Brazilian guideline for the use of immunobiologicals in chronic rhinosinusitis with nasal polyps ‒ 2024 update.

INTRODUCTION: Biologics targeting type 2 inflammation have revolutionized the way we treat patients with Chronic Rhinosinusitis with Nasal Polyps (CRSwNP). Particularly in severe and difficult-to-control cases, these drugs have provided a new reality for these patients, allowing for the effective and safe treatment of extensive diseases that were not completely managed with the typical strategy of surgery and topical medications. OBJECTIVES: The experience achieved with the approval of these medications by ANVISA for use in CRSwNP and the knowledge obtained regarding outcomes, adverse effects, and the ideal patient profile prompted the update of the previously published guideline, with a detailed review of the most recent scientific literature, the personal experiences of experts, and the adaptation to the reality of the Brazilian healthcare system, both public and private. RESULTS: We proposed a new eligibility criterion for biologics in patients with CRSwNP based on four pillars of indication: the impact of the disease on the patient's life, whether in the presence of specific symptoms or in overall quality of life; the extent of sinonasal disease; the presence of type 2 comorbidities, considering other associated diseases that may also benefit from anti-T2 biologics, and the presence of biomarkers to define type 2 inflammation, especially those associated with worse disease prognoses. CONCLUSIONS: This innovative and pioneering method has two major advantages. First, it ensures a comprehensive evaluation of patients; second, it is flexible, as advancements in our understanding of the disease and changes in cost-effectiveness can be addressed by simply adjusting the required score for indication, without the need to modify the entire evaluation scheme.

Brazilian guideline for the use of immunobiologicals in chronic rhinosinusitis with nasal polyps ‒ 2024 update

Abstract Introduction Biologics targeting type 2 inflammation have revolutionized the way we treat patients with Chronic Rhinosinusitis with Nasal Polyps (CRSwNP). Particularly in severe and difficult-to-control cases, these drugs have provided a new reality for these patients, allowing for the effective and safe treatment of extensive diseases that were not completely managed with the typical strategy of surgery and topical medications. Objectives The experience achieved with the approval of these medications by ANVISA for use in CRSwNP and the knowledge obtained regarding outcomes, adverse effects, and the ideal patient profile prompted the update of the previously published guideline, with a detailed review of the most recent scientific literature, the personal experiences of experts, and the adaptation to the reality of the Brazilian healthcare system, both public and private. Results We proposed a new eligibility criterion for biologics in patients with CRSwNP based on four pillars of indication: the impact of the disease on the patient's life, whether in the presence of specific symptoms or in overall quality of life; the extent of sinonasal disease; the presence of type 2 comorbidities, considering other associated diseases that may also benefit from anti-T2 biologics, and the presence of biomarkers to define type 2 inflammation, especially those associated with worse disease prognoses. Conclusions This innovative and pioneering method has two major advantages. First, it ensures a comprehensive evaluation of patients; second, it is flexible, as advancements in our understanding of the disease and changes in cost-effectiveness can be addressed by simply adjusting the required score for indication, without the need to modify the entire evaluation scheme.

Dupilumabe na urticária crônica espontânea refratária ao omalizumabe / Dupilumab in chronic spontaneous urticaria refractory to omalizumab

A urticária é uma lesão cutânea eritematosa, edematosa e pruriginosa, mais prevalente em mulheres entre 30 a 50 anos de idade, sendo classificada em aguda ou crônica. O quadro clínico da urticária crônica espontânea é desencadeado independentemente de estímulos exógenos, podendo ser acompanhado de angioedema em 40% dos casos. O diagnóstico é clínico e a doença pode ser monitorada com escores. O tratamento da urticária crônica espontânea é baseado em anti-histamínicos H1 de segunda geração como primeira linha. A segunda linha se baseia no aumento da dose de anti-histamínicos H1 em até quatro vezes a dose habitual, a terceira linha consiste na associação de imunobiológicos como o omalizumabe, e a quarta linha no uso de ciclosporina. Este relato de caso teve como objetivo analisar a eficácia e segurança do tratamento com dupilumabe na urticária crônica espontânea refratária ao omalizumabe, utilizando os escores de atividade da urticária e o questionário de qualidade de vida em dermatologia. A partir dos resultados obtidos, verificou-se sucesso terapêutico com dupilumabe, que se manteve mesmo após suspensão do medicamento. O uso off label do dupilumabe justificou-se pelo seu mecanismo de ação na fisiopatologia da doença. Este é o primeiro relato de caso brasileiro do uso de dupilumabe para urticária crônica espontânea refratária ao omalizumabe.

Urticaria is an erythematous, edematous, and pruritic skin lesion, most prevalent in women between 30 and 50 years of age, and classified as acute or chronic. The clinical features of spontaneous chronic urticaria are triggered regardless of exogenous stimuli and may be accompanied by angioedema in 40% of cases. The diagnosis is clinical and the disease can be monitored with scores. The first-line treatment of spontaneous chronic urticaria is based on second-generation H1 antihistamines. The second-line treatment is based on increasing the dose of H1 antihistamines by up to four times the standard dose, the third line consists of the association with biologics such as omalizumab, and the fourth line consists of the use of cyclosporine. The present case report aimed to analyze the efficacy and safety of dupilumab treatment for chronic spontaneous urticaria refractory to omalizumab, quantifying clinical improvement and quality of life using urticaria activity scores and a dermatology quality of life questionnaire, respectively. The results obtained showed therapeutic success with dupilumab, which was maintained even after drug suspension. Offlabel use of dupilumab was justified by its mechanism of action in the pathophysiology of the disease. This is the first Brazilian case report of the use of dupilumab for chronic spontaneous urticaria refractory to omalizumab.

Does current evidence on disease-modifying antirheumatic drugs for psoriatic arthritis reinforce an effect on radiographic progression? Results from a systematic review and meta-analysis.

This study aims to estimate the effect of synthetic and biologic disease-modifying antirheumatic drugs (DMARDs) on radiographic progression and quality of life in adult patients with psoriatic arthritis. A comprehensive search was performed using MEDLINE, Embase, Web of Science, Scopus, and Cochrane Central Register of Controlled Trials (CCRCT). Clinical trials comparing DMARDs with placebo for ≥ 12 weeks were included. The meta-analysis was conducted with a random-effects model using mean differences (MD). A total of 16 trials with overall moderate quality of evidence were included. Exposure to a biologic agent reduced radiographic progression at 24 weeks of treatment (MD: - 0.66; [95% CI - 0.97 to - 0.34]; P < .00001; I2 = 100%). The reduction of the baseline score was more than two times higher for TNF blockers compared with IL-17 and IL-12/IL-23 inhibitors (MD: - 0.94 vs - 0.41). Improvement in health-related quality of life scores was observed in biologic-treated populations (MD: - 0.21; [95% CI - 0.25 to - 0.18]; P < .00001; I2 = 97%). No sufficient data were available regarding conventional synthetic agents. Our data analyses suggest a better control of radiological damage with bDMARDs, as compared to placebo, after 24 weeks of treatment. However, the accuracy of these results in real life are jeopardized by the exceedingly high level of heterogeneity exhibited within and across included studies, and the true intervention effect cannot be determined with confidence. Further research is required to assess long-term outcomes and to control heterogeneity in the evaluation of treatments for psoriatic arthritis. PROSPERO registration number: CRD42019122223. Key Points • Radiographic progression is not the primary outcome for most efficacy studies in psoriatic arthritis; hence, baseline data are substantially diverse in major clinical trials. • The best available evidence on this particular outcome is currently at a moderate risk of bias. • Existing reports of the effect of DMARDs on structural damage must be taken with caution. • Further research is required to assess long-term outcomes and to control heterogeneity between studies.

Lokivetmab: uma nova opção para o tratamento e o controle da dermatite atópica canina: revisão / Lokivetmab: a new option for the treatment and control of canine atopic dermatitis: review / Lokivetmab: una alternativa para el tratamiento y control de la dermatitis atópica canina: revisión

Os anticorpos monoclonais são tema de pesquisa na medicina humana. Eles têm como alvo receptores específicos ou determinadas citocinas e são altamente específicos e eficazes no bloqueio de sua molécula-alvo. O lokivetmab é um anticorpo monoclonal caninizado anti-IL-31 que se liga especificamente à IL-31 circulante, e foi recentemente aprovado para o tratamento da dermatite atópica canina. Atualmente, o lokivetmab é o primeiro anticorpo monoclonal terapêutico utilizado na medicina veterinária. Este trabalho teve como objetivo revisar e atualizar os clínicos sobre esse novo anticorpo monoclonal que está disponível para tratamento da dermatite atópica canina.

Monoclonal antibodies have been studied in human medicine for a while. They target specific receptors and cytokines, and are highly specific and effective in blocking their target molecule. Lokivetmab is a monoclonal caninised anti-IL-31 antibody that was recently approved for the treatment of atopic dermatitis in dogs. Currently, no other therapeutic monoclonal antibody is used in veterinary medicine. The goal of this review of literature is to update clinicians on this new biological option for the treatment of canine atopic dermatitis.

Los anticuerpos monoclonales son tema de investigación en la medicina humana, y tienen como blancos receptores específicos o determinadas citoquinas. Son muy específicos y eficientes en el bloqueo de su molécula blanco. El lokivetmab es un anticuerpo monoclonal caninizado anti-IL-31 que se une específicamente a la IL-31 circulante, que fue aprobado recientemente para el tratamiento de la dermatitis atópica canina. Actualmente este fármaco representa el primer anticuerpo monoclonal terapéutico que se utiliza en medicina veterinaria. Este trabajo tiene como objetivo revisar y actualizar las informaciones científicas sobre este nuevo anticuerpo monoclonal que se encuentra disponible para el tratamiento de la dermatitis atópica en perros.

Lokivetmab: uma nova opção para o tratamento e o controle da dermatite atópica canina: revisão / Lokivetmab: a new option for the treatment and control of canine atopic dermatitis: review / Lokivetmab: una alternativa para el tratamiento y control de la dermatitis atópica canina: revisión

Os anticorpos monoclonais são tema de pesquisa na medicina humana. Eles têm como alvo receptores específicos ou determinadas citocinas e são altamente específicos e eficazes no bloqueio de sua molécula-alvo. O lokivetmab é um anticorpo monoclonal caninizado anti-IL-31 que se liga especificamente à IL-31 circulante, e foi recentemente aprovado para o tratamento da dermatite atópica canina. Atualmente, o lokivetmab é o primeiro anticorpo monoclonal terapêutico utilizado na medicina veterinária. Este trabalho teve como objetivo revisar e atualizar os clínicos sobre esse novo anticorpo monoclonal que está disponível para tratamento da dermatite atópica canina.(AU)

Monoclonal antibodies have been studied in human medicine for a while. They target specific receptors and cytokines, and are highly specific and effective in blocking their target molecule. Lokivetmab is a monoclonal caninised anti-IL-31 antibody that was recently approved for the treatment of atopic dermatitis in dogs. Currently, no other therapeutic monoclonal antibody is used in veterinary medicine. The goal of this review of literature is to update clinicians on this new biological option for the treatment of canine atopic dermatitis.(AU)

Los anticuerpos monoclonales son tema de investigación en la medicina humana, y tienen como blancos receptores específicos o determinadas citoquinas. Son muy específicos y eficientes en el bloqueo de su molécula blanco. El lokivetmab es un anticuerpo monoclonal caninizado anti-IL-31 que se une específicamente a la IL-31 circulante, que fue aprobado recientemente para el tratamiento de la dermatitis atópica canina. Actualmente este fármaco representa el primer anticuerpo monoclonal terapéutico que se utiliza en medicina veterinaria. Este trabajo tiene como objetivo revisar y actualizar las informaciones científicas sobre este nuevo anticuerpo monoclonal que se encuentra disponible para el tratamiento de la dermatitis atópica en perros.(AU)

New and Potential Treatments for Atopic Dermatitis: Biologicals and Small Molecules.

PURPOSE OF REVIEW: An update on new therapies currently approved or potentially useful in the future for the management of patients suffering moderate-to-severe atopic dermatitis. RECENT FINDINGS: New pathogenic mechanisms involved in atopic dermatitis have permitted to propose novel therapeutic approaches devised to control the inflammatory process observed in involved cutaneous tissues by neutralizing mediators, cytokines, and their receptors. Recent research findings have disclosed important and previously unrecognized pathogenic mechanisms that have resulted in innovative targeted therapies, such as dupilumab, and potentially other biologicals and small molecules. Further studies should permit the sub-classification of patients according to the relevance of different mediators and inflammatory cells. It can be concluded that the treatment of atopic dermatitis has entered into the era of personalized/precision medicine.

[Safe use of biological therapies for the treatment of rheumatoid arthritis and spondyloarthritides]. / Segurança do uso de terapias biológicas para o tratamento de artrite reumatoide e espondiloartrites.

The treatment of autoimmune rheumatic diseases has gradually improved over the last half century, which has been expanded with the contribution of biological therapies or immunobiopharmaceuticals. However, we must be alert to the possibilities of undesirable effects from the use of this class of medications. The Brazilian Society of Rheumatology (Sociedade Brasileira de Reumatologia/SBR) produced a document based on a comprehensive literature review on the safety aspects of this class of drugs, specifically with regard to the treatment of rheumatoid arthritis (RA) and spondyloarthritides. The themes selected by the participating experts, on which considerations have been established as the safe use of biological drugs, were: occurrence of infections (bacterial, viral, tuberculosis), infusion reactions, hematological, neurological, gastrointestinal and cardiovascular reactions, neoplastic events (solid tumors and hematologic neoplasms), immunogenicity, other occurrences and vaccine response. For didactic reasons, we opted by elaborating a summary of safety assessment in accordance with the previous themes, by drug class/mechanism of action (tumor necrosis factor antagonists, T-cell co-stimulation blockers, B-cell depletors and interleukin-6 receptor blockers). Separately, general considerations on safety in the use of biologicals in pregnancy and lactation were proposed. This review seeks to provide a broad and balanced update of that clinical and experimental experience pooled over the last two decades of use of immunobiological drugs for RA and spondyloarthritides treatment.

Segurança do uso de terapias biológicas para o tratamento de artrite reumatoide e espondiloartrites / Safe use of biological therapies for the treatment of rheumatoid arthritis and spondyloarthritides

O tratamento das doenças reumáticas autoimunes sofreu uma progressiva melhora ao longo da última metade do século passado, que foi expandida com a contribuição das terapias biológicas ou imunobiológicos. No entanto, há que se atentar para as possibilidades de efeitos indesejáveis advindos da utilização dessa classe de medicações. A Sociedade Brasileira de Reumatologia (SBR) elaborou um documento, baseado em ampla revisão da literatura, sobre os aspectos relativos à segurança dessa classe de fármacos, mais especificamente no que diz respeito ao tratamento da artrite reumatoide (AR) e das espondiloartrites. Os temas selecionados pelos especialistas participantes, sobre os quais foram estabelecidas considerações quanto à segurança do uso de drogas biológicas, foram: ocorrência de infecções (bacterianas, virais, tuberculose), reações infusionais, reações hematológicas, neurológicas, gastrointestinais, cardiovasculares, ocorrências neoplásicas (neoplasias sólidas e da linhagem hematológica), imunogenicidade, outras ocorrências e reposta vacinal. Optou-se, por motivos didáticos, por se fazer um resumo da avaliação de segurança, de acordo com os tópicos anteriores, por classe de drogas/mecanismo de ação (antagonistas do fator de necrose tumoral, bloqueador da co-estimulação do linfócito T, depletor de linfócito B e bloqueador do receptor de interleucina-6). Em separado, foram tecidas considerações gerais sobre segurança do uso de biológicos na gravidez e na lactação. Esta revisão procura oferecer uma atualização ampla e equilibrada das experiências clínica e experimental acumuladas nas últimas duas décadas de uso de medicamentos imunobiológicos para o tratamento da AR e espondiloartrites.

The treatment of autoimmune rheumatic diseases has gradually improved over the last half century, which has been expanded with the contribution of biological therapies or immunobiopharmaceuticals. However, we must be alert to the possibilities of undesirable effects from the use of this class of medications. The Brazilian Society of Rheumatology (Sociedade Brasileira de Reumatologia) produced a document based on a comprehensive literature review on the safety aspects of this class of drugs, specifically with regard to the treatment of rheumatoid arthritis and spondyloarthritides. The themes selected by the participating experts, on which considerations have been established as the safe use of biological drugs, were: occurrence of infections (bacterial, viral, tuberculosis), infusion reactions, hematological, neurological, gastrointestinal and cardiovascular reactions, neoplastic events (solid tumors and hematologic neoplasms), immunogenicity, other occurrences and vaccine response. For didactic reasons, we opted by elaborating a summary of safety assessment in accordance with the previous themes, by drug class/mechanism of action (tumor necrosis factor antagonists, T-cell co-stimulation blockers, B-cell depletors and interleukin-6 receptor blockers). Separately, general considerations on safety in the use of biologicals in pregnancy and lactation were proposed. This review seeks to provide a broad and balanced update of that clinical and experimental experience pooled over the last two decades of use of immunobiological drugs for RA and spondyloarthritides treatment.

Evaluation of the agreement between Swiss Webster and B6D2F1 mice lineages in the potency test of Recombinant Human Erythropoietin (rhEPO): the Brazilian National Control Laboratory experience / Avaliação da concordância entre as linhagens de camundongos Swiss Webster e B6D2F1 no teste de potência da Eritropoietina Humana Recombinante (rhEPO): a experiência do Laboratório Nacional de Controle

The recombinant human erythropoietin (rhEPO) is a glycoprotein hormone. In face of the broad range of rhEPO-containing products in the market, the scope of their therapeutic indication and the characteristics of the rhEPO users, the biological activity testing is of high relevance for their batches releasing process. The potency testing is a laboratory evaluation for assessing the effectiveness of the final product, recommended by the European Pharmacopoeia (Ph. Eur.). This paper aimed at evaluating the agreement between the biological activity results obtained when the strain of mice-B6D2F1, recommended by Ph. Eur., was used in comparison to the Swiss Webster (SW). Twenty-two batches were assayed using these two mice strains, and a total of 44 valid assays were obtained with satisfactory results. In none of these analyses, neither repeating assays nor results combination were needed. The inter-strains variation and the accuracy were evaluated, and the following results were detected: Coefficient of Variation (VC) 10 % and Relative Error % (RE) 10 %, respectively. The tested lineage provided homogeneous results, and no statistically significant difference between them was found. The SW strain might be used as an alternative in place of B6D2F1 for performing the biological potency evaluation of rhEPO.(AU)

A eritropoietina humana recombinante (rhEPO) é um hormônio glicoproteico. Diante da gama de produtos contendo rhEPO disponíveis no mercado, da abrangência da indicação terapêutica e das características dos usuários de rhEPO, o ensaio de atividade biológica é de grande importância para o processo de liberação de lotes deste produto. O teste de potência é uma avaliação laboratorial para averiguar a eficácia do produto final, recomendada pela Farmacopeia Europeia (Ph. Eur.). Este trabalho teve como objetivo avaliar a concordância entre os valores de potência biológica obtidos quando a linhagem de camundongos preconizada pela Ph. Eur. (B6D2F1) foi utilizada em comparação com a Swiss Webster (SW). Vinte e dois lotes foram testados usando-se estas duas linhagens, e 44 ensaios válidos foram obtidos com resultados satisfatórios. Em nenhuma das análises houve necessidade de efetuar repetição de ensaios, bem como a combinação de resultados. A variação entre linhagens e a veracidade foram avaliadas, obtendo-se os seguintes resultados: Coeficiente de Variação (CV) 10 %; Erro Relativo % (ER %) 10 %, respectivamente. As linhagens testadas geraram resultados homogêneos sem diferença estatisticamente significativa entre elas. A linhagem SW mostrou características adequadas para ser empregada como alternativa à linhagem B6D2F1 na avaliação da potência biológica de rhEPO.(AU)

Avanços recentes no emprego de imunobiológicos nas doenças alérgicas / Recent advances in the use of biologicals in allergic diseases

O uso de imunobiológicos, já consagrados como importantes avanços terapêuticos na Reumatologia, para o tratamento de pacientes com doenças autoimunes do tecido conjuntivo, e na Gastroenterologia, no manejo de pacientes com doenças intestinais inflamatórias, inicia uma trajetória também muito promissora no controle mais eficaz de várias condições em Alergia-Imunologia, incluindo asma grave eosinofílica, urticária crônica espontânea, dermatite atópica, e esofagite eosinofílica. É possível que futuramente, tal como na Oncologia, possam ser empregadas várias combinações de drogas visando um melhor controle da alergia, baseado sempre que possível na caracterização dos diversos endótipos e fenótipos estabelecidos. No presente artigo, é feita uma revisão objetiva e atualizada de vários agentes imunobiológicos em Alergia: omalizumabe (anti-IgE), anti-IL-5 (mepolizumabe, reslizumabe e benralizumabe), dupilumabe (anti-subunidade alfa do receptor de IL-4), quilizumabe (anti-receptor M1 prime de membrana da IgE nas células-alvo), anti-TSLP (AMG 157), e lebrikizumabe (anti-IL-13). Futuramente, novos agentes imunoterapêuticos poderão surgir, com potencial de melhorar as atuais estratégias para tratamento das doenças alérgicas mais complexas e graves, de difícil controle...

The use of biologicals, currently recognized as an important therapeutic advance in the fields of rheumatology – in the treatment of patients with autoimmune connective tissue disorders – and gastroenterology – in the management of patients with inflammatory bowel disease – has also shown promising results in terms of a more effective control of different conditions in the field of allergy and immunology, including severe eosinophilic asthma, chronic spontaneous urticaria, atopic dermatitis and eosinophilic esophagitis. Similarly to what has been seen in oncology, it is possible that, in the future, several drug combinations can be used with the aim of better controlling atopic conditions, whenever possible based on the characterization of established endotypes and phenotypes. This article presents an objective, up-to-date review of the use of different biologicals in allergy, namely, omalizumab (anti-IgE), anti-IL-5 (mepolizumab, reslizumab,and benralizumab), dupilumab (anti-alpha subunit of the IL-4 receptor), quilizumab (anti-M1 prime membrane receptor of IgE in target cells), anti-TSLP (AMG 157), and lebrikizumab (anti-IL-13). In the future, other biological agents may be developed, with the potential to improve the treatment strategies currently available for more severe, complex, difficult-to-control allergic diseases...

Níveis séricos pré-operatórios dos marcadores CEA e CA19-9 e imunoexpressão tecidual do marcador CA19-9 no carcinoma colorretal: relação com os aspectos morfológicos da neoplasia / Pre-operative sera levels of CEA and CA19-9 and tissular distribution of tumor marker CA19-9 in colorectal carcinoma: correlation with morphological features of neoplasia

OBJETIVO: Comparar os níveis séricos de CA19-9 e CEA e a expressão tecidual do CA19-9 e relacioná-los com os aspectos morfológicos do carcinoma colorretal. MÉTODOS: Quarenta e cinco pacientes com carcinoma colorretal foram operados com coleta de CEA e CA19-9 séricos pré-operatórios. Valores séricos de CEA = 5,0ng/mL e de CA19-9 = 37UI/mL foram considerados aumentados. A avaliação da imunoexpressão do CA19-9 no tecido neoplásico foi realizada por meio de estudo imunoistoquímico com anticorpo monoclonal anti-CA19-9. A intensidade de expressão do CA19-9 no tecido neoplásico foi semiquantificada em leve(+/+++), moderada(++/+++), intensa(+++/+++) e ausente. RESULTADOS: Os valores do CA19-9 sérico foram progressivamente maiores conforme o aumento da expressão do CA19-9 no tecido neoplásico, porém sem significância (p=0,06). O aumento do nível sérico do CA19-9 foi acompanhado de elevação significante (p<0,001) do nível sérico do CEA. O nível sérico do CA19-9, a imunoexpressão tecidual do CA19-9 e o nível sérico do CEA não apresentaram associação significante com características morfológicas do carcinoma colorretal. CONCLUSÃO: As expressões sérica e tissular do CA19-9 demonstraram relação diretamente proporcional entre si, enquanto que os aspectos morfológicos da neoplasia não tiveram influência no CEA e CA19-9 séricos ou na imunoexpressão do CA19-9 tissular.

OBJECTIVE: To compare sera levels of CEA and CA19-9 and tissular expression of the CA19-9 and to correlate these with morphological features of the colorectal carcinoma. METHODS: Forty five patients with colorectal carcinoma underwent surgical treatment following measurement of pre-operative levels of CA19-9 and CEA. Sera levels of CEA = 5.0ng/ml and CA19-9 = 37UI were deemed high values. Evaluation of CA19-9 immunoexpression in neoplastic tissue was carried through by means of immunohistochemical study with monoclonal antibody anti-CA19-9. The intensity of expression of CA19-9 in neoplastic areas was semi-quantified in each area of tumor differentiation into mild(+/+++), moderate(++/+++), intense(+++/+++) or absent. RESULTS: Sera CA19-9 values were progressively higher in the presence of elevated CA19-9 immunoexpression in colorectal carcinoma tissue, although not significant (p=0.06). Increased sera CA19-9 levels were found to be associated with significantly elevated (p<0.001) sera CEA levels. Levels of sera CA19-9, tissular immunoexpression of CA19-9 and sera levels of CEA presented no significant association with morphological features of the colorectal carcinoma. CONCLUSION: Sera and tissular levels of the CA19-9 marker exhibited, each other, a directly proportional relationship. The morphological features of the neoplasia had no influence on sera CEA or CA19-9 levels or tissular immunoexpression of CA19-9.