A membrane can be idealized as a film that readily passes solvents and small solutes but retains large solutes above a particular size. UF (Ultrafiltration) membranes retain solutes with hydraulic diameters in the 5–150 nm range. This roughly corresponds to molecular weights in the 1–1000 kDa range covering most proteins, nucleic acids, nanoparticles, viruses, and some polymers. In the field of membranes, the term nanofiltration refers to membranes tighter than ultrafiltration but more open than reverse osmosis (Figure 1.1). However, in biotechnology, it has come to refer to virus-retaining membranes that fall in the open ultrafiltration (roughly 100 kDa) to tight microfiltration range (roughly 0.1 μm).

In a biopharmaceutical manufacturing process, biopharmaceutical products are expressed in a bioreactor (for mammalian cells) or fermentor (for bacterial or yeast cells). Ultrafiltration has been used to retain colloids and cell debris while passing the expressed product. In a similar way, ultrafiltration has been used after a refold pool to retain refold aggregates while passing the refolded product. Following clarification, ultrafiltration has been used to remove the largest contaminant – water – by retaining the product in a concentration step. This can be to reduce the size of subsequent steps, which may have to be sized based on the batch volume rather than on product mass. In addition, volume reduction facilitates transport and storage. This can provide flexibility to a manufacturing operation by decoupling the upstream from downstream operations.

Membranes are encased in modules for ease-of-operation. One could run the membrane in a static or dialysis mode where small buffer solutes can be exchanged by diffusion across the membrane (Figure 1.2). This is convenient at the bench scale but economical commercial operation requires bulk flow. UF can also be run in NFF (normal flow filtration) or TFF (tangential flow filtration) modes. NFF (Figure 1.2a) is the most common type of filtration. NFF mode involves passing the solvent through the filter under pressure where the fluid velocity is perpendicular (or normal) to the plane of the membrane. As the fluid passes through the membrane, it drags solutes with it to the membrane surface where they accumulate and cause the filter hydraulic resistance to increase. For high concentrations of retained solutes, NFF operation leads to relatively rapid plugging and low filter capacities. NFF is used at bench scale where low capacities pose less of a concern and the ease-of-use is convenient. NFF is also used for virus filtration.