Filson 2016.
Study characteristics | |||
Patient sampling | Aim of the study: to evaluate the performance of MRI‐TBx in diagnosing clinically significant PCa Type of study: prospective cohort Selection: consecutive selection Enrolled/eligible: 1042/1042 (328 Bx‐naïve‐, 324 prior‐negative Bx‐ and 390 active surveillance men) Inclusion period: September 2009‐February 2015 |
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Patient characteristics and setting | Inclusion criteria: elevated PSA level or abnormal DRE or 2) confirmation of low‐risk PCa for men considering active surveillance Exclusion criteria: none reported Setting: Los Angeles, USA. University hospital Age*: median (IQR) 64.4 years (58.5‐69.4); 65.7 (59.3‐70.2) PSA*: median (IQR) 5.8 ng/mL (4.4‐8.1); 7,6 (5‐11.5) Prostate volume*: median (IQR) 45 mL (33‐61.5); 57.7 (39.8‐83.5) *respectively, for the Bx‐naïve‐ and prior‐negative Bx participant groups |
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Index tests | Index tests 1: MRI‐pathway: a 3 Tesla MRI machine (Trio Trim/Somatom, Philips) was used, with T2, DWI and DCE sequences. An in‐house Likert 1‐5 score was used, with threshold ≥ 3 for positivity. MRI‐TBx (Artemis fusion device (Eigen, Grass Valley, Calif) were taken first in case of a suspicious lesion, then SBx were taken Index test 2: transrectal 12‐core SBx were taken in all participants, after MRI‐TBx. No blinding for MRI is reported |
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Target condition and reference standard(s) | No reference standard is used in this agreement analyses study (MRI‐pathway vs SBx), therefore the reference standard domain is not applicable and disregarded. | ||
Flow and timing | All participants underwent the same reference test. All participants were included in the analysis. | ||
Comparative | |||
Notes | Participants on active surveillance (n = 390) were excluded from our analysis. Although in text 328 participants are reported in the biopsy‐naïve group, in the data tables 329 participants are reported | ||
Methodological quality | |||
Item | Authors' judgement | Risk of bias | Applicability concerns |
DOMAIN 1: Patient Selection | |||
Was a consecutive or random sample of patients enrolled? | Yes | ||
Did the study avoid inappropriate exclusions? | Yes | ||
Low | Low | ||
DOMAIN 2: Index Test SBx | |||
Was the MRI assessed without knowledge of the results of the (reference or other index) biopsies? | |||
Were the MRI‐TBx performed independent of the (reference or other index) biopsies? | |||
Was the performance of the SBx not influenced by the performance of the (reference or other index) biopsies? | Unclear | ||
Unclear | Low | ||
DOMAIN 2: Index Test MRI‐pathway | |||
Was the MRI assessed without knowledge of the results of the (reference or other index) biopsies? | Yes | ||
Were the MRI‐TBx performed independent of the (reference or other index) biopsies? | Yes | ||
Was the performance of the SBx not influenced by the performance of the (reference or other index) biopsies? | |||
Low | Low | ||
DOMAIN 3: Reference Standard | |||
Is the reference standards likely to correctly classify the target condition? | Yes | ||
Was the reference standard performed independent from the index test? | Yes | ||
Low | Low | ||
DOMAIN 4: Flow and Timing | |||
Did all patients receive the same reference standard? | Yes | ||
Were all enrolled patients included in the analysis, or were exclusions explained and not leading to a relevant bias? | Yes | ||
Low |