Structural and kinetic studies of mutants can give much insight into the function of an enzyme. We report the detection of possible proton transfer pathways into the active site of a number Of Mutants of the enzyme human carbonic anhydrase II (HCA II). Using a recently developed method of path search in the protein conformational space, we identify hydrogen-bonded networks (or proton paths) that can dynamically connect the protein surface to the active site through fluctuations in protein structure and hydration. The feasibility of establishing such dynamical connectivities is assessed by computing the change in free energy of conformational fluctuations and compared to those identified earlier in the wild type enzyme. It is found that the point mutation facilitates or suppresses one or more of the alternative pathways. Our results allow the use of a generic set of pathways to correlate qualitatively the residual activity in the mutants to the molecular mechanism of proton transfer in the absence of His at position 64. We also demonstrate how the detected pathways may be used to compare the efficiencies of the mutants His-64-Ala/Asn-62-His and His-64-Ala/Asn-67-His using the empirical valence bond theory.