl Gainesville
- Master ID
- 2048252379/2524
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- Characteristic
- ILLE, ILLEGIBLE
- Site
- N403
- Date Loaded
- 05 Jun 1998
- UCSF Legacy ID
- djs65e00
Document Images
rrom' acan sk rax A o- Loreen wicaipin
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Source of Funding and Outcome of Clinical Trials
RICHARD A. DAVIDSON, MD, MPH'
D.cau.e o( r.oent ccac.rar about coalifah of latats.t aad
prbUai.d r+s.areb. the artbar a.aysed JQ7 ceaholl.d
cUntca/ trfaL. 3tudf.s were claads.d as (a.oriap.ftia a
s.+w tb.rarFr or a tmdltioaal tb.wpy. and as b.lsp sr~
pxt.j by a pbarmoeaatktitl =z*ufacftu%w er aa belag Ora-
.ec11T sappotted. S.v..ltms p.r e.st of tbe tr9da lv.at.d
sew tb.ev*.:: 43% e! tb....a0 tasd.d b7 piazaac~..-
tical ti..ow OI the J1 Mals fa.ortap hodiH.ed tL.evpt.
.ay foat (19%t wae iupporl.d b7 a pharaenslfcal tErom.
7iee* was a stoltstteQly .fp.ificant aarociattoa b.ews.a
the aotrce d(oadisp and the oatcome el the stStdy (p a
8.0QL. Few trlala ssppoat.d by pharaaac.utlcal .m.afoc-
tsarrs favorrd leedttlasal tfna"r soese no.aas tas fhts

rromacan s rax i o- Loreen ivicaipin
4
1ss
7S(71 %)
Favored new therapy
33(43%)
Phanrxacsutiaaliy
supported
un~c. . ...,... ~ .. . ....... ....ti.......
j,aS/%Ql0I7. SOUPCE OF FUNIXNG ANO SiUOY U7TCOME
107 trials
31(25%)
Favorod traditional therapy
43(57%) 403%)
Q.w.ra/!y fh.rssa..rt)cally
supported suOPortad
Chl sq.r. = 9.045, p =.002
Trials were then classified by funding source.
A trial was considered "pharmacwutically sup-
pocted,, if a drug company .vas noted in the ac-
kisowled9ements as having provided support for
the study or any of its investigators (a study was
not classified as pharmaceutically supported if a
drug company provided only drugs or placebos).
All other studies were classified as generally sup-
ported, whether funding sources were noted or not.
Statistical analysis was by chi square.
RESULTS
One hundred and twenty-six trials were re-
viewed; 107 trials met the final inclusion criteria.
Of the remaining 19 triaL, 13 were published in
symposia, two were actually caselcontrol studies,
two used pooled data, one measured no clinical
outcomes, and one compared different dosages of
the same drug.
There was a statistically significant associa-
tion between the source of funding and the outcome
of the study (p = 0.002), with studies supported by
pharmaceutical manufacturers favoring new ther-
apies in comparison with generally supported
studies (Fig. I). The distribution of studies by jour-
nal, results, and funding source is shown in Table
1. The ratios of articles favoring new to those fa-
voring traditional therapies varied from 6 to 1 in
the Annals of Internal Medicine to 1 to 1.4 in the
American Journal of Medicine.
Twenty-two studies evaluated non-pharma-
cologic therapies such as sclerotherapy," hypno-
therapy, t' or oxorcise." If such studies more fre-
quently had negative results, the analysis could
have been biased, since phoanaceutical firms are
much more likely to fund studies of pharmaceutical
agents. In fact, 60% of studies of non-pharmaco-
logic therapies favored the new therapy in com-
parison with 71% of the overall group, and only one
2 7(a7%)
Gen.ra)ly
srpported
17pucs t. D=atptla
of 107 aInlal trtslsk
of the 22 was pharmaceutically supported. For this
reason. an analysis that included pharrnacologic
studies only was prepared. Tha strength of the as-
sociation between funding and results dscreassd
somewhat but remained statistically significant (p
= 0.007).
Analysis of sample size per group revealed no
significant differences between the pbazmac.ufi-
cally supported and generally supported studies
(Table 2). With regard to blinding, 67.5% of the
pharmaceutically supported studies specificallY
mentioned that blinding was carried out, compared
with only 41.8% of the generally supported studies
(p - 0.01). However, this was a reflection of the
non-pharmacologic studies, which utilized inter-
ventions that could not easily be blinded. Analysis
(PhG
outc
f.ct
alon
souz
ship
!ry f
clast
Imn.
3tud:
that
conh
what
ical t
tria2.
ment
less
studi
thesw
ative
smai
error
snt).'
tors.
samF
to de
feren
journ
icant
mace
P
sults
of pharmacologic studies alone revealed no sig- I Sour
nificant difference in rates of blinding between the
two funding sources. (p = 0.46).
Among the four pharmaceutically supported
studies favoring traditional therapies, one sug-
gosted that the therapy, v.hile not improving over-
all survival, ". .. may be helpful early in the course
of the disease and in c.rtaia subgroups of pa-
tients:'10 Another compared two therapies mcmu-
factured by the sponsoring drug company.'S The
other two studiee, one comparing the lipid-reduc-
ing effects of d- and 1-thyroxine," and the other a
decision-analysis study evaluating the cost-eff.o-
tiveness of two antibiotics," were funded by com-
panies that did not produce any of the drugs
investigated. In no case wai a therapeutic agent
manufactured by the sponsoring company found to
*w Eij
PS
G5
txXar
PS
GS
Mnals a
PS
QS
PS
c=
be inferior to an alternative product manufacturQd ar
by another company. ~
~ .~
DISCUSSION I - r.)
Ln
~~
This study has demonstrated a statisticaitf ~
~
significant association between source of fundinQ ncrnt
na

~ ~
d-
JauRW oF GExcs+u tecrMAL t.teflKrrt. Vdume 1(AIayUune). 15196
(phcamaceutical firm versus Qeneral support) a.nd
outcome of published clinical trials. Cause and ef-
f.et cannot be inferred on the basis of this study
aion:. Other factors associaied with both funding
source and outcome may confound the relation-
ship. Also, it is possible that the chatacterisation
by funding source may have inadvertently mis-
datsified some studi.s becaus. of inaccurate ac-
knowledgements, underestimating the number of
studies funded by pharmaceutical firms.
"Publicati.on biaa." in this case a gceata chance
that a study will be accepted for publication if it
contains a positive result, may d.termine, in part,
what appears in journals. One discussion of clin-
ical triaL'' suggested that for every clearly positive
triai, there are five to ten trials comparing treat-
ments that o=e equally effective. It is possible that
1as well-known journals might publish negative
studies more frequently, and thus ha.* more of
th.se studies submitted. Furthermore, many neg-
ative studies are methodologically weakened by
small sample sises and the possibility of a Type II
error (the inability to detect a true difference if pres-
nt).1r This may make them less attractive to edi-
toss. It is possible that funding may influence
sample sise, which in turn might aff.ct the ability
eo detect clinically or statistically significant dif-
ieseaces, or the chance of publication in a major
journal. In fact, in this study there were no siQnif-
icant differences in sample siae between phar-
maceutically and generally supported studies.
Publication bias alone cannot explain the re-
sults of the current study, as there .vas a higher
TABLE I
Sourc@s of Fundkq arad Outmmes of 107 Ciinical Trta(s by Journal
~ ~ r ~En.glxr'd Jovrnal of Medicine
Cs
s-
1 ~ tazxC
e i PS
~ GS
~ , Mn~1s of lnterna/ McYlklne
!( PS
C.S
Favorinu
Naw
Tmtment Favaina
Traditlonal
Trsatttwnt
ToLaf
~ 1 to
9 8 17
8 0 8
Zz 10 32
6 1 7
6 1 7
3 2 5
2 5 7
7 0 7
4 3 7
Ti1fi.E 2
Sarnple Size psr Grow Rt mumamtk* Slspportsd
and Qrsrs{!y Suppostsd CHna! Trtsls
157
Sarrrpf. stae
p.r c.rmip Phwmaceutic.t S4port (%)
(n = 37) GWWat 9upport (%)
(n - 70)
s15 6(16) 15 (21)
1 t~r5o 18(49) 28(40)
>50 13(35) 27(39)
No siQNncant Offirance betwem Pnam,acastsotly suppoctna and
generaity wppattaa trtaLL
proportion of published studies favoring nevw ther-
apies funded by drug companies compared with
those getting general support. Whilo it is possible
that editors and reviewers preferentially rtjsct
negative pharmaiceuticallT supported studies, an
alternative (and more likely) explanation is ::iat
fewer of these studies are submitted.
DruQ companms may select foc study drugs that
have been previously shown to be efficacious, in
some cases in other eountries; these trials aze more
likely to favor tha therapy. As a study pnoQresses,
and the accumulatinQ resuits appear negatie.,
companies may conserve funds by discontinuing
the study prior to exclusion of a Type II error. In-
vestigators may fear discontinued funding if neg-
ative trials are submitted and published. and may
be pressured not to submit such trials. The com-
bination of these occurrences could contsibute to
the high publication rate of pharmaceutically sup-
ported studies favoring new rather than traditional
therapies.
While it seems unlikely that conspiracies to
suppress unfavorable results of clinical trials exist,
a de facto exclusion of negative results may be
occurring. There are almost certainly many causes
for this exclusion. related to decisions by phar-
maceutical firms, investigators, and editors. The
characterization of the factors leading to publica-
tion has been recently addressed by Shapiro. who
noted that "To publish on drug effects is to risk the
anger or pleasure of ... practicing physicians, the
research community, regulatory agencies. drug
manufacturers, and the public. Each constituency
has its own unique interests, and consciously or
unconsciously exerts its own unique pres.eures.",0
Further investigation into the fate of phar-
maceutically supported studies would be aa ap-
propriate next step. Research divisions of phar-
maceutical firms could provide information
regarding the numbers of studies funded and com-
pleted, results, and publication outcomes. Critical
review and analysia of thia type of informatioa could
help ensure the objectivity of scientific research.
PS = study whdry or partialfy funded by a pharsnaceutkal firm.
The awtor xknwrledges the uig vrxe of 5opfiia Smlth in dve pcrforrtvnce of this
GS = generai support (no evidence of support by a pharmaceutical
study. George Granasas in the review of the manusrs(pL and Evelyn Lea in the
km)-
preparaGon of rhe nunuxript.

ISa
DavioWn. SouRa OF Furvanc A+w STUOr OuRa.+e
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REFLECTIONS
[nowl.dQv oad Wisdom, fm from beinQ one,
Eiavn ofttims no conn.xion. KnowledQe dw.lls
In haads r.rpiet..vith thoughts of oth.c men;
Wisdom in minds attentive to their own.
Knowledge is proud that he has lamn'd so much;
Wisdom is humble that he knows no maz..
Wu.uas~ CoWPEt
"Th. Task"
copied from Poeticd WorJri, voL II,
Little. Brown, Bo.ton. 1859
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