Intravesical Therapy: Old trials, new agents and new approaches

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Intravesical Therapy Old trials, new agents and new approaches Hugh Mostafid North Hampshire Hospital, Basingstoke

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A presentation is a part of a BJUI.org Virtual Edition on Intravesical therapies. View the whole open access article on www.bjui.org.

Transcript of Intravesical Therapy: Old trials, new agents and new approaches

Page 1: Intravesical Therapy: Old trials, new agents and new approaches

Intravesical Therapy

Old trials, new agents and new approaches

Hugh Mostafid

North Hampshire Hospital, Basingstoke

Page 2: Intravesical Therapy: Old trials, new agents and new approaches

What can the old trials tell us?

Outcome

• Recurrence

• Progression

Factors which affect it

• Single Dose• Timing• Induction• Maintenance• Which Drug• Drug optimisation

Page 3: Intravesical Therapy: Old trials, new agents and new approaches

What can the old trials tell us?

Single Dose

• Meta-analysis of 7 RCTs• 1476 pts with IC within 24 hours

• Single instillation reduced recurrence rate from 48.4 to 36.7%

• No difference between MMC, Epirubicin and Doxorubicin

Sylvester 2004

Timing• Recurrence lower if given within 6 hours cf. 24 hours

• If instillation > 24 hours, recurrence rate is doubledKaasinen 2002

Page 4: Intravesical Therapy: Old trials, new agents and new approaches

Survey of UK intravesical chemotherapy practice

527 consultant questionnaires produced 313 evaluable responses

• 244 (82%) advocated single dose of MMC• 155 (64%) use within 24 hours• 10 (4%) use immediately

69 Don’t give single dose 84 give single dose > 24 hours

• 23 (8%) use MMC as 1st line for G3 pT1• 20 (7%) use MMC as 1st line for CIS

Clarke 2006

153 consultants outside EAU guidelines

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What can the old trials tell us?

EAU guidelines 2006 • Unnecessary for solitary G1/2 pTa tumours (50%)

• Necessary for large (>3 cm) and mutifocal tumours (35%)

• High risk tumours (G3 pT1 , CIS) require BCG (15%)

Based on meta-analysis of EORTC and MRC trials Pawinski 1996

Induction therapy (6 courses)

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What can the old trials tell us?

Maintenance therapy

Meta-analysis of 9 RCTs

• 1774 pts, maintenance MMC• Recurrence rate (RR) 38% with maintenance cf. 54% in TURBT only group Nilsson 2001

2 EORTC trials (MMC and Doxorubicin)

• Monthly instillations for 6 or 12 months• No effect on RR if 1st instillation given after TURBT Bouffioux 1995

To date no prospective studies show a difference in RR or time to recurrence between induction and maintenance Rx

Malmstrom 2004

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What can the old trials tell us?

Which Drug?

No differenceThiotepa 44%Adriamycin 39%Mitomycin C 36%Epirubicin 39% Kamat 2000

MMC superior?• Stratified data from meta-analysis of 8 RCTs comparing

intravesical chemotherapy with BCGHuncharek 2004

Recurrence rate

Page 8: Intravesical Therapy: Old trials, new agents and new approaches

Optimising intravesical chemotherapy

• RCT 119 pts: 6/52 Standard vs Optimised RxNaHCO3 to urine pH

Overnight fasting to U.O

Bladder residual emptied

40 mg MMC given

• At 5yrs

Time to recurrence % Recurrence free

Optimized MMC 29.1 41

Standard MMC 11.8 24.6

Au 2001

MMC optimized treatment

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Optimising intravesical chemotherapy

Turning the patient?

• No mention in any trial, paper, abstract,review or guideline

• Often difficult to achieve practically

Better to focus on

• Timing of single dose

• Maintenance instillations Fasting for 6 hours

Empty bladder residual

(Alkalinisation of urine)

Page 10: Intravesical Therapy: Old trials, new agents and new approaches

Optimising intravesical chemotherapy

Synergistic effect?

• 137 pts with G3pT1

• Combined MMC and Epirubicin maintenance

• Significantly lower RR than MMC, doxorubicin or Epirubicin

aloneSeretta

2004

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What can the old trials tell us?

1. Does intravesical chemotherapy alone prevent progression?

No - EORTC / MRC meta-analysis Pawinski 1996

No proof that any chemotherapeutic agent alone, either as early instillation or maintenance prevents progression or improves

disease-specific survivalOkeke 2005

Progression

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What can the old trials tell us?

2. Is BCG superior to intravesical chemotherapy at preventing progression?

Only if maintenance BCG given:Meta-analysis of 24 RCTs, 4863 patients Sylvester 2002

Meta-analysis of 9 RCTs, 2410 patients Bohle 2004

Differences due to failure to control for prior chemotherapy RxMeta-analysis of 8 RCTs, 2427 patients Huncharek 2004

Progression

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Mode of action

• Prevent reseeding Zincke 1983

• Destroys residual tumour- ‘Chemoresection’ Masters 1999

• Not able to compensate for incomplete resection Divrick 2006

• May provoke significant alterations in the normal

urothelium which could be mistaken for malignant

lesions Mazzucchelli 2005

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Complications of Intravesical Chemotherapy

Adverse effects • Chemical cystitis 40% • Allergic skin reactions 16%

Systemic complications• Severe Myelosuppression: A few reported cases after v.high

doses or early instillation after v.large resection area Thrasher 1992

• Maintenance has higher incidence of adverse events owing to higher cumulative doses Schenkman 2004

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Complications of Intravesical Chemotherapy

Severe local complications after early instillation of MMC• 6 case reports• Only 2 required surgical intervention • No long term sequelae

Severe complications after MMC maintenance Rx• 4 case reports• None required surgery• No long term sequelae

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New Agents - Phase I studies

Pirirubicin Okamura 2002

Valrubicin Steinberg 2000

Vinorelbine Bonfil 2001

Meglumine -linolenic acid Harris 2002

Recombinant human interleukin-12 Weiss 2003

Suramin Ord 2005

Docetaxel McKiernan 2006

Ethics of phase II studies in high risk BCG failures

Costs of phase III studies

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New Agents

Gemcitabine Lilly Pharmaceuticals

Phase II marker lesion studies • 6 weeks instillations: 56% CR Gontero 2004

• In total 6 phase II studies, total of 184 pts, CR 44-66%

Phase III studies• German co-operative group, immediate post-op gemcitabine

Will reach target of 328 patients in a few months• SWOG study, target 340 patients, starting soon

• No plans to license gemcitabine for intravesical use(coming off patent)

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New Agents

Apaziquone (EOquin) Spectrum Pharmaceuticals

• Phase II study in 46 patients: 6 instillations produced

67% CR of marker lesion Van der Heijden 2006

• Awaiting £350K funding and EORTC support for 800

patient Phase III study

• 6-8 years from completion

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New Approaches

• PDT 5-ALA Berger 2003

• Oral chemopreventionCelecoxib Mohammed 2006

Tegafur (5-FU precursor) Kubota 1999

Verapamil + adriamycin Tsushima 1994

• Chemosensitivity testsIn vitro sensitivity assays Burgues 2005

• Bioadhesive microspheres

Adheres to urothelium

Releases Placitaxel LeVisage 2004

• Microwave Hyperthemia Colombo 2003

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New Approaches

•ElectroMotive Drug Administration

BCG once a week for 6 weeks (n=105) BCG infused once a week for 2 weeks, followed by 40 mg EMDA MMC for three weeks (n=107)

212 Stage pT1 patients

BCG once a month for 10 months 40 mg EMDA MMC once a month for 2 months followed by BCG once a month as 1 cycle, for 3 cycles

DiStasi 2006

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New Approaches

‘BCG-induced inflammation might increase the permeability of the bladder mucosa such that mitomycin can reach the target tissue more easily and exert its anticancer effect.’

DiStasi 2006

EMDA MMC + BCG

BCG Difference

Disease free interval (months)

69 21 48 p=0.0012

Recurrence %

41.9 57.9 16 p=0.0012

Progression %

9.3 21.9 12.6 p=0.004

Overall mortality %

21.5 32.4 10.9 p=0.045

Disease-specific mortality %

5.6 16.2 10.6 p=0.01

EMDA MMC/ BCG vs BCG:

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New Approaches

Problems of ward based intravesical chemotherapy

• Timing - giving drug within 6 hours

• Communication

• Who gives it ?

• Special precautions ≠ Open ward environment

• Monitoring patient

• Releasing drug after 1 hour

• Cytotoxic disposal

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Theatre administration

Advantages• Its been given!

• Urologist takes responsibility

• Administered in a controlled environment

• Pts are fasted for 6 hours: concentrates urine

• Known ‘no residual volume’

• Irrigation not required

• Patient asleep/drowsy for most of the hour

• Monitored continuously in recovery

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Results

• 16% not suitable: Deep resection

Large resection area

Invasive tumour

Heavy bleeding

• 195 instillations in 170 patients, Historical control group

Median follow-up (months)

Recurrence rate (%)

Theatre MMC 16 37.5

TURBT only 20 55.9

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Results

Complications

• 1 Spillage of MMC in recovery

• 1 Abdo pain in recovery MMC released early

• Discomfort same as post-op catheterised pts without MMC

• 12 trusts giving MMC in theatre: No reported adverse events

• Further 16 awaiting protocol clearance

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The future

• Chemo-resectionForthcoming EORTC trial

Pts choice: Immediate single dose MMC at Dx versus TURBT

• Antisense oligodeoxynucleotidesCauses chemosensitisation and increases cytotoxic potential of MMC

• Oncolytic retrovirus therapy Hanel 2004

Kausch 2006

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Conclusions

• No new drugs in the near future

Improve the effectiveness of what we have

• One immediate post-operative instillationAll patients: single, multi-focal or recurrent

In theatre or within 6 hours, fasting, no residual

• EMDA MMC/BCG for high risk non muscle invasive TCC

• Chemo-resection - will TURBT go the way of TURP?

Level I evidence