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干扰素的代价 [复制链接]

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发表于 2009-1-18 05:53
From "Management of Chronic Hepatitis B",Number 174,prepared by Minnesota Evidence-based Practice Center, Minneapolis, Minnesota for Agency for Healthcare Research and Quality, U.S. Department of Health and Human Services, October 2008.   

Question 2a. What is the efficacy (or effectiveness) of interferon therapy, oral therapy, and various combinations in treating hepatitis B with defined or continuous courses of treatment?

Clinical outcomes.

Mortality. Antiviral medications did not reduce mortality versus placebo, other antiviral medications, or in combination with corticosteroids, regardless of baseline HBeAg or cirrhosis status in 14 RCTs that were not designed to test long-term clinical outcomes.

Cirrhosis. A small trial failed to demonstrate that interferon alfa-2b prevented cirrhosis in HBeAg-positive patients.  Another small RCT found no significant difference in histologically confirmed cirrhosis after interferon alfa-2b alone or with simultaneous prednisone.  No data were available from RCTs for other antiviral drugs or longer followup.

Hepatic decompensation was not prevented by lamivudine compared to placebo or entecavir compared to lamivudine in three underpowered trials.

Hepatocellular carcinoma was not prevented in four studies with inadequate size and duration.   In one RCT, analysis that adjusted for country, sex, baseline ALT level, Child-Pugh score, and Ishak fibrosis score and excluded five individuals who developed HCC within the first year of the study found a borderline significant effect of lamivudine.  This study noted a nonsignificant increase in all cause mortality.

Intermediate outcomes. Evidence suggested drug effects on viral load or replication, liver enzymes, and histology at end-of-treatment and lasting from at least 6 months off treatment. No one treatment improved all examined outcomes and few assessed complete response or sustained outcomes (i.e., at >6 months off treatment).

HBV DNA clearance was assessed using assays with different sensitivities to detect HBV DNA. Adefovir and lamivudine increased HBV DNA clearance at end of treatment versus placebo. Entecavir increased clearance versus lamivudine with inconsistent effect size. Lamivudine was less effective than adefovir in lamivudine-resistant patients and less effective than telbivudine in HBeAg-positive patients.  Limited evidence suggested that HBV DNA clearance was maintained at followup off therapy ranging from 18-24 weeks after interferon alfa-2b,  lamivudine,  or adefovir administration.

HBeAg loss was assessed in 35 trials.  HBeAg clearance off treatment was demonstrated for interferon alfa- 2b.  Lamivudine for 52 weeks versus placebo increased HBeAg loss at 16 weeks off therapy.   HBeAg loss at 24 weeks post treatment was greater after peginterferon alfa-2a versus lamivudine.

HBeAg seroconversion was assessed in 36 studies.  Lamivudine or adefovir increased HBeAg seroconversion versus placebo.  Interferon alfa-2b64,83 increased post-treatment seroconversion. Lamivudine monotherapy failed to sustain seroconversion.  Interferon alfa- 2b plus lamivudine demonstrated inconsistent effects on seroconversion at 6-28 weeks of followup with significant benefit in a pooled analysis from four RCTs using individual patient data.  Telbivudine versus adefovir or peginterferon alfa-2a versus lamivudine increased post treatment HBeAg seroconversion. Peginterferon alfa-2a plus lamivudine increased HBeAg seroconversion versus lamivudine alone but not versus peginterferon alfa-2a alone.

HBsAg clearance. Nine studies compared active drugs with placebo or no treatment.  Only one RCT of HBeAg-positive patients found a significant increase in HBsAg loss after interferon alfa-2b.  Steroid pretreatment followed by interferon alfa-2b versus no antiviral drugs increased HBsAg loss at the end of treatments.  Active treatments compared to each other did not demonstrate differences post-treatment HBsAg loss or combined outcomes that included loss HBsAg clearance.

ALT normalization was greater after adefovir versus placebo.  Lamivudine increased rates of ALT normalization versus placebo at 24 weeks off treatment in HBeAg-negative patients.  Interferon Alfa-2b at doses 35 million units (MU)/week compared to no antiviral treatment increased rates of ALT normalization at 8-24 weeks of followup.  Sustained ALT 6 normalization at 24 weeks off treatment was greater after peginterferon alfa-2a compared to lamivudine and after combined therapy of peginterferon alfa-2a with lamivudine compared to lamivudine alone.

Histological improvement off treatment in necroinflammatory scores was reported in only one RCT95 after peginterferon alfa-2a compared to lamivudine in HBeAg-negative patients.

Combined virologic and biochemical outcomes. Low to moderate evidence suggested that some examined drugs or their combinations improved combined virologic and biochemical outcomes immediately after and post treatment.

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发表于 2009-1-18 13:03
好久没上来了,大家新年好!
最近在家打针,因为把500万单位改成300万的了,反应小很多,生活也基本上正常了,所以来上面少了.
说说我最近的感受:如果有打干扰素反应太大受不了的,特别是一个月后还是反应大的.我到是建议改小剂量打,因为大剂量严重影响到生活话,还是不妥,而且本来干扰素治疗的时间长,经历半年以上那种痛苦我反正是受不了,所以我改成300万单位的了。
我现在能够自己打针了,其实打了第一针后就不怕了,有打PP打怕了的战友可以试试打肚皮,原来没有打的时候很怕,认为要打到肠子怎么办,其实没那么严重,而且打肚子只一点点痛,比打PP好多了,自己打的时候推药时可以掌握快慢,觉得痛了就推慢些,这样打下来,不会象护士打针那样痛。我一直没有去检查DNA,准备过年后去查一次。
好就说这些,祝大家过个好年!(还有个事,我打了快三个月的干扰素了,发烧等症状到是有,就是没掉过头发,看来掉头发也只是个别现象)

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发表于 2009-1-20 19:36
我刚打赛若金500万单位一个月,白细胞和血小板下降得厉害,现在在吃生血宁,不知道还能不能继续打下去(ALT由40多升到65再到100,感觉IFN对我可能比较有效,今天血常规白细胞又下降了,血小板已经到下限值了

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发表于 2009-1-20 20:36

与大家分享,有空交流118043369群67341317

ALT             AST                                  HBV—DNA
住院时(一直在服联苯)          56             193                                    10的8次方
点滴甘利欣且停服联苯一周后      正常              正常
担心转氨酶正常不利干扰,
私自建议医生停“甘利欣”
一周后反跳为                    220            183
此时开始打干扰素                220            183                                         
干扰第一周                      103            56     (点滴“甘利欣”)                     未检查
干扰第二周                      272            220    (不同意点滴保肝降酶)                 未检查
干扰第三周                      320            187    (期间服用“益肝灵软胶囊”)           未检查
干扰第四周                      未检查            未检查   (( 服“益肝灵软胶囊”)             未检查
干扰第五周                      未检查            未检查   (停服“益肝灵软胶囊”)             未检查  
干扰40天后                      201            123     (停服“益肝灵软胶囊已有13天)       未检查   
干扰第65天                     228            127      (只打干扰素)                     DNA  10的6次方
干扰第105天                     414            225                                     未检查
干扰4个月半                      169            105                                    DNA转阴(大三变成一五阳)

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发表于 2009-2-3 15:18
呵呵 MM 好久不见了吧
我可是很久都没有来过论坛了
我没在哈尔滨  就一直没怎么上网
状态还挺好 能吃能喝的  头发掉的也少了 还有3个月就1年了
另外 我的头发 感觉不怎么掉了  而且白头发居然都变黑了 。。。。奇怪
过几天回哈尔滨 正好贺普丁3个月完事  去复查
过来给MM拜个晚年 不会怪我把
命里有时终须有,命里无时莫强求

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发表于 2009-2-6 21:56
洋洋下雪,新年好!!
不知你的检查结果如何

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发表于 2009-2-8 09:36
我3月份才去化验
正好买药
不知道这次情况怎么样  该怎么样就怎么样
我发现我现在状态特别的好·1
命里有时终须有,命里无时莫强求

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发表于 2009-2-8 11:08
原帖由 洋洋下雪 于 2009-2-8 09:36 发表
我3月份才去化验
正好买药
不知道这次情况怎么样  该怎么样就怎么样
我发现我现在状态特别的好·1

祝福你啊!希望3月能听到你的好消息,呵呵

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发表于 2009-2-10 16:44
我三月份也要去检查开药

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发表于 2009-2-10 21:34
呵呵 我现在都是自己去买药
自己化验 一切都是自己搞定
记得刚开始的时候害怕 胆小 现在无所谓了 心态刚刚的
命里有时终须有,命里无时莫强求
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