CHAPTER 33  Hematopoietic Tumors  707


           protocols that bias the overall result, making it a less comparable   relapse after chemotherapy include inadequate dosing and/or fre-
           outcome. Widespread  application of these  standardized criteria   quency of administration of chemotherapy, failure to achieve high
                                                                 concentrations of chemotherapeutic drugs in certain sites such as
           should permit more suitable comparisons in the future. True iCR
  VetBooks.ir  rarely occur in dogs with lymphoma; documenting iCRs is lim-  the CNS, and initial treatment with prednisone alone.
                                                                   At the first recurrence of lymphoma, it is recommended that
           ited to investigative trials striving to achieve them because we lack
           meaningful therapeutic options.                       reinduction be attempted first by reintroducing the induction pro-
             Improved methods of detecting minimal residual disease (MRD)   tocol that was initially successful, provided the recurrence occurred
           or early recurrence have been investigated in dogs with lymphoma   temporally far enough from the conclusion of the initial protocol
           and include advanced imaging and detection of molecular and bio-  (e.g., ≥2 months) to make reinduction likely. The cumulative dose
           logic markers of MRD. Advanced functional and anatomic imag-  of DOX that will result from reinduction, baseline cardiac assess-
           ing techniques (i.e., PET/CT) are the current standard for assessing   ment, the use of cardioprotectants, alternative drug choices, and
           treatment response and early relapse of lymphoma in humans and   client education should all be considered. In general, the dura-
           have also been investigated in dogs (see Fig. 33.10). 221,223–226  As   tion of reinduction remission will be half that encountered in the
           these techniques become available to a broader veterinary popu-  initial therapy; however, a subset of animals will enjoy long-term
           lation, their clinical application will surely increase. Molecular   reinductions, especially if the dog completed the initial induction
           detection of MRD applies clonality and PCR techniques. Beyond   treatment protocol and was currently not receiving chemotherapy
           diagnostic applications, these techniques have been applied to deter-  for several months when relapse occurred. Reinduction rates of
           mine cytoreductive efficacy of various chemotherapeutic drugs and   nearly 80% to 90% can be expected in dogs that have completed
           to document and predict early relapse in patients before more con-  CHOP-based protocols and then relapse while not receiving ther-
           ventional methods. 123,217,246,287–293  Regarding biomarkers of MRD,   apy. 232,300  The duration of a second CHOP-based remission in
           preliminary investigations have suggested serum lactate dehydroge-  one report was predicted by the duration of the interval between
           nase activity, thymidine kinase 1 activity, haptoglobin, and serum   protocols and the duration of the first remission. 123,300
           C-reactive protein may be candidates in the dog. 202–206,294  If reinduction fails or the dog does not respond to the initial
             As we become more proficient at defining MRD, the pressing   induction, the use of so-called “rescue” agents or “rescue” protocols
           clinical question becomes how we use this information. Theoreti-  may be attempted. These are single drugs or drug combinations
           cally, such information could suggest when more aggressive ther-  that are typically not found in standard CHOP protocols and are
           apy or alternative therapy should be instituted in patients who   withheld for use in the drug-resistant setting. The most common
           have not achieved a “molecular remission” or who are undergoing   rescue protocols used in dogs include single-agent use or a combi-
           early relapse; however, until we determine what these interven-  nation of rabacfosadine, actinomycin D, mitoxantrone, DOX (if
           tions should be based on prospective trial assessment, the clinical   DOX was not part of the original induction protocol), dacarba-
           utility of MRD analytics remain theoretical.          zine (DTIC), temozolomide, lomustine (CCNU), l-asparaginase,
                                                                 mechlorethamine, vincristine, vinblastine, procarbazine, predni-
           Reinduction and Rescue Chemotherapy                   sone, and etoposide. Some rescue protocols are relatively simple
                                                                 and convenient single-agent treatments, whereas others are more
           Eventually, the vast majority of dogs that achieve a remission will   complicated (and expensive) multiagent protocols, such as MOPP.
           relapse or experience recrudescence of lymphoma. This usually   Overall rescue response rates of 40% to 90% are reported; however,
           represents the emergence of tumor clones or tumor stem cells   responses are usually not durable with median response durations
           (see  Chapter 2) that are inherently more resistant to chemo-  of 1.5 to 2.5 months being typical regardless of the complexity of
           therapy than the original tumor, the so-called MDR clones that   the protocol. A small (<20%) subset of animals will enjoy longer
           either were initially drug resistant or became so after exposure to   rescue durations. Table 33.5 provides a summary of canine res-
           selected chemotherapy agents. 295  Evidence suggests that in dogs   cue protocols and published results. 270,301–320  Current published
           with relapsed lymphoma, tumor cells are more likely to express   data from rescue protocols do not include sufficient numbers for
           genes (e.g., MDR1) that encode ABC-transporter protein trans-  adequate statistical power, nor do they compare protocols in a
           membrane drug pumps often associated with MDR. 196,197,296–299    controlled, randomized prospective fashion. Therefore compara-
           MDR1 represents only one of the plethora of mechanisms that   tive evaluations of efficacy among various protocols are subject
           lead to drug-resistant disease (see Chapter 12). Other causes of   to substantial bias, making direct comparisons difficult. Choice



            TABLE 33.5     Summary of Response for Rescue Protocols a
                                                                     Median
                            Number of   Overall Response   Complete   Response     Median Duration of
             PRIVATE Protocol  Animals  (%)            Response (%)  Duration c    Complete Response  References
             Actinomycin-D  25           0              0            0 days        0 days           316
             Actinomycin-D  49 b        41             41            129 days      129 days         310
             Dacarbazine    40          35              3            43 days       144 days         313
             Dacarbazine or   63        71             55            45 days       NR               311
               temozolomide-
               anthracycline
                                                                                                            Continued