丙肝用药单一，已经硬化的能否进来聊聊经验和症状。

liver411

Investigational HCV Protease Inhibitor BI 201335 Exhibits Promising Antiviral Activity

By Liz Highleyman

Given the limited efficacy and side effects of interferon-based therapy for chronic hepatitis C virus (HCV) infection -- especially among patients with hard-to-treat HCV genotype 1 -- investigators have explored several small molecule agents (dubbed "STAT-C") that directly target various steps of the viral lifecycle.

One such candidate, BI201335, is an HCV NS3 protease inhibitor being developed by Boehringer-Ingelheim. Two posters with results from a Phase 1b study of BI201335 were presented last week at the 59th Annual Meeting of the American Association for the Study of Liver Diseases (AASLD 2008) in San Francisco.

Treatment-naive Patients

Study 1220.2 is a multinational clinical trial evaluating the pharmacokinetics, safety, and antiviral activity of multiple ascending doses of BI201335 monotherapy for 14 days, followed by triple therapy with BI201335 + pegylated interferon + ribavirin for an additional 14 days.

The first analysis looked at 34 treatment-naive patients with genotype 1 chronic hepatitis C in the U.S., France, Germany, and Spain. Most participants (27) were men, all but 1 were white, the mean age was about 49 years, and Metavir fibrosis scores were 0-3.

Participants were randomly assigned to receive placebo or 1 of 4 doses of once-daily BI201335: 20 mg (n=8), 48 mg (n=9), 120 mg (n=9), or 240 mg (n=8). BI201335 was given as monotherapy for 14 days. Patients with less than a 1 log10 decrease in HCV RNA at day 10 had BI201335 discontinued after day 14. Those with at least a 1 log10 decrease at day 10 continued on BI201335, adding 180 mcg/week pegylated interferon alfa-2a (Pegasys) + weight-adjusted ribavirin from day 15 through Day 28.

Results

    • A rapid decline in HCV viral load was observed in all patients, with maximal decline 2-4 days after starting BI201335.

    • With the exception of 1 patient in the 20 mg group, all participants receiving BI201335 (96.2%) achieved > 2 log10 decline in HCV RNA during the monotherapy period.

    • 100% of patients in the 48 mg, 120 mg, and 240 mg BI201335 dose groups achieved > 2.8 log10 drop in HCV viral load during the first few days of monotherapy.

    • Median maximal reductions in viral load during the 14-day monotherapy period were 3.0 log10 in the 20 mg arm, 3.6 log10 in the 48 mg arm, 3.7 log10 in the 120 mg arm, and 4.2 log10 in the 240 mg arm, versus no significant change in the placebo group.

    • A majority of patients in all dose groups experienced viral load rebound during the first 14 days of monotherapy.

    • Population sequencing of the NS3/NS4A protease at baseline and after viral rebound revealed selection of HCV variants previously shown to confer resistance to BI201335 in vitro.

    • BI201335 was generally well-tolerated, with no observed dose-dependent increases in adverse events (AEs).

    • No patients discontinued treatment during the monotherapy period due to AEs.

    • AEs observed while on combination therapy were typical for pegylated interferon + ribavirin.

    • Changes in bilirubin were observed with increasing doses of BI 201335.

    • One serious AE (asthenia, or muscle weakness) occurred in an individual in the 20 mg dose arm 6 days after starting pegylated interferon + ribavirin.

In conclusion, the investigators stated, "BI 201335 as monotherapy for 14 days followed by combination with [pegylated interferon + ribavirin] for [an] additional 14 days was well tolerated, and induced a strong and rapid antiviral response."

"The results support further study of BI201335 as a once-daily potent antiviral for treatment-naive HCV patients," they added.

Medizinische Hochschule Hannover Zentrum Innere Medizin, Hannover, Germany; Hopital Saint Joseph, Marseille, France; Hopital Pitie Salpetriere, Paris, France; California Pacific Medical Center Research Institute, San Francisco, CA; Charité Berlin Campus Virchow-Klinikum, Berlin, Germany; Hopital Hotel Dieu, Lyon, France; Central Texas Clinical Research, Austin, TX; Hopital Cochin, Paris, France; Boehringer Ingelheim Pharma, Ridgefield, CT; Hospital Universitario Puerta de Hierro, Madrid, Spain.

Treatment-experienced Patients

Study 1220.2 also included a cohort of 19 treatment-experienced patients with genotype 1 chronic hepatitis C who experienced confirmed virological failure (< 2 log reduction in HCV RNA from baseline) during or after previous combination therapy with approved doses of pegylated interferon + ribavirin. Here, too, a majority of participants were men, all were white, and the mean age was 49 years.

This part of the study was open-label, and all patients received BI201335 at doses of 48, 120, or 480 mg once-daily in combination with standard doses of Pegasys + ribavirin for 28 days (none received monotherapy or 20 mg BI201335).

Results

    • Here again, a rapid dose-related decline in HCV RNA was observed in all patients.

    • All participants treated with BI201335 + pegylated interferon + ribavirin achieved > 2 log10 decline in HCV viral load.

    • Median maximal declines in HCV RNA during 28-day combination therapy were 4.8 log10 in the 48 mg arm, 5.2 log10 in the 120 mg arm, and 5.3 log10 in the 240 mg arm.

    • 2 of 6 patients (33%) in the 48 mg group and 1 of 7 (14%) in the 120 mg group experienced virological rebound during the first 28 days of triple combination therapy.

    • In these patients, sequencing of the NS3/4A protease revealed variants with known BI201335 resistance mutations.

    • No viral rebound during treatment was seen in the 240 mg dose arm, and 5 of 6 patients (83%) in this group had HCV RNA < 25 IU/mL at day 28.

    • Again, BI201335 was well-tolerated and no serious drug-related AEs were observed.

    • AEs were typical for pegylated interferon + ribavirin.

    • 1 participant discontinued treatment due to anxiety.

"BI201335 given once-daily in combination therapy with [pegylated interferon + ribavirin] for 28 days was well tolerated, and induced a strong and rapid antiviral response," the researchers concluded. "The results support further study of BI201335 as a potent protease inhibitor for [pegylated interferon + ribavirin] treatment-experienced HCV patients."

Medizinische Hochschule Hannover Zentrum Innere Medizin, Hannover, Germany; Hopital Saint Joseph, Marseille, France; Hopital Pitie Salpetriere, Paris, France; I. Med. Klinik und Poliklinik, Mainz, Germany; Universitätsklinikum Düsseldorf, Düsseldorf, Germany; Hopital Cochin, Paris, France; California Pacific Medical Center Research Institute, San Francisco, CA; Boehringer Ingelheim Pharmaceuticals, Inc, Ridgefield, CT.

11/11/08

References
MP Manns, M Bourliere, Y Benhamou, and others. Safety and antiviral activity of BI201335, a new HCV NS3 protease inhibitor, in treatment-naive patients with chronic hepatitis C genotype-1 infection given as monotherapy and in combination with Peginterferon alfa 2a (P) and Ribavirin (R). 59th Annual Meeting of the American Association for the Study of Liver Diseases (AASLD 2008). San Francisco. October 31-November 4, 2008. Abstract 1849.

MP Manns, M Bourliere, Y Benhamou, and others. Safety and antiviral activity of BI201335, a new HCV NS3 protease inhibitor, in combination therapy with Peginterferon alfa 2a (P) and Ribavirin (R) for 28 days in P+R treatment-experienced patients with chronic hepatitis C genotype-1 infection. 59th Annual Meeting of the American Association for the Study of Liver Diseases (AASLD 2008). San Francisco. October 31-November 4, 2008. Abstract 1882.

liver411

很多试验性治疗/试药在管道中..


HCV Experimental Treatments
ACH 806 (HCV Protease Inhibitor)
Albumin Interferon
BI 201335 (protease inhibitor)
Boceprevir (aka SCH 503034)
Celgosivir
GS 9132 and GS 9190
HCV 759 (HCV Polymerase Inhibitor)
HCV-796 (HCV Polymerase Inhibitor) *Development Halted April, 2008
ITMN 191
MK-0608
R-1626 and R-7128
STAT-C Agents
Telaprevir (aka VX-950)
TMC435350
Valopicitabine (aka NM 283)
Viramidine (aka Taribavirin)

ACH 806 (HCV Protease Inhibitor)

In Vitro Studies Suggest Promising Outcomes with New HCV Protease Inhibitor ACH 806 in Combination with Interferon, Telaprevir, or NM 107 - 5/05/07


Albumin Interfern

Albumin Interferon (Albuferon) Administered Once Every 2-4 Weeks May Be As Effective as Once-weekly Pegylated Interferon - 9/23/08

Safety and Activity of Once-Monthly Albinterferon Alfa-2b (Albuferon) in Genotype 2/3 Chronic Hepatitis C Patients - 5/23/08

Antiviral Activity, Pharmacodynamics, and Quality of Life in Genotype 1 Hepatitis C Patients Treated with Albinterferon (Albuferon) - 5/23/08

Albuferon Dose in Ongoing Trials is Lowered Due to Safety Concerns - 1/25/08

Albumin Interferon May Be as Effective as Pegylated Interferon with Less Frequent Dosing - 5/05/07


BI 201335 (protease inhibitor)

Investigational HCV Protease Inhibitor BI 201335 Exhibits Promising Antiviral Activity - 11/11/2008

Safety and antiviral activity of BI 201335, a new HCV NS3 protease inhibitor, in treatment-naïve patients with chronic hepatitis C genotype 1 infection given as monotherapy and in combination with peginterferon alfa-2a (P) and ribavirin (R) - 11/05/2008

Safety and antiviral activity of BI 201335, a new HCV NS3 protease inhibitor, in combination therapy with peginterferon alfa-2a (P) and ribavirin (R) for 28 days in P+R treatment-experienced patients with chronic hepatitis C genotype 1 infection - 11/05/2008


Boceprevir (aka SCH 503034)

HCV Protease Inhibitor Boceprevir plus Pegylated Interferon/Ribavirin Increases Sustained Virological Response Rate: SPRINT-1 Study - 11/04/2008

74 Percent of Genotype 1 HCV Patients in Experimental HCV PI Boceprevir Phase II Study Achieve Sustained Virologic Response (SVR) at 48 Weeks - 8/05/2008

Schering Plough Initiates Phase 3 Studies with Experimental Oral HCV Protease Inhibitor Boceprevir in Treatment-naive HCV Patients and in Those Who Failed Prior Treatment - 5/23/08

Boceprevir (NS3 Protease Inhibitor) Combination Therapy in Non Responders: Phase II Dose Finding Study - 4/29/08
E Schiff and others. EASL 2008.

Interim Results from HCV SPRINT-1: RVR/EVR from Phase 2 Study of Boceprevir Plus Peginterferon alfa-2b/Ribavirin in Treatment-Naïve Subjects with Genotype-1 CHC - 4/29/08
K Lawitz and others. EASL 2008.

Boceprevir Added to Pegylated Interferon/Ribavirin Increases Sustained Response in Treatment-naive Patients and Some Prior Non-responders - 4/29/08

Polymerase Inhibitor NM107 and Protease Inhibitor Boceprevir Show Enhanced Anti-HCV Activity in Combination - 12/07/07

Combination Therapy with HCV Protease Inhibitor Boceprevir Produces a High Rate of Early Virological Response in Genotype 1 Hepatitis C Patients - 10/23/07

Enhanced Clinical Effects and Favorable Resistance Profile with Combination of Boceprevir Plus HCV-796   - 5/20/07

Schering’s Experimental Oral HCV Protease Inhibitor Boceprevir Appears Safe in Patients with Varying Degrees of Liver Impairment - 5/05/07

Mutations That Confer Resistance to HCV Protease Inhibitors 5/05/07

Combining Experimental HCV Inhibitors Boceprevir and NM 107 Enhances Anti-HCV Activity and Suppresses Emergence of Resistance - 5/05/07

Mutations That Confer Resistance to HCV Protease Inhibitors 5/01/07

In Vitro Studies Suggest Promising Outcomes with New HCV Protease Inhibitor ACH 806 in Combination with Interferon, Telaprevir, or NM 107 4/05/07

Update on Clinical Development Program for HCV Protease Inhibitor SCH 503034 - 4/28/06

THE HCV NS3 PROTEASE INHIBITOR SCH 503034 IN COMBINATION WITH PEG-IFN-ALPHA-2B IN THE TREATMENT OF HCV-1 PEG-IFN-ALPHA-2B NON-RESPONDERS: ANTIVIRAL ACTIVITY AND HCV VARIANT ANALYSIS - 4/28/06

Open Clinical Trial of New PI SCH 503034 Plus PegIntron in HCV Patients Nonresponsive to Prior Treatment with Peginterferon Plus Ribavirin - 2/17/06

Celgosivir

Adding Celgosivir to Standard Hepatitis C Therapy Increases the Likelihood of Early Response Rate in Prior Non-responders - 5/05/07

Celgosivir: Well-Tolerated, but Minimal Anti-HCV Activity as Monotherapy - 6/06/06

GS 9132 and GS 9190

Experimental HCV Polymerase Inhibitor GS 9190 Shows Promising Antiviral Activity but Possible Cardiac Side Effects in Phase 1 Study - 12/11/07

Despite Promising Early Data, Companies Discontinue Experimental HCV Protease Inhibitor GS 9132 - 2/13/07

Gilead and Achillion Announce Start of Phase 1 Clinical Trial of GS 9132, an HCV Protease Inhibitor for the Treatment of Hepatitis C - 8/24/05

HCV-796 (HCV Polymerase Inhibitor)

Naturally Occurring Resistance to HCV Protease and Polymerase Inhibitors in Treatment-naive Hepatitis C Patients - 1/09/2009

Natural Prevalence of Resistance to HCV Protease Inhibitors - 9/25/08

ViroPharma and Wyeth Halt Development of HCV-796 for Hepatitis C - 4/24/08

Novel HCV Polymerase Inhibitor VCH-759 Monotherapy Demonstrates Promising Antiviral Activity - 12/07/07

Experimental Polymerase Inhibitor HCV-796 is Safe and Effective in Combination with PegIntron or Pegasys - 12/07/07

HCV-796 Plus PegIntron Shows Greater Antiviral Activity Across All HCV Genotypes Than Either Agent Used Alone   - 5/20/07

Enhanced Clinical Effects and Favorable Resistance Profile with Combination of Boceprevir Plus HCV-796   - 5/20/07

HCV-796 Shows Antiviral Activity in Combination with Pegylated Interferon - 5/05/07

Experimental Agent HCV-796 Shows Activity in Preclinical Studies - 10/03/06

HCV Polymerase Inhibitor VCH-759

Naturally Occurring Resistance to HCV Protease and Polymerase Inhibitors in Treatment-naive Hepatitis C Patients - 1/09/2009

Natural Prevalence of Resistance to HCV Protease Inhibitors - 9/25/08

Novel HCV Polymerase Inhibitor VCH-759 Monotherapy Demonstrates Promising Antiviral Activity - 12/07/07

ITMN 191 and ANA598 (HCV Polymerase Inhibitor)

Natural Prevalence of Resistance to HCV Protease Inhibitors - 9/25/08

InterMune and Anadys Begin Phase 1 Clinical Trials of Experimental HCV Therapies ITMN-191 and ANA598 - 6/06/08

InterMune Presents Top-line Results from Phase 1b Trial of HCV Protease Inhibitor ITMN-191 Monotherap - 4/04/08

InterMune Announces Progress on HCV Protease Inhibitor ITMN-191 - 1/11/08

Preclinical Study Shows ITMN-191 Plus Pegasys is Active against HCV In Vitro   11/10/06

Roche and InterMune to Collaborate on HCV Protease Inhibitor ITMN-191   10/24/06

Preclinical Data on New HCV Protease Inhibitor ITMN 191- 6/02/06

MK-06080 (HCV Nucleoside Inhibitor)

Experimental Nucleoside Inhibitor MK-0608 Suppresses HCV Replication in Chimpanzees   9/29/06

R-1626 and R7128 (HCV Polymerase Inhibitor)  

HCV Polymerase Inhibitor R7128 Demonstrates Good Antiviral Activity in Genotype 2 or 3 Prior Non-responders and Relapsers - 11/14/2008

R7128 plus ITMN-191 Perform Well in Laboratory Study; STAT-C Combination Clinical Trial Now Underway - 11/14/2008

Combination Therapy with Investigational HCV Polymerase Inhibitor R7128 Produces Rapid Response in Patients with Genotype 2/3 HCV - 9/12/2008

Pharmasset Releases Preliminary Data from Phase 1 Study of Investigational HCV Polymerase Inhibitor R7128 - 8/08/2008

R7128 Demonstrates Potent Anti-HCV Activity in Combination with Pegylated Interferon/Ribavirin; Ongoing Trial to be Expanded - 4/29/08

HCV Polymerase Inhibitor R1626 Produces Good Response with Pegylated Interferon/Ribavirin and Has High Barrier to Resistance - 4/29/08

Pharmasset Announces Promising 4-Week Data on Combination Therapy with HCV Polymerase Inhibitor R7128 - 1/11/08

HCV Polymerase Inhibitor R7128 Demonstrates Antiviral Activity in Prior Non-responders - 12/14/07

Pharmasset Completes Enrollment for Phase 1 Study of Experimental Nucleoside Polymerase Inhibitor R7128 for Treatment of Chronic Hepatitis C   - 8/07/07

Pharmasset and Roche Initiate New Toxicology Studies of HCV Polymerase Inhibitor R7128    - 7/13/07

Roche Polymerase Inhibitor R1626 Demonstrates Antiviral Activity and Good Safety in Phase I Study   11/10/06

HCV Polymerase Inhibitor R-1626 Advances to Phase II Study 10/17/06


STAT-C Agents

Three New STAT-C Agents Show Promise in Preclinical Studies and Early Clinical Trials: MK-7009, ANA598, and IDX375 - 11/25/2008

R7128 plus ITMN-191 Perform Well in Laboratory Study; STAT-C Combination Clinical Trial Now Underway - 11/14/2008

Several “STAT-C” Agents Discussed at the Liver Meeting - 11/07/2008

Valopicitabine (HCV Polymerase Inhibitor)

Two Studies Yield Mixed Results for HCV Polymerase Inhibitor Valopicitabine - 5/05/07

Valopicitabine Dosed in Combination with Pegylated Interferon Alfa-2a (Pegasys) Leads to Rapid Virologic Response in 93 percent of Genotype 1 Hepatitis C Patients - 1/05/06

Lower Dose of Valopicitabine plus Pegylated Interferon Shows Antiviral Activity with Fewer Side Effects - 11/15/06

Valopicitabine plus Peginterferon Alfa-2a (Pegasys) Is More Effective in Nonresponders Compared to Peginterferon alfa-2a/Ribavirin Combination Treatment - 5/12/06

Randomized Trial of Valopicitabine (NM 283), Alone or with Peginterferon, vs Retreatment with Peginterferon Plus Ribavirin in Nonresponders to Peginterferon Alfa - 11/14/05

No Effect of Pegylated Interferon Alfa-2b (PegIntron) on the Pharmacokinetics of Valopicitabine (NM 283) in Chronic HCV Patients - 11/14/05

Encouraging Interim Results of Phase II Study of Valopicitabine (NM-283) in Combination with Peginterferon Alfa in Patients with HCV Genotype 1 - 1/05/05

Viramidine (Taribavirin)

Prodrug Taribavirin Produces Equivalent Response, but Less Anemia than Ribavirin at 48 Weeks - 12/02/2008

Taribavirin Efficacy Similar to Ribavirin in Combination Therapy for Hepatitis C, but with Less Anemia - 5/09/08

Valeant Reports Promising 12-week Phase IIb Data on Taribavirin - 4/01/08

Virological Response and Safety Outcomes in Chronic Hepatitis C Patients Treated with Pegylated Interferon plus Taribavirin (Viramidine)   - 8/10/07

Hepatitis C Drug Viramidine Fails Pivotal Phase III Trial, Again   9/15/06

Valeant Announces Results of Phase 3 VISER 1 Trial Results of Viramidine versus Ribavirin - 3/24/06


TMC435350

Experimental HCV Protease Inhibitor TMC435350 Demonstrates Favorable Safety and Efficacy in Phase 2a Trial - 11/11/2008

Experimental HCV Protease Inhibitor TMC435350 Demonstrates Promising Activity and Tolerability in Early Clinical Trial - 5/13/08


Telaprevir (aka VX-950)  monotherapy / combination

HCV Protease Inhibitor Telaprevir (VX-950) Continues to Perform Well in PROVE Trials - 11/11/2008

Tibotec Begins Enrolling Phase III Study of HCV Protease Inhibitor Telaprevir for Hepatitis C Patients with Prior Treatment Failure - 10/24/2008

Vertex Reports Encouraging Data from PROVE3 Trial of HCV Protease Inhibitor Telaprevir (VX-950) - 6/13/08

Telaprevir plus Pegylated Interferon and Ribavirin Allows Shorter Therapy for Patients with Genotype 1 HCV - 4/26/08

Vertex to Start Phase 3 Trials of HCV Protease Inhibitor Telaprevir (VX-950) - 2/01/08

Telaprevir plus Pegylated Interferon Is Effective against Both Wild-type and Drug-resistant HCV Strains   - 8/17/07

Mutations That Confer Resistance to HCV Protease Inhibitors 5/01/07

Telaprevir-based Therapy for HCV May Shorten Treatment Duration from 48 to 24 Weeks for Some Genotype 1 Patients - 4/17/07

In Vitro Studies Suggest Promising Outcomes with New HCV Protease Inhibitor ACH 806 in Combination with Interferon, Telaprevir, or NM 107 4/05/07

Telaprevir Demonstrates Safety and Anti-HCV Activity in 12-week Interim Analysis 1/05/07

Telaprevir Resistance Mutations Observed in Laboratory Studies  12/05/06

Updated Results from Patients Receiving Standard HCV Therapy Following Telaprevir  12/01/06

Telaprevir plus Pegylated Interferon Suppresses Wild-type and Resistant HCV Over 14 Days  11/03/06

Rapid Decline of HCV RNA in Patients Treated with VX-950 10/02/06

这病头疼

感谢411老师的关心，您总是能给我们指导和建议，您发的外文我看不懂，但我知道您的意思，坚持就是胜利治疗的药物在不断的发展，您是这个意思吧。呵呵您放心大家都在努力，毕竟生命可贵。感谢您的关心指导。

这病头疼

今天拿上化验单不由的又愁上心头，情况不好。谷丙95    谷草68    总胆36     直胆11   间胆26     白细胞4.2          血小板55
今天要打干扰素了，可现在不能打了，因为过节，医院没人，只有等上班才能去住院，在家现在吃这优思弗和升血小板胶囊。怎么会突然这样，有可能是干扰素没用了，现在的情况说明已经开始肝损害了。下星期去化验病毒就知道结果如何了，哎年过的都不安生。这两天觉的没劲，就感觉到了不好。干扰素停了下面真就不知道该怎么办了。哎，顺其自然吧，其实也想到了这天，不过没想会这么快。

这病头疼

住了十来天医院，昨天回到家了。一切又回到前面的情况。检查病毒还是阴性，就是脾又大了点。干扰素还在打，b超结果肝静脉走行不规则，变细，门静脉1.0cm.《以前是1.2是否有误差我不知道，但愿是真的》。医生说不用做胃镜，虽然在我的要求要做的情况下还是没让做，他很自信。脾厚4.0cm长径12.9cm脾静脉0.8cm.《ct检查说9个肋骨，不知道怎么换算》，b超说是脾稍大，cd说是巨脾，真不知道该相信谁。胆囊多发性息肉样病变。ct结果肝脏略缩小，肝裂略增宽，肝实质密度呈弥漫小结节状改变。肝硬化巨脾。
出院检查转氨酶正常黄疸正常，血小板67白细胞2.7继续用干扰素。现在吃药血小板白细胞都上不去了，打的是利生素和胸腺肽。医生说情况不错，是这样吗也许吧，对于病重的，我当然是情况不错了。住院的时间医生们救了一个重肝患者，30天花了30多万，医生很欣慰，对于生命来说30多万不算什么，可又有几个可以承受的起呢。
这次回来好像有点麻木了，不知道该高兴还是难过，总的来说我还可以继续活着就是幸福不是吗，我还在坚持着。这次住院也有好消息，遇上了一位干扰素3针就转阴的乙肝战友，他是老师。和一位自然转阴的乙肝战友，连医生都说是特例，他是搞水利的常年野外。呵呵，有时间不能不相信生命是有奇迹的。加油吧战友们。

这病头疼

很长时间没上来了，看着论坛愁多囍少，心情也不怎么好了，可是这里总是个牵挂，同命相连吧。我还是老样子，还是白细胞血小板低，白细胞在2.6.血小板这两个星期到正常了，因为喝了花生皮的汤。现在汤也减了星期5开始喝喝到星期一化验停。其他还是老样子，黄疸一吃利巴韦林就上，上了就停，开始吃降黄药。每星期化验一次，干扰素第39针了。头发少了很多。还是不相信门脉小了，在过半年在查了看吧，10月份一定要做个胃镜，就是医生不让我也要坚持做个，现在老是觉的不做心里不踏实。我要坚持打上一年半干扰素，希望老天能给我这个机会，同时希望佩乐能可以进入医保，在派罗欣失败后可以用佩乐能，呵呵最好派罗欣不要失败，老天保佑。

lxiaolan

www.healthoo.net里有个丙肝论坛

王国春

我爸爸也是一样的,95年输血感染的,2007年打了一年的派罗欣和利巴,病毒清除了,效果还好!现在还是代尝期硬化

这病头疼

又过了1个月了，刚拿上化验单，谷丙转氨酶77谷草转氨酶53总胆31白细胞3.4血小板65，一切都是反反复复。要打干扰素44针了，利巴韦林已经停了1个月了，现在不吃利巴韦林黄疸也在升高了，现在一直吃这优思弗，只要停了黄疸就会上，还有4针就1年了，不想半途而废。看样子优思弗要一直吃了。转氨酶老是起起伏伏不知道是怎么回事，最近老是感觉肝有点坠的感觉，反正是不怎么舒服，到底是什么感觉还真不好说。谢谢楼上的回复，写了有人看或有人回复，总是让我感到点欣慰，希望能帮别人点，也希望有人能帮我。这可能就是这个论坛的乐趣吧。同是不幸总希望留下点什么，哪怕是句问候。战友们努力吧。
每次要跑1500多公里去住个院好累啊，现在根本就不想出门，哎本地的医生好，谁又会跑那么远呢，劳命伤财。

这病头疼

1年了，去年这个时候，得知自己肝硬化了，一年的奔波治疗，昨天打了第48针。肝功检查转氨酶稍微高一点，白细胞血小板还是低，准备在过一个月去复查了。但最近两肋不舒服，感觉明显了，想想就头疼。准备在坚持打半年，希望不要反复。
马上就要512了，在记忆中512那天我在病房看着新闻，神情恍惚心里像被压了块石头，让我喘不过气来，512的前两天跟医生聊到很晚，因为他职晚班，详细告诉我了我的病情，说如果治疗失败，也就是2年到3年的时间，那一刻才突然发现，我是如此的眷恋活着感觉，才发现生命这么的脆弱，才发觉对身边亲人的依恋。茫然的看着新闻里奔跑人们，当时并不知道会死这么多的人，只是觉的跑什么啊。因为我就住在地震带，1年最少要晃那么2次，已经习惯了。随着时间的发展看见灾情的发展，让我震惊。那一个多月的时间，在医院我都不知道是怎么过来的，天天如同行尸走肉，看着新闻眼泪根本就控制不住，流泪是为了那些逝去的人们和我自己。那一刻我才发现我的情感是那么的脆弱。30多年流的泪，没有那一个月的多。
512了在此一周年的日子里，让逝去的人们一路走好，让我们这些还在活着的人们好好的珍惜活着的感觉，让我们这些被疾病缠绕的人们尽量的快乐的过好每一天，为了逝去的人们，为了我们自己，为了亲人，为了爱人，为了朋友。